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首页> 外文期刊>The Journal of biological chemistry >Vesicle-associated Membrane Protein 8 (VAMP8) Is a SNARE (Soluble N-Ethylmaleimide-sensitive Factor Attachment Protein Receptor) Selectively Required for Sequential Granule-to-granule Fusion
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Vesicle-associated Membrane Protein 8 (VAMP8) Is a SNARE (Soluble N-Ethylmaleimide-sensitive Factor Attachment Protein Receptor) Selectively Required for Sequential Granule-to-granule Fusion

机译:囊泡相关膜蛋白8(Vamp8)是序列颗粒 - 颗粒融合所需的圈套(可溶性的N-乙基马来酰亚胺敏感因子附着蛋白受体)

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Compound exocytosis is found in many cell types and is the major form of regulated secretion in acinar and mast cells. Its key characteristic is the homotypic fusion of secretory granules. These then secrete their combined output through a single fusion pore to the outside. The control of compound exocytosis remains poorly understood. Although soluble N-ethylmaleimide-sensitive factor attachment protein receptors (SNAREs) such as syntaxin 2, SNAP23 (synaptosome-associated protein of 23 kDa), and SNAP25 have been suggested to play a role, none has been proven. Vesicle-associated membrane protein 8 (VAMP8) is a SNARE first associated with endocytic processes but more recently has been suggested as an R-SNARE in regulated exocytosis. Secretion in acinar cells is reduced when VAMP8 function is inhibited and is less in VAMP8 knock-out mice. Based on electron microscopy experiments, it was suggested that VAMP8 may be involved in compound exocytosis. Here we have tested the hypothesis that VAMP8 controls homotypic granule-to-granule fusion during sequential compound exocytosis. We use a new assay to distinguish primary fusion events (fusion with the cell membrane) from secondary fusion events (granule-granule fusion). Our data show the pancreatic acinar cells from VAMP8 knock-out animals have a specific reduction in secondary granule fusion but that primary granule fusion is unaffected. Furthermore, immunoprecipitation experiments show syntaxin 2 association with VAMP2, whereas syntaxin 3 associates with VAMP8. Taken together our data indicate that granule-to-granule fusion is regulated by VAMP8 containing SNARE complexes distinct from those that regulate primary granule fusion.
机译:复合卵细胞症在许多细胞类型中被发现,并且是丙氨酸和肥大细胞中的主要分泌物的主要形式。其关键特征是分泌颗粒的均型融合。然后,这些通过单个融合孔到外部分泌它们的组合输出。对复合卵尿精的控制仍然尚不敏感。虽然可溶性N-乙基马来酰亚胺敏感因子附着蛋白受体(SNARES)如语法2,SNAP23(23kDA的突触体相关蛋白)和SNAP25已经提出发挥作用,但没有被证明。囊泡相关的膜蛋白8(Vamp8)是与内吞过程相关的圈套,但最近已经提出了在受管制的外毒性中的R-SNARe。当Vamp8函数被抑制并且在Vamp8敲除小鼠中较少时,减少了丙氨酸细胞中的分泌。基于电子显微镜实验,建议Vamp8可以参与复合卵尿胞症。在这里,我们已经测试了Vamp8在顺序化合物外尿胞症期间对偶拷贝颗粒对颗粒融合进行了假设。我们使用新的测定从二级融合事件(颗粒 - 颗粒融合)区分初级融合事件(融合细胞膜)。我们的数据显示来自Vamp8敲除动物的胰腺缩醛细胞具有次级颗粒融合的特异性降低,但原颗粒融合不受影响。此外,免疫沉淀实验显示了与VAMP2的棘突2关联,而Syntaxin 3与Vamp8相关联。我们的数据表明,颗粒 - 颗粒融合由含有纳雷复合物的VAMP8调节,不同于调节初级颗粒融合的VAME。

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