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腺苷脱氨酶样蛋白 1(ADAL1):在 N(6)-或 O(6)取代嘌呤或 2-氨基嘌呤核苷单磷酸水解中的特性和底物特异性。

Adenosine deaminase-like protein 1 (ADAL1): characterization and substrate specificity in the hydrolysis of N(6)- or O(6)-substituted purine or 2-aminopurine nucleoside monophosphates.

机构信息

Pharmasset, Inc., 303A College Road East, Princeton, New Jersey 08540, USA.

出版信息

J Med Chem. 2011 Aug 25;54(16):5902-14. doi: 10.1021/jm200650j. Epub 2011 Jul 22.

Abstract

Human N(6)-methyl-AMP/dAMP aminohydrolase has been shown to be involved in metabolism of pharmacologically important N(6)-substituted purine nucleosides and 5'-monophosphate prodrugs thereof. This enzyme was cloned and expressed in E. coli, and mass spectroscopic analysis followed by amino acid sequence analyses indicated that the protein was adenosine deaminase-like protein isoform 1 (ADAL1). An extensive structure-activity relationship study showed that ADAL1 was able to catalyze removal of different alkyl groups not only from N(6)-substituted purine or 2-aminopurine nucleoside monophosphates but also from O(6)-substituted compounds. The ADAL1 activity was susceptible to modifications in the phosphate moiety but not to changes in the sugar moiety. Overall, our data indicated that ADAL1 specifically acts at the 6-position of purine and 2-aminopurine nucleoside monophosphates. Our results may help designing of new therapeutic nucleoside/nucleotide prodrugs with desired metabolic profiles. Furthermore, amino acid sequence analysis in conjunction with crystallographic data and metal analysis suggested that ADAL1 contains a catalytic zinc ion. Finally, a potential physiological role of ADAL1 is discussed.

摘要

人 N(6)-甲基-AMP/dAMP 氨基水解酶已被证明参与药理学上重要的 N(6)-取代嘌呤核苷和其 5'-单磷酸前药的代谢。该酶在大肠杆菌中被克隆和表达,质谱分析和氨基酸序列分析表明该蛋白是腺苷脱氨酶样蛋白 1 同工型(ADAL1)。广泛的结构-活性关系研究表明,ADAL1 不仅能够催化 N(6)-取代嘌呤或 2-氨基嘌呤核苷单磷酸上不同烷基的去除,还能够催化 O(6)-取代化合物的去除。ADAL1 活性易受磷酸部分修饰的影响,但不易受糖部分变化的影响。总的来说,我们的数据表明 ADAL1 特异性作用于嘌呤和 2-氨基嘌呤核苷单磷酸的 6 位。我们的结果可能有助于设计具有所需代谢特征的新型治疗性核苷/核苷酸前药。此外,氨基酸序列分析结合晶体学数据和金属分析表明,ADAL1 含有催化锌离子。最后,讨论了 ADAL1 的潜在生理作用。

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