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胰岛素受体的核转位。胰岛素长期效应的一种可能介导物。

Nuclear translocation of the insulin receptor. A possible mediator of insulin's long term effects.

作者信息

Podlecki D A, Smith R M, Kao M, Tsai P, Huecksteadt T, Brandenburg D, Lasher R S, Jarett L, Olefsky J M

出版信息

J Biol Chem. 1987 Mar 5;262(7):3362-8.

PMID:3546306
Abstract

The translocation of occupied surface insulin receptors to the nuclei of isolated hepatocytes was studied using the biologically active photosensitive insulin derivative, B2(2-nitro-4-azidophenylacetyl)-des-PheB1-insulin (NAPA-DP-insulin). When hepatocytes were photolabeled at 4 degrees C, extensively washed, and then further incubated at 37 degrees C for 1 h, photolabeled insulin receptors, which were initially localized to the cell surface, accumulated in the subsequently isolated nuclei. When the isolated nuclei were solubilized and subjected to polyacrylamide gel electrophoresis and radioautography, labeled proteins with Mr identical to the cell surface insulin receptor were detected. Light microscopic radioautography of nuclei isolated from cells incubated for 1 ha at 37 degrees C demonstrated that 28% of these nuclei were specifically labeled with one or more grains. Electron microscopic radioautography of intact cultured hepatocytes, incubated 60 min at 37 degrees C, revealed that 26% of the thin-sectioned nuclei contained at least a single grain and 8.3% of the total cell-associated associated grains were located over the nuclei. Only 1.6% of grains were localized to lysosomes. In contrast, if photolabeled hepatocytes were incubated at 4 degrees C for up to 2 h, negligible accumulation of nuclear radioactivity was observed by polyacrylamide gel electrophoresis on light or electron microscopic radioautography. Conclusions are as follows. Occupied cell surface insulin receptors can internalize and translocate to the nucleus of intact hepatocytes by a time- and temperature-dependent mechanism. Accumulation and possible degradation of insulin receptors in lysosomes involves only a small percentage of the receptors internalized. Nuclear translocation of occupied cell surface insulin receptors may be a mechanism which mediates insulin's long term effects.

摘要

利用具有生物活性的光敏胰岛素衍生物B2(2-硝基-4-叠氮苯乙酰基)-去苯丙氨酸B1-胰岛素(NAPA-DP-胰岛素),研究了占据的表面胰岛素受体向分离的肝细胞细胞核的转位情况。当肝细胞在4℃下进行光标记、充分洗涤,然后在37℃下进一步孵育1小时时,最初定位于细胞表面的光标记胰岛素受体在随后分离的细胞核中积累。当分离的细胞核被溶解并进行聚丙烯酰胺凝胶电泳和放射自显影时,检测到分子量与细胞表面胰岛素受体相同的标记蛋白。对在37℃下孵育1小时的细胞分离出的细胞核进行光学显微镜放射自显影显示,这些细胞核中有28%被一个或多个银粒特异性标记。对完整培养的肝细胞在37℃下孵育60分钟后进行电子显微镜放射自显影,结果显示,26%的薄切片细胞核至少含有一个银粒,且与细胞相关的银粒总数的8.3%位于细胞核上。只有1.6%的银粒定位于溶酶体。相比之下,如果将光标记的肝细胞在4℃下孵育长达2小时,通过聚丙烯酰胺凝胶电泳、光学或电子显微镜放射自显影观察到的核放射性积累可以忽略不计。结论如下。占据的细胞表面胰岛素受体可通过一种时间和温度依赖性机制内化并转位至完整肝细胞的细胞核。胰岛素受体在溶酶体中的积累及可能的降解仅涉及内化受体的一小部分。占据的细胞表面胰岛素受体的核转位可能是介导胰岛素长期效应的一种机制。

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