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Syntaxin-11 而非 syntaxin-2 或 syntaxin-4 对于血小板分泌是必需的。

Syntaxin-11, but not syntaxin-2 or syntaxin-4, is required for platelet secretion.

机构信息

Department of Molecular and Cellular Biochemistry, University of Kentucky College of Medicine, Lexington, KY, USA.

出版信息

Blood. 2012 Sep 20;120(12):2484-92. doi: 10.1182/blood-2012-05-430603. Epub 2012 Jul 5.

Abstract

The platelet release reaction plays a critical role in thrombosis and contributes to the events that follow hemostasis. Previous studies have shown that platelet secretion is mediated by Soluble NSF Attachment Protein Receptor (SNARE) proteins from granule and plasma membranes. The SNAREs form transmembrane complexes that mediate membrane fusion and granule cargo release. Although VAMP-8 (v-SNARE) and SNAP-23 (a t-SNARE class) are important for platelet secretion, the identity of the functional syntaxin (another t-SNARE class) has been controversial. Previous studies using anti-syntaxin Abs in permeabilized platelets have suggested roles for both syntaxin-2 and syntaxin-4. In the present study, we tested these conclusions using platelets from syntaxin-knockout mouse strains and from a Familial Hemophagocytic Lymphohistiocytosis type 4 (FHL4) patient. Platelets from syntaxin-2 and syntaxin-4 single- or double-knockout mice had no secretion defect. Platelets from a FHL4 patient deficient in syntaxin-11 had a robust defect in agonist-induced secretion although their morphology, activation, and cargo levels appeared normal. Semiquantitative Western blotting showed that syntaxin-11 is the more abundant syntaxin in both human and murine platelets. Coimmunoprecipitation experiments showed that syntaxin-11 can form SNARE complexes with both VAMP-8 and SNAP-23. The results of the present study indicate that syntaxin-11, but not syntaxin-2 or syntaxin-4, is required for platelet exocytosis.

摘要

血小板释放反应在血栓形成中起着关键作用,并促进止血后的事件发生。先前的研究表明,血小板分泌是由来自颗粒和质膜的可溶性 NSF 附着蛋白受体 (SNARE) 蛋白介导的。SNARE 形成跨膜复合物,介导膜融合和颗粒货物释放。尽管 VAMP-8(v-SNARE)和 SNAP-23(t-SNARE 类)对于血小板分泌很重要,但功能突触蛋白(另一种 t-SNARE 类)的身份一直存在争议。先前使用透化血小板中的抗突触蛋白 Abs 进行的研究表明,突触蛋白-2 和突触蛋白-4 都具有作用。在本研究中,我们使用突触蛋白敲除小鼠品系和家族性噬血细胞性淋巴组织细胞增多症 4 型(FHL4)患者的血小板来检验这些结论。突触蛋白-2 和突触蛋白-4 单敲除或双敲除小鼠的血小板没有分泌缺陷。来自缺乏突触蛋白-11 的 FHL4 患者的血小板在激动剂诱导的分泌中存在严重缺陷,尽管它们的形态、激活和货物水平似乎正常。半定量 Western blot 显示,突触蛋白-11 是人类和鼠血小板中更丰富的突触蛋白。免疫共沉淀实验表明,突触蛋白-11 可以与 VAMP-8 和 SNAP-23 形成 SNARE 复合物。本研究的结果表明,突触蛋白-11(而不是突触蛋白-2 或突触蛋白-4)是血小板胞吐作用所必需的。

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本文引用的文献

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