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Platelet receptor proteolysis: GPVI and ADAM10

机译:血小板受体蛋白水解:GPVI和ADAM10

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摘要

Glycoprotein VI (GPVI) is a platelet collagen receptor that, together with the von Willebrand factor receptor, GPlb-IX-V, initiates platelet thrombus formation at arterial shear rates. Levels of GPVI also may act as a marker of acute coronary syndrome. GPVI is a member of the immunoreceptor family, and contains two extracellular immunoglobulin domains, a mucin core, a transmembrane domain and a C-terminal cytoplasmic tail. Ligand-induced signaling involves association of calmodulin and Src kinases with the cytoplasmic tail, and co-association with the immunoreceptor tyrosine-based activation motif (ITAM)-bearing Fc receptor gamma-chain (FcRgamma), that utilizes the Syk kinase pathway. Divergent signaling by GPVI activates integrin alpha_(llb)beta_3 that mediates platelet aggregation, and calmodulin-mediated metalloproteinase (ADAM 10)-dependent ectodomain shedding, producing an ~55-kDa soluble fragment and an ~10-kDa platelet-associated remnant. Current studies are revealing how ADAM10 and GPVI shedding are regulated, with broader implications to the regulation of receptor expression on other cells.
机译:糖蛋白VI(GPVI)是一种血小板胶原蛋白受体,与血管性血友病因子受体GPlb-IX-V一起以动脉剪切速率引发血小板血栓形成。 GPVI的水平也可以作为急性冠状动脉综合征的标志。 GPVI是免疫受体家族的成员,并包含两个细胞外免疫球蛋白结构域,一个粘蛋白核心,一个跨膜结构域和一个C端细胞质尾巴。配体诱导的信号传导涉及钙调蛋白和Src激酶与细胞质尾部的缔合,以及与带有免疫受体酪氨酸的活化基序(ITAM)的Fc受体γ链(FcRgamma)的关联,后者利用Syk激酶途径。 GPVI的发散信号激活了整合素α_(11b)beta_3,后者介导血小板聚集,钙调蛋白介导的金属蛋白酶(ADAM 10)依赖性胞外域脱落,产生〜55 kDa的可溶性片段和〜10 kda的血小板相关残基。当前的研究揭示了如何调节ADAM10和GPVI脱落,对其他细胞上受体表达的调节具有更广泛的意义。

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