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XIAP as a ubiquitin ligase in cellular signaling.

机译:XIAP作为细胞信号传导中的泛素连接酶。

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摘要

The ability of the vertebrate X-linked inhibitor of apoptosis (XIAP) protein to directly suppress apoptotic cell death pathways has been the subject of much research. Studies of this broadly expressed protein have largely focused on the unique interactions between XIAP and caspases - proteases that conduct and participate in the ordered disassembly of the cell during apoptosis. However, relatively less attention has been given to the RING domain of XIAP, which functions as an E3 ligase to catalyze the ubiquitination of substrate proteins. Here, we discuss the evidence implicating the RING domain of XIAP in the ubiquitin-mediated regulation of three, somewhat arbitrarily divided, categories of substrate: XIAP itself, XIAP-interacting proteins involved in apoptosis, and other targets whose physiological roles likely extend beyond cell death. Collectively, these multiple activities of XIAP show that this enigmatic protein participates in a range of cellular activities beyond apoptotic suppression.
机译:脊椎动物X连锁凋亡抑制剂(XIAP)蛋白直接抑制凋亡细胞死亡途径的能力已成为许多研究的主题。这种广泛表达的蛋白质的研究主要集中在XIAP和胱天蛋白酶之间的独特相互作用。胱天蛋白酶是在细胞凋亡过程中进行并参与细胞有序分解的蛋白酶。但是,对XIAP的RING结构域的关注相对较少,该结构域作为E3连接酶来催化底物蛋白的泛素化。在这里,我们讨论了在泛素介导的三种底物类别的调控中涉及XIAP的RING域的证据:XIAP本身,参与凋亡的XIAP相互作用蛋白以及其他靶标的生理作用可能超出细胞死亡。总的来说,XIAP的这些多种活性表明,这种神秘的蛋白质参与了细胞凋亡以外的一系列细胞活动。

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