- ICH GCP
- Yhdysvaltain kliinisten tutkimusten rekisteri
- Kliininen tutkimus NCT00829166
A Study of Trastuzumab Emtansine Versus Capecitabine + Lapatinib in Participants With HER2-positive Locally Advanced or Metastatic Breast Cancer (EMILIA)
lauantai 10. syyskuuta 2016 päivittänyt: Hoffmann-La Roche
A Randomized, Multicenter, Phase III Open-label Study of the Efficacy and Safety of Trastuzumab MCC-DM1 vs. Capecitabine + Lapatinib in Patients With HER2-Positive Locally Advanced or Metastatic Breast Cancer Who Have Received Prior Trastuzumab-Based Therapy
This is a Phase III, randomized, multicenter, international, 2-arm, open-label clinical trial designed to compare the safety and efficacy of trastuzumab emtansine (T-DM1) with that of capecitabine + lapatinib in participants with human epidermal growth factor receptor 2 (HER2)-positive locally advanced or metastatic breast cancer.
Participants will be treated until disease progression (PD), unmanageable toxicity, or study termination.
Once disease progression is reported, all participants will be followed for survival every 3 months until death, loss to follow-up, withdrawal of consent, or study termination.
Tutkimuksen yleiskatsaus
Tila
Valmis
Ehdot
Interventio / Hoito
Opintotyyppi
Interventio
Ilmoittautuminen (Todellinen)
991
Vaihe
- Vaihe 3
Yhteystiedot ja paikat
Tässä osiossa on tutkimuksen suorittajien yhteystiedot ja tiedot siitä, missä tämä tutkimus suoritetaan.
Opiskelupaikat
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Banja Luka, Bosnia ja Hertsegovina, 78000
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Sarajewo, Bosnia ja Hertsegovina, 71000
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Belo Horizonte, Brasilia, 30150-281
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Curitiba, Brasilia, 80530-010
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Goiania, Brasilia, 74605-070
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Itajai, Brasilia, 88301-220
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JAU, Brasilia, 17210-080
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Joao Pessoa, Brasilia, 58040280
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Porto Alegre, Brasilia, 90610-000
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Porto Alegre, Brasilia, 91350-200
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Porto Alegre, Brasilia, 90430-090
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Porto Alegre - Rs, Brasilia, 90050-170
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Rio de Janeiro, Brasilia, 20560-120
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Rio de Janeiro, Brasilia, 22260-020
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Santo Andre, Brasilia, 09060-870
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Sao Paulo, Brasilia, 1323020
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Sao Paulo, Brasilia, 01317-000
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Plovdiv, Bulgaria, 4000
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Sofia, Bulgaria, 1756
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Sofia, Bulgaria, 1784
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Varna, Bulgaria, 9002
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Barcelona, Espanja, 08035
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Córdoba, Espanja, 14004
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Lerida, Espanja, 25198
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Madrid, Espanja, 28046
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Madrid, Espanja, 28041
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Santander, Espanja, 39008
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Sevilla, Espanja, 41013
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Valencia, Espanja, 46009
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Zaragoza, Espanja, 50009
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Diliman, Quezon City, Filippiinit, 1100
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Quezon City, Luzon, Filippiinit, 1101
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Hong Kong, Hong Kong
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Bangalore, Intia, 560027
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Gurgaon, Intia, 122001
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Kolkata, Intia, 700 053
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New Delhi, Intia, 110029
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Pune, Intia, 411004
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Aviano, Italia, 33081
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Bologna, Italia, 40138
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Candiolo, Italia, 10060
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Genova, Italia, 16132
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Meldola, Italia, 47014
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Milano, Italia, 20133
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Milano, Italia, 20141
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Napoli, Italia, 80131
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Negrar, Italia, 37024
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Pisa, Italia, 56100
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Reggio Emilia, Italia, 42100
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Roma, Italia, 00168
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Rozzano, Italia, 20089
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Sassari, Italia, 07100
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Terni, Italia, 05100
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Alberta
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Calgary, Alberta, Kanada, T2N 4N2
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Edmonton, Alberta, Kanada, T6G 1Z2
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British Columbia
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Kelowna, British Columbia, Kanada, V1Y 5L3
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Vancouver, British Columbia, Kanada, V5Z 1H5
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Nova Scotia
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Halifax, Nova Scotia, Kanada, B3H 2Y9
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Ontario
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Ottawa, Ontario, Kanada, K1H 8L6
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Sudbury, Ontario, Kanada, J9P 3Y1
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Toronto, Ontario, Kanada, M4N 3M5
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Quebec
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Greenfield Park, Quebec, Kanada, J4V 2H1
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Montreal, Quebec, Kanada, H1T 2M4
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Montreal, Quebec, Kanada, H3T 1E2
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Montreal, Quebec, Kanada, H2W 1T8
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Bogota, Kolumbia
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Bogota, Kolumbia, 49 00
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Monteria, Kolumbia
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Kyunggi-do, Korean tasavalta, 411-769
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Seoul, Korean tasavalta, 110-744
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Seoul, Korean tasavalta, 120-752
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Seoul, Korean tasavalta, 135-710
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Acapulco, Meksiko, 39670
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Oaxaca, Meksiko, 68000
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Toluca, Meksiko, 50180
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Coimbra, Portugali, 3000-075
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Lisboa, Portugali, 1649-035
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Porto, Portugali, 4200-072
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Bialystok, Puola, 15-027
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Gdansk, Puola, 80-952
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Krakow, Puola, 31-531
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Lublin, Puola, 20-090
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Opole, Puola, 45-060
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Poznan, Puola, 61-866
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Warszawa, Puola, 02-781
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Avignon, Ranska, 84082
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Bordeaux, Ranska, 33076
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Brest, Ranska, 29609
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Caen, Ranska, 14076
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Dijon, Ranska, 21079
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La Roche Sur Yon, Ranska, 85925
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Montpellier, Ranska, 34298
