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首现缺失的雄性基因(MOF):从果蝇到人类

Males absent on the first (MOF): from flies to humans.

作者信息

Rea S, Xouri G, Akhtar A

机构信息

Gene Expression Programme, European Molecular Biology Laboratory, Heidelberg, Germany.

出版信息

Oncogene. 2007 Aug 13;26(37):5385-94. doi: 10.1038/sj.onc.1210607.

Abstract

Histone modifications such as acetylation, methylation and phosphorylation have been implicated in fundamental cellular processes such as epigenetic regulation of gene expression, organization of chromatin structure, chromosome segregation, DNA replication and DNA repair. Males absent on the first (MOF) is responsible for acetylating histone H4 at lysine 16 (H4K16) and is a key component of the MSL complex required for dosage compensation in Drosophila. The human ortholog of MOF (hMOF) has the same substrate specificity and recent purification of the human and Drosophila MOF complexes showed that these complexes were also highly conserved through evolution. Several studies have shown that loss of hMOF in mammalian cells leads to a number of different phenotypes; a G2/M cell cycle arrest, nuclear morphological defects, spontaneous chromosomal aberrations, reduced transcription of certain genes and an impaired DNA repair response upon ionizing irradiation. Moreover, hMOF is involved in ATM activation in response to DNA damage and acetylation of p53 by hMOF influences the cell's decision to undergo apoptosis instead of a cell cycle arrest. These data, highlighting hMOF as an important component of many cellular processes, as well as links between hMOF and cancer will be discussed.

摘要

组蛋白修饰,如乙酰化、甲基化和磷酸化,已涉及到一些基本的细胞过程,如基因表达的表观遗传调控、染色质结构的组织、染色体分离、DNA复制和DNA修复。第一雄性缺失蛋白(MOF)负责组蛋白H4赖氨酸16位点(H4K16)的乙酰化,并且是果蝇剂量补偿所需的MSL复合物的关键组成部分。MOF的人类直系同源物(hMOF)具有相同的底物特异性,最近对人类和果蝇MOF复合物的纯化表明,这些复合物在进化过程中也高度保守。多项研究表明,哺乳动物细胞中hMOF的缺失会导致多种不同的表型;G2/M期细胞周期停滞、核形态缺陷、自发染色体畸变、某些基因的转录减少以及电离辐射后DNA修复反应受损。此外,hMOF参与DNA损伤时的ATM激活,hMOF对p53的乙酰化影响细胞是选择凋亡而非细胞周期停滞的决定。本文将讨论这些突出hMOF作为许多细胞过程重要组成部分的数据,以及hMOF与癌症之间的联系。

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