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von Willebrand disease: advances in pathogenetic understanding, diagnosis, and therapy

机译:von Willebrand病:在病原学理解,诊断和治疗方面的进展

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摘要

von Willebrand disease (VWD) is the most common autosomally inherited bleeding disorder. The disease represents a range of quantitative and qualitative pathologies of the adhesive glycoprotein von Willebrand factor (VWF). The pathogenic mechanisms responsible for the type 2 qualitative variants of VWF are now well characterized, with most mutations representing missense substitutions influencing VWF multimer structure and interactions with platelet GPIbα and collagen and with factor VIII. The molecular pathology of type 3 VWD has been similarly well characterized, with an array of different mutation types producing either a null phenotype or the production of VWF that is not secreted. In contrast, the pathogenetic mechanisms responsible for type 1 VWD remain only partially resolved. In the hemostasis laboratory, the measurement of VWF:Ag and VWF:RCo are key components in the diagnostic algorithm for VWD, although the introduction of direct GPIbα-binding assays may become the functional assay of choice. Molecular genetic testing can provide additional benefit, but its utility is currently limited to type 2 and 3 VWD. The treatment of bleeding in VWD involves the use of desmopressin and plasma-derived VWF concentrates and a variety of adjunctive agents. Finally, a new recombinant VWF concentrate has just completed clinical trial evaluation and has demonstrated excellent hemostatic efficacy and safety.
机译:von Willebrand病(VWD)是最常见的自体遗传性出血病。该疾病代表了粘附性糖蛋白von Willebrand因子(VWF)的一系列定量和定性病理。现在已经很好地表征了导致VWF 2型定性变异的致病机制,大多数突变代表影响VWF多聚体结构以及与血小板GPIbα和胶原蛋白以及与VIII因子相互作用的错义替换。 3型VWD的分子病理学已得到相似的良好表征,具有一系列不同的突变类型,它们会产生无效表型或产生未被分泌的VWF。相比之下,造成1型VWD的致病机制仅部分解决。在止血实验室中,VWF:Ag和VWF:RCo的测量是VWD诊断算法的关键组成部分,尽管引入直接GPIbα结合测定法可能会成为功能测定法。分子遗传学检测可以提供额外的好处,但是其实用性目前仅限于2型和3型VWD。 VWD出血的治疗涉及使用去氨加压素和血浆衍生的VWF浓缩物以及各种辅助剂。最后,一种新的重组VWF浓缩物刚刚完成临床试验评估,并显示出优异的止血功效和安全性。

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