A Safety and Efficacy Study of the Combination Estradiol and Progesterone to Treat Vasomotor Symptoms (REPLENISH)
A Phase 3 Study Safety and Efficacy Study of the Combination Estradiol and Progesterone to Treat Vasomotor Symptoms in Postmenopausal Women With an Intact Uterus
調査の概要
詳細な説明
Postmenopausal subjects with an intact uterus who meet the study entry criteria will be randomized to one of five treatment arms (four active and one placebo) and followed for 12 months. During the Screening period all subjects will be provided with a diary to self-assess the frequency and severity of their vasomotor symptoms. Subjects experiencing a minimum daily frequency of ≥7 (or ≥50 per week) moderate to severe hot flushes will participate in a VMS Substudy during the first 12 weeks of treatment. The Substudy subjects will be stratified by treatment arm within the sites, and only Substudy subjects have the possibility of being randomized to placebo. Subjects who qualify for the study except for experiencing a minimum daily frequency of ≥7 (or ≥50 per week) moderate to severe hot flushes will be stratified within sites to one of the four active treatment arms and followed for 12 months, but will not participate in the VMS Substudy. (However, VMS information will be collected from all subjects during the first 12 weeks of treatment.) All Study Subjects: Postmenopausal women with an intact uterus who seek relief from hot flushes and meet all other inclusion/exclusion criteria are eligible for 12 months of study treatment.
VMS Substudy Subjects: A subset of All Study Subjects who have ≥7 per day or ≥50 per week moderate to severe hot flushes (as determined during Screening) are eligible for the 12-week VMS Substudy and for a total of 12 months of study treatment.
Clinical evaluations will be performed at the following time points:
- Screening Period (Week: - 8.5) (up to -60 Days)
- Visit 1 Randomization (Week 0) (Day 1)
- Visit 2 Interim (Week 4)
- Visit 3 Interim (Week 8)
- Visit 4 Interim (Week 12)
- Visit 5 Interim (Month 6)
- Visit 6 Interim (Month 9)
- Visit 7 End of Treatment (Month 12)
研究の種類
入学 (実際)
段階
- フェーズ 3
連絡先と場所
研究場所
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Alabama
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Birmingham、Alabama、アメリカ、35211
- Simon Williamson Clinic
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Huntsville、Alabama、アメリカ、35801
- Medical Affiliated Research Center
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Mobile、Alabama、アメリカ、36608
- Coastal Clinical Research
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Mobile、Alabama、アメリカ、36608
- Mobile Ob-Gyn, P.C.
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Montgomery、Alabama、アメリカ、36117
- Montgomery Women's Health
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Arizona
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Glendale、Arizona、アメリカ、85308
- Advanced Research Associates
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Mesa、Arizona、アメリカ、85209
- Cactus Clinical Research
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Phoenix、Arizona、アメリカ、85032
- Precision Trials
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Tucson、Arizona、アメリカ、85712
- Radiant Research (Tucson)
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Tucson、Arizona、アメリカ、85712
- Visions Clinical Research Tucson
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Arkansas
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Hot Springs、Arkansas、アメリカ、71913
- Health Star Research, LLC
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California
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Berkeley、California、アメリカ、94705
- Sutter East Bay Medical Foundation
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La Mesa、California、アメリカ、91942
- Grossmont Center for Clinical Research
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Norwalk、California、アメリカ、90650
- Futura Research
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San Diego、California、アメリカ、92108
- Medical Center for Clinical Research
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San Diego、California、アメリカ、92111
- Women's Health Care Research Corp.
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Santa Rosa、California、アメリカ、95405
- Radiant Research, Inc.
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Walnut Creek、California、アメリカ、94598
- Diablo Clinical Research
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Colorado
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Denver、Colorado、アメリカ、80209
- Downtown Women's Healthcare
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Denver、Colorado、アメリカ、80220
- Horizon's Clinical Research Center
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Lakewood、Colorado、アメリカ、80228
- Red Rocks OB/Gyn
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Connecticut
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Milford、Connecticut、アメリカ、06460
- Clinical Research Consulting
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New London、Connecticut、アメリカ、06320
- Coastal Connecticut Research
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Florida
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Aventura、Florida、アメリカ、33180
- South Florida Medical Research
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Crystal River、Florida、アメリカ、34429
- Nature Coast Clinical Research
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Fort Myers、Florida、アメリカ、33916
- Clinical Physiology Associates
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Gainesville、Florida、アメリカ、32607
- Southeastern Integrated Medical, PL, d/b/a Florida Medical Research
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Jacksonville、Florida、アメリカ、32207
- UF College of Medicine-Jacksonville, Dept. of Obstetrics and Gynecology
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Margate、Florida、アメリカ、33063
- Suncoast Research
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Melbourne、Florida、アメリカ、32934
- Accelovance
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New Port Richey、Florida、アメリカ、34652
- Suncoast Clinical Research, Inc
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North Miami、Florida、アメリカ、33161
- Segal Institute
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North Miami Beach、Florida、アメリカ、33162
- Ideal Clinical Research
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Orlando、Florida、アメリカ、32806
- Compass Research
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Pinellas Park、Florida、アメリカ、33781
- Radiant Research (St. Petersburg)
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Plantation、Florida、アメリカ、33324
- All Women's Healthcare of West Broward Discovery Clinical Research
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West Palm Beach、Florida、アメリカ、33409
- Comprehensive Clinical Trials
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Georgia
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Atlanta、Georgia、アメリカ、30342
- Women's Health Associates
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Atlanta、Georgia、アメリカ、30328
- Radiant Research (Atlanta)
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Decatur、Georgia、アメリカ、30034
- Soapstone Center for Clinical Research
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Sandy Springs、Georgia、アメリカ、30328
- Wake Research - Mount Vernon Clinical Research
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Savannah、Georgia、アメリカ、31406
- Fellows Research Alliance
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Idaho
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Blackfoot、Idaho、アメリカ、83221
- Elite Clinical Trials
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Meridian、Idaho、アメリカ、83642
- Advanced Clinical Research
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Illinois
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Addison、Illinois、アメリカ、60101
- Biofortis
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Champaign、Illinois、アメリカ、61820
- Women's Health Practice
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Chicago、Illinois、アメリカ、60654
- Radiant Research (Chicago)
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Indiana
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Granger、Indiana、アメリカ、46530
- The South Bend Clinic Granger
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Indianapolis、Indiana、アメリカ、46250
- Davis Clinic
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Kansas
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Wichita、Kansas、アメリカ、67226
- Cypress Medical Research Center, LLC
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Kentucky
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Lexington、Kentucky、アメリカ、40509
- Central Kentucky Research Associates
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Louisville、Kentucky、アメリカ、40291
- Bluegrass Clinical Research
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Louisiana
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Eunice、Louisiana、アメリカ、70535
- Horizon Research Group
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Maryland
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Lutherville、Maryland、アメリカ、21093
- Maryland Center for Sexual Health
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Michigan
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Bingham Farms、Michigan、アメリカ、48025
- Quest Research Institute
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Grand Rapids、Michigan、アメリカ、49503
- Female Pelvic Medicine & Urogynecology
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Kalamazoo、Michigan、アメリカ、49009
- Beyer Research
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Saginaw、Michigan、アメリカ、48604
- Saginaw Valley Medical Research Group
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Missouri
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Saint Louis、Missouri、アメリカ、63141
- Radiant Research (St. Louis)
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Montana
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Billings、Montana、アメリカ、59102
- Montana Health
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Billings、Montana、アメリカ、59101
- Billings Clinical Research
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Nebraska
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Lincoln、Nebraska、アメリカ、68510
- Women's Clinic of Lincoln
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Nevada
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Las Vegas、Nevada、アメリカ、89128
- Affiliated Clinical Research
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Las Vegas、Nevada、アメリカ、89113
- Affiliated Clinical Research INC
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New Jersey
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Lawrenceville、New Jersey、アメリカ、08648
- Lawrence OB-GYN Clinical Research
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New Mexico
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Albuquerque、New Mexico、アメリカ、87102
- Albuquerque Clinical Trials, Inc.
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Albuquerque、New Mexico、アメリカ、87109
- Bosque Women's Care
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Albuquerque、New Mexico、アメリカ、87109
- Southwest Clinical Research
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New York
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New York、New York、アメリカ、10032
- Columbia University
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Port Jefferson、New York、アメリカ、11777
- Suffolk OB/GYN
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Williamsville、New York、アメリカ、14221
- Upstate Clinical Research Associates
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North Carolina
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Durham、North Carolina、アメリカ、27713
- Women's Wellness Clinic
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High Point、North Carolina、アメリカ、27262
- Carolina Medical Trials
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Raleigh、North Carolina、アメリカ、27607
- Centre OBGYN
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Raleigh、North Carolina、アメリカ、27612
- Wake County Research
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Salem、North Carolina、アメリカ、27103
- Lyndhurst Clinical Research
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Winston-Salem、North Carolina、アメリカ、27103
- Carolina Medical Trials
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Winston-Salem、North Carolina、アメリカ、27103
- Hawthorne Research
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Winston-Salem、North Carolina、アメリカ、27103
- Triad Ob-Gyn
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North Dakota
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Fargo、North Dakota、アメリカ、58103
- Lillestol Research
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Ohio
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Akron、Ohio、アメリカ、44311
- Radiant Research (Akron)
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Cincinnati、Ohio、アメリカ、45267-0457
- University of Cincinnati Physicians Company
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Cleveland、Ohio、アメリカ、44122
- Rapid Medical Research
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Columbus、Ohio、アメリカ、43213
- Columbus Center for Women's Health Research
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Englewood、Ohio、アメリカ、45322
- HWC Women's Research Center
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Oklahoma
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Oklahoma City、Oklahoma、アメリカ、73112
- Lynn Health Science Institute
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Oregon
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Medford、Oregon、アメリカ、97504
- Sunstone Medical Research
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Pennsylvania
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Jenkintown、Pennsylvania、アメリカ、19046
- The Clinical Trial Center
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Philadelphia、Pennsylvania、アメリカ、19114
- Clinical Research of Philadelphia
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Pittsburgh、Pennsylvania、アメリカ、15206
- Clinical Trials Research Services, LLC
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Rhode Island
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Warwick、Rhode Island、アメリカ、02886
- Omega Medical Research
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South Carolina
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Bluffton、South Carolina、アメリカ、29910
- Fellows Research Group
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Columbia、South Carolina、アメリカ、29201
- Vista Clinical Research
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Greenville、South Carolina、アメリカ、29615
- Upstate Pharmaceutical Research
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Mount Pleasant、South Carolina、アメリカ、29464
- Coastal Carolina Research Center
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Tennessee
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Chattanooga、Tennessee、アメリカ、37404
- Chattanooga Medical Research
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Knoxville、Tennessee、アメリカ、37920
- Volunteer Research Group/NOCCR
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Texas
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Bryan、Texas、アメリカ、77802
- DiscoveResearch, Inc.
