The Pharmacogenomic Control of Clopidogrel Response in Acute Coronary Syndromes

急性冠脉综合征中氯吡格雷反应的药物基因组学控制

• 批准号: 8704960
• 负责人: Stuart Alexander Scott
• 金额: $ 19.45万
• 依托单位: ICAHN SCHOOL OF MEDICINE AT MOUNT SINAI
• 依托单位国家: 美国
• 财政年份: 2013
• 资助国家: 美国
• 起止时间: 2013-08-01 至 2017-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8704960
• 关键词: ABCB1 gene; Accounting; Adoption; Advisory Committees; Aftercare; Alleles; American; Ancillary Study; Anticoagulants; Antiplatelet Drugs; Applications Grants; Aspirin; Award; Basic Science; Benchmarking; Biology; Blood Platelets; Candidate Disease Gene; Cardiology; Cardiovascular system; Caring; Clinical; Clinical Research; Clinical Sciences; Clinical Services; Clinical Trials; Clinical Trials Design; Clinical and Translational Science Awards; Collaborations; Committee Members; Complex; Cytochrome P450; DNA Sequence; Data; Data Analyses; Disease; Doctor of Medicine; Doctor of Philosophy; Drug Kinetics; Effectiveness; Enrollment; Environment; Enzymes; Epidemiologist; Equipment; Event; Faculty; Foundations; Frequencies; Funding; Future; Gene Frequency; Gene Mutation; Genes; Genetic; Genetic Polymorphism; Genetic Variation; Genetic screening method; Genomics; Genotype; Goals; Human Genetics; Hybrids; Institutes; Laboratories; Legal patent; Medical Genetics; Medicine; Mentored Patient-Oriented Research Career Development Award; Mentors; Mentorship; Meta-Analysis; Molecular; Network-based; Outcome; Outcomes Research; Patients; Pharmaceutical Preparations; Pharmacodynamics; Pharmacogenetics; Pharmacogenomics; Phenotype; Platelet aggregation; Play; Practice Guidelines; Principal Investigator; Programmed Instruction; Publications; Quality Control; Research; Research Personnel; Research Project Grants; Resistance; Resources; Risk; Role; Sampling; Science; Serious Adverse Event; Single Nucleotide Polymorphism; Stents; Testing; Thrombosis; Time; Training; Translational Research; Treatment Efficacy; Variant; Warfarin; acute coronary syndrome; base; career; career development; clinically relevant; clopidogrel; cohort; design; exome sequencing; experience; genetic variant; genome wide association study; genome-wide; loss of function; medical schools; next generation; novel; patient oriented; percutaneous coronary intervention; pharmacogenetic testing; programs; public health relevance; response; skills; standard of care; trait; uptake

