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MYST家族组蛋白乙酰转移酶Esa1中的催化位点突变。

Catalytic-site mutations in the MYST family histone Acetyltransferase Esa1.

作者信息

Decker Peter V, Yu David Y, Iizuka Masayoshi, Qiu Qifeng, Smith M Mitchell

机构信息

Department of Microbiology, University of Virginia Cancer Center, University of Virginia Health System, Charlottesville, Virginia 22908, USA.

出版信息

Genetics. 2008 Mar;178(3):1209-20. doi: 10.1534/genetics.107.080135. Epub 2008 Feb 1.

Abstract

Esa1 is the only essential histone acetyltransferase (HAT) in budding yeast. It is the catalytic subunit of at least two multiprotein complexes, NuA4 and Piccolo NuA4 (picNuA4), and its essential function is believed to be its catalytic HAT activity. To examine the role of Esa1 in DNA damage repair, we isolated viable esa1 mutants with a range of hypersensitivities to the toposide camptothecin. Here we show that the sensitivity of these mutants to a variety of stresses is inversely proportional to their level of histone H4 acetylation, demonstrating the importance of Esa1 catalytic activity for resistance to genotoxic stress. Surprisingly, individual mutations in two residues directly involved in catalysis were not lethal even though the mutant enzymes appear catalytically inactive both in vivo and in vitro. However, the double-point mutant is lethal, demonstrating that the essential function of Esa1 relies on residues within the catalytic pocket but not catalysis. We propose that the essential function of Esa1 may be to bind acetyl-CoA or lysine substrates and positively regulate the activities of NuA4 and Piccolo NuA4.

摘要

Esa1是芽殖酵母中唯一必需的组蛋白乙酰转移酶(HAT)。它是至少两种多蛋白复合物NuA4和小NuA4(picNuA4)的催化亚基,其基本功能被认为是其催化HAT活性。为了研究Esa1在DNA损伤修复中的作用,我们分离出了对拓扑异构酶喜树碱具有一系列超敏反应的存活esa1突变体。在这里我们表明,这些突变体对多种应激的敏感性与它们的组蛋白H4乙酰化水平成反比,这证明了Esa1催化活性对抵抗基因毒性应激的重要性。令人惊讶的是,即使突变酶在体内和体外似乎都没有催化活性,但直接参与催化的两个残基中的单个突变并不致命。然而,双点突变体是致命的,这表明Esa1的基本功能依赖于催化口袋内的残基而不是催化作用。我们提出,Esa1的基本功能可能是结合乙酰辅酶A或赖氨酸底物,并正向调节NuA4和小NuA4的活性。

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