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Corpus Christi、Texas、アメリカ、78414
- Advanced Research Associates
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Dallas、Texas、アメリカ、75234
- Research Across America
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Fort Worth、Texas、アメリカ、76104
- Brownstone Clinical Trials
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Houston、Texas、アメリカ、77030
- Advances In Health
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Houston、Texas、アメリカ、77054
- TMC Life Research
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Houston、Texas、アメリカ、77054
- The Women's Hospital of Texas
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Hurst、Texas、アメリカ、76054
- Protenium Clinical Research
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Irving、Texas、アメリカ、75062
- MacArthur OB/GYN
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San Antonio、Texas、アメリカ、78229
- Clinical Trials of Texas
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San Antonio、Texas、アメリカ、78258
- Stone Oak, LLC dba Discovery Clinical Trials
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Schertz、Texas、アメリカ、78154
- NECRSA
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Utah
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Draper、Utah、アメリカ、84020
- PRO/ Salt Lake Women's Center
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Salt Lake City、Utah、アメリカ、84124
- Jean Brown Research
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Salt Lake City、Utah、アメリカ、84107
- Wasatch Clinical Research, LLC
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Virginia
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Charlottesville、Virginia、アメリカ、22908
- UVA/Midlife Health at North Ridge
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Norfolk、Virginia、アメリカ、23507
- Clinical Research Center Eastern Virginia Medical School
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Richmond、Virginia、アメリカ、23233
- Virginia Women's Center
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Richmond、Virginia、アメリカ、23294
- National Clinical Research-Richmond, Inc
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Virginia Beach、Virginia、アメリカ、23456
- Tidewater Clinical Research
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Washington
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Seattle、Washington、アメリカ、98105
- Seattle Women's Health Research, Gynecology
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Spokane、Washington、アメリカ、99027
- North Spokane Women's Health
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参加基準
適格基準
就学可能な年齢
健康ボランティアの受け入れ
受講資格のある性別
説明
Inclusion Criteria:
- Be a female between the ages of 40 and 65 years (at the time of randomization) who is willing to participate in the study, as documented by signing the informed consent form.
Be a postmenopausal woman with an intact uterus and a Screening serum estradiol level of ≤50 pg/mL. Postmenopausal is defined herein as:
- ≥ 12 months of spontaneous amenorrhea, or
- at least 6 months of spontaneous amenorrhea with a Screening serum FSH level of >40 mIU/ml, or
- ≥ 6 weeks postsurgical bilateral oophorectomy.
- Be seeking treatment or relief for vasomotor symptoms associated with menopause.
To participate in the VMS Substudy, a subject must also report ≥7 moderate to severe hot flushes per day, or ≥50 per week, at the baseline assessment during Screening (subjects whose hot flushes are less frequent may still participate as non-Substudy subjects.
Note: A minimum of 14 consecutive days of complete hot flush diary data are required during the baseline assessment at Screening, and these consecutive days must occur within the last 14 days prior to the Randomization visit (not counting the Randomization visit day itself). The most recent 7 consecutive days of data prior to randomization (Day -7 to Day -1) will be used to determine the baseline number of mild, moderate and severe hot flushes for each subject.
- Have a Body Mass Index (BMI) less than or equal to 34 kg/mP2P. (BMI values should be rounded to the nearest integer [e.g., 34.4 rounds down to 34, while 26.5 rounds up to 27]).
- Be willing to abstain from using products (other than study medication) that contain estrogen, progestin, or progesterone throughout study participation.
Be judged by the principal or sub-investigator physician as being in otherwise generally good health based on a medical evaluation performed during the Screening period prior to the initial dose of study medication. The medical evaluation findings must include:
- a normal or non-clinically significant physical examination, including vital signs (sitting blood pressure, heart rate, respiratory rate and temperature). Sitting systolic blood pressure is ≤140 mmHg and diastolic blood pressure ≤90 mmHg at Screening. A subject may be taking up to two antihypertensive medications.
- a normal or non-clinically significant pelvic examination.
- a mammogram that shows no sign of significant disease (can be performed within previous 6 months prior to initial dose of study medication). Subjects must have a BI-RADS 1 or 2 to enroll in the study. An incomplete mammogram result, i.e. BI-RADS 0, is not acceptable. The site must obtain a copy of the official report for the subject's study file, and it must be verified that the mammogram itself is available if needed for additional assessment.
- a normal or non-clinically significant clinical breast examination. An acceptable breast examination is defined as no masses or other findings identified that are suspicious of malignancy.
- a normal Screening Papanicolaou ("Pap") smear. (Subjects with findings of atypical glandular cells [AGC], AGUS, ASCUS with high risk HPV type upon reflex testing, LSIL, ASC-H, HSIL, dysplastic cells, or malignant cells must be excluded from randomization.)
- an acceptable result from an evaluable Screening endometrial biopsy. The endometrial biopsy reports by the two central pathologists at Screening must each specify one of the following: proliferative endometrium; weakly proliferative endometrium; disordered proliferative pattern; secretory endometrium; endometrial tissue other (including benign, inactive or atrophic fragments of endometrial epithelium, glands, stroma, etc); endometrial tissue insufficient for diagnosis; no endometrium identified; or no tissue identified. However, at least one pathologist must identify sufficient tissue to evaluate the biopsy. Additionally, the endometrial biopsy reports by the two central pathologists of Other Findings at Screening must each specify one of the following: endometrial polyp not present; benign endometrial polyp; or polyp other. (See Exclusion criterion #27)
- a normal or non-clinically significant 12-lead ECG.
Exclusion Criteria:
To participate in the study, a subject must NOT:
- Be currently hospitalized.
- Have a history of thrombosis of deep veins or arteries or a thromboembolic disorder.
- Have a history of coronary artery or cerebrovascular disease (e.g., myocardial infarction, angina, stroke, TIA).
- Have a history of a chronic liver or kidney dysfunction/disorder (e.g., Hepatitis C or chronic renal failure).
- Have a history of a malabsorption disorder (e.g., gastric bypass, Crohn's disease).
- Have a history of gallbladder dysfunction/disorders (e.g., cholangitis, cholecystitis), unless gallbladder has been removed.
- Have a history of diabetes, thyroid disease or any other endocrinological disease. (Subjects with diet-controlled diabetes or controlled hypothyroid disease at Screening are not excluded.)
- Have a history of estrogen-dependent neoplasia.
- Have a history of atypical ductal hyperplasia of the breast.
- Have a finding of clinically significant uterine fibroids at Screening.
- Have had a uterine ablation.
- Have a history of undiagnosed vaginal bleeding.
- Have any history of endometrial hyperplasia, melanoma, or uterine/endometrial, breast or ovarian cancer.
- Have any history of other malignancy within the last 5 years, with the exception of basal cell (excluded if within 1 year) or non-invasive squamous cell (excluded if within 1 year) carcinoma of the skin.
- Have a history of any other cardiovascular, hepatic, renal, pulmonary, hematologic, gastrointestinal, endocrine, immunologic, dermatologic, neurologic, psychological (e.g., bipolar disorder, schizophrenia, major depressive disorder), or musculoskeletal disease or disorder that is clinically significant in the opinion of the Principal Investigator or Medical Sub-Investigator.
Have any of the following clinical laboratory values at Screening:
- fasting triglyceride of ≥300 mg/dL and/or total cholesterol of ≥300mg/dL
- positive laboratory finding for Factor V Leiden mutation
- AST or ALT ≥1.5 times the upper limit of normal (ULN)
- fasting glucose >125 mg/dL
- Be known to be pregnant or have a positive urine pregnancy test. (Note: A pregnancy test is not required for subjects who have had bilateral tubal ligation, bilateral oophorectomy, or are 55 years old or greater and have experienced cessation of menses for at least 1 year.)
- Have contraindication to estrogen and/or progestin therapy or allergy to the use of estradiol and/or progesterone or any components of the investigational drugs.
- Use 15 or more cigarettes per day or currently use any electronic cigarettes.
- Have a history of drug and/or alcohol abuse within one year of start of study.
