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泛素缀合系统与内吞途径在生长激素受体配体诱导的内化中的联系。

Linkage of the ubiquitin-conjugating system and the endocytic pathway in ligand-induced internalization of the growth hormone receptor.

作者信息

Govers R, van Kerkhof P, Schwartz A L, Strous G J

机构信息

Department of Cell Biology, Faculty of Medicine and Institute of Biomembranes, Utrecht University, The Netherlands.

出版信息

EMBO J. 1997 Aug 15;16(16):4851-8. doi: 10.1093/emboj/16.16.4851.

Abstract

The major function of the ubiquitin-conjugating system is the targeting of cytosolic and nuclear proteins for degradation by the proteasome. Recently, ubiquitin conjugation has been implicated in the downregulation of signalling receptors such as the mammalian growth hormone receptor (GHR) and the alpha-factor receptor in yeast. By examining truncated receptors, the internalization-deficient receptor mutant F327A and conditions under which clathrin-mediated GHR endocytosis is inhibited, we show here that GHR ubiquitination and ligand-induced GHR internalization are coupled events. Previously, we had shown that GHR endocytosis is dependent on an intact ubiquitination system. Here we present evidence that GHR ubiquitination depends on an intact endocytic pathway. Our data indicate that the ubiquitin-conjugating system and the endocytic pathway interact at the cytoplasmic tail of the GHR at the plasma membrane, where they cooperate to regulate internalization of the GHR.

摘要

泛素缀合系统的主要功能是将胞质和核蛋白靶向蛋白酶体进行降解。最近,泛素缀合已被认为与信号受体的下调有关,如哺乳动物生长激素受体(GHR)和酵母中的α-因子受体。通过检查截短的受体、内化缺陷型受体突变体F327A以及网格蛋白介导的GHR内吞作用被抑制的条件,我们在此表明GHR泛素化和配体诱导的GHR内化是偶联事件。此前,我们已表明GHR内吞作用依赖于完整的泛素化系统。在此我们提供证据表明GHR泛素化依赖于完整的内吞途径。我们的数据表明泛素缀合系统和内吞途径在质膜上GHR的细胞质尾部相互作用,它们在那里协同调节GHR的内化。

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