Cbl 通过调节早期内体融合控制 EGFR 命运。
Cbl controls EGFR fate by regulating early endosome fusion.
机构信息
Department of Pharmacology, University of Iowa, Iowa City, IA 52242, USA.
出版信息
Sci Signal. 2009 Dec 22;2(102):ra86. doi: 10.1126/scisignal.2000217.
Abstract
Amino acid residues 1 to 434 of the E3 ubiquitin ligase Cbl control signaling of the epidermal growth factor receptor (EGFR) by enhancing its ubiquitination, down-regulation, and lysosomal degradation. This region of Cbl comprises a tyrosine kinase-binding domain, a linker region, a really interesting new gene finger (RF), and a subset of the residues of the RF tail. In experiments with full-length alanine substitution mutants, we demonstrated that the RF tail of Cbl regulated biochemically distinct checkpoints in the endocytosis of EGFR. The Cbl- and ubiquitin-dependent degradation of the regulator of internalization hSprouty2 was compromised by the Val(431)--> Ala mutation, whereas the Cbl- and EGFR-dependent dephosphorylation or degradation of the endosomal trafficking regulator Hrs was compromised by the Phe(434)--> Ala mutation. Deregulated phosphorylation of Hrs correlated with inhibition of the fusion of early endosomes and of the degradation of EGFR. This study provides the first evidence that Cbl regulates receptor fate by controlling the fusion of sorting endosomes. We postulate that it does so by modulating the abundance of tyrosine-phosphorylated Hrs.
摘要
E3 泛素连接酶 Cbl 的第 1 至 434 个氨基酸残基通过增强其泛素化、下调和溶酶体降解来控制表皮生长因子受体 (EGFR) 的信号。Cbl 的这一区域包含一个酪氨酸激酶结合域、一个连接区、一个真正有趣的新基因指(RF)和 RF 尾部的一部分残基。在全长丙氨酸取代突变体的实验中,我们证明 Cbl 的 RF 尾部调节 EGFR 内吞作用中生化上不同的检查点。Cbl 和泛素依赖性的内吞调节因子 hSprouty2 的降解受到 Val(431)-->Ala 突变的影响,而 Cbl 和 EGFR 依赖性的内体运输调节剂 Hrs 的去磷酸化或降解受到 Phe(434)-->Ala 突变的影响。Hrs 的去磷酸化失调与早期内体融合和 EGFR 降解的抑制有关。这项研究首次提供了证据表明 Cbl 通过控制分拣内体的融合来调节受体命运。我们假设它通过调节酪氨酸磷酸化 Hrs 的丰度来实现这一点。
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