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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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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。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。 VAMP-8(-/-)小鼠的血小板在激动剂诱导的分泌中具有显着缺陷,尽管信号传导,形态和货物水平似乎正常。相反,VAMP-2(+/-),VAMP-3(-/-)和VAMP-2(+ /-/)VAMP-3(-/-)血小板未显示缺陷。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(-/-)小鼠将成为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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