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首页> 外文期刊>Biochimica et biophysica acta: international journal of biochemistry and biophysics >Two MAD tails: what the recent knockouts of Mad1 and Mxi1 tell us about the MYC/MAX/MAD network.
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Two MAD tails: what the recent knockouts of Mad1 and Mxi1 tell us about the MYC/MAX/MAD network.

机译:MAD有两条尾巴:Mad1和Mxi1的最近淘汰赛告诉我们有关MYC / MAX / MAD网络的信息。

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摘要

Members of the MAD/MXI protein family heterodimerize with MAX and repress transcription by recruiting a chromatin-modifying co-repressor complex to specific DNA target genes. Repression mediated by MAD is thought to antagonize the transcriptional activation and proliferation-promoting functions of MYC-MAX heterodimers. Because they are induced during differentiation, it has been suggested that MAD proteins act to limit cell proliferation during terminal differentiation. There is also controversial evidence that these proteins may function as tumor suppressors. Recently, targeted gene deletions of two members of this gene family, Mad1 and Mxi1, have been carried out in mice. Although these animals display what appear to be quite different phenotypes, further analysis supports the view that both these proteins function in cell-cycle exit during terminal differentiation, and that at least MXI1 can act as a tumor suppressor.
机译:MAD / MXI蛋白家族的成员与MAX异源二聚体,并通过向特定的DNA靶基因募集染色质修饰的共阻遏物复合物来抑制转录。由MAD介导的抑制被认为拮抗MYC-MAX异二聚体的转录激活和增殖促进功能。由于它们是在分化过程中诱导的,因此有人提出MAD蛋白在终末分化过程中起着限制细胞增殖的作用。也有争议的证据表明这些蛋白质可能起抑癌作用。最近,已经在小鼠中进行了该基因家族的两个成员Mad1和Mxi1的靶向基因删除。尽管这些动物表现出似乎完全不同的表型,但进一步的分析支持以下观点:这两种蛋白均在终末分化过程中在细胞周期出口起作用,并且至少MXI1可以充当肿瘤抑制因子。

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