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首页> 外文期刊>Journal of molecular histology >Ultrastructural immunolocalization of basic fibroblast growth factor in endothelial cells: morphologic evidence for unconventional secretion of a novel protein.
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Ultrastructural immunolocalization of basic fibroblast growth factor in endothelial cells: morphologic evidence for unconventional secretion of a novel protein.

机译:碱性成纤维细胞生长因子在内皮细胞中的超微结构免疫定位:新蛋白非常规分泌的形态学证据。

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Basic fibroblast growth factor (bFGF) is one of the most potent angiogenic factors. Unlike many other growth factors, bFGF lacks a classic peptide sequence for its secretion. Recent studies suggest that there is an unconventional secretory pathway for this growth factor. The aim of this study was to identify the specific location of bFGF in endothelial cells and to find morphologic evidences concerning its synthesis, storage and release from endothelial cells. The capillaries in hippocampus, adrenal gland, kidney, peripheral nerves as well as the vessels in connective tissues were analysed by using immunogold labeling techniques at electron microscope level. Results show that endogenous bFGF is mainly located in the nuclei of endothelial cells. Slight immunoreactivity is found in the cytoplasm. Immunolabeling is notably absent in pinocytotic vesicles, Golgi complexes, endoplasmic reticulum, nuclear membrane and intercellular junctions. These results provide morphologic evidence suggesting that endothelial cells might export bFGF via unique cellular pathways that are clearly distinct from classical signal peptide mediated secretion and/or release of this protein could be directly through mechanically induced disruptions of these cells. The current study support the recent hypothesis related with unconventional secretory pathway for bFGF as some other "cargo" proteins.
机译:碱性成纤维细胞生长因子(bFGF)是最有效的血管生成因子之一。与许多其他生长因子不同,bFGF缺乏分泌经典的肽序列。最近的研究表明,该生长因子存在非常规的分泌途径。这项研究的目的是鉴定bFGF在内皮细胞中的特定位置,并寻找有关bFGF合成,储存和从内皮细胞释放的形态学证据。使用电子显微镜水平的免疫金标记技术分析海马,肾上腺,肾,周围神经以及结缔组织中的血管的毛细血管。结果表明,内源性bFGF主要位于内皮细胞核中。在细胞质中发现轻微的免疫反应性。在胞吞小泡,高尔基复合体,内质网,核膜和细胞间连接中明显没有免疫标记。这些结果提供了形态学证据,表明内皮细胞可能通过独特的细胞途径输出bFG​​F,而这些细胞途径明显不同于经典的信号肽介导的分泌和/或释放该蛋白,可以直接通过机械诱导这些细胞的破坏。当前的研究支持与bFGF作为其他“货物”蛋白的非常规分泌途径有关的最新假说。

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