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利用核苷酸类似物探究人MTH1蛋白的底物识别机制。

Probing the substrate recognition mechanism of the human MTH1 protein by nucleotide analogs.

作者信息

Kamiya Hiroyuki, Yakushiji Hiroyuki, Dugué Laurence, Tanimoto Mitsuhide, Pochet Sylvie, Nakabeppu Yusaku, Harashima Hideyoshi

机构信息

Graduate School of Pharmaceutical Sciences, Hokkaido University, Kita-12, Nishi-6, Kita-ku, Sapporo 060-0812, Japan.

出版信息

J Mol Biol. 2004 Feb 27;336(4):843-50. doi: 10.1016/j.jmb.2003.12.060.

Abstract

To examine the substrate recognition mechanism of the human MTH1 protein, which hydrolyzes 2-hydroxy-dATP, 8-hydroxy-dATP, and 8-hydroxy-dGTP, ten nucleotide analogs (8-bromo-dATP, 8-bromo-dGTP, deoxyisoinosine triphosphate, 8-hydroxy-dITP, 2-aminopurine-deoxyriboside triphosphate, 2-amino-dATP, deoxyxanthosine triphosphate, deoxyoxanosine triphosphate, dITP, and dUTP) were incubated with the MTH1 protein. Of these, the former five nucleotides were hydrolyzed with various efficiencies. The fact that the syn-oriented brominated nucleotides were hydrolyzed suggests that the MTH1 protein binds to deoxynucleotides adopting the syn-conformation. However, 8-hydroxy-dITP, which lacks the 2-amino group of 8-hydroxy-dGTP, was degraded with tenfold less efficiency as compared with 8-hydroxy-dGTP. In addition, deoxyisoinosine triphosphate, lacking the 6-amino group of 2-hydroxy-dATP, was hydrolyzed as efficiently as 8-hydroxy-dGTP, but less efficiently than 2-hydroxy-dATP. These results clarify the effects of the anti/syn conformation and the functional groups on the 2 and 6 positions of the purine ring on the recognition by the human MTH1 protein.

摘要

为研究水解2-羟基-dATP、8-羟基-dATP和8-羟基-dGTP的人MTH1蛋白的底物识别机制,将十种核苷酸类似物(8-溴-dATP、8-溴-dGTP、脱氧异肌苷三磷酸、8-羟基-dITP、2-氨基嘌呤-脱氧核糖核苷三磷酸、2-氨基-dATP、脱氧黄苷三磷酸、脱氧氧杂核苷三磷酸、dITP和dUTP)与人MTH1蛋白一起孵育。其中,前五种核苷酸以不同效率被水解。同向排列的溴化核苷酸被水解这一事实表明,MTH1蛋白与采用同向构象的脱氧核苷酸结合。然而,缺乏8-羟基-dGTP的2-氨基基团的8-羟基-dITP,其降解效率比8-羟基-dGTP低十倍。此外,缺乏2-羟基-dATP的6-氨基基团的脱氧异肌苷三磷酸,其水解效率与8-羟基-dGTP相同,但低于2-羟基-dATP。这些结果阐明了反式/同向构象以及嘌呤环2位和6位上的官能团对人MTH1蛋白识别的影响。

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