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Writing and erasing MYC ubiquitination and SUMOylation

机译:编写和擦除MYC泛素化和SUMOylation

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The transcription factor c-MYC (MYC thereafter) controls diverse transcription programs and plays a key role in the development of many human cancers. Cells develop multiple mechanisms to ensure that MYC levels and activity are precisely controlled in normal physiological context. As a short half-lived protein, MYC protein levels are tightly regulated by the ubiquitin proteasome system. Over a dozen of ubiquitin ligases have been found to ubiquitinate MYC whereas a number of deubiquitinating enzymes counteract this process. Recent studies show that SUMOylation and deSUMOylation can also regulate MYC protein stability and activity. Interestingly, evidence suggests an intriguing crosstalk between MYC ubiquitination and SUMOylation. Deregulation of the MYC ubiquitination-SUMOylation regulatory network may contribute to tumorigenesis. This review is intended to provide the current understanding of the complex regulation of the MYC biology by dynamic ubiquitination and SUMOylation and their crosstalk.
机译:转录因子c-MYC(此后称为MYC)控制多种转录程序,并在许多人类癌症的发展中发挥关键作用。细胞发展出多种机制来确保在正常生理环境中精确控制MYC水平和活性。作为半衰期短的蛋白质,MYC蛋白质水平受到泛素蛋白酶体系统的严格调控。已经发现超过十二种泛素连接酶使MYC泛素化,而许多去泛素化酶抵消了这一过程。最近的研究表明SUMOylation和deSUMOylation也可以调节MYC蛋白的稳定性和活性。有趣的是,证据表明MYC泛素化和SUMOylation之间的串扰。 MYC泛素化-SUMOylation调节网络的失调可能有助于肿瘤发生。这篇综述旨在通过动态泛素化和SUMOylation及其串扰提供对MYC生物学复杂调控的当前理解。

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