首页> 外文期刊>Archives of Biochemistry and Biophysics >Relationship between calcium mobilization and platelet alpha- and delta-granule secretion. A role for TRPC6 in thrombin-evoked delta-granule exocytosis
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Relationship between calcium mobilization and platelet alpha- and delta-granule secretion. A role for TRPC6 in thrombin-evoked delta-granule exocytosis

机译:钙动员与血小板α-和δ-颗粒分泌之间的关系。 TRPC6在凝血酶诱发的三角粒子胞吐作用中的作用

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摘要

Changes in cytosolic Ca2+ concentration ([Ca2+](c)) regulate granule secretion in different cell types. Thrombin activates PAR1 and PAR4 receptors and promotes release of Ca2+ from distinct intracellular stores, which, in turn, activates store-operated Ca2+ entry (SOCE). A crucial step during platelet function is the release of physiological agonists stored in secretory granules to the extracellular compartment during activation. We aim to study the role of Ca2+ mobilization from the extracellular compartment or from different intracellular stores in platelet granule secretion. By using flow cytometry, we have found that alpha- and delta-granules are secreted in thrombin-stimulated platelets in the absence of extracellular Ca2+, and in a concentration-dependent manner. Our findings show that thrombin-stimulated granule secretion depends on Ca2+ mobilization from intracellular stores. Analysis of the kinetics of granule secretion reveals that platelet stimulation with thrombin results in rapid release of alpha-granules which precedes the secretion of delta-granules. Incubation of platelets with a specific antibody, which recognizes the extracellular amino acid sequence 573-586 of TRPC6, inhibited thrombin-evoked delta-granule exocytosis. Our results indicate that the mechanisms underlying thrombin-induced alpha- and delta-granule secretion show differences in dependency on Ca2+ mobilization. (C) 2015 Elsevier Inc. All rights reserved.
机译:胞质Ca2 +浓度([Ca2 +](c))的变化调节了不同细胞类型中颗粒的分泌。凝血酶激活PAR1和PAR4受体,并促进Ca2 +从不同的细胞内存储中释放,进而激活存储操作的Ca2 +进入(SOCE)。血小板功能过程中的关键步骤是活化过程中将储存在分泌颗粒中的生理激动剂释放到细胞外区室。我们旨在研究钙离子从细胞外区室或血小板颗粒分泌中不同细胞内存储中动员的作用。通过使用流式细胞仪,我们发现在不存在细胞外Ca2 +的情况下,凝血酶刺激的血小板中会分泌α-和delta-颗粒,并且呈浓度依赖性。我们的发现表明,凝血酶刺激的颗粒分泌取决于细胞内存储的Ca2 +动员。颗粒分泌动力学的分析表明,凝血酶对血小板的刺激会导致α-颗粒的快速释放,而δ-颗粒的分泌要早于α-颗粒的释放。用识别TRPC6的细胞外氨基酸序列573-586的特异性抗体孵育血小板,可抑制凝血酶诱发的δ-颗粒胞吐作用。我们的结果表明,凝血酶诱导的α-和δ-颗粒分泌的潜在机制显示了对Ca2 +动员的依赖性的差异。 (C)2015 Elsevier Inc.保留所有权利。

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