- Have used, within 28 days prior to the initial dose of study medication at Visit 1, any medication known to induce or inhibit CYP3A4 enzyme activity that may affect estrogen and/or progestin drug metabolism. (See 48TUSection 4.3U48T)
- Have used, within 28 days prior to Screening, or plan to use during the study, any prescription or over-the-counter (OTC) medications (including herbal products, such as St. John's Wort) that would be expected to alter progesterone or estrogen activity or is being used to treat vasomotor symptoms. (See Section 4.3U48T)
Have used estrogen alone or estrogen/progestin, SERM (selective estrogen receptor modulator), testosterone, or estrogen/testosterone for any of the following time periods:
- Vaginal nonsystemic hormonal products (rings, creams, gels) within 7 days prior to Screening, or vaginal systemic products (e.g., FemRing) within 28 days prior to Screening.
- Transdermal estrogen alone or estrogen/progestin products within 8 weeks prior to Screening.
- Oral estrogen and/or progestin and/or SERM therapy within 8 weeks prior to Screening.
- Progestational implants, estrogen or estrogen/progestational injectable drug therapy within 3 months prior to Screening.
- Estrogen pellet therapy or progestational injectable drug therapy within 6 months prior to Screening.
- Percutaneous estrogen lotions/gels within 8 weeks prior to Screening.
- Oral, topical, vaginal, patch, implantable or injectable androgen therapy within 8 weeks prior to Screening.
- Have used an intrauterine device (IUD) within the 12 weeks prior to Screening.
- For subjects in the VMS Substudy only: use of medication that may affect the outcome of the vasomotor symptom endpoints within 28 days prior to Screening (e.g. SSRIs [selective serotonin reuptake inhibitors], SNRIs [serotonin and norepinephrine reuptake inhibitors], aldomet, dopaminergic or antidopaminergic drugs, gabapentin, clonidine, or bellergal.)
- Have any reason which, in the opinion of the Principal Investigator or Medical Sub-Investigator, would prevent the subject from safely participating in the study or complying with protocol requirements.
- Have a Screening endometrial biopsy sample that is found by both primary pathologists to have endometrial tissue insufficient for diagnosis, no endometrium identified, or no tissue identified. (With the approval of the Medical Monitor, the Screening endometrial biopsy may be repeated once.)
- Endometrial polyps with atypical nuclei reported by at least 1 central pathologist.
- Have contraindication to any planned study assessments (e.g., endometrial biopsy).
- Have participated in another clinical trial within 30 days prior to Screening, have received an investigational drug within the three months prior to the initial dose of study medication, or be likely to participate in a clinical trial or receive another investigational medication during the study.
- Currently use marijuana.
研究計画
研究はどのように設計されていますか?
デザインの詳細
- 主な目的:処理
- 割り当て:ランダム化
- 介入モデル:並列代入
- マスキング:トリプル
武器と介入
参加者グループ / アーム |
介入・治療 |
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実験的:Treatment 1
Combined Estradiol 1 mg / Progesterone 100 mg softgel capsule formulation and placebo taken orally once a day for twelve months.
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実験的:Treatment 2
Combined Estradiol 0.5 mg / Progesterone 100 mg softgel capsule formulation and placebo taken orally once a day for twelve months.
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他の名前:
他の名前:
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実験的:Treatment 3
Combined Estradiol 0.5 mg / Progesterone 50 mg softgel capsule formulation and placebo, taken orally once a day for twelve months.
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他の名前:
他の名前:
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実験的:Treatment 4
Combined Estradiol 0.25 mg / Progesterone 50 mg softgel capsule formulation and placebo, taken orally once a day for twelve months.
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他の名前:
他の名前:
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プラセボコンパレーター:Placebo
Two Placebo softgel capsules taken orally once a day for twelve months.
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この研究は何を測定していますか?
主要な結果の測定
結果測定 |
メジャーの説明 |
時間枠 |
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Co-Primary Efficacy Endpoint: Frequency of Moderate to Severe Vasomotor Symptoms (MITT-VMS)
時間枠:Baseline and Week 4
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Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 4. The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
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Baseline and Week 4
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Co-Primary Efficacy Endpoint: Frequency of Moderate to Severe Vasomotor Symptoms (MITT-VMS)
時間枠:Baseline and Week 12
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Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 12.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
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Baseline and Week 12
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Co-Primary Efficacy Endpoint: Severity of Moderate to Severe Vasomotor Symptoms (MITT-VMS)
時間枠:Baseline and Week 4
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Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 4. The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
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Baseline and Week 4
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Co-Primary Efficacy Endpoint: Severity of Moderate to Severe Vasomotor Symptoms (MITT-VMS)
時間枠:Baseline and Week 12
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Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 12.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
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Baseline and Week 12
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Primary Safety Endpoint: Endometrial Protection - Hyperplasia
時間枠:Baseline and Month 12
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Endometrial biopsies centrally evaluated by 2 primary pathologists using criteria from Blaustein's Pathology text.
Pathologists classified bx into 1 of following 3 categories: Cat.1: Non-endometrial malignancy/non-hyperplasia; Cat.2: Endometrial hyperplasia; Cat.3: Endometrial malignancy.
Consensus reached when 2 primary pathologist agreed on any of above categories; if primary pathologists disagreed on presence of hyperplasia, result of 3rd pathologist was utilized and final decision regarding presence of hyperplasia was based on diagnosis of majority.
If all 3 reads disparate, final diagnosis based on most severe dx.
Incidence rate calculated as: I=A/B where I=incidence rate at M12 evaluation, A=all new subjects with biopsies positive for endometrial hyperplasia during study but post-Baseline, B=all subjects w/biopsies following M11 meeting criteria specified plus all subjects w/biopsies positive for endometrial hyperplasia by any pathologists before M11.
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Baseline and Month 12
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二次結果の測定
結果測定 |
メジャーの説明 |
時間枠 |
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Endometrial Protection - Hyperplasia
時間枠:Baseline and Month 12
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Endometrial biopsies centrally evaluated by 3 primary pathologists using criteria described in Blaustein's Pathology text.
Pathologists classified biopsy into 1 of following 3 categories: Cat.1: Non-endometrial malignancy/non-hyperplasia; Cat.2: Endometrial hyperplasia; Cat.3: Endometrial malignancy.
Consensus was reached when the 2 of 3 pathologist readers agreed on any of the above categories; if all three reads were disparate, the final diagnosis was based on the most severe diagnosis.
Incidence rate calculated as: I=A/B where I=incidence rate at M12 evaluation, A=all new subjects with biopsies positive for endometrial hyperplasia during study but post-Baseline, B=all subjects with biopsies following M11 meeting the criteria specified plus all subjects with biopsies positive for endometrial hyperplasia by any of the pathologists before M11.
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Baseline and Month 12
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Frequency of Moderate to Severe Vasomotor Symptoms - Week 1 (MITT-VMS)
時間枠:Baseline and Week 1
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 1.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 1
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 2 (MITT-VMS)
時間枠:Baseline and Week 2
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 2. The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 2
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 3 (MITT-VMS)
時間枠:Baseline and Week 3
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 3. The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 3
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 4 (MITT-VMS)
時間枠:Baseline and Week 4
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 4. The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 4
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 5 (MITT-VMS)
時間枠:Baseline and Week 5
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 5.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 5
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 6 (MITT-VMS)
時間枠:Baseline and Week 6
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 6.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 6
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 7 (MITT-VMS)
時間枠:Baseline and Week 7
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 7. The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 7
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 8 (MITT-VMS)
時間枠:Baseline and Week 8
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 8.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 8
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 9 (MITT-VMS)
時間枠:Baseline and Week 9
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 9.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 9
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 10 (MITT-VMS)
時間枠:Baseline and Week 10
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 10.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 10
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 11 (MITT-VMS)
時間枠:Baseline and Week 11
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 11.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 11
|
Frequency of Moderate to Severe Vasomotor Symptoms - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 12.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of moderate to severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of moderate to severe hot flushes for the subject week.
|
Baseline and Week 12
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 1 (MITT-VMS)
時間枠:Baseline and Week 1
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 1.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 1
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 2 (MITT-VMS)
時間枠:Baseline and Week 2
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 2. The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 2
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 3 (MITT-VMS)
時間枠:Baseline and Week 3
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 3. The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 3
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 4 (MITT-VMS)
時間枠:Baseline and Week 4
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 4. The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 4
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 5 (MITT-VMS)
時間枠:Baseline and Week 5
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 5.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 5
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 6 (MITT-VMS)
時間枠:Baseline and Week 6
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 6.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 6
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 7 (MITT-VMS)
時間枠:Baseline and Week 7
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 7. The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 7
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 8 (MITT-VMS)
時間枠:Baseline and Week 8
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 8.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 8
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 9 (MITT-VMS)
時間枠:Baseline and Week 9
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 9.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 9
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 10 (MITT-VMS)
時間枠:Baseline and Week 10
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 10.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 10
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 11 (MITT-VMS)
時間枠:Baseline and Week 11
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 11.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 11
|
Severity of Moderate to Severe Vasomotor Symptoms - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Mean change in severity of moderate to severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 12.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score = (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of moderate to severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 12
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 1 (MITT-VMS)
時間枠:Baseline and Week 1
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 1.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 1
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 2 (MITT-VMS)
時間枠:Baseline and Week 2
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 2. The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 2
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 3 (MITT-VMS)
時間枠:Baseline and Week 3
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 3. The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 3
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 4 (MITT-VMS)
時間枠:Baseline and Week 4
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 4. The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 4
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 5 (MITT-VMS)
時間枠:Baseline and Week 5
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 5.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 5
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 6 (MITT-VMS)
時間枠:Baseline and Week 6
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 6.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 6
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 7 (MITT-VMS)
時間枠:Baseline and Week 7
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 7. The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 7
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 8 (MITT-VMS)
時間枠:Baseline and Week 8
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 8.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 8
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 9 (MITT-VMS)
時間枠:Baseline and Week 9
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 9.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 9
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 10 (MITT-VMS)
時間枠:Baseline and Week 10
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 10.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 10
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 11 (MITT-VMS)
時間枠:Baseline and Week 11
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 11.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 11
|
Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Mean change in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 12.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The weekly frequency of mild, moderate and severe hot flushes was calculated from the daily diary record using a forward counting process of 7 day intervals beginning with the baseline date.
