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首页> 外文期刊>Journal of cell biology >Vamp-7 Mediates Vesicular Transport from Endosomes to Lysosomes
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Vamp-7 Mediates Vesicular Transport from Endosomes to Lysosomes

机译:Vamp-7介导从内体到溶酶体的囊泡运输。

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A more complete picture of the molecules that are critical for the organization of membrane compartments is beginning to emerge through the characterization of proteins in the vesicle-associated membrane protein (also called synaptobrevin) family of membrane trafficking proteins. To better understand the mechanisms of membrane trafficking within the endocytic pathway, we generated a series of monoclonal and polyclonal antibodies against the cytoplasmic domain of vesicle-associated membrane protein 7 (VAMP-7). The antibodies recognize a 25-kD membrane-associated protein in multiple tissues and cell lines. Immunohistochemical analysis reveals colocalization with a marker of late endosomes and lysosomes, lysosome-associated membrane protein 1 (LAMP-1), but not with other membrane markers, including p115 and transferrin receptor. Treatment with nocodozole or brefeldin A does not disrupt the colocalization of VAMP-7 and LAMP-1. Immunoelectron microscopy analysis shows that VAMP-7 is most concentrated in the trans -Golgi network region of the cell as well as late endosomes and transport vesicles that do not contain the mannose-6 phosphate receptor. In streptolysin- O–permeabilized cells, antibodies against VAMP-7 inhibit the breakdown of epidermal growth factor but not the recycling of transferrin. These data are consistent with a role for VAMP-7 in the vesicular transport of proteins from the early endosome to the lysosome.
机译:通过膜转运蛋白的与囊泡相关的膜蛋白(也称为突触短纤维蛋白)家族中的蛋白的表征,对膜间隔组织至关重要的分子的更完整的图片开始出现。为了更好地理解内吞途径内膜运输的机制,我们产生了一系列针对囊泡相关膜蛋白7(VAMP-7)胞质域的单克隆和多克隆抗体。抗体识别多种组织和细胞系中的25 kD膜相关蛋白。免疫组织化学分析显示与晚期内体和溶酶体的标记物,溶酶体相关的膜蛋白1(LAMP-1)共定位,但与其他膜标记物(包括p115和转铁蛋白受体)共定位。诺考唑或布雷菲德菌素A的治疗不会破坏VAMP-7和LAMP-1的共定位。免疫电子显微镜分析显示,VAMP-7最集中在细胞的反式-高尔基体网络区域以及不包含甘露糖6磷酸受体的晚期内体和转运囊泡中。在经链球菌溶血素-O渗透的细胞中,针对VAMP-7的抗体可抑制表皮生长因子的降解,但不能抑制转铁蛋白的循环。这些数据与VAMP-7在蛋白质从早期内体到溶酶体的囊泡运输中的作用一致。

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