Schuetz Anja, Min Jinrong, Allali-Hassani Abdellah, Schapira Matthieu, Shuen Michael, Loppnau Peter, Mazitschek Ralph, Kwiatkowski Nick P, Lewis Timothy A, Maglathin Rebecca L, McLean Thomas H, Bochkarev Alexey, Plotnikov Alexander N, Vedadi Masoud, Arrowsmith Cheryl H
Structural Genomics Consortium, University of Toronto, Toronto, Ontario M5G 1L5, Canada.
J Biol Chem. 2008 Apr 25;283(17):11355-63. doi: 10.1074/jbc.M707362200. Epub 2008 Feb 19.
Histone deacetylases (HDACs) are protein deacetylases that play a role in repression of gene transcription and are emerging targets in cancer therapy. Here, we characterize the structure and enzymatic activity of the catalytic domain of human HDAC7 (cdHDAC7). Although HDAC7 normally exists as part of a multiprotein complex, we show that cdHDAC7 has a low level of deacetylase activity which can be inhibited by known HDAC inhibitors. The crystal structures of human cdHDAC7 and its complexes with two hydroxamate inhibitors are the first structures of the catalytic domain of class IIa HDACs and demonstrate significant differences with previously reported class I and class IIb-like HDAC structures. We show that cdHDAC7 has an additional class IIa HDAC-specific zinc binding motif adjacent to the active site which is likely to participate in substrate recognition and protein-protein interaction and may provide a site for modulation of activity. Furthermore, a different active site topology results in modified catalytic properties and in an enlarged active site pocket. Our studies provide mechanistic insights into class IIa HDACs and facilitate the design of specific modulators.
组蛋白去乙酰化酶(HDACs)是一类蛋白质去乙酰化酶,在基因转录抑制中发挥作用,正成为癌症治疗的新兴靶点。在此,我们对人HDAC7催化结构域(cdHDAC7)的结构和酶活性进行了表征。尽管HDAC7通常作为多蛋白复合物的一部分存在,但我们发现cdHDAC7具有较低水平的去乙酰化酶活性,且可被已知的HDAC抑制剂抑制。人cdHDAC7及其与两种异羟肟酸酯抑制剂复合物的晶体结构是IIa类HDACs催化结构域的首个结构,显示出与先前报道的I类和IIb类HDAC结构存在显著差异。我们发现cdHDAC7在活性位点附近有一个额外的IIa类HDAC特异性锌结合基序,它可能参与底物识别和蛋白质 - 蛋白质相互作用,并可能为活性调节提供一个位点。此外,不同的活性位点拓扑结构导致催化特性改变以及活性位点口袋扩大。我们的研究为IIa类HDACs提供了机制性见解,并有助于设计特异性调节剂。