Weekly frequency equals total number of mild, moderate and severe hot flushes for the subject week.
|
Baseline and Week 12
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 1 (MITT-VMS)
時間枠:Baseline and Week 1
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 1.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 1
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 2 (MITT-VMS)
時間枠:Baseline and Week 2
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 2. The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 2
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 3 (MITT-VMS)
時間枠:Baseline and Week 3
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 3. The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 3
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 4 (MITT-VMS)
時間枠:Baseline and Week 4
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 4. The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 4
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 5 (MITT-VMS)
時間枠:Baseline and Week 5
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 5.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 5
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 6 (MITT-VMS)
時間枠:Baseline and Week 6
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 6.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 6
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 7 (MITT-VMS)
時間枠:Baseline and Week 7
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 7. The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 7
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 8 (MITT-VMS)
時間枠:Baseline and Week 8
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 8.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 8
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 9 (MITT-VMS)
時間枠:Baseline and Week 9
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 9.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 9
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 10 (MITT-VMS)
時間枠:Baseline and Week 10
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 10.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 10
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 11 (MITT-VMS)
時間枠:Baseline and Week 11
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 11.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 11
|
Severity of Mild, Moderate and Severe Vasomotor Symptoms - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Mean change in severity of mild, moderate and severe vasomotor symptoms at Baseline to mild, moderate to severe vasomotor symptoms at Week 12.
The baseline was the most recent 7 consecutive days of data prior to randomization.
The severity score was derived as follows: mild = 1, moderate = 2, severe = 3. Baseline Weekly Severity Score =(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
On Treatment Weekly Severity Score = [(number of mild hot flushes for 7 days) x 1 + (number of moderate hot flushes for 7 days) x 2 + (number of severe hot flushes for 7 days) x 3] / (total number of mild, moderate and severe hot flushes over 7 days).
|
Baseline and Week 12
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 1 (MITT-VMS)
時間枠:Baseline and Week 1
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe VMS from Baseline to Week 1.
|
Baseline and Week 1
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 2 (MITT-VMS)
時間枠:Baseline and Week 2
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 2.
|
Baseline and Week 2
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 3 (MITT-VMS)
時間枠:Baseline and Week 3
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 3.
|
Baseline and Week 3
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 4 (MITT-VMS)
時間枠:Baseline and Week 4
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 4.
|
Baseline and Week 4
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 5 (MITT-VMS)
時間枠:Baseline and Week 5
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 5.
|
Baseline and Week 5
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 6 (MITT-VMS)
時間枠:Baseline and Week 6
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 6.
|
Baseline and Week 6
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 7 (MITT-VMS)
時間枠:Baseline and Week 7
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 7.
|
Baseline and Week 7
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 8 (MITT-VMS)
時間枠:Baseline and Week 8
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 8.
|
Baseline and Week 8
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 9 (MITT-VMS)
時間枠:Baseline and Week 9
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 9.
|
Baseline and Week 9
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 10 (MITT-VMS)
時間枠:Baseline and Week 10
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 10.
|
Baseline and Week 10
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 11 (MITT-VMS)
時間枠:Baseline and Week 11
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 11.
|
Baseline and Week 11
|
Reduction of Frequency of Moderate to Severe Vasomotor Symptoms - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of moderate to severe vasomotor symptoms from Baseline to Week 12.
|
Baseline and Week 12
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 1 - (MITT-VMS)
時間枠:Baseline and Week 1
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 1.
|
Baseline and Week 1
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 2 - (MITT-VMS)
時間枠:Baseline and Week 2
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 2.
|
Baseline and Week 2
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 3 - (MITT-VMS)
時間枠:Baseline and Week 3
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 3.
|
Baseline and Week 3
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 4 - (MITT-VMS)
時間枠:Baseline and Week 4
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 4.
|
Baseline and Week 4
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 5 - (MITT-VMS)
時間枠:Baseline and Week 5
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 5.
|
Baseline and Week 5
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 6 - (MITT-VMS)
時間枠:Baseline and Week 6
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 6.
|
Baseline and Week 6
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 7 - (MITT-VMS)
時間枠:Baseline and Week 7
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 7.
|
Baseline and Week 7
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 8 - (MITT-VMS)
時間枠:Baseline and Week 8
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 8.
|
Baseline and Week 8
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 9 - (MITT-VMS)
時間枠:Baseline and Week 9
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 9.
|
Baseline and Week 9
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 10 - (MITT-VMS)
時間枠:Baseline and Week 10
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 10.
|
Baseline and Week 10
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 11 - (MITT-VMS)
時間枠:Baseline and Week 11
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 11.
|
Baseline and Week 11
|
Reduction of Frequency of Mild, Moderate and Severe Vasomotor Symptoms - Week 12 - (MITT-VMS)
時間枠:Baseline and Week 12
|
Number of Subjects with >=50%, and separately, >=75% reduction in frequency of mild, moderate and severe vasomotor symptoms from Baseline to Week 12.
|
Baseline and Week 12
|
Clinical Global Impression (CGI) - Week 4 (MITT-VMS)
時間枠:Baseline and Week 4
|
The number and percentage of subjects for each possible response to the CGI at Week 4. The CGI score is a seven point scale where subjects were asked to rate the total improvement, whether or not in her judgment it was due entirely to drug treatment, compared to her condition at admission to the study.
Scale: Very much improved, Much improved, Minimally improved, No change, Minimally worse, Much worse, Very much worse.
Results for the top two responses (Very Much Improved and Much Improved) and No Change or Worsening (Minimally worse, Much worse, Very much worse) were combined for each group and active treatment groups compare to placebo.
|
Baseline and Week 4
|
Mean Change in Frequency of Moderate to Severe VMS for the Respective CGI Category - Week 4 (MITT-VMS)
時間枠:Baseline and Week 4
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 4 for the respective CGI category.
The CGI score is a seven point scale where subjects were asked to rate the total improvement, whether or not in her judgment it was due entirely to drug treatment, compared to her condition at admission to the study.
Scale: Very much improved, Much improved, Minimally improved, No change, Minimally worse, Much worse, Very much worse.
Results for the top two responses (Very Much Improved and Much Improved) and No Change or Worsening (Minimally worse, Much worse, Very much worse) were combined for each group and active treatment groups compare to placebo.
|
Baseline and Week 4
|
Clinical Global Impression (CGI) - Week 8 (MITT-VMS)
時間枠:Baseline and Week 8
|
The number and percentage of subjects for each possible response to the CGI at Week 8.
The CGI score is a seven point scale where subjects were asked to rate the total improvement, whether or not in her judgment it was due entirely to drug treatment, compared to her condition at admission to the study.
Scale: Very much improved, Much improved, Minimally improved, No change, Minimally worse, Much worse, Very much worse.
Results for the top two responses (Very Much Improved and Much Improved) and No Change or Worsening (Minimally worse, Much worse, Very much worse) were combined for each group and active treatment groups compare to placebo.
|
Baseline and Week 8
|
Mean Change in Frequency of Moderate to Severe VMS for the Respective CGI Category - Week 8 (MITT-VMS)
時間枠:Baseline and Week 8
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 8 for the respective CGI category.
The CGI score is a seven point scale where subjects were asked to rate the total improvement, whether or not in her judgment it was due entirely to drug treatment, compared to her condition at admission to the study.
Scale: Very much improved, Much improved, Minimally improved, No change, Minimally worse, Much worse, Very much worse.
Results for the top two responses (Very Much Improved and Much Improved) and No Change or Worsening (Minimally worse, Much worse, Very much worse) were combined for each group and active treatment groups compare to placebo.
|
Baseline and Week 8
|
Clinical Global Impression (CGI) - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
The number and percentage of subjects for each possible response to the CGI at Week 12.
The CGI score is a seven point scale where subjects were asked to rate the total improvement, whether or not in her judgment it was due entirely to drug treatment, compared to her condition at admission to the study.
Scale: Very much improved, Much improved, Minimally improved, No change, Minimally worse, Much worse, Very much worse.
Results for the top two responses (Very Much Improved and Much Improved) and No Change or Worsening (Minimally worse, Much worse, Very much worse) were combined for each group and active treatment groups compare to placebo.
|
Baseline and Week 12
|
Mean Change in Frequency of Moderate to Severe VMS for the Respective CGI Category - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Mean change in frequency of moderate to severe vasomotor symptoms from Baseline to Week 12 for the respective CGI category.
The CGI score is a seven point scale where subjects were asked to rate the total improvement, whether or not in her judgment it was due entirely to drug treatment, compared to her condition at admission to the study.
Scale: Very much improved, Much improved, Minimally improved, No change, Minimally worse, Much worse, Very much worse.
Results for the top two responses (Very Much Improved and Much Improved) and No Change or Worsening (Minimally worse, Much worse, Very much worse) were combined for each group and active treatment groups compare to placebo.
|
Baseline and Week 12
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 1 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 1 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 2 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 2 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 3 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 3 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 4 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 4 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 5 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 5 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 6 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 6 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 7 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 7 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 8 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 8 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 9 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 9 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 10 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 10 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 11 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 11 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:Cycle 12 to 13
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
Cycle 12 to 13
|
Number of Subjects Without Bleeding for Consecutive Cycles
時間枠:The 13th Cycle
|
No bleeding was defined as the absence of bleeding.
