Karnes Jason H
Department of Pharmacy Practice & Science, University of Arizona College of Pharmacy, Tucson, AZ 85721, USA.
Sarver Heart Center, Department of Medicine, University of Arizona College of Medicine - Tucson, Tucson, AZ 85721, USA.
Pharmacogenomics. 2018 Dec;19(18):1413-1422. doi: 10.2217/pgs-2018-0147. Epub 2018 Nov 6.
Heparin-induced thrombocytopenia (HIT) is a life-threatening, immune-mediated adverse reaction to heparin anticoagulants. The inability to predict HIT represents a considerable liability associated with heparin administration. Genetic studies of HIT are challenging due to the scarcity of true HIT cases, potential for misclassification, and many environmental risk factors. Genetic studies have not consistently identified risk alleles for HIT, the production of platelet factor 4/heparin antibodies or the thromboembolic complications of HIT. Genes implicated in HIT and platelet factor 4/heparin antibody levels include FCGR2A, TDAG8, HLA-DR and others. Compelling evidence also suggests that the FCGR2A H131R polymorphism is associated with HIT-related thrombosis. There is a need for well-powered, multiethnic studies with laboratory confirmation of HIT, detailed patient- and drug-specific data, and inclusion of both serologic and thromboembolic outcomes. Genomic biomarkers identified from such studies offer the possibility of shifting current clinical practice paradigms from early detection and treatment to prevention.
肝素诱导的血小板减少症(HIT)是一种危及生命的、由免疫介导的针对肝素抗凝剂的不良反应。无法预测HIT是与肝素给药相关的一项重大风险。由于真正的HIT病例稀缺、存在错误分类的可能性以及许多环境风险因素,HIT的基因研究具有挑战性。基因研究尚未一致地确定HIT的风险等位基因、血小板因子4/肝素抗体的产生或HIT的血栓栓塞并发症。与HIT和血小板因子4/肝素抗体水平相关的基因包括FCGR2A、TDAG8、HLA-DR等。有力的证据还表明,FCGR2A H131R多态性与HIT相关的血栓形成有关。需要开展有充足样本量的多民族研究,对HIT进行实验室确认,提供详细的患者和药物特异性数据,并纳入血清学和血栓栓塞结局。从此类研究中确定的基因组生物标志物有可能将当前的临床实践模式从早期检测和治疗转变为预防。