DESCRIPTION (provided by applicant): CANDIDATE: Stuart A. Scott, Ph.D., is a clinical molecular geneticist in the Mount Sinai Genetic Testing Laboratory, certified by the American Board of Medical Genetics (ABMG), who has drawn on his training and experience in clinical and basic science to develop a research program focused on translational pharmacogenomics. His previous pharmacogenetics research centered on the anticoagulant warfarin and the antiplatelet clopidogrel, and he has co-authored clinical pharmacogenetic practice guidelines for both of these agents. He now seeks a focused four-year K23 Award to support 85% protected time from his clinical responsibilities to initiate a whole-exome sequencing pharmacogenomics research project with related career development as he completes his two-year Institutional KL2 Faculty Scholar award in translational science. CAREER DEVELOPMENT: The long-term goal of the Candidate is to become an independently funded Principal Investigator in the field of translational pharmacogenomics research. This goal will be accomplished through Clinical and Translational Science Award (CTSA)/Pharmacogenomics Research Network (PGRN)- based co-mentorship, collaboration, and the practical and didactic mechanisms outlined in this application. INSTITUTIONAL ENVIRONMENT: The Department of Genetics and Genomic Sciences at the Mount Sinai School of Medicine (MSSM) is a hybrid basic science and clinical department that offers a broad-based program of instruction, research, and clinical services in translational genetics and genomic sciences. The MSSM Institute for Genomics and Multiscale Biology is a central resource for all the equipment and computational support necessary to accomplish modern genomics research. As such, the institutional environment at MSSM is ideal for the proper execution of the studies outlined in this application. RESEARCH PROJECT: Dual antiplatelet therapy (DAPT) with clopidogrel and aspirin is standard of care for patients with acute coronary syndromes (ACS) and/or for those undergoing percutaneous coronary intervention (PCI)~ however, substantial interindividual variability in platelet inhibition and clinical response is commonly observed. Cytochrome P450-2C19 (CYP2C19) is a key enzyme involved in clopidogrel bioactivation and patients who carry CYP2C19 loss-of-function alleles have reduced therapeutic efficacy and increased risks for serious adverse cardiovascular events. However, CYP2C19 only accounts for ~12% of the variability in clopidogrel response. The proposed research project will use whole-exome sequencing and genome-wide genotyping in carefully selected extreme phenotype cohorts of DAPT-treated ACS/PCI patients to identify novel genetic variants, which could facilitate the adoption of genetically guided antiplatelet therapy into routine interventional cardiology practice for more personalized and effective care. The identification of additioal genes and variants will not only influence the uptake of personalized antiplatelet therapy, but could provide a benchmark for other pharmacogenomic studies on drugs and medications with variable responses.

描述（由申请人提供）： 候选人：Stuart A. Scott博士是由美国医学遗传学委员会（ABMG）认证的西奈山基因测试实验室中的临床分子遗传学家，他借鉴了他在临床和基础科学领域的培训和经验，以开发以转化为基础药物基因组学的研究计划。他以前的药物遗传学研究集中在抗凝华法林和抗血小板质地质葡萄膜上，并为这两种药物共同撰写了临床药物遗传学实践指南。 现在，他寻求重点的四年K23奖，以支持85％的临床责任，以启动一项全面的测序药物基因组学研究项目，并获得了相关的职业发展项目，因为他填写了他的两年年度KL2教职员工学者奖。 职业发展：候选人的长期目标是成为转化药物基因组学领域的独立资助的首席研究员。该目标将通过临床和转化科学奖（CTSA）/药物基因组学研究网络（PGRN）基于基于本应用程序中概述的实用和教学机制。 机构环境：西奈山医学院（MSSM）的基因与基因组科学系是一个混合基础科学和临床部，提供了基于广泛的教学，研究和临床服务计划，领域是转化遗传学和基因组科学的临床服务。 MSSM基因组和多尺度生物学研究所是完成现代基因组学研究所需的所有设备和计算支持的中心资源。 因此，MSSM的机构环境非常适合正确执行本应用程序中概述的研究。 研究项目：氯吡格雷和阿司匹林的双抗血小板治疗（DAPT）是急性冠状动脉综合征（ACS）患者和/或接受经皮冠状动脉疗法（PCI）〜的患者的护理标准，但是，通常观察到血小板抑制和临床反应的实质性差异。细胞色素P450-2C19（CYP2C19）是参与氯吡格雷生物活化的关键酶，携带CYP2C19功能丧失等位基因的患者的治疗功效降低，风险增加了严重的不良心血管事件。 但是，CYP2C19仅占氯吡格雷反应变异性的约12％。 拟议的研究项目将在精心选择的DAPT治疗的ACS/PCI患者的极端表型同类中使用全外活体测序和全基因组基因分型，以鉴定新型的遗传变异，这可以促进遗传性导高的抗血小板疗法在常规介入心脏病学实践中，以实现更加个性化的实践，以实现更加个性化和有效的护理。 添加基因和变体的鉴定不仅会影响个性化抗血小板疗法的摄取，而且可以为其他具有可变反应的药物和药物的药物基因组学研究提供基准。