Cumulative rates for no bleeding was defined as the percentage of women who reported consecutive cycles of no bleeding for a given cycle of time.
|
The 13th Cycle
|
Number of Subjects With Cumulative Amenorrhea From Cycle 1 to 13
時間枠:Cycle 1 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 1 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 1 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 2 to 13
時間枠:Cycle 2 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 2 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 2 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 3 to 13
時間枠:Cycle 3 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 3 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 3 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 4 to 13
時間枠:Cycle 4 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 4 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 4 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 5 to 13
時間枠:Cycle 5 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 5 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 5 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 6 to 13
時間枠:Cycle 6 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 6 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 6 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 7 to 13
時間枠:Cycle 7 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 7 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 7 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 8 to 13
時間枠:Cycle 8 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 8 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 8 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 9 to 13
時間枠:Cycle 9 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 9 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 9 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 10 to 13
時間枠:Cycle 10 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 10 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 10 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 11 to 13
時間枠:Cycle 11 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 11 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 11 to 13
|
Number of Subjects With Cumulative Amenorrhea From Cycle 12 to 13
時間枠:Cycle 12 to 13
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from Cycle 12 to 13 was calculated and compared between active and placebo treatments.
|
Cycle 12 to 13
|
Number of Subjects With Cumulative Amenorrhea From the 13th Cycle
時間枠:The 13th Cycle
|
Cumulative amenorrhea is defined as the absence of bleeding or spotting for a cumulative period.
Cumulative rates of amenorrhea were defined as the percentage of women who reported consecutive cycles of amenorrhea for a given cycle of time.
Within each treatment arm, the percentage of subjects with cumulative amenorrhea from the 13th Cycle was calculated and compared between active and placebo treatments.
|
The 13th Cycle
|
Subject Incidence With Spotting - Trimester 1 (Safety Pop.)
時間枠:Trimester 1
|
Summary of subject incidence with spotting per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 1
|
Subject Incidence With Spotting - Trimester 2 (Safety Pop.)
時間枠:Trimester 2
|
Summary of subject incidence with spotting per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 2
|
Subject Incidence With Spotting - Trimester 3 (Safety Pop.)
時間枠:Trimester 3
|
Summary of subject incidence with spotting per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 3
|
Subject Incidence With Spotting - Trimester 4 (Safety Pop.)
時間枠:Trimester 4
|
Summary of subject incidence with spotting per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 4
|
Number of Days With Spotting - Trimester 1 (Safety Pop.)
時間枠:Trimester 1
|
Summary of the number of days with spotting per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 1
|
Number of Days With Spotting - Trimester 2 (Safety Pop.)
時間枠:Trimester 2
|
Summary of the number of days with spotting per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 2
|
Number of Days With Spotting - Trimester 3 (Safety Pop.)
時間枠:Trimester 3
|
Summary of the number of days with spotting per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 3
|
Number of Days With Spotting - Trimester 4 (Safety Pop.)
時間枠:Trimester 4
|
Summary of the number of days with spotting per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 4
|
Subject Incidence With Bleeding - Trimester 1 (Safety Pop.)
時間枠:Trimester 1
|
Summary of subject incidence with bleeding per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 1
|
Subject Incidence With Bleeding - Trimester 2 (Safety Pop.)
時間枠:Trimester 2
|
Summary of subject incidence with bleeding per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 2
|
Subject Incidence With Bleeding - Trimester 3 (Safety Pop.)
時間枠:Trimester 3
|
Summary of subject incidence with bleeding per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 3
|
Subject Incidence With Bleeding - Trimester 4 (Safety Pop.)
時間枠:Trimester 4
|
Summary of subject incidence with bleeding per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 4
|
Number of Days With Bleeding - Trimester 1 (Safety Pop.)
時間枠:Trimester 1
|
Summary of the number of days with bleeding per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 1
|
Number of Days With Bleeding - Trimester 2 (Safety Pop.)
時間枠:Trimester 2
|
Summary of the number of days with bleeding per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 2
|
Number of Days With Bleeding - Trimester 3 (Safety Pop.)
時間枠:Trimester 3
|
Summary of the number of days with bleeding per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 3
|
Number of Days With Bleeding - Trimester 4 (Safety Pop.)
時間枠:Trimester 4
|
Summary of the number of days with bleeding per trimester as recorded in a daily diary.
A trimester is defined as every 90 days since Day 1.
|
Trimester 4
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Vasomotor Domain Score - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Changes in Vasomotor Domain Score from Baseline to Week 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Vasomotor domain score is mean of = Q1,Q2, Q3, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Week 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Vasomotor Domain Score - Month 6 (MITT-VMS)
時間枠:Baseline and Month 6
|
Changes in Vasomotor Domain Score from Baseline to Month 6.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Vasomotor domain score is mean of = Q1,Q2, Q3, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 6
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Vasomotor Domain Score - Month 12 (MITT-VMS)
時間枠:Baseline and Month 12
|
Changes in Vasomotor Domain Score from Baseline to Month 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Vasomotor domain score is mean of = Q1,Q2, Q3, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Psychosocial Domain Score - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Changes in Psychosocial Domain Score from Baseline to Week 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Psychosocial domain score is mean of = Q4 to Q10, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Week 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Psychosocial Domain Score - Month 6 (MITT-VMS)
時間枠:Baseline and Month 6
|
Changes in Psychosocial Domain Score from Baseline to Month 6.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Psychosocial domain score is mean of = Q4 to Q10, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 6
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Psychosocial Domain Score - Month 12 (MITT-VMS)
時間枠:Baseline and Month 12
|
Changes in Psychosocial Domain Score from Baseline to Month 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Psychosocial domain score is mean of = Q4 to Q10, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Physical Domain Score - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Changes in Physical Domain Score from Baseline to Week 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Physical domain score is mean of = Q11 to Q26, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Week 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Physical Domain Score - Month 6 (MITT-VMS)
時間枠:Baseline and Month 6
|
Changes in Physical Domain Score from Baseline to Month 6.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Physical domain score is mean of = Q11 to Q26, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 6
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Physical Domain Score - Month 12 (MITT-VMS)
時間枠:Baseline and Month 12
|
Changes in Physical Domain Score from Baseline to Month 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Physical domain score is mean of = Q11 to Q26, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Sexual Domain Score - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Changes in Sexual Domain Score from Baseline to Week 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Sexual domain score is mean of = Q27 to Q29, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Week 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Sexual Domain Score - Month 6 (MITT-VMS)
時間枠:Baseline and Month 6
|
Changes in Sexual Domain Score from Baseline to Month 6.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Sexual domain score is mean of = Q27 to Q29, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 6
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Sexual Domain Score - Month 12 (MITT-VMS)
時間枠:Baseline and Month 12
|
Changes in Sexual Domain Score from Baseline to Month 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Sexual domain score is mean of = Q27 to Q29, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Overall Scores - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Changes in Overall Scores from Baseline to Week 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The Overall Score is the mean of the 4 domain scores with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Week 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Overall Scores - Month 6 (MITT-VMS)
時間枠:Baseline and Month 6
|
Changes in Overall Scores from Baseline to Month 6.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The Overall Score is the mean of the 4 domain scores with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 6
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Overall Scores - Month 12 (MITT-VMS)
時間枠:Baseline and Month 12
|
Changes in Overall Scores from Baseline to Month 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The Overall Score is the mean of the 4 domain scores with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Sleep Scale - Total Sleep Score - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Total Sleep Score as compared w/Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Total score includes items Q1, 3, 4, 5, 6, 7, 8, 9, & 12. Scoring method: Answers to Q3, 5, 6, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q1, 4, & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Total score= average of item scores; ranges =0 to 100, where higher score means worse outcome.
If any of individual questions used to obtain total score is missing, total score will be set to missing value.
|
Baseline and Week 12
|
Medical Outcomes Sleep Study (MOS) Sleep Scale - Total Sleep Score - Month 6 (MITT-VMS)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Total Sleep Score as compared w/Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Total score includes items Q1, 3, 4, 5, 6, 7, 8, 9, & 12. Scoring method: Answers to Q3, 5, 6, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q1, 4, & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Total score= average of item scores; ranges =0 to 100, where higher score means worse outcome.
If any of individual questions used to obtain total score is missing, total score will be set to missing value.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Sleep Scale - Total Sleep Score - Month 12 (MITT-VMS)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Total Sleep Score as compared w/Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Total score includes items Q1, 3, 4, 5, 6, 7, 8, 9, & 12. Scoring method: Answers to Q3, 5, 6, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q1, 4, & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Total score= average of item scores; ranges =0 to 100, where higher score means worse outcome.
If any of individual questions used to obtain total score is missing, total score will be set to missing value.
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Disturbance - Week 12 (MITT-VMS)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Disturbance individual score as compared with Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep disturbance includes items Q1, Q3, Q7, Q8.
Scoring method: Answer to Q1 is rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25.
Answers to Q3, 7, 8 are reversed & rescaled to realign to be same direction and range(0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Score is average of item scores; score range=0 to 100, where higher score means worse outcome.
|
Baseline and Week 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Disturbance - Month 6 - (MITT-VMS)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Disturbance individual score as compared with Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep disturbance includes items Q1, Q3, Q7, Q8.
Scoring method: Answer to Q1 is rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25.
