Feasibility of the Hemophilia INHIBIT Trial

血友病 INHIBIT 试验的可行性

• 批准号: 8352123
• 负责人: MARGARET VICTORIA RAGNI
• 金额: $ 37.65万
• 依托单位: UNIVERSITY OF PITTSBURGH AT PITTSBURGH
• 依托单位国家: 美国
• 财政年份: 2012
• 资助国家: 美国
• 起止时间: 2012-08-20 至 2014-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8352123
• 关键词: A-factor (Streptomyces); Adult; Antibodies; Antigens; Biological Assay; Blood specimen; Body cavities; Case Report Form; Child; Childhood; Clinical; Clinical Research; Clinical Trials; Clinical Trials Design; Commit; Communication; Communities; Consensus; Contracts; Data; Development; Disease; Enrollment; Event; Factor VIII; Feedback; Future; Goals; Grant; Guidelines; Hemophilia A; Hemorrhage; Hemostatic function; IL2RA gene; Immune system; Infection; Inflammation; Injection of therapeutic agent; Institutional Review Boards; Intervention; Interview; Joints; Laboratories; Link; Manuals; Methods; Morbidity - disease rate; Muscle; NIH Program Announcements; Nurses; Online Systems; Operative Surgical Procedures; Parents; Patients; Phase; Phase III Clinical Trials; Physicians; Prevention; Prophylactic treatment; Protocols documentation; Randomized; Randomized Clinical Trials; Randomized Controlled Clinical Trials; Randomized Controlled Trials; Recruitment Activity; Regulatory T-Lymphocyte; Research; Research Design; Research Infrastructure; Research Personnel; Research Project Grants; Resource Development; Resources; Risk; Safety; Sampling; Science; Shipping; Ships; Signal Transduction; Site; Societies; Structure; Study Subject; System; T cell response; T-Lymphocyte; Testing; Thrombosis; Time; Tissues; U-Series Cooperative Agreements; Validation; Work; abstracting; antibody inhibitor; body cavity; clinical practice; cost; design; enzyme linked immunospot assay; inhibitor/antagonist; innovation; meetings; member; open label; operation; prevent; randomized trial; recombinant antihemophilic factor VIII; repository; response; treatment center; trial comparing

DESCRIPTION (provided by applicant): Hemophilia A is an X-linked bleeding disorder resulting from deficiency of factor VIII, and characterized by bleeding into joints, muscles, and body cavities. Among the most serious complications of hemophilia treatment is inhibitor formation, that is, the development of antibodies directed against infused factor VIII Inhibitor antibodies occur in 25-35% of patients and result in uncontrolled bleeding and significant morbidity. Inhibitor risk is associated with intensive treatment, such as given for major bleeds or surgeries, in which tissue damage and inflammation activate the immune system. Increasing evidence suggests if so-called "danger" signals could be avoided, inhibitor formation could be prevented. The purpose of this U34 Exploratory Clinical Research Grant is to establish the feasibility of conducting a Phase III trial of recombinant factor VIII (rF.VIII) begun preemptively weekly before the first bleed versus standard three-times weekly rF.VIII begun after the first bleed in children with severe hemophilia A. The original concept for this study was developed as one of four clinical trial concepts by six hemophilia treatment center (HTC) physicians, members of the NHBLI State of the Science (SoS) Hemophilia Subcommittee, who are members of the Steering Committee for this study. We hypothesize that recombinant F.VIII (rF.VIII) prophylaxis given preemptively before the first bleed, in the absence of "danger", will prevent inhibitor formation, as compared with standard three times weekly prophylaxis begun after the first bleed. This is an innovative concept as it challenges current treatment, and, if successful, will be practice-changing. It is also innovative in evaluating F.VIII-specific T cell responses by ELISPOT assay to determine the mechanism of inhibitor formation and tolerance. The ultimate goal of this project is to identify and resolve barriers to the conduct of a future phase III randomized, controlled clinical trial, the specific aims of which are: Aim 1. To establish an HTC infrastructur of 60+ HTC physicians to jointly build consensus on trial design, subject recruitment and participation to assure a sufficient number of eligible subjects to conduct a future R01 48-week randomized trial to compare preemptive weekly vs. standard three times weekly rF.VIII prophylaxis in the prevention of inhibitor formation in children with severe hemophilia A. The HTC network will be operationalized by 1) conducting facilitated structured interviews with HTC physicians and with parents to determine acceptability of trial design and participation potential; 2) collaborating with a Steering Committee and the U24 Clinical Resource to optimize trial design, recruitment strategy, and to prepare case report forms and a manual of operations; 3) developing and pilot-testing a web-based data entry system; 4) conducting exploratory meetings with foreign HTC physicians to determine potential for trial participation and subject recruitment; and 5) hiring two dedicated nurse coordinators to prepare IRB submissions and contracts for HTCs. Aim 2. To determine the feasibility of a phase III 48-week, open-label, randomized clinical trial comparing preemptive weekly rF.VIII prophylaxis begun before the first bleed versus standard three times weekly rF.VIII prophylaxis begun after the first bleed in children with severe hemophilia A, F.VIII<0.01 U/ml, enrolled at local HTCs. This will be accomplished by 1) validating and optimizing the anti-F.VIII inhibitor antibody, the primary endpoint, for pediatric volumes, low- and high-titer antibodies, and shipping; 2) validating the F.VIII-specific T cell ELISPOT assay, a secondary endpoint to assess inhibitor mechanism, in adult inhibitor samples and optimizing it for pediatric volumes and shipping; 3) establishing safety stopping guidelines to assure safety of the intervention, to minimize bleeding events and central line infections; 4) setting up a repository of blood samples linked to study subject data via web-based data entry; and 5) seeking advice of a community advisory board to provide feedback and promote communication regarding the future phase III trial. PUBLIC HEALTH RELEVANCE: The purpose of this U34 proposal is to determine the feasibility of a randomized trial to compare prophylaxis (factor VIII to prevent bleeds) given preemptively, once weekly, before the first bleed vs. standard three times weekly prophylaxis beginning after the first bleed to prevent inhibitor formation in children with severe hemophilia A If successful, our approach could reduce morbidity and cost, and change clinical practice. We will recruit hemophilia center investigators, conduct structured interviews with HTC physicians and parents, groups, and finalize protocol design, set up an infrastructure to accomplish IRB and contract approval for 60+ HTCs, and explore foreign HTC participation, to assure the feasibility of a future Phase III randomized trial. (End of Abstract)

