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E2F1通过HCF-1和组蛋白甲基转移酶的MLL家族介导DNA损伤和细胞凋亡。

E2F1 mediates DNA damage and apoptosis through HCF-1 and the MLL family of histone methyltransferases.

作者信息

Tyagi Shweta, Herr Winship

机构信息

Center for Integrative Genomics, University of Lausanne, Génopode, Lausanne, Switzerland.

出版信息

EMBO J. 2009 Oct 21;28(20):3185-95. doi: 10.1038/emboj.2009.258. Epub 2009 Sep 17.

Abstract

E2F1 is a key positive regulator of human cell proliferation and its activity is altered in essentially all human cancers. Deregulation of E2F1 leads to oncogenic DNA damage and anti-oncogenic apoptosis. The molecular mechanisms by which E2F1 mediates these two processes are poorly understood but are important for understanding cancer progression. During the G1-to-S phase transition, E2F1 associates through a short DHQY sequence with the cell-cycle regulator HCF-1 together with the mixed-lineage leukaemia (MLL) family of histone H3 lysine 4 (H3K4) methyltransferases. We show here that the DHQY HCF-1-binding sequence permits E2F1 to stimulate both DNA damage and apoptosis, and that HCF-1 and the MLL family of H3K4 methyltransferases have important functions in these processes. Thus, HCF-1 has a broader role in E2F1 function than appreciated earlier. Indeed, sequence changes in the E2F1 HCF-1-binding site can modulate both up and down the ability of E2F1 to induce apoptosis indicating that HCF-1 association with E2F1 is a regulator of E2F1-induced apoptosis.

摘要

E2F1是人类细胞增殖的关键正向调节因子,其活性在几乎所有人类癌症中都会发生改变。E2F1失调会导致致癌性DNA损伤和抗肿瘤凋亡。E2F1介导这两个过程的分子机制尚不清楚,但对于理解癌症进展很重要。在G1期到S期转换过程中,E2F1通过一个短的DHQY序列与细胞周期调节因子HCF-1以及组蛋白H3赖氨酸4(H3K4)甲基转移酶的混合谱系白血病(MLL)家族结合。我们在此表明,DHQY HCF-1结合序列使E2F1能够刺激DNA损伤和凋亡,并且HCF-1和H3K4甲基转移酶的MLL家族在这些过程中具有重要功能。因此,HCF-1在E2F1功能中的作用比之前认为的更广泛。实际上,E2F1 HCF-1结合位点的序列变化可以上调和下调E2F1诱导凋亡的能力,表明HCF-1与E2F1的结合是E2F1诱导凋亡的一个调节因子。

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