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Paris, Ranska, 75248
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Saint Brieuc, Ranska, 22015
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Saint Herblain, Ranska, 44805
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Vandoeuvre-les-nancy, Ranska, 54511
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Eskilstuna, Ruotsi, 63188
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Gaelve, Ruotsi, 80187
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Goteborg, Ruotsi, 40036
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Aschaffenburg, Saksa, 63739
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Berlin, Saksa, 10367
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Berlin, Saksa, 13125
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Berlin, Saksa, 4169
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Bonn, Saksa, 53113
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Dortmund, Saksa, 44137
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Freiburg, Saksa, 79106
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Fuerstenwalde, Saksa, 15517
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Hamburg, Saksa, 20357
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Karlsruhe, Saksa, 76135
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Kiel, Saksa, 24105
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Offenbach, Saksa, 63069
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Stralsund, Saksa, 18435
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Singapore, Singapore, 119074
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Singapore, Singapore, 169610
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Ljubljana, Slovenia, 1000
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Helsinki, Suomi, 00180
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Tampere, Suomi, 33520
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Turku, Suomi, 20520
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Luzern, Sveitsi, 6004
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St. Gallen, Sveitsi, 9007
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Kaohsung, Taiwan, 883
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Taichung, Taiwan, 404
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Taichung, Taiwan, 407
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Taipei, Taiwan, 112
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Taoyuan, Taiwan, 333
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Herlev, Tanska, 2730
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København, Tanska, 2100
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Odense, Tanska, 5000
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Newtown, Uusi Seelanti, 6021
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Palmerston North, Uusi Seelanti, 4442
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Kemerovo, Venäjän federaatio, 650036
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Moscow, Venäjän federaatio, 121356
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St Petersburg, Venäjän federaatio, 197758
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Bournemouth, Yhdistynyt kuningaskunta, BH7 7DW
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Cardiff, Yhdistynyt kuningaskunta, CF14 2TL
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Denbigh, Yhdistynyt kuningaskunta, LL18 5UJ
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London, Yhdistynyt kuningaskunta, SE1 7EH
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London, Yhdistynyt kuningaskunta, SW3 6JJ
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Manchester, Yhdistynyt kuningaskunta, M20 4BX
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New Castle Upon Tyne, Yhdistynyt kuningaskunta, NE7 7DN
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Northwood, Yhdistynyt kuningaskunta, HA6 2RN
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Poole, Yhdistynyt kuningaskunta, BH15 2JB
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Preston, Yhdistynyt kuningaskunta, PR2 9HT
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Romford, Yhdistynyt kuningaskunta, RM7 0AG
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Sutton, Yhdistynyt kuningaskunta, SM2 5PT
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Weston Super Mare, Yhdistynyt kuningaskunta, BS23 4TQ
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Arizona
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Chandler, Arizona, Yhdysvallat, 85224
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Tucson, Arizona, Yhdysvallat, 85719
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California
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Anaheim, California, Yhdysvallat, 92801
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Anaheim, California, Yhdysvallat, 92807
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Bakersfield, California, Yhdysvallat, 93309
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Baldwin Park, California, Yhdysvallat, 91706
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Bellflower, California, Yhdysvallat, 90706
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Duarte, California, Yhdysvallat, 91010
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Fontana, California, Yhdysvallat, 92335
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Hayward, California, Yhdysvallat, 94545
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Irvine, California, Yhdysvallat, 92618
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La Jolla, California, Yhdysvallat, 92093
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La Mesa, California, Yhdysvallat, 91942
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Loma Linda, California, Yhdysvallat, 92354
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Long Beach, California, Yhdysvallat, 90806
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Los Angeles, California, Yhdysvallat, 90025
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Los Angeles, California, Yhdysvallat, 90057
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Los Angeles, California, Yhdysvallat, 90095-1772
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Los Angeles, California, Yhdysvallat, 90034
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Montebello, California, Yhdysvallat, 90640
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Newport Beach, California, Yhdysvallat, 92660
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Oakland, California, Yhdysvallat, 94611
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Panorama City, California, Yhdysvallat, 91402
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Riverside, California, Yhdysvallat, 92505
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Roseville, California, Yhdysvallat, 95661
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Sacramento, California, Yhdysvallat, 95825
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San Diego, California, Yhdysvallat, 92123
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San Diego, California, Yhdysvallat, 92120
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San Francisco, California, Yhdysvallat, 94115
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San Jose, California, Yhdysvallat, 95119
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Santa Clara, California, Yhdysvallat, 95051
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Santa Maria, California, Yhdysvallat, 93454
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Santa Monica, California, Yhdysvallat, 90404
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South San Francisco, California, Yhdysvallat, 94080
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Thousand Oaks, California, Yhdysvallat, 91360
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Vallejo, California, Yhdysvallat, 94589
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Walnut Creek, California, Yhdysvallat, 94596
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Woodland Hills, California, Yhdysvallat, 91367
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Colorado
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Fort Collins, Colorado, Yhdysvallat, 80528
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Connecticut
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Norwalk, Connecticut, Yhdysvallat, 06856
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Norwich, Connecticut, Yhdysvallat, 06360
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Stamford, Connecticut, Yhdysvallat, 06902
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District of Columbia
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Washington, District of Columbia, Yhdysvallat, 20010
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Florida
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Boca Raton, Florida, Yhdysvallat, 33486
