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Ubc13 and COOH Terminus of Hsp70-interacting Protein (CHIP) Are Required for Growth Hormone Receptor Endocytosis

机译:Hb70相互作用蛋白(CHIP)的Ubc13和COOH总站是生长激素受体内吞作用所必需的

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摘要

Growth hormone receptor (GHR) endocytosis is a highly regulated process that depends on the binding and activity of the multimeric ubiquitin ligase, SCFβTrCP (Skp Cullin F-box). Despite a specific interaction between β-transducin repeat-containing protein (βTrCP) and the GHR, and a strict requirement for ubiquitination activity, the receptor is not an obligatory target for SCFβTrCP-directed Lys48 polyubiquitination. We now show that also Lys63-linked ubiquitin chain formation is required for GHR endocytosis. We identified both the ubiquitin-conjugating enzyme Ubc13 and the ubiquitin ligase COOH terminus of Hsp70 interacting protein (CHIP) as being connected to this process. Ubc13 activity and its interaction with CHIP precede endocytosis of GHR. In addition to βTrCP, CHIP interacts specifically with the cytosolic tails of the dimeric GHR, identifying both Ubc13 and CHIP as novel factors in the regulation of cell surface availability of GHR.
机译:生长激素受体(GHR)的内吞作用是一个高度受控的过程,取决于多聚体泛素连接酶SCF βTrCP(Skp Cullin F-box)的结合和活性。尽管包含β-转导蛋白重复序列​​的蛋白(βTrCP)和GHR之间存在特定的相互作用,并且对泛素化活性有严格要求,但该受体并不是SCF βTrCP指导的Lys 的强制性靶标。 48 多聚泛素化。现在我们显示,GHR内吞还需要Lys 63 连接的泛素链形成。我们确定Hsp70相互作用蛋白(CHIP)的泛素结合酶Ubc13和泛素连接酶COOH末端都与此过程相关。 Ubc13活性及其与CHIP的相互作用先于GHR的内吞作用。除βTrCP以外,CHIP还与二聚体GHR的胞质尾部特异性相互作用,从而将Ubc13和CHIP均视为调节GHR细胞表面可用性的新因素。

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