Institut de Rhythmologie et de Modélisation Cardiaque, Plateforme Technologique d'Innovation Biomédicale, Hôpital Xavier Arnozan, Pessac, France.
Blood Rev. 2019 Jul;36:10-22. doi: 10.1016/j.blre.2019.03.004. Epub 2019 Mar 20.
In contrast to the inherited platelet disorder given by mutations in the ITGA2B and ITGB3 genes, mucocutaneous bleeding from a spontaneous inhibition of normally expressed αIIbβ3 characterizes acquired Glanzmann thrombasthenia (GT). Classically, it is associated with autoantibodies or paraproteins that block platelet aggregation without causing a fall in platelet count. However, inhibitory antibodies to αIIbβ3 are widely associated with primary immune thrombocytopenia (ITP), occur in secondary ITP associated with leukemia and related disorders, solid cancers and myeloma, other autoimmune diseases, following organ transplantation while cytoplasmic dysregulation of αIIbβ3 function features in myeloproliferative and myelodysplastic syndromes. Antibodies to αIIbβ3 occur during viral and bacterial infections, while drug-dependent antibodies reacting with αIIbβ3 are a special case. Direct induction of acquired GT is a feature of therapies that block platelets in coronary artery disease. This review looks at these conditions, emphasizing molecular mechanisms, therapy, patient management and future directions for research.
与由 ITGA2B 和 ITGB3 基因突变引起的遗传性血小板疾病相反,由正常表达的 αIIbβ3 自发抑制引起的黏膜皮肤出血是获得性 Glanzmann 血小板无力症(GT)的特征。经典地,它与自身抗体或副蛋白相关联,这些自身抗体或副蛋白阻断血小板聚集而不会导致血小板计数下降。然而,αIIbβ3 的抑制性抗体广泛与原发性免疫性血小板减少症(ITP)相关,在与白血病和相关疾病、实体瘤和骨髓瘤、其他自身免疫性疾病相关的继发性 ITP 中发生,在器官移植后,αIIbβ3 功能的细胞质调节障碍在骨髓增生性和骨髓发育不良综合征中发生。在病毒和细菌感染期间会出现针对 αIIbβ3 的抗体,而与药物相关的抗体与 αIIbβ3 反应则是一种特殊情况。在治疗冠状动脉疾病中阻断血小板的治疗会直接诱导获得性 GT。这篇综述探讨了这些情况,强调了分子机制、治疗、患者管理和未来研究方向。
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