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Fernandina Beach, Florida, Yhdysvallat, 32034
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Fort Myers, Florida, Yhdysvallat, 33916
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Ft. Lauderdale, Florida, Yhdysvallat, 33316
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Hollywood, Florida, Yhdysvallat, 33021
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Jacksonville, Florida, Yhdysvallat, 32205
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Jacksonville, Florida, Yhdysvallat, 32256
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Jacksonville, Florida, Yhdysvallat, 32207
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Jacksonville, Florida, Yhdysvallat, 32258
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Kissimmee, Florida, Yhdysvallat, 34741
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Lakeland, Florida, Yhdysvallat, 33804-1057
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Miami, Florida, Yhdysvallat, 33136
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Miami, Florida, Yhdysvallat, 33176
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Miami, Florida, Yhdysvallat, 33133
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Orange Park, Florida, Yhdysvallat, 32073
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Pembroke Pines, Florida, Yhdysvallat, 33028
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Georgia
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Athens, Georgia, Yhdysvallat, 30607
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Atlanta, Georgia, Yhdysvallat, 30342
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Atlanta, Georgia, Yhdysvallat, 30322
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Atlanta, Georgia, Yhdysvallat, 30341
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Atlanta, Georgia, Yhdysvallat, 30318
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Carrolton, Georgia, Yhdysvallat, 30117
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Cartersville, Georgia, Yhdysvallat, 30121
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Decatur, Georgia, Yhdysvallat, 30033
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Douglasville, Georgia, Yhdysvallat, 30134
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Macon, Georgia, Yhdysvallat, 31217
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Marietta, Georgia, Yhdysvallat, 30060
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Idaho
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Boise, Idaho, Yhdysvallat, 83712
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Meridian, Idaho, Yhdysvallat, 83642
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Nampa, Idaho, Yhdysvallat, 83686
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Post Falls, Idaho, Yhdysvallat, 83854
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Twin Falls, Idaho, Yhdysvallat, 83301
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Illinois
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Chicago, Illinois, Yhdysvallat, 60612
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Decatur, Illinois, Yhdysvallat, 62526
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Effingham, Illinois, Yhdysvallat, 62526
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Joliet, Illinois, Yhdysvallat, 60435
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Morris, Illinois, Yhdysvallat, 60450
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Peoria, Illinois, Yhdysvallat, 61615-7828
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Skokie, Illinois, Yhdysvallat, 60076
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Zion, Illinois, Yhdysvallat, 60099
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Iowa
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Bettendorf, Iowa, Yhdysvallat, 52722
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Kansas
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Wichita, Kansas, Yhdysvallat, 67214-3728
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Kentucky
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Paducah, Kentucky, Yhdysvallat, 42001
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Louisiana
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Covington, Louisiana, Yhdysvallat, 70433
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Lafayette, Louisiana, Yhdysvallat, 70503
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Marrero, Louisiana, Yhdysvallat, 70072
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Metairie, Louisiana, Yhdysvallat, 70006
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New Orleans, Louisiana, Yhdysvallat, 70115
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Maine
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Kittery, Maine, Yhdysvallat, 03904
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Wells, Maine, Yhdysvallat, 04090
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York, Maine, Yhdysvallat, 03909
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Maryland
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Baltimore, Maryland, Yhdysvallat, 21202
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Baltimore, Maryland, Yhdysvallat, 21237
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Bethesda, Maryland, Yhdysvallat, 20817
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Rockville, Maryland, Yhdysvallat, 20850
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Massachusetts
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Boston, Massachusetts, Yhdysvallat, 02215
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Boston, Massachusetts, Yhdysvallat, 02114
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Boston, Massachusetts, Yhdysvallat, 02118
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Boston, Massachusetts, Yhdysvallat, 02115
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Burlington, Massachusetts, Yhdysvallat, 01805
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Peabody, Massachusetts, Yhdysvallat, 01960
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Michigan
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Brownstown, Michigan, Yhdysvallat, 48183
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Dearborn, Michigan, Yhdysvallat, 48126
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Detroit, Michigan, Yhdysvallat, 48201
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Detroit, Michigan, Yhdysvallat, 48202
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Saint Joseph, Michigan, Yhdysvallat, 49085
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West Bloomfield, Michigan, Yhdysvallat, 48322
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Minnesota
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Edina, Minnesota, Yhdysvallat, 55414
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Maplewood, Minnesota, Yhdysvallat, 55109
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Minneapolis, Minnesota, Yhdysvallat, 55454
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Saint Louis Park, Minnesota, Yhdysvallat, 55426
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Saint Paul, Minnesota, Yhdysvallat, 55101
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St. Louis Park, Minnesota, Yhdysvallat, 55426
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Missouri
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Joplin, Missouri, Yhdysvallat, 64804
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Kansas City, Missouri, Yhdysvallat, 64111
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Saint Louis, Missouri, Yhdysvallat, 63110
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Saint Peters, Missouri, Yhdysvallat, 63110
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St. Louis, Missouri, Yhdysvallat, 63141
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St. Peters, Missouri, Yhdysvallat, 63376
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Montana
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Missoula, Montana, Yhdysvallat, 59802
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Nebraska
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Omaha, Nebraska, Yhdysvallat, 68114
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Nevada
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Henderson, Nevada, Yhdysvallat, 89052
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New Jersey
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Cherry Hill, New Jersey, Yhdysvallat, 08002
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Hackensack, New Jersey, Yhdysvallat, 07601
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Morristown, New Jersey, Yhdysvallat, 07962
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Parsippany, New Jersey, Yhdysvallat, 07054
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Voorhees, New Jersey, Yhdysvallat, 08043
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New Mexico
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Santa Fe, New Mexico, Yhdysvallat, 87505
