Methotrexate-Inadequate Response Autoinjector Device Sub Study (MTX-IR)
2015년 6월 30일 업데이트: Bristol-Myers Squibb
Substudy-A Phase IIIB Multicenter, Randomized, Double-Blind, Double-Dummy Study to Compare the Efficacy and Safety of Abatacept Administered Subcutaneously and Intravenously in Subjects With Rheumatoid Arthritis, Receiving Background Methotrexate, and Experiencing an Inadequate Response to Methotrexate
The purpose of this study is to implement a substudy in approximately 120 rheumatoid arthritis (RA) subjects to compare the steady-state serum trough concentration (Cminss), Cmax and area under the curve (AUC) during the dosing interval (TAU) of subcutaneous (SC) Abatacept injection of 125 mg via the autoinjector and via the BD Hypak™ Physiolis prefilled syringe.
연구 개요
상세 설명
Study Classification:
- Safety: show if the drug is safe under conditions of proposed use
- Efficacy: measure of an intervention's influence on a disease or health condition
- Safety/Efficacy
- Pharmacokinetics: the action of a drug in the body over a period of time including the process of absorption, distribution and localization in tissue, biotransformation, and excretion of the compound.
연구 유형
중재적
등록 (실제)
120
단계
- 3단계
참여기준
연구원은 적격성 기준이라는 특정 설명에 맞는 사람을 찾습니다. 이러한 기준의 몇 가지 예는 개인의 일반적인 건강 상태 또는 이전 치료입니다.
자격 기준
공부할 수 있는 나이
18년 이상 (성인, 고령자)
건강한 자원 봉사자를 받아들입니다
아니
연구 대상 성별
모두
설명
For more information regarding BMS clinical trial participation, please visit www.BMSStudyConnect.com
Inclusion Criteria:
- Subjects who have been treated in the long term (LT) with open-label SC Abatacept for at least 3 months
- Must continue to meet inclusion criteria specified in main IM101-174 Study Protocol
Exclusion Criteria:
- Participation in previous device substudy (implemented by Amendment 10)
- Must continue to meet exclusion criteria specified in main IM101-174 Study Protocol
공부 계획
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디자인 세부사항
- 주 목적: 치료
- 할당: 해당 없음
- 중재 모델: 단일 그룹 할당
- 마스킹: 없음(오픈 라벨)
무기와 개입
참가자 그룹 / 팔 |
개입 / 치료 |
|---|---|
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실험적: Abatacept (Autoinjector and Prefilled Syringe)
Abatacept (prefilled syringe) 125 mg/device solution subcutaneously weekly for 3 months Abatacept (autoinjector) 125 mg/device solution subcutaneously weekly for 1 month |
다른 이름들:
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연구는 무엇을 측정합니까?
주요 결과 측정
결과 측정 |
측정값 설명 |
기간 |
|---|---|---|
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Pharmacokinetic (PK) Analysis: Adjusted Geometric Mean Observed Serum Trough Concentration at Steady State (Cminss) of Abatacept Using a Prefilled Syringe (Measured on Day 29) and Using an Autoinjector (Measured on Day 113)
기간: Day 29, Day 113
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Abatacept SC was self-administered with a prefilled syringe every 7 days for the first 4 weeks until Day 29; Blood samples for PK were taken pre-dose (0 hour) on Days 29 and 113.
Serum concentrations of abatacept were analyzed using a validated enzyme-linked immunosorbent assay (ELISA).
Steady-state trough observed concentration in serum (Cminss) was measured in micrograms/milliliter (μg/mL).
Adjusted geometric mean and 90% confidence interval (CI) are presented.
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Day 29, Day 113
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2차 결과 측정
결과 측정 |
측정값 설명 |
기간 |
|---|---|---|
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PK Analysis: Geometric Mean of Maximum Observed Serum Concentration (Cmax) of Abatacept During the Sampling Period Between Substudy Days 22 and 29 for the Prefilled Syringe and Between Substudy Days 106 and Day 113 for the Autoinjector
기간: Days 22, 24, 25, 26, 29 (prefilled syringe); Days 106, 108, 109, 110, 113 (autoinjector)
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Abatacept SC was self-administered with a BD Hypak™ Physiolis prefilled syringe every 7 days for the first 4 weeks of the substudy until Day 29; Blood samples for PK were taken on Days 1 and 22 at 0 hour (predose), Day 24 at 48 hour (h) post dose, Day 25 at 72 h post dose, Day 26 at 96 h post dose and Day 29 at 0 h (predose).
On substudy Day 29, participants were switched from the prefilled syringe to the autoinjector.
Participants continued to self-administer abatacept with the autoinjector every 7 days following Day 29 for the remaining 3 months of the substudy; Blood samples for PK were taken on Day 108 at 48 h post dose, Day 109 at 72 h post dose, Day 110 at 96 h post dose and at Day 113 0h (predose).
Serum concentrations of abatacept were analyzed using a validated ELISA.
Cmax was measured in μg/mL.
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Days 22, 24, 25, 26, 29 (prefilled syringe); Days 106, 108, 109, 110, 113 (autoinjector)
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PK Analysis: Median Time to Achieve Cmax (Tmax) During the Sampling Period Between Days 22 and 29 for the Prefilled Syringe and Between Days 106 and Day 113 for the Autoinjector
기간: Days 22, 24, 25, 26, 29 (prefilled syringe); Days 106, 108, 109, 110,113 (autoinjector)
|
Abatacept SC was self-administered with a BD Hypak™ Physiolis prefilled syringe every 7 days for the first 4 weeks of the substudy until Day 29; Blood samples for PK were taken on Days 1 and 22 at 0 hour (predose), Day 24 at 48 hour (h) post dose, Day 25 at 72 h post dose, Day 26 at 96 h post dose and Day 29 at 0 h (predose).
