动态调节的 HDAC2 类泛素化控制 p53 的去乙酰化作用，并限制遗传毒性应激后的细胞凋亡。

Dynamically regulated sumoylation of HDAC2 controls p53 deacetylation and restricts apoptosis following genotoxic stress.

机构信息

Center for Molecular Biomedicine, Institute for Biochemistry and Biophysics, Department of Biochemistry, Friedrich Schiller University of Jena, Hans-Knöll-Straße 2, 07745 Jena, Germany.

出版信息

J Mol Cell Biol. 2012 Oct;4(5):284-93. doi: 10.1093/jmcb/mjs013. Epub 2012 Apr 5.

DOI:10.1093/jmcb/mjs013

PMID:22493095

Abstract

Histone deacetylase 2 (HDAC2) is relevant for homeostasis and plays a critical role in gastrointestinal cancers. Here, we report that post-translational modification of endogenous HDAC2 with small ubiquitin-related modifier 1 (SUMO1) is a new regulatory switch for the tumor suppressor p53. Sumoylation of HDAC2 at lysine 462 allows binding of HDAC2 to p53. Moreover, sumoylated HDAC2 is a previously not recognized biologically relevant site-specific deacetylase for p53. Deacetylation of p53 at lysine 320 by sumoylated HDAC2 blocks recruitment of p53 into promoter-associated complexes and p53-dependent expression of genes for cell cycle control and apoptosis. Thereby, catalytically active sumoylated HDAC2 restricts p53 functions and attenuates DNA damage-induced apoptosis. Genotoxic stress evokes desumoylation of HDAC2, enabling p53-dependent gene expression. Our data show a new molecular mechanism involving a dynamically controlled HDAC2-sumoylation/p53-acetylation switch that regulates cell fate decisions following genotoxic stress.

摘要

组蛋白去乙酰化酶 2（HDAC2）与内源性的 SUMO1 发生翻译后修饰，与细胞内稳态相关，并在胃肠道癌症中发挥关键作用。我们在此报道，HDAC2 的赖氨酸 462 残基的 SUMO1 化修饰成为肿瘤抑制因子 p53 的新调控开关。SUMO1 化修饰的 HDAC2 可与 p53 结合。此外，SUMO1 化的 HDAC2 是 p53 的一个以前未被识别的、具有生物学意义的、特异性去乙酰化酶。SUMO1 化的 HDAC2 对 p53 的赖氨酸 320 进行去乙酰化修饰，阻止 p53 募集到与启动子相关的复合物中，以及 p53 依赖的细胞周期控制和凋亡基因的表达。因此，具有催化活性的 SUMO1 化的 HDAC2 限制了 p53 的功能，并减弱了 DNA 损伤诱导的细胞凋亡。遗传毒性应激会引发 HDAC2 的去 SUMO 化，从而使 p53 依赖的基因表达。我们的数据显示了一种新的分子机制，涉及到一个动态调控的 HDAC2-SUMO1 化/p53 乙酰化开关，该开关调节了遗传毒性应激后细胞命运的决定。