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New York
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Brockport, New York, Yhdysvallat, 14420
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Canandaigua, New York, Yhdysvallat, 14424
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Fresh Meadows, New York, Yhdysvallat, 11366
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Geneva, New York, Yhdysvallat, 14456
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Greece, New York, Yhdysvallat, 14626
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Lake Success, New York, Yhdysvallat, 11042
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Mount Kisco, New York, Yhdysvallat, 10549
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Rochester, New York, Yhdysvallat, 14626
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Stony Brook, New York, Yhdysvallat, 11794
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North Carolina
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Charlotte, North Carolina, Yhdysvallat, 28203
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Durham, North Carolina, Yhdysvallat, 27710
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Hickory, North Carolina, Yhdysvallat, 28602
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Kinston, North Carolina, Yhdysvallat, 28501
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Washington, North Carolina, Yhdysvallat, 27889
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Ohio
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Cleveland, Ohio, Yhdysvallat, 44195
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Cleveland, Ohio, Yhdysvallat, 44106
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Columbus, Ohio, Yhdysvallat, 43215
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Columbus, Ohio, Yhdysvallat, 43219
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Columbus, Ohio, Yhdysvallat, 43228
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Middletown, Ohio, Yhdysvallat, 45042
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Newark, Ohio, Yhdysvallat, 43055
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Sandusky, Ohio, Yhdysvallat, 44870
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Oregon
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Portland, Oregon, Yhdysvallat, 97227
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Pennsylvania
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Philadelphia, Pennsylvania, Yhdysvallat, 19124
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Philadelphia, Pennsylvania, Yhdysvallat, 19106
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Pittsburgh, Pennsylvania, Yhdysvallat, 15232
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Pittsburgh, Pennsylvania, Yhdysvallat, 15213
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Rhode Island
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East Providence, Rhode Island, Yhdysvallat, 02915
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South Carolina
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Columbia, South Carolina, Yhdysvallat, 29210
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North Charleston, South Carolina, Yhdysvallat, 29425
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Tennessee
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Memphis, Tennessee, Yhdysvallat, 38120
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Nashville, Tennessee, Yhdysvallat, 37203
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Texas
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Austin, Texas, Yhdysvallat, 78731
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Bryan, Texas, Yhdysvallat, 77802
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Cypress, Texas, Yhdysvallat, 77429
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Dallas, Texas, Yhdysvallat, 75230
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El Paso, Texas, Yhdysvallat, 79902
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Houston, Texas, Yhdysvallat, 77090
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Shenandoah, Texas, Yhdysvallat, 77384
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Temple, Texas, Yhdysvallat, 76501
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Virginia
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Fairfax, Virginia, Yhdysvallat, 22031
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Washington
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Gig Harbor, Washington, Yhdysvallat, 98332
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Lakewood, Washington, Yhdysvallat, 98499
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Puyallup, Washington, Yhdysvallat, 98372
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Tacoma, Washington, Yhdysvallat, 98405
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Wisconsin
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Milwaukee, Wisconsin, Yhdysvallat, 53226
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Wausau, Wisconsin, Yhdysvallat, 54401
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Osallistumiskriteerit
Tutkijat etsivät ihmisiä, jotka sopivat tiettyyn kuvaukseen, jota kutsutaan kelpoisuuskriteereiksi. Joitakin esimerkkejä näistä kriteereistä ovat henkilön yleinen terveydentila tai aiemmat hoidot.
Kelpoisuusvaatimukset
Opintokelpoiset iät
18 vuotta ja vanhemmat (Aikuinen, Vanhempi Aikuinen)
Hyväksyy terveitä vapaaehtoisia
Ei
Sukupuolet, jotka voivat opiskella
Kaikki
Kuvaus
Inclusion Criteria:
- HER2 status must be prospectively, centrally tested and be HER2-positive based on central laboratory assay results
- Histologically or cytologically confirmed invasive breast cancer
- Prior treatment for breast cancer in the adjuvant, unresectable, locally advanced, or metastatic setting must include both a taxane, alone or in combination with another agent, and trastuzumab, alone or in combination with another agent
- Documented progression (which occur during or after most recent treatment or within 6 months after completing of adjuvant therapy) of incurable, unresectable, locally advanced or metastatic breast cancer, defined by the investigator
- Measurable and/or nonmeasurable disease; participants with central nervous system-only disease are excluded
- Cardiac ejection fraction greater than or equal to (>/=) 50 percent (%) by either echocardiogram or multi-gated acquisition scan
- Eastern Cooperative Oncology Group (ECOG) performance status of 0 or 1
- For women of childbearing potential and men with partners of childbearing potential, agreement to use a highly effective, non-hormonal form of contraception; contraception use should continue for the duration of the study treatment and for at least 6 months after the last dose of study treatment
Exclusion Criteria:
- History of treatment with trastuzumab emtansine
- Prior treatment with lapatinib or capecitabine
- Peripheral neuropathy of Grade >/= 3 per National Cancer Institute Common Terminology Criteria for Adverse Events (NCI-CTCAE), Version 3.0
- History of other malignancy within the last 5 years, except for appropriately treated carcinoma in situ of the cervix, non-melanoma skin carcinoma, Stage 1 uterine cancer, synchronous or previously diagnosed HER2-positive breast cancer, or cancers with a similar curative outcome as those mentioned above
- History of receiving any anti-cancer drug/biologic or investigational treatment within 21 days prior to randomization except hormone therapy, which could be given up to 7 days prior to randomization; recovery of treatment-related toxicity consistent with other eligibility criteria
- History of radiation therapy within 14 days of randomization
- Brain metastases that are untreated, symptomatic, or require therapy to control symptoms, as well as any history of radiation, surgery, or other therapy, including steroids, to control symptoms from brain metastases within 2 months (60 days) of randomization
- History of symptomatic congestive heart failure or serious cardiac arrhythmia requiring treatment
- History of myocardial infarction or unstable angina within 6 months of randomization
- Current dyspnea at rest due to complications of advanced malignancy or current requirement for continuous oxygen therapy
- Current severe, uncontrolled systemic disease (for example, clinically significant cardiovascular, pulmonary, or metabolic disease)
- Pregnancy or lactation
- Current known active infection with human immunodeficiency virus (HIV), hepatitis B virus, or hepatitis C virus
- Presence of conditions that could affect gastrointestinal absorption: Malabsorption syndrome, resection of the small bowel or stomach, and ulcerative colitis
- History of intolerance (such as Grade 3-4 infusion reaction) to trastuzumab
- Known hypersensitivity to 5-fluorouracil or known dihydropyrimidine dehydrogenase deficiency
- Current treatment with sorivudine or its chemically related analogs, such as brivudine
Opintosuunnitelma
Tässä osiossa on tietoja tutkimussuunnitelmasta, mukaan lukien kuinka tutkimus on suunniteltu ja mitä tutkimuksella mitataan.
