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Cbl-c Ubiquitin Ligase Activity Is Increased via the Interaction of Its RING Finger Domain with a LIM Domain of the Paxillin Homolog Hic 5

机译:CBL-C泛素连接酶的活动是通过其环指结构域与桩蛋白同源嗝5的LIm域相互作用增加

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摘要

Cbl proteins (Cbl, Cbl-b and Cbl-c) are ubiquitin ligases that are critical regulators of tyrosine kinase signaling. In this study we identify a new Cbl-c interacting protein, Hydrogen peroxide Induced Construct 5 (Hic-5). The two proteins interact through a novel interaction mediated by the RING finger of Cbl-c and the LIM2 domain of Hic-5. Further, this interaction is mediated and dependent on specific zinc coordinating complexes within the RING finger and LIM domain. Binding of Hic-5 to Cbl-c leads to an increase in the ubiquitin ligase activity of Cbl-c once Cbl-c has been activated by Src phosphorylation or through an activating phosphomimetic mutation. In addition, co-transfection of Hic-5 with Cbl-c leads to an increase in Cbl-c mediated ubiquitination of the EGFR. These data suggest that Hic-5 enhances Cbl-c ubiquitin ligase activity once Cbl-c has been phosphorylated and activated. Interactions between heterologous RING fingers have been shown to activate E3s. This is the first demonstration of enhancement of ubiquitin ligase activity of a RING finger ubiquitin ligase by the direct interaction of a LIM zinc coordinating domain.
机译:Cbl蛋白(Cbl,Cbl-b和Cbl-c)是泛素连接酶,是酪氨酸激酶信号转导的关键调节剂。在这项研究中,我们确定了一种新的Cbl-c相互作用蛋白,过氧化氢诱导的构建体5(Hic-5)。两种蛋白质通过Cbl-c的RING指和Hic-5的LIM2结构域介导的新型相互作用进行相互作用。此外,这种相互作用是由RING指和LIM域内的特定锌配位复合物介导的。一旦通过Src磷酸化或通过激活的拟磷酸化突变激活了Cbl-c,Hic-5与Cbl-c的结合将导致Cbl-c的泛素连接酶活性增加。另外,Hic-5与Cbl-c的共转染导致Cbl-c介导的EGFR泛素化的增加。这些数据表明,一旦Cbl-c被磷酸化并被激活,Hic-5就会增强Cbl-c泛素连接酶的活性。异源RING指之间的相互作用已显示可激活E3。这是通过LIM锌配位域的直接相互作用增强RING手指泛素连接酶的泛素连接酶活性的首次证明。

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