Answers to Q3, 7, 8 are reversed & rescaled to realign to be same direction and range(0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Score is average of item scores; score range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Disturbance - Month 12 - (MITT-VMS)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Disturbance individual score as compared with Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep disturbance includes items Q1, Q3, Q7, Q8.
Scoring method: Answer to Q1 is rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25.
Answers to Q3, 7, 8 are reversed & rescaled to realign to be same direction and range(0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Score is average of item scores; score range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Snoring - Week 12 - (MITT-VMS)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Snoring individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Snoring item is Q10.
Scoring method: Answer to Q10 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
|
Baseline and Week 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Snoring - Month 6 - (MITT-VMS)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Snoring individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Snoring item is Q10.
Scoring method: Answer to Q10 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Individual Score for Snoring - Month 12 - (MITT-VMS)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Snoring individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Snoring item is Q10.
Scoring method: Answer to Q10 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Short of Breath or Headache - Week 12 - (MITT-VMS)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Short of Breath or Headache(SOBHA) individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
SOBHA item is Q5.
Scoring method: Answer to Q5 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
|
Baseline and Week 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Short of Breath or Headache - Month 6 - (MITT-VMS)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Short of Breath or Headache(SOBHA) individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
SOBHA item is Q5.
Scoring method: Answer to Q5 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Short of Breath or Headache - Month 12 - (MITT-VMS)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Short of Breath or Headache(SOBHA) individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
SOBHA item is Q5.
Scoring method: Answer to Q5 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Adequacy - Week 12 - (MITT-VMS)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Adequacy individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Adequacy includes items Q4, Q12.
Scoring method: Answers for Q4 and Q12 are reversed and rescaled to 0-100 as follows: MOS_4_new = (6-MOS_4_old) x 20; MOS_12_new = (6-MOS_12_old) x 20.
Score is the average of item scores; score range = 0 to 100, where higher score means better outcome.
|
Baseline and Week 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Adequacy - Month 6 - (MITT-VMS)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Adequacy individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Adequacy includes items Q4, Q12.
Scoring method: Answers for Q4 and Q12 are reversed and rescaled to 0-100 as follows: MOS_4_new = (6-MOS_4_old) x 20; MOS_12_new = (6-MOS_12_old) x 20.
Score is the average of item scores; score range = 0 to 100, where higher score means better outcome.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Adequacy - Month 12 - (MITT-VMS)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Adequacy individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Adequacy includes items Q4, Q12.
Scoring method: Answers for Q4 and Q12 are reversed and rescaled to 0-100 as follows: MOS_4_new = (6-MOS_4_old) x 20; MOS_12_new = (6-MOS_12_old) x 20.
Score is the average of item scores; score range = 0 to 100, where higher score means better outcome.
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Somnolence - Week 12 - (MITT-VMS)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Somnolence individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Somnolence items include Q6, Q9, Q11.
Scoring method: Answers to Q6, Q 9 and Q11 are reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Week 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Somnolence - Month 6 - (MITT-VMS)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Somnolence individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Somnolence items include Q6, Q9, Q11.
Scoring method: Answers to Q6, Q 9 and Q11 are reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Somnolence - Month 12 - (MITT-VMS)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Somnolence individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Somnolence items include Q6, Q9, Q11.
Scoring method: Answers to Q6, Q 9 and Q11 are reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index I - Week 12 - (MITT-VMS)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Problems Index I individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index I includes items Q4, Q5, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q, 5, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q4, & 12 are rescaled to 0-100 as follows: MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Week 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index I - Month 6 - (MITT-VMS)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Problems Index I individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index I includes items Q4, Q5, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q, 5, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q4, & 12 are rescaled to 0-100 as follows: MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index I - Month 12 - (MITT-VMS)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Problems Index I individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index I includes items Q4, Q5, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q, 5, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q4, & 12 are rescaled to 0-100 as follows: MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index II - Week 12 - (MITT-VMS)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Problems Index II individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index II items include Q1, Q3, Q4, Q5, Q6, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q3, 5, 6, 7, 8, & 9 are reversed & rescaled to realign to be same direction and range 0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20, for n=Q3, 5, 6, 7, 8, and 9. Answers to Q1, 4 & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Week 12
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index II - Month 6 - (MITT-VMS)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Problems Index II individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index II items include Q1, Q3, Q4, Q5, Q6, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q3, 5, 6, 7, 8, & 9 are reversed & rescaled to realign to be same direction and range 0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20, for n=Q3, 5, 6, 7, 8, and 9. Answers to Q1, 4 & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index II - Month 12 - (MITT-VMS)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Problems Index II individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index II items include Q1, Q3, Q4, Q5, Q6, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q3, 5, 6, 7, 8, & 9 are reversed & rescaled to realign to be same direction and range 0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20, for n=Q3, 5, 6, 7, 8, and 9. Answers to Q1, 4 & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Optimal Sleep - Week 12 - (MITT-VMS)
時間枠:Baseline and Week 12
|
Change from Baseline (BL) to Week 12 in MOS Optimal Sleep Score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items measuring 6 dimensions of sleep over the past 4 wks.
Optimal sleep is based on Q2 (self-reported average hrs sleep per night in past 4 wks).
Scoring method: hrs of sleep coded 0 (non-optimal) or 1 (optimal) where 1-6 hrs & 9-23 hrs = 0, 7-8 hrs = 1.
Change from BL: subject sleeps 7-8 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = -1; subject sleeps 1-6 or 9-23 hrs at BL & 7-8 hrs at follow-up, change = +1; subject sleeps 1-6 or 9-23 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = 0. Mean change from BL: changes are summed to give the Net Total (equivalent to the number subjects w/ improved sleep hrs minus the number subjects w/ worsened sleep hrs), which is divided by the number of subjects to give the mean proportion of net change, where >0 = overall improvement and <0 = overall worsening in the study arm.
|
Baseline and Week 12
|
Medical Outcomes Sleep Study (MOS) Optimal Sleep - Month 6 - (MITT-VMS)
時間枠:Baseline and Month 6
|
Change from Baseline (BL) to Month 6 in MOS Optimal Sleep Score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items measuring 6 dimensions of sleep over the past 4 wks.
Optimal sleep is based on Q2 (self-reported average hrs sleep per night in past 4 wks).
Scoring method: hrs of sleep coded 0 (non-optimal) or 1 (optimal) where 1-6 hrs & 9-23 hrs = 0, 7-8 hrs = 1.
Change from BL: subject sleeps 7-8 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = -1; subject sleeps 1-6 or 9-23 hrs at BL & 7-8 hrs at follow-up, change = +1; subject sleeps 1-6 or 9-23 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = 0. Mean change from BL: changes are summed to give the Net Total (equivalent to the number subjects w/ improved sleep hrs minus the number subjects w/ worsened sleep hrs), which is divided by the number of subjects to give the mean proportion of net change, where >0 = overall improvement and <0 = overall worsening in the study arm.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Optimal Sleep - Month 12 - (MITT-VMS)
時間枠:Baseline and Month 12
|
Change from Baseline (BL) to Month 12 in MOS Optimal Sleep Score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items measuring 6 dimensions of sleep over the past 4 wks.
Optimal sleep is based on Q2 (self-reported average hrs sleep per night in past 4 wks).
Scoring method: hrs of sleep coded 0 (non-optimal) or 1 (optimal) where 1-6 hrs & 9-23 hrs = 0, 7-8 hrs = 1.
Change from BL: subject sleeps 7-8 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = -1; subject sleeps 1-6 or 9-23 hrs at BL & 7-8 hrs at follow-up, change = +1; subject sleeps 1-6 or 9-23 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = 0. Mean change from BL: changes are summed to give the Net Total (equivalent to the number subjects w/ improved sleep hrs minus the number subjects w/ worsened sleep hrs), which is divided by the number of subjects to give the mean proportion of net change, where >0 = overall improvement and <0 = overall worsening in the study arm.
|
Baseline and Month 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Vasomotor Domain Score - Week 12 (MITT)
時間枠:Baseline and Week 12
|
Changes in Vasomotor Domain Score from Baseline to Week 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Vasomotor domain score is mean of = Q1,Q2, Q3, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Week 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Vasomotor Domain Score - Month 6 (MITT)
時間枠:Baseline and Month 6
|
Changes in Vasomotor Domain Score from Baseline to Month 6.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Vasomotor domain score is mean of = Q1,Q2, Q3, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 6
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Vasomotor Domain Score - Month 12 (MITT)
時間枠:Baseline and Month 12
|
Changes in Vasomotor Domain Score from Baseline to Month 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Vasomotor domain score is mean of = Q1,Q2, Q3, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Psychosocial Domain Score - Week 12 (MITT)
時間枠:Baseline and Week 12
|
Changes in Psychosocial Domain Score from Baseline to Week 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Psychosocial domain score is mean of = Q4 to Q10, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Week 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Psychosocial Domain Score - Month 6 (MITT)
時間枠:Baseline and Month 6
|
Changes in Psychosocial Domain Score from Baseline to Month 6.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Psychosocial domain score is mean of = Q4 to Q10, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 6
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Psychosocial Domain Score - Month 12 (MITT)
時間枠:Baseline and Month 12
|
Changes in Psychosocial Domain Score from Baseline to Month 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Psychosocial domain score is mean of = Q4 to Q10, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Physical Domain Score - Week 12 (MITT)
時間枠:Baseline and Week 12
|
Changes in Physical Domain Score from Baseline to Week 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Physical domain score is mean of = Q11 to Q26, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Week 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Physical Domain Score - Month 6 (MITT)
時間枠:Baseline and Month 6
|
Changes in Physical Domain Score from Baseline to Month 6.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Physical domain score is mean of = Q11 to Q26, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 6
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Physical Domain Score - Month 12 (MITT)
時間枠:Baseline and Month 12
|
Changes in Physical Domain Score from Baseline to Month 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Physical domain score is mean of = Q11 to Q26, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Sexual Domain Score - Week 12 (MITT)
時間枠:Baseline and Week 12
|
Changes in Sexual Domain Score from Baseline to Week 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Sexual domain score is mean of = Q27 to Q29, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Week 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Sexual Domain Score - Month 6 (MITT)
時間枠:Baseline and Month 6
|
Changes in Sexual Domain Score from Baseline to Month 6.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Sexual domain score is mean of = Q27 to Q29, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 6
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Sexual Domain Score - Month 12 (MITT)
時間枠:Baseline and Month 12
|
Changes in Sexual Domain Score from Baseline to Month 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
Each domain is scored separately.