Miten tutkimus on suunniteltu?
Suunnittelun yksityiskohdat
- Ensisijainen käyttötarkoitus: Hoito
- Jako: Satunnaistettu
- Inventiomalli: Rinnakkaistehtävä
- Naamiointi: Ei mitään (avoin tarra)
Aseet ja interventiot
Osallistujaryhmä / Arm |
Interventio / Hoito |
---|---|
Kokeellinen: Trastuzumab emtansine
Participants will receive trastuzumab emtansine 3.6 milligrams per kilogram (mg/kg) intravenous (IV) infusion over 30-90 minutes on Day 1 of each 21-day treatment cycle until disease progression (PD) (as assessed by the investigator), unmanageable toxicity, or study termination.
|
Trastuzumab emtansine 3.6 mg/kg IV infusion over 30-90 minutes on Day 1 of each 21-day treatment cycle.
Muut nimet:
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Active Comparator: Lapatinib + Capecitabine
Participants will receive lapatinib 1250 mg (five 250 mg tablets) orally once daily during each 21-day cycle + capecitabine 1000 milligrams per square meter (mg/m^2) orally twice daily on Days 1-14 of each 21-day treatment cycle until PD (as assessed by the investigator), unmanageable toxicity, or study termination.
Eligible participants will cross over to receive trastuzumab emtansine if second interim analysis demonstrates statistically significant overall survival benefit in favor of trastuzumab emtansine.
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Lapatinib 1250 mg (five 250 mg tablets) orally once daily during each 21-day cycle.
Muut nimet:
Capecitabine 1000 mg/m^2 orally twice daily on Days 1-14 of each 21-day treatment cycle.
Muut nimet:
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Mitä tutkimuksessa mitataan?
Ensisijaiset tulostoimenpiteet
Tulosmittaus |
Toimenpiteen kuvaus |
Aikaikkuna |
---|---|---|
Percentage of Participants With PD or Death as Assessed by an Independent Review Committee (IRC)
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
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PD was assessed by an IRC using modified Response Evaluation Criteria in Solid Tumors (RECIST).
All measurable lesions up to a maximum of 5 per organ and 10 in total were identified as target lesions (TLs) and recorded at baseline.
TLs should be selected on the basis of their size (those with the longest diameter) and their suitability for accurate repeated measurements either by imaging or clinically.
A sum of the longest diameter for all TLs was calculated as baseline sum longest diameter (SLD).
All other lesions (or sites of disease) should be identified as non-TLs and recorded at baseline.
PD for TLs was defined as greater than or equal to (>/=) 20 percent (%) increase in SLD, taking as reference smallest SLD recorded since treatment started or appearance of 1 or more new lesions.
PD for non-TLs was defined as appearance of 1 or more new lesions and/or unequivocal progression of existing non-TLs.
Percentage of Participants with PD by IRC or death from any cause was reported.
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From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
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Progression-free Survival (PFS) as Assessed by an IRC (Co-primary Endpoint)
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
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Tumor response was assessed by an IRC according to modified RECIST.
All measurable lesions up to a maximum of 5 per organ and 10 in total were identified as TLs (on the basis of their size and their suitability for accurate repeated measurements either by imaging or clinically) and recorded at baseline.
A sum of the longest diameter for all TLs was calculated as baseline SLD.
All other lesions were identified as non-TLs and recorded at baseline.
PD for TLs: >/= 20% increase in the SLD, taking as reference the smallest SLD recorded since treatment started or appearance of 1 or more new lesions.
PD for non-TLs: appearance of 1 or more new lesions and/or unequivocal progression of existing non-TLs.
PFS: time from randomization to first documented PD by IRC or death from any cause (whichever occurred earlier).
The median duration of PFS was estimated using Kaplan-Meier method.
The 95% confidence interval (CI) was computed using the method of Brookmeyer and Crowley.
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From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
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Percentage of Participants Who Died: Second Interim Analysis
Aikaikkuna: From the date of randomization through the data cut-off date of 31 Jul 2012 (up to 3 years, 5 months)
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The percentage of participants who died from any cause was reported.
The results are reported from second interim analysis, which deemed to be the confirmatory.
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From the date of randomization through the data cut-off date of 31 Jul 2012 (up to 3 years, 5 months)
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Overall Survival: Second Interim Analysis (Co-primary Endpoint)
Aikaikkuna: From the date of randomization through the data cut-off date of 31 Jul 2012 (up to 3 years, 5 months)
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OS was defined as the time from the date of randomization to the date of death from any cause.
The median duration of OS was estimated using Kaplan-Meier method.
The 95% CI was computed using the method of Brookmeyer and Crowley.
The results are reported from second interim analysis, which deemed to be the confirmatory.
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From the date of randomization through the data cut-off date of 31 Jul 2012 (up to 3 years, 5 months)
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Percentage of Participants Who Died: Final Analysis
Aikaikkuna: From the date of randomization through the data cut-off date of 31 Dec 2014 (up to 5 years, 11 months)
|
The percentage of participants who died from any cause was reported.
The results reported are from the final analysis.
The final analysis is descriptive.
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From the date of randomization through the data cut-off date of 31 Dec 2014 (up to 5 years, 11 months)
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Overall Survival: Final Analysis
Aikaikkuna: From the date of randomization through the data cut-off date of 31 Dec 2014 (up to 5 years, 11 months)
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OS was defined as the time from the date of randomization to the date of death from any cause.
The median duration of OS was estimated using Kaplan-Meier method.
The 95% CI was computed using the method of Brookmeyer and Crowley.
The results reported are from the final analysis.
The final analysis is descriptive.
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From the date of randomization through the data cut-off date of 31 Dec 2014 (up to 5 years, 11 months)
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Percentage of Participants Who Were Alive at Year 1
Aikaikkuna: Year 1
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1 year survival was defined as the percentage of participants alive 1 year after starting treatment.
The results reported are from the final analysis.
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Year 1
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Percentage of Participants Who Were Alive at Year 2
Aikaikkuna: Year 2
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2 year survival was defined as the percentage of participants alive 2 years after starting treatment.
