首页> 美国卫生研究院文献>The EMBO Journal >VAMP-2 and cellubrevin are expressed in pancreatic beta-cells and are essential for Ca(2+)-but not for GTP gamma S-induced insulin secretion.
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VAMP-2 and cellubrevin are expressed in pancreatic beta-cells and are essential for Ca(2+)-but not for GTP gamma S-induced insulin secretion.

机译:VAMP-2和cellubrevin在胰腺β细胞中表达对于Ca(2+)是必不可少的但对于GTPγS诱导的胰岛素分泌却不是。

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摘要

VAMP proteins are important components of the machinery controlling docking and/or fusion of secretory vesicles with their target membrane. We investigated the expression of VAMP proteins in pancreatic beta-cells and their implication in the exocytosis of insulin. cDNA cloning revealed that VAMP-2 and cellubrevin, but not VAMP-1, are expressed in rat pancreatic islets and that their sequence is identical to that isolated from rat brain. Pancreatic beta-cells contain secretory granules that store and secrete insulin as well as synaptic-like microvesicles carrying gamma-aminobutyric acid. After subcellular fractionation on continuous sucrose gradients, VAMP-2 and cellubrevin were found to be associated with both types of secretory vesicle. The association of VAMP-2 with insulin-containing granules was confirmed by confocal microscopy of primary cultures of rat pancreatic beta-cells. Pretreatment of streptolysin-O permeabilized insulin-secreting cells with tetanus and botulinum B neurotoxins selectively cleaved VAMP-2 and cellubrevin and abolished Ca(2+)-induced insulin release (IC50 approximately 15 nM). By contrast, the pretreatment with tetanus and botulinum B neurotoxins did not prevent GTP gamma S-stimulated insulin secretion. Taken together, our results show that pancreatic beta-cells express VAMP-2 and cellubrevin and that one or both of these proteins selectively control Ca(2+)-mediated insulin secretion.
机译:VAMP蛋白是控制分泌小泡与其靶膜对接和/或融合的机制的重要组成部分。我们调查了胰腺β细胞中VAMP蛋白的表达及其在胰岛素胞吐中的意义。 cDNA克隆表明,VAMP-2和cellubrevin,但不是VAMP-1,在大鼠胰岛中表达,其序列与从大鼠脑中分离的序列相同。胰腺β细胞含有储存和分泌胰岛素的分泌颗粒,以及带有γ-氨基丁酸的突触样微泡。在连续的蔗糖梯度下进行亚细胞分级分离后,发现VAMP-2和Cellubrevin与两种类型的分泌囊泡有关。通过共聚焦显微镜观察大鼠胰腺β细胞的原代培养,证实了VAMP-2与含胰岛素的颗粒的缔合。破伤风和肉毒杆菌B神经毒素对链球菌溶血素O透化的胰岛素分泌细胞的预处理选择性裂解VAMP-2和Cellubrevin,并废除了Ca(2+)诱导的胰岛素释放(IC50约为15 nM)。相比之下,破伤风和肉毒杆菌B神经毒素的预处理不能阻止GTPγS刺激的胰岛素分泌。两者合计,我们的结果表明,胰腺β细胞表达VAMP-2和Cellubrevin,并且这些蛋白质中的一个或两个选择性地控制Ca(2+)介导的胰岛素分泌。

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