描述(申请人提供)：血友病A是一种X连锁出血性疾病，由因子VIII缺乏引起，其特征是关节、肌肉和体腔出血。血友病治疗最严重的并发症之一是抑制物的形成，即针对输注的第八因子抑制物抗体的抗体的产生发生在25%-35%的患者中，并导致无法控制的出血和显著的发病率。抑制剂风险与强化治疗有关，如对大出血或 外科手术，其中组织损伤和炎症激活免疫系统。越来越多的证据表明，如果能够避免所谓的“危险”信号，就可以防止抑制剂的形成。U34探索性临床研究基金的目的是确定先发制人开始的重组因子(rF.VIII)进行第三阶段试验的可行性 在严重血友病A的儿童第一次出血后开始的每周三次rF.VIII与标准的每周三次rF.VIII本研究的原始概念是由六名血友病治疗中心(HTC)医生开发的四个临床试验概念之一，他们是NHBLI科学状况(SOS)血友病小组委员会的成员，也是本研究指导委员会的成员。我们假设，与第一次出血后开始的标准的每周三次预防相比，在第一次出血之前预先给予重组F.VIII(rF.VIII)预防，在没有“危险”的情况下，将防止抑制剂的形成。这是一个创新的概念，因为它挑战了目前的治疗方法，如果成功，将改变实践。它在用ELISPOT法评估F.VIII特异性T细胞反应以确定抑制物形成和耐受的机制方面也是创新的。该项目的最终目标是确定和解决未来第三阶段随机对照临床试验的实施障碍，其具体目标是：目标1.建立一个由60多名HTC医生组成的HTC基础设施，共同就试验设计、受试者招募和参与达成共识，以确保有足够数量的合格受试者进行未来R01 48周随机试验，比较先发制人的每周和标准的每周三次rF.VIII预防在严重血友病A儿童中抑制物形成的作用。HTC网络将通过1)与HTC医生和父母进行便利的结构化访谈来确定试验设计和参与的可接受性； 2)与指导委员会和U24临床资源中心合作，优化试验设计、招募策略，并准备病例报告表和操作手册；3)开发和试点基于网络的数据输入系统；4)与外国HTC医生举行探索性会议，以确定参与试验和招募受试者的潜力；以及5)聘请两名专门的护士协调员为HTC准备IRB提交文件和合同。目的2.确定一项为期48周、开放标签、随机的III期临床试验的可行性，比较在当地HTCS登记的重度血友病A，F.VIII和0.01U/ml的重度血友病儿童在第一次出血前开始每周预防性rF.VIII预防和在第一次出血后开始标准的每周三次rF.VIII预防的可行性。这将通过以下方式实现：1)验证和优化抗F.VIII抑制物抗体，这是儿科容量、低和高滴度抗体和运输的主要终点；2)在成人抑制物样本中验证F.VIII特异性T细胞ELISPOT试验，这是评估抑制机制的次要终点，并针对儿科容量和运输进行优化；3)建立安全停止指南，以确保干预的安全性，将出血事件和中心线感染降至最低；4)建立血样储存库，通过基于网络的数据输入链接到研究对象数据；以及5)寻求社区咨询委员会的建议，以提供反馈并促进关于未来第三阶段试验的沟通。 公共卫生相关性：这项U34提案的目的是确定一项随机试验的可行性，比较首次出血前每周预先给予一次预防措施(预防出血因素)与首次出血后开始每周三次标准预防措施以防止严重血友病A儿童抑制物形成的可行性。如果成功，我们的方法将可以降低发病率和成本，并改变临床实践。我们将招募血友病中心调查人员，对HTC医生和家长、小组进行结构化访谈，并最终确定方案设计，建立基础设施以完成60多个HTC的IRB和合同审批，并探索HTC的外国参与，以确保未来第三阶段随机试验的可行性。(摘要结束)