The results reported are from the final analysis.
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Year 2
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Toissijaiset tulostoimenpiteet
Tulosmittaus |
Toimenpiteen kuvaus |
Aikaikkuna |
---|---|---|
Percentage of Participants With PD or Death as Assessed by the Investigator
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
PD was assessed by the investigator using modified RECIST.
All measurable lesions up to a maximum of 5 per organ and 10 in total were identified as TLs and recorded at baseline.
A sum of the longest diameter for all TLs was calculated as baseline SLD.
PD for TLs was defined as >/=20% increase in the SLD, taking as reference the smallest SLD recorded since treatment started or the appearance of 1 or more new lesions.
PD for non-TLs was defined as appearance of 1 or more new lesions and/or unequivocal progression of existing non-TLs.
The percentage of participants who died or experienced PD by Investigator was reported.
|
From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
PFS as Assessed by the Investigator
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Tumor response was assessed by the investigator according to modified RECIST.
All measurable lesions up to a maximum of 5 per organ and 10 in total were identified as TLs and recorded at baseline.
A sum of the longest diameter for all TLs was calculated as baseline SLD.
PD for TLs was defined as >/=20% increase in the SLD, taking as reference the smallest SLD recorded since treatment started or the appearance of 1 or more new lesions.
PD for non-TLs was defined as appearance of 1 or more new lesions and/or unequivocal progression of existing non-TLs.
PFS was defined as the time from randomization to first documented PD by Investigator or death from any cause (whichever occurred earlier).
The median duration of PFS was estimated using Kaplan-Meier method.
The 95% CI was computed using the method of Brookmeyer and Crowley.
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From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Percentage of Participants With Objective Response (OR) as Assessed by an IRC
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Tumor response was assessed by an IRC according to modified RECIST.
OR was defined as the percentage of participants with a complete response (CR) or partial response (PR).
All measurable lesions up to a maximum of 5 per organ and 10 in total were identified as TLs and recorded at baseline.
A sum of the longest diameter for all TLs was calculated as baseline SLD.
For TLs, a CR was defined as the disappearance of all TLs and a PR was defined as >/= 30% decrease in the SLD of TLs, taking as reference the baseline SLD.
For non-TLs, a CR was defined as the disappearance of all non-TLs and a PR was defined as the persistence of 1 or more non-TLs.
Confirmation of response at a consecutive tumor assessment at least 4 weeks apart was required.
Participants without a post-baseline tumor assessment were considered non-responders.
The percentage of participants with CR or PR by IRC was reported.
The 95% CI was computed using Blyth-Still Casella exact CI method.
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From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Duration of Objective Response (DOR) as Assessed by an IRC
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Tumor response was assessed by an IRC according to modified RECIST.
DOR was defined as the time from first documented OR to first documented PD or death from any cause, whichever occurred earlier.
OR was defined as a CR or PR determined on 2 consecutive tumor assessments at least 4 weeks apart.
For TLs, CR was defined as the disappearance of all TLs; PR was defined as >/=30% decrease in the SLD of TLs, taking as reference the baseline SLD; and PD was defined as >/=20% increase in the SLD, taking as reference the smallest SLD recorded since treatment started or the appearance of 1 or more new lesions.
For non-TLs, CR was defined as the disappearance of all non-TLs; PR was defined as the persistence of 1 or more non-TLs; and PD was defined as appearance of 1 or more new lesions and/or unequivocal progression of existing non-TLs.
The 95% CI was computed using the method of Brookmeyer and Crowley.
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From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
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Percentage of Participants With Clinical Benefit as Assessed by an IRC
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Tumor response was assessed by an IRC according to modified RECIST.
Participants were considered as experienced clinical benefit if they had an OR or maintained stable disease (SD) for at least 6 months from randomization.
OR: CR or PR determined on 2 consecutive tumor assessments >/=4 weeks apart.
For TLs, CR: disappearance of all TLs; PR: >/=30% decrease in the SLD of TLs, taking as reference the baseline SLD; PD: >/=20% increase in the SLD, taking as reference the smallest SLD recorded since treatment started or appearance of 1 or more new lesions; and SD: neither sufficient shrinkage to qualify for PR nor sufficient increase to qualify for PD.
For non-TLs, CR: disappearance of all non-TLs; PR/SD: persistence of 1 or more non-TLs; and PD: appearance of 1 or more new lesions and/or unequivocal progression of existing non-TLs.
Participants without a post-baseline tumor assessment were considered non-responders.
The 95% CI was computed using Blyth-Still Casella exact CI method.
|
From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Percentage of Participants With Treatment Failure
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Treatment failure was defined as discontinuation of treatment for any reason, including PD (per investigator review), treatment toxicity, or death from any cause.
For "Lapatinib + Capecitabine" arm, a participant was considered as treatment failure only if both drugs were discontinued.
For TLs, PD was defined as >/=20% increase in the SLD, taking as reference the smallest SLD recorded since treatment started or the appearance of 1 or more new lesions.
For non-TLs, PD was defined as appearance of 1 or more new lesions and/or unequivocal progression of existing non-TLs.
Percentage of participants with treatment failure was reported.
|
From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Time to Treatment Failure
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Time to treatment failure was defined as the time from randomization to discontinuation of treatment for any reason, including PD (per investigator review), treatment toxicity, or death from any cause.
For "Lapatinib + Capecitabine" arm, a participant was considered as treatment failure only if both drugs were discontinued with treatment failure date as the later of the 2 discontinuation dates.
For TLs, PD was defined as >/=20% increase in the SLD, taking as reference the smallest SLD recorded since treatment started or the appearance of 1 or more new lesions.
For non-TLs, PD was defined as appearance of 1 or more new lesions and/or unequivocal progression of existing non-TLs.
The median time to treatment failure was estimated using Kaplan-Meier method.