On substudy Day 29, participants were switched from the prefilled syringe to the autoinjector.
Participants continued to self-administer abatacept with the autoinjector every 7 days following Day 29 for the remaining 3 months of the substudy; Blood samples for PK were taken on Day 108 at 48 h post dose, Day 109 at 72 h post dose, Day 110 at 96 h post dose and at Day 113 0h (predose).
Serum concentrations of abatacept were analyzed using a validated ELISA.
Tmax was measured in hours (h).
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Days 22, 24, 25, 26, 29 (prefilled syringe); Days 106, 108, 109, 110,113 (autoinjector)
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Geometric Mean of Area Under Serum Concentration-time (AUC) During a Dosing Interval (TAU) of Abatacept During the Sampling Period Between Days 22 and 29 for the Prefilled Syringe and Between Days 106 and Day 113 for the Autoinjector
기간: Days 22, 24, 25, 26,29 (prefilled syringe); Days 106, 108, 109, 110, 113 (autoinjector)
|
Abatacept SC was self-administered with a BD Hypak™ Physiolis prefilled syringe every 7 days for the first 4 weeks of the substudy until Day 29; Blood samples for PK were taken on Days 1 and 22 at 0 hour (predose), Day 24 at 48 hour (h) post dose, Day 25 at 72 h post dose, Day 26 at 96 h post dose and Day 29 at 0 h (predose).
On substudy Day 29, participants were switched from the prefilled syringe to the autoinjector.
Participants continued to self-administer abatacept with the autoinjector every 7 days following Day 29 for the remaining 3 months of the substudy; Blood samples for PK were taken on Day 106 at 0 h (predose), Day 108 at 48 h post dose, Day 109 at 72 h post dose, Day 110 at 96 h post dose and at Day 113 0h (predose).
Serum concentrations of abatacept were analyzed using a validated ELISA.
AUC(TAU) where TAU = 168 hours was calculated in µg*h/mL
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Days 22, 24, 25, 26,29 (prefilled syringe); Days 106, 108, 109, 110, 113 (autoinjector)
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Geometric Mean of Trough Serum Concentration (Cmin) Over Time and During the Switch From Prefilled Syringe to Autoinjector on Days 22, 29, 57, 85, 106, and 113
기간: Days 22, 29, 57, 85, 106, and 113
|
Abatacept SC was self-administered with a BD Hypak™ Physiolis prefilled syringe every 7 days for the first 4 weeks of the substudy until Day 29; Blood samples for PK were taken at 0 hour (predose).
On substudy Day 29, participants were switched from the prefilled syringe to the autoinjector.
Participants continued to self-administer abatacept with the autoinjector every 7 days following Day 29 for the remaining 3 months of the substudy.
Blood samples for PK were taken at 0 hour (predose).
Serum concentrations of abatacept were analyzed using a validated ELISA.
Steady-state trough observed concentration in serum (Cminss) was measured in micrograms/milliliter (μg/mL).
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Days 22, 29, 57, 85, 106, and 113
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Number of Participants With Positive Anti-Abatacept or Anti-CTLA4 Antibody Responses by Electrochemiluminescence (ECL) on Day 29 and Day 113.
기간: Days 29 and 113
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Serum samples for immunogenicity were evaluated for presence of anti-abatacept antibodies using a validated bridging ECL on Day 29 and Day 113.
The ECL assay differentiated between 2 antibody specificities: the immunoglobulin (Ig) G and/or junction region and cytotoxic leukocyte antigen 4 (CTLA4) and possibly Ig.
A positive immunogenicity response relative to baseline was defined as: A missing baseline immunogenicity measurement and a positive analytical laboratory reported immunogenicity response post-baseline; A negative baseline immunogenicity response and a positive analytical laboratory reported immunogenicity response post-baseline; A positive baseline immunogenicity response and a positive analytical laboratory reported immunogenicity response post-baseline that has a titer value strictly greater than the baseline titer value.
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Days 29 and 113
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여기에서 이 연구와 관련된 사람과 조직을 찾을 수 있습니다.
연구 기록 날짜
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연구 주요 날짜
연구 시작
2013년 4월 1일
기본 완료 (실제)
2014년 7월 1일
연구 완료 (실제)
2014년 7월 1일
연구 등록 날짜
최초 제출
2013년 4월 5일
QC 기준을 충족하는 최초 제출
2013년 4월 29일
처음 게시됨 (추정)
2013년 5월 3일
연구 기록 업데이트
마지막 업데이트 게시됨 (추정)
2015년 7월 23일
QC 기준을 충족하는 마지막 업데이트 제출
2015년 6월 30일
마지막으로 확인됨
2015년 6월 1일
추가 정보
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류마티스 관절염에 대한 임상 시험
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Azienda Unita Sanitaria Locale di PiacenzaUniversity of Parma모병특발성 폐 섬유증(IPF) | 전신 질환으로 인한 간질성 폐질환(장애) | Reumatoid Arthritis | 결합 조직 질환 (CTD)체코, 이탈리아
아바타셉트에 대한 임상 시험
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Kashiv BioSciences, LLC완전한
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Washington University School of MedicineIncyte Corporation모병
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Center for International Blood and Marrow Transplant...Incyte Corporation; National Marrow Donor Program모병림프종 | 골수 섬유증 | MDS(골수이형성 증후군) | 만성골수단구성백혈병(CMML) | CLL(만성 림프구성 백혈병) | 급성 백혈병(분류) | 급성 림프성 백혈병(ALL) | 전림프구성 백혈병 | 골수 증식성 신생물(MPN) | CML(만성 골수성 백혈병) | AML(급성 골수성 백혈병)미국