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人对氧磷酶 1 是负责水解毛果芸香碱的酶。

Human paraoxonase 1 is the enzyme responsible for pilocarpine hydrolysis.

机构信息

Drug Metabolism and Toxicology, Faculty of Pharmaceutical Sciences, Kanazawa University, Kakuma-machi, Kanazawa 920-1192, Japan.

出版信息

Drug Metab Dispos. 2011 Aug;39(8):1345-52. doi: 10.1124/dmd.111.038141. Epub 2011 Apr 26.

Abstract

Pilocarpine has been widely used in ophthalmic preparations for the treatment of glaucoma and in oral preparations for the treatment of radiation-induced xerostomia and Sjögren syndrome. The major metabolic pathways of pilocarpine in human are hydrolysis and hydroxylation. It was found that CYP2A6 is responsible for the 3-hydroxylation, but the enzymes responsible for the hydrolysis have not been characterized. In this study, we attempted to identify esterases responsible for pilocarpine hydrolysis. Pilocarpine hydrolase activities in human liver microsomes and plasma were stimulated by the addition of CaCl(2), suggesting that the calcium-dependent esterase, paraoxonase (PON), was responsible for pilocarpine hydrolysis. To confirm this hypothesis, the pilocarpine hydrolase activity was measured using the recombinant human PONs (PON1, PON2, and PON3) established in this study, and the result was that only PON1 showed pilocarpine hydrolase activity. The effect of PON1 polymorphism (Q192R) on pilocarpine hydrolase activity was analyzed using recombinant human PON1 192Q and 192R and human plasma from 50 volunteers. The results showed that recombinant PON1 192R revealed significantly higher catalytic efficiency than PON1 192Q. In human plasma, the activity of the R/R genotype (117.0 ± 25.2 pmol · min(-1) · μl(-1), n = 23) was significantly higher than those of the Q/R and Q/Q genotypes (97.3 ± 21.0 pmol · min(-1) · μl(-1), n = 20 and 90.4 ± 26.2 pmol · min(-1) · μl(-1), n = 7, respectively). It is suggested that this polymorphism affects pilocarpine hydrolase activity. In this study, we found that human PON1 is the major enzyme for the catalytic efficiency of pilocarpine hydrolysis.

摘要

毛果芸香碱被广泛应用于眼科制剂治疗青光眼和口服制剂治疗放射性口干症和干燥综合征。毛果芸香碱在人体内的主要代谢途径是水解和羟化。研究发现 CYP2A6 负责 3-羟化,但负责水解的酶尚未被确定。在这项研究中,我们试图确定负责毛果芸香碱水解的酯酶。在人肝微粒体和血浆中,毛果芸香碱水解酶活性可被氯化钙促进,提示钙依赖性酯酶,对氧磷酶(PON),负责毛果芸香碱水解。为了证实这一假说,使用本研究建立的重组人 PONs(PON1、PON2 和 PON3)测量毛果芸香碱水解酶活性,结果仅 PON1 显示毛果芸香碱水解酶活性。使用重组人 PON1 192Q 和 192R 以及来自 50 名志愿者的人血浆分析 PON1 多态性(Q192R)对毛果芸香碱水解酶活性的影响。结果表明,重组 PON1 192R 显示出明显更高的催化效率比 PON1 192Q。在人血浆中,R/R 基因型(117.0 ± 25.2 pmol·min(-1)·μl(-1),n = 23)的活性明显高于 Q/R 和 Q/Q 基因型(97.3 ± 21.0 pmol·min(-1)·μl(-1),n = 20 和 90.4 ± 26.2 pmol·min(-1)·μl(-1),n = 7,分别)。这表明这种多态性影响毛果芸香碱水解酶活性。在这项研究中,我们发现人 PON1 是毛果芸香碱水解催化效率的主要酶。

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