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Regulation of TGF–β signal transduction by mono- and deubiquitylation of Smads

机译:粉刺单体和脱硫的TGF-β信号转导

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摘要

Polyubiquitylation leading to proteasomal degradation is a well-established mechanism for regulating TGF-β signal transduction components such as receptors and Smads. Recently, an equally important role was suggested for monoubiquitylation of both Smad4 and Receptor-associated Smads that regulates their function without protein degradation. Monoubiquitylation of Smads was discovered following the identification of deubiquitylases required for TGF-β signaling, suggesting that continuous cycles of Smad mono- and deubiquitylation are required for proper TGF-β signal transduction. Here we summarize and discuss recent work on Smad mono- and deubiquitylation.
机译:导致蛋白酶体降解的多辅基金是用于调节TGF-β信号转导组分如受体和Smads的良好结构机制。最近,建议对Smad4和受体相关的血液的单相腹进行同样重要的作用,其在没有蛋白质降解的情况下调节其功能。在鉴定TGF-β信号传导所需的氘基酶后发现了Smads的Monoubiquitylations,表明适当的TGF-β信号转导需要连续的Smad单次和脱硫的循环。在这里,我们总结了并讨论了最近对Smad单音和脱硫的工作。

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