Sexual domain score is mean of = Q27 to Q29, with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Overall Scores - Week 12 (MITT)
時間枠:Baseline and Week 12
|
Change in Overall Scores from Baseline to Week 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The Overall Score is the mean of the 4 domain scores with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Week 12
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Overall Scores - Month 6 (MITT)
時間枠:Baseline and Month 6
|
Change in Overall Scores from Baseline to Month 6.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The Overall Score is the mean of the 4 domain scores with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 6
|
Menopause-specific Quality of Life Questionnaire (MENQOL) - Overall Scores - Month 12 (MITT)
時間枠:Baseline and Month 12
|
Change in Overall Scores from Baseline to Month 12.
The MENQOL is self-administered questionnaire which assessed changes in quality of life over a one-month period.
It is composed of 29 questions indicating if subject experienced the problem (Yes/No) and if Yes, rating scale ranged from 0=Not bothered at all to 6=Extremely bothered.
The scale contains four domains: vasomotor, psychosocial, physical and sexual.
For analysis, the original scores were converted to the analysis score ranging from 1-8 where No=1, 0=2, 1=3...and 6=8.
The Overall Score is the mean of the 4 domain scores with 1 being "not at all bothered" and 8 being "extremely bothered".
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Sleep Scale - Total Sleep Score - Week 12 (MITT)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Total Sleep Score as compared w/Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Total score includes items Q1, 3, 4, 5, 6, 7, 8, 9, & 12. Scoring method: Answers to Q3, 5, 6, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q1, 4, & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Total score= average of item scores; ranges =0 to 100, where higher score means worse outcome.
If any of individual questions used to obtain total score is missing, total score will be set to missing value.
|
Baseline and Week 12
|
Medical Outcomes Sleep Study (MOS) Sleep Scale - Total Sleep Score - Month 6 (MITT)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Total Sleep Score as compared w/Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Total score includes items Q1, 3, 4, 5, 6, 7, 8, 9, & 12. Scoring method: Answers to Q3, 5, 6, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q1, 4, & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Total score= average of item scores; ranges =0 to 100, where higher score means worse outcome.
If any of individual questions used to obtain total score is missing, total score will be set to missing value.
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Baseline and Month 6
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Medical Outcomes Sleep Study (MOS) Sleep Scale - Total Sleep Score - Month 12 (MITT)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Total Sleep Score as compared w/Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Total score includes items Q1, 3, 4, 5, 6, 7, 8, 9, & 12. Scoring method: Answers to Q3, 5, 6, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q1, 4, & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Total score= average of item scores; ranges =0 to 100, where higher score means worse outcome.
If any of individual questions used to obtain total score is missing, total score will be set to missing value.
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Baseline and Month 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Disturbance - Week 12 - (MITT)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Disturbance individual score as compared with Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep disturbance includes items Q1, Q3, Q7, Q8.
Scoring method: Answer to Q1 is rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25.
Answers to Q3, 7, 8 are reversed & rescaled to realign to be same direction and range(0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Score is average of item scores; score range=0 to 100, where higher score means worse outcome.
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Baseline and Week 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Disturbance - Month 6 - (MITT)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Disturbance individual score as compared with Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep disturbance includes items Q1, Q3, Q7, Q8.
Scoring method: Answer to Q1 is rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25.
Answers to Q3, 7, 8 are reversed & rescaled to realign to be same direction and range(0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Score is average of item scores; score range=0 to 100, where higher score means worse outcome.
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Baseline and Month 6
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Disturbance - Month 12 - (MITT)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Disturbance individual score as compared with Placebo.
MOS-Sleep Self Report Questionnaire is 12 items that measure 6 dimensions of sleep over past 4 wks.
Q1 scored on scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 self-reported hrs of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep disturbance includes items Q1, Q3, Q7, Q8.
Scoring method: Answer to Q1 is rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25.
Answers to Q3, 7, 8 are reversed & rescaled to realign to be same direction and range(0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Score is average of item scores; score range=0 to 100, where higher score means worse outcome.
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Baseline and Month 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Snoring - Week 12 - (MITT)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Snoring individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Snoring item is Q10.
Scoring method: Answer to Q10 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
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Baseline and Week 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Snoring - Month 6 - (MITT)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Snoring individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Snoring item is Q10.
Scoring method: Answer to Q10 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
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Baseline and Month 6
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Medical Outcomes Sleep Study (MOS) Individual Score for Snoring - Month 12 - (MITT)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Snoring individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Snoring item is Q10.
Scoring method: Answer to Q10 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
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Baseline and Month 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Short of Breath or Headache - Week 12 - (MITT)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Short of Breath or Headache(SOBHA) individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
SOBHA item is Q5.
Scoring method: Answer to Q5 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
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Baseline and Week 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Short of Breath or Headache - Month 6 - (MITT)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Short of Breath or Headache(SOBHA) individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
SOBHA item is Q5.
Scoring method: Answer to Q5 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
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Baseline and Month 6
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Short of Breath or Headache - Month 12 - (MITT)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Short of Breath or Headache(SOBHA) individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
SOBHA item is Q5.
Scoring method: Answer to Q5 is reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score range=0 to 100, where higher score means worse outcome.
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Baseline and Month 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Adequacy - Week 12 - (MITT)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Adequacy individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Adequacy includes items Q4, Q12.
Scoring method: Answers for Q4 and Q12 are reversed and rescaled to 0-100 as follows: MOS_4_new = (6-MOS_4_old) x 20; MOS_12_new = (6-MOS_12_old) x 20.
Score is the average of item scores; score range = 0 to 100, where higher score means better outcome.
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Baseline and Week 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Adequacy - Month 6 - (MITT)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Adequacy individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Adequacy includes items Q4, Q12.
Scoring method: Answers for Q4 and Q12 are reversed and rescaled to 0-100 as follows: MOS_4_new = (6-MOS_4_old) x 20; MOS_12_new = (6-MOS_12_old) x 20.
Score is the average of item scores; score range = 0 to 100, where higher score means better outcome.
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Baseline and Month 6
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Adequacy - Month 12 - (MITT)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Adequacy individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Adequacy includes items Q4, Q12.
Scoring method: Answers for Q4 and Q12 are reversed and rescaled to 0-100 as follows: MOS_4_new = (6-MOS_4_old) x 20; MOS_12_new = (6-MOS_12_old) x 20.
Score is the average of item scores; score range = 0 to 100, where higher score means better outcome.
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Baseline and Month 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Somnolence - Week 12 - (MITT)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Somnolence individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Somnolence items include Q6, Q9, Q11.
Scoring method: Answers to Q6, Q 9 and Q11 are reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
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Baseline and Week 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Somnolence - Month 6 - (MITT)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Somnolence individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Somnolence items include Q6, Q9, Q11.
Scoring method: Answers to Q6, Q 9 and Q11 are reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 6
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Somnolence - Month 12 - (MITT)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Somnolence individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-Q12 are scored 1-6 ranging from 1=All of the time to 6=None of the time.
Sleep Somnolence items include Q6, Q9, Q11.
Scoring method: Answers to Q6, Q 9 and Q11 are reversed & rescaled to 0 to 100 such that 0="best possible" & 100="worst possible".
MOS_n_new <- (6-MOS_n_old) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
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Baseline and Month 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index I - Week 12 - (MITT)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Problems Index I individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index I includes items Q4, Q5, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q, 5, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q4, & 12 are rescaled to 0-100 as follows: MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
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Baseline and Week 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index I - Month 6 - (MITT)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Problems Index I individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index I includes items Q4, Q5, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q, 5, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q4, & 12 are rescaled to 0-100 as follows: MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
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Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index I - Month 12 - (MITT)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Problems Index I individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self-reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index I includes items Q4, Q5, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q, 5, 7, 8, 9 are reversed & rescaled to realign to be same direction and range (0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20.
Answers to Q4, & 12 are rescaled to 0-100 as follows: MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 12
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Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index II - Week 12 - (MITT)
時間枠:Baseline and Week 12
|
Change from Baseline to Wk 12 in MOS Sleep Problems Index II individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index II items include Q1, Q3, Q4, Q5, Q6, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q3, 5, 6, 7, 8, & 9 are reversed & rescaled to realign to be same direction and range 0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20, for n=Q3, 5, 6, 7, 8, and 9. Answers to Q1, 4 & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
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Baseline and Week 12
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Medical Outcomes Sleep Study (MOS) Sleep Problems Index II - Month 6 - (MITT)
時間枠:Baseline and Month 6
|
Change from Baseline to Month 6 in MOS Sleep Problems Index II individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index II items include Q1, Q3, Q4, Q5, Q6, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q3, 5, 6, 7, 8, & 9 are reversed & rescaled to realign to be same direction and range 0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20, for n=Q3, 5, 6, 7, 8, and 9. Answers to Q1, 4 & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Individual Score for Sleep Problems Index II - Month 12 - (MITT)
時間枠:Baseline and Month 12
|
Change from Baseline to Month 12 in MOS Sleep Problems Index II individual score as compared with Placebo.