The 95% CI was computed using the method of Brookmeyer and Crowley.
|
From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Percentage of Participants With Symptom Progression
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Symptom progression was defined as the documentation of a >/= 5-point decrease from baseline in the scoring of responses as measured by the Functional Assessment of Cancer Therapy-for participants with Breast Cancer (FACT-B) questionnaire with the Trial Outcomes Index-Physical/Functional/Breast (TOI-PFB) subscale.
The FACT-B TOI-PFB subscale contained 24 items from 3 subsections of the FACT-B questionnaire: Physical well-being, functional well-being, and additional concerns for breast cancer participants (breast cancer subscale [BCS]).
All items in the questionnaire were rated by the participant on a 5-point scale ranging from 0 ("not at all") to 4 ("very much").
The total score ranged from 0 to 96 with higher score indicating better perceived quality of life.
The percentage of participants with symptom progression was reported.
|
From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Time to Symptom Progression
Aikaikkuna: From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
|
Time to symptom progression was defined as the time from randomization to the first documentation of a >/= 5-point decrease from baseline in the scoring of responses as measured by the FACT-B questionnaire with the TOI-PFB subscale.
The FACT-B TOI-PFB subscale contained 24 items from 3 subsections of the FACT-B questionnaire: Physical well-being, functional well-being, and additional concerns for breast cancer participants (BCS).
All items in the questionnaire were rated by the participant on a 5-point scale ranging from 0 ("not at all") to 4 ("very much").
The total score ranged from 0 to 96 with higher score indicating better perceived quality of life.
The median time to symptom progression was estimated using Kaplan-Meier method.
The 95% CI was computed using the method of Brookmeyer and Crowley.
|
From the date of randomization through the data cut-off date of 14 Jan 2012 (up to 2 years, 11 months)
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Yhteistyökumppanit ja tutkijat
Täältä löydät tähän tutkimukseen osallistuvat ihmiset ja organisaatiot.
Sponsori
Julkaisuja ja hyödyllisiä linkkejä
Tutkimusta koskevien tietojen syöttämisestä vastaava henkilö toimittaa nämä julkaisut vapaaehtoisesti. Nämä voivat koskea mitä tahansa tutkimukseen liittyvää.
Yleiset julkaisut
- Scott AM, Wolchok JD, Old LJ. Antibody therapy of cancer. Nat Rev Cancer. 2012 Mar 22;12(4):278-87. doi: 10.1038/nrc3236.
- Dieras V, Miles D, Verma S, Pegram M, Welslau M, Baselga J, Krop IE, Blackwell K, Hoersch S, Xu J, Green M, Gianni L. Trastuzumab emtansine versus capecitabine plus lapatinib in patients with previously treated HER2-positive advanced breast cancer (EMILIA): a descriptive analysis of final overall survival results from a randomised, open-label, phase 3 trial. Lancet Oncol. 2017 Jun;18(6):732-742. doi: 10.1016/S1470-2045(17)30312-1. Epub 2017 May 16. Erratum In: Lancet Oncol. 2017 Aug;18(8):e433. Lancet Oncol. 2018 Dec;19(12):e667.
- Verma S, Miles D, Gianni L, Krop IE, Welslau M, Baselga J, Pegram M, Oh DY, Dieras V, Guardino E, Fang L, Lu MW, Olsen S, Blackwell K; EMILIA Study Group. Trastuzumab emtansine for HER2-positive advanced breast cancer. N Engl J Med. 2012 Nov 8;367(19):1783-91. doi: 10.1056/NEJMoa1209124. Epub 2012 Oct 1. Erratum In: N Engl J Med. 2013 Jun 20;368(25):2442.
Opintojen ennätyspäivät
Nämä päivämäärät seuraavat ClinicalTrials.gov-sivustolle lähetettyjen tutkimustietueiden ja yhteenvetojen edistymistä. National Library of Medicine (NLM) tarkistaa tutkimustiedot ja raportoidut tulokset varmistaakseen, että ne täyttävät tietyt laadunvalvontastandardit, ennen kuin ne julkaistaan julkisella verkkosivustolla.
Opi tärkeimmät päivämäärät
Opiskelun aloitus
Sunnuntai 1. helmikuuta 2009
Ensisijainen valmistuminen (Todellinen)
Sunnuntai 1. heinäkuuta 2012
Opintojen valmistuminen (Todellinen)
Tiistai 1. syyskuuta 2015
Opintoihin ilmoittautumispäivät
Ensimmäinen lähetetty
Torstai 22. tammikuuta 2009
Ensimmäinen toimitettu, joka täytti QC-kriteerit
Torstai 22. tammikuuta 2009
Ensimmäinen Lähetetty (Arvio)
Maanantai 26. tammikuuta 2009
Tutkimustietojen päivitykset
Viimeisin päivitys julkaistu (Arvio)
Maanantai 31. lokakuuta 2016
Viimeisin lähetetty päivitys, joka täytti QC-kriteerit
Lauantai 10. syyskuuta 2016
Viimeksi vahvistettu
Torstai 1. syyskuuta 2016
Lisää tietoa
Tähän tutkimukseen liittyvät termit
Muita asiaankuuluvia MeSH-ehtoja
- Ihosairaudet
- Neoplasmat
- Neoplasmat sivustoittain
- Rintojen sairaudet
- Rintojen kasvaimet
- Farmakologisen vaikutuksen molekyylimekanismit
- Entsyymin estäjät
- Antimetaboliitit, antineoplastiset
- Antimetaboliitit
- Antineoplastiset aineet
- Tubuliinimodulaattorit
- Antimitoottiset aineet
- Mitoosin modulaattorit
- Antineoplastiset aineet, fytogeeniset
- Antineoplastiset aineet, immunologiset
- Proteiinikinaasin estäjät
- Trastutsumabi
- Kapesitabiini
- Maytansine
- Ado-Trastutsumab Emtansine
- Lapatinib
Muut tutkimustunnusnumerot
- BO21977
- TDM4370g (Muu tunniste: Genentech)
Nämä tiedot haettiin suoraan verkkosivustolta clinicaltrials.gov ilman muutoksia. Jos sinulla on pyyntöjä muuttaa, poistaa tai päivittää tutkimustietojasi, ota yhteyttä register@clinicaltrials.gov. Heti kun muutos on otettu käyttöön osoitteessa clinicaltrials.gov, se päivitetään automaattisesti myös verkkosivustollemme .
