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Endobrevin/VAMP-8 Is the Primary v-SNARE for the Platelet Release Reaction

机译:Endobrevin / VAMP-8是血小板释放反应的主要v-SNARE

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摘要

Platelet secretion is critical to hemostasis. Release of granular cargo is mediated by soluble NSF attachment protein receptors (SNAREs), but despite consensus on t-SNAREs usage, it is unclear which Vesicle Associated Membrane Protein (VAMPs: synaptobrevin/VAMP-2, cellubrevin/VAMP-3, TI-VAMP/VAMP-7, and endobrevin/VAMP-8) is required. We demonstrate that VAMP-8 is required for release from dense core granules, alpha granules, and lysosomes. Platelets from VAMP-8−/− mice have a significant defect in agonist-induced secretion, though signaling, morphology, and cargo levels appear normal. In contrast, VAMP-2+/−, VAMP-3−/−, and VAMP-2+/−/VAMP-3−/− platelets showed no defect. Consistently, tetanus toxin had no effect on secretion from permeabilized mouse VAMP-3−/− platelets or human platelets, despite cleavage of VAMP-2 and/or -3. Tetanus toxin does block the residual release from permeabilized VAMP-8−/− platelets, suggesting a secondary role for VAMP-2 and/or -3. These data imply a ranked redundancy of v-SNARE usage in platelets and suggest that VAMP-8−/− mice will be a useful in vivo model to study platelet exocytosis in hemostasis and vascular inflammation.
机译:血小板分泌对于止血至关重要。颗粒状货物的释放是由可溶性NSF附着蛋白受体(SNARE)介导的,但尽管在使用t-SNARE方面已达成共识,但尚不清楚哪种囊泡相关膜蛋白(VAMP:synaptobrevin / VAMP-2,cellubrevin / VAMP-3,TI- VAMP / VAMP-7和endobrevin / VAMP-8)。我们证明VAMP-8是从致密核心颗粒,α颗粒和溶酶体释放所必需的。尽管信号,形态和货物水平正常,但来自VAMP-8 -/-小鼠的血小板在激动剂诱导的分泌中具有明显的缺陷。相反,VAMP-2 +/- ,VAMP-3 -/-和VAMP-2 + /-/- / VAMP-3 < sup>-/-血小板无缺陷。一致地,尽管VAMP-2和/或-3被切割,但破伤风毒素对透化的小鼠VAMP-3 -/-血小板或人血小板的分泌没有影响。破伤风毒素确实阻止了通透的VAMP-8 -/-血小板的残留释放,表明VAMP-2和/或-3具有次要作用。这些数据暗示了v-SNARE在血小板中的使用具有一定的冗余度,并表明VAMP-8 -/-小鼠将是研究止血和血管炎症中血小板胞吐作用的有用的体内模型。

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