The MOS-Sleep Self Report Questionnaire is composed of 12 items that measure 6 dimensions of sleep over the past 4 weeks.
Q1 is scored on a scale 1-5: 1=0-15 min, 2=16-30 min...5=>60 mins.
Q2 is self reported hours of sleep per night.
Q3-12 scored 1-6 where 1=All of the time to 6=None of the time.
Sleep Problems Index II items include Q1, Q3, Q4, Q5, Q6, Q7, Q8, Q9, Q12.
Scoring method: Answers to Q3, 5, 6, 7, 8, & 9 are reversed & rescaled to realign to be same direction and range 0 to 100 with 0="best possible" & 100="worst possible" as follows: MOS_n_new = (6-MOS_n_old) x 20, for n=Q3, 5, 6, 7, 8, and 9. Answers to Q1, 4 & 12 are rescaled to 0-100 as follows: MOS_1_new =(MOS_1_old - 1) x 25; MOS_4_new =(MOS_4_old - 1) x 20; MOS_12_new=(MOS_12_old - 1) x 20.
Score is the average of item scores; score range range=0 to 100, where higher score means worse outcome.
|
Baseline and Month 12
|
Medical Outcomes Sleep Study (MOS) Optimal Sleep - Week 12 - (MITT)
時間枠:Baseline and Week 12
|
Change from Baseline (BL) to Wk 12 in MOS Optimal Sleep Score as compared with Placebo.The MOS-Sleep Self Report Questionnaire is composed of 12 items measuring 6 dimensions of sleep over the past 4 wks.
Optimal sleep is based on Q2 (self-reported average hrs sleep per night in past 4 wks).
Scoring method: hrs of sleep coded 0 (non-optimal) or 1 (optimal) where 1-6 hrs & 9-23 hrs = 0, 7-8 hrs = 1.
Change from BL: subject sleeps 7-8 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = -1; subject sleeps 1-6 or 9-23 hrs at BL & 7-8 hrs at follow-up, change = +1; subject sleeps 1-6 or 9-23 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = 0. Mean change from BL: changes are summed to give the Net Total (equivalent to the number subjects w/ improved sleep hrs minus the number subjects w/ worsened sleep hrs), which is divided by the number of subjects to give the mean proportion of net change, where >0 = overall improvement and <0 = overall worsening in the study arm.
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Baseline and Week 12
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Medical Outcomes Sleep Study (MOS) Optimal Sleep - Month 6 - (MITT)
時間枠:Baseline and Month 6
|
Change from Baseline (BL) to Month 6 in MOS Optimal Sleep Score as compared with Placebo.The MOS-Sleep Self Report Questionnaire is composed of 12 items measuring 6 dimensions of sleep over the past 4 wks.
Optimal sleep is based on Q2 (self-reported average hrs sleep per night in past 4 wks).
Scoring method: hrs of sleep coded 0 (non-optimal) or 1 (optimal) where 1-6 hrs & 9-23 hrs = 0, 7-8 hrs = 1.
Change from BL: subject sleeps 7-8 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = -1; subject sleeps 1-6 or 9-23 hrs at BL & 7-8 hrs at follow-up, change = +1; subject sleeps 1-6 or 9-23 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = 0. Mean change from BL: changes are summed to give the Net Total (equivalent to the number subjects w/ improved sleep hrs minus the number subjects w/ worsened sleep hrs), which is divided by the number of subjects to give the mean proportion of net change, where >0 = overall improvement and <0 = overall worsening in the study arm.
|
Baseline and Month 6
|
Medical Outcomes Sleep Study (MOS) Optimal Sleep - Month 12 - (MITT)
時間枠:Baseline and Month 12
|
Change from Baseline (BL) to Month 12 in MOS Optimal Sleep Score as compared with Placebo.The MOS-Sleep Self Report Questionnaire is composed of 12 items measuring 6 dimensions of sleep over the past 4 wks.
Optimal sleep is based on Q2 (self-reported average hrs sleep per night in past 4 wks).
Scoring method: hrs of sleep coded 0 (non-optimal) or 1 (optimal) where 1-6 hrs & 9-23 hrs = 0, 7-8 hrs = 1.
Change from BL: subject sleeps 7-8 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = -1; subject sleeps 1-6 or 9-23 hrs at BL & 7-8 hrs at follow-up, change = +1; subject sleeps 1-6 or 9-23 hrs at BL & 1-6 or 9-23 hrs at follow-up, change = 0. Mean change from BL: changes are summed to give the Net Total (equivalent to the number subjects w/ improved sleep hrs minus the number subjects w/ worsened sleep hrs), which is divided by the number of subjects to give the mean proportion of net change, where >0 = overall improvement and <0 = overall worsening in the study arm.
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Baseline and Month 12
|
協力者と研究者
スポンサー
捜査官
- スタディディレクター:Sebastian Mirkin, MD、TherapeuticsMD
出版物と役立つリンク
一般刊行物
- Revicki D, Hays RD, Cella D, Sloan J. Recommended methods for determining responsiveness and minimally important differences for patient-reported outcomes. J Clin Epidemiol. 2008 Feb;61(2):102-9. doi: 10.1016/j.jclinepi.2007.03.012. Epub 2007 Aug 3.
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- Spritzer, K. L. & Hays, R. D. (2003, November). MOS Sleep Scale: A Manual for Use and Scoring, Version 1.0. Los Angeles, CA.
- Kurman RJ, Ellenson L H, and Ronnett B.M., ed. Blaustein's Pathology of the Female Genital Tract. 6th ed. New York, NY: Springer; 2011:305-452.
- Hays RD and Stewart AL. Sleep measures. In AL Stewart & JE Ware (eds), Measuring functioning and well-being: The Medical Outcomes Study approach (pp 235-259). Durham, NC: Duke University Press, 1992.
- McClung MR, Kagan R, Graham S, Bernick B, Mirkin S, Constantine G. Effects of E2/P4 oral capsules on bone turnover in women with vasomotor symptoms. Menopause. 2022 Feb 14;29(3):304-308. doi: 10.1097/GME.0000000000001915.
- Constantine GD, Simon JA, Kaunitz AM, Pickar JH, Revicki DA, Graham S, Bernick B, Mirkin S. TX-001HR is associated with a clinically meaningful effect on severity of moderate to severe vasomotor symptoms in the REPLENISH trial. Menopause. 2020 Nov;27(11):1236-1241. doi: 10.1097/GME.0000000000001602.
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- Kaunitz AM, Bitner D, Constantine GD, Bernick B, Graham S, Mirkin S. 17beta-estradiol/progesterone in a single, oral, softgel capsule (TX-001HR) significantly increased the number of vasomotor symptom-free days in the REPLENISH trial. Menopause. 2020 Dec;27(12):1382-1387. doi: 10.1097/GME.0000000000001615.
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- Mirkin S, Graham S, Revicki DA, Bender RH, Bernick B, Constantine GD. Relationship between vasomotor symptom improvements and quality of life and sleep outcomes in menopausal women treated with oral, combined 17beta-estradiol/progesterone. Menopause. 2019 Jan 9;26(6):637-642. doi: 10.1097/GME.0000000000001294.
- Kagan R, Constantine G, Kaunitz AM, Bernick B, Mirkin S. Improvement in sleep outcomes with a 17beta-estradiol-progesterone oral capsule (TX-001HR) for postmenopausal women. Menopause. 2018 Dec 21;26(6):622-628. doi: 10.1097/GME.0000000000001278.
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- Mirkin S, Amadio JM, Bernick BA, Pickar JH, Archer DF. 17beta-Estradiol and natural progesterone for menopausal hormone therapy: REPLENISH phase 3 study design of a combination capsule and evidence review. Maturitas. 2015 May;81(1):28-35. doi: 10.1016/j.maturitas.2015.02.266. Epub 2015 Mar 9.
研究記録日
主要日程の研究
研究開始 (実際)
一次修了 (実際)
研究の完了 (実際)
試験登録日
最初に提出
QC基準を満たした最初の提出物
最初の投稿 (見積もり)
学習記録の更新
投稿された最後の更新 (実際)
QC基準を満たした最後の更新が送信されました
最終確認日
詳しくは
本研究に関する用語
キーワード
追加の関連 MeSH 用語
その他の研究ID番号
- TXC12-05
- REPLENISH Trial (その他の識別子:Sponsor)
この情報は、Web サイト clinicaltrials.gov から変更なしで直接取得したものです。研究の詳細を変更、削除、または更新するリクエストがある場合は、register@clinicaltrials.gov。 までご連絡ください。 clinicaltrials.gov に変更が加えられるとすぐに、ウェブサイトでも自動的に更新されます。
プラセボの臨床試験
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Palacky University完了
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Universidade Federal do ParaConselho Nacional de Desenvolvimento Científico e Tecnológico完了
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Advice Pharma Group srl積極的、募集していない肥満 | 栄養障害 | 体重 | 減量 | 食生活 | 太りすぎと肥満 | 健康行動 | ダイエット、健康 | ダイエット習慣 | ライフスタイル | 栄養、健康 | 行動障害イタリア
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University Hospital, Strasbourg, France積極的、募集していない