Kliiniset tutkimukset Rintasyöpä
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Gangnam Severance HospitalRekrytointiHER2 Rikastettu alatyyppi Breast Cancer, Herzuma, PAM50 -tutkimusKorean tasavalta
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Novartis PharmaceuticalsValmisMetastaattinen rintasyöpä (MBC) | Locally Advance Breast Cancer (LABC)Yhdistynyt kuningaskunta, Espanja
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BioNTech SESeventh Framework ProgrammeValmisRintasyöpä (TNBC (Triple Negative Breast Cancer))Ruotsi, Saksa
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Jonsson Comprehensive Cancer CenterNational Cancer Institute (NCI); National Institutes of Health (NIH)Ei vielä rekrytointiaAnatomisen vaiheen II rintasyöpä AJCC v8 | Anatomisen vaiheen III rintasyöpä AJCC v8 | Varhaisen vaiheen rintasyöpä | Anatomic Stage I Breast Cancer American Joint Committee on Cancer (AJCC) v8Yhdysvallat
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Emory UniversityNational Cancer Institute (NCI)PeruutettuPrognostisen vaiheen IV rintasyöpä AJCC v8 | Metastaattinen pahanlaatuinen kasvain aivoissa | Metastaattinen rintasyöpä | Anatominen vaihe IV Breast Cancer American Joint Committee on Cancer (AJCC) v8
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Fudan UniversityRekrytointiRintasyöpä | Rintojen kasvain | Rintojen kasvaimet | HER2-positiivinen rintasyöpä | Paikallisesti edennyt rintasyöpä | HER2-negatiivinen rintasyöpä | Hormonireseptoripositiivinen kasvain | Hormonireseptorinegatiivinen kasvain | Varhaisvaiheen rintasyöpä | Triple-negative Breast Cancer (TNBC)Kiina
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NRG OncologyNational Cancer Institute (NCI)Aktiivinen, ei rekrytointiAnatomisen vaiheen IV rintasyöpä AJCC v8 | Prognostisen vaiheen IV rintasyöpä AJCC v8 | Metastaattinen pahanlaatuinen kasvain luussa | Metastaattinen pahanlaatuinen kasvain imusolmukkeissa | Metastaattinen pahanlaatuinen kasvain maksassa | Metastaattinen rintasyöpä | Metastaattinen pahanlaatuinen kasvain... ja muut ehdotYhdysvallat, Kanada, Saudi-Arabia, Korean tasavalta
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Gynecologic Oncology GroupNational Cancer Institute (NCI)ValmisLymfaödeema | Perioperatiiviset/postoperatiiviset komplikaatiot | Vaiheen II Vulvar Cancer AJCC v7 | Vaihe IIIA Vulvar Cancer AJCC v7 | Vaihe IIIB Vulvar Cancer AJCC v7 | Vaihe IIIC Vulvar Cancer AJCC v7 | Stage IVA Vulvar Cancer AJCC v7 | Vaihe IA Vulvar Cancer AJCC v7 | Vaihe IB Vulvar Cancer AJCC v7 | Vaihe...Yhdysvallat
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National Cancer Institute (NCI)NCIC Clinical Trials Group; Cancer and Leukemia Group B; North Central Cancer... ja muut yhteistyökumppanitAktiivinen, ei rekrytointiHormonireseptori positiivinen | Vaiheen IA rintasyöpä AJCC v7 | Vaiheen IB rintasyöpä AJCC v7 | Stage IIA Breast Cancer AJCC v6 ja v7 | Vaiheen IIB rintasyöpä AJCC v6 ja v7 | Vaiheen IIIB rintasyöpä AJCC v7 | Rintojen adenokarsinoomaYhdysvallat, Kanada, Australia, Puerto Rico, Uusi Seelanti, Irlanti, Peru, Yhdistynyt kuningaskunta
Kliiniset tutkimukset Trastuzumab emtansine
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Nancy Lin, MDGenentech, Inc.Aktiivinen, ei rekrytointiHER2-positiivinen metastaattinen rintasyöpä | Keskushermoston metastaasitYhdysvallat
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Genentech, Inc.Valmis
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Fox Chase Cancer CenterNational Comprehensive Cancer Network; Puma Biotechnology, Inc.Rekrytointi
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QuantumLeap Healthcare CollaborativeRekrytointiKiinteä kasvain | Metastaattinen syöpä | Metastaattinen rintasyöpä | Kolminkertainen negatiivinen rintasyöpä | HER2-positiivinen rintasyöpä | Kiinteä kasvain, aikuinen | Kiinteä karsinooma | HER2-positiivinen metastaattinen rintasyöpä | Progesteronireseptoripositiivinen rintasyöpä | HER2-negatiivinen rintasyöpä | Estrogeenireseptoripositiivinen kasvain ja muut ehdotYhdysvallat
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Enliven TherapeuticsRekrytointiHER2-positiivinen metastaattinen rintasyöpä | HER2-geenimutaatio | HER2-mutantti ei-pienisoluinen keuhkosyöpä | HER2:n vahvistusYhdysvallat, Espanja, Korean tasavalta, Taiwan, Italia, Australia, Ranska
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Dana-Farber Cancer InstitutePuma Biotechnology, Inc.; Translational Breast Cancer Research ConsortiumAktiivinen, ei rekrytointi
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Dana-Farber Cancer InstituteGenentech, Inc.RekrytointiRintasyöpä | HER2-positiivinen rintasyöpä | Hormonireseptoripositiivinen rintasyöpä | Invasiivinen rintasyöpä | Solmu negatiivinen rintasyöpä | Mikrometastaasi RintasyöpäYhdysvallat