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对羟基苯甲酸酯(尼泊金酯)在人肠道(Caco-2)细胞中的酯交换反应

Transesterification of p-hydroxybenzoate esters (parabens) by human intestinal (Caco-2) cells.

作者信息

Lakeram M, Paine A J, Lockley D J, Sanders D J, Pendlington R, Forbes B

机构信息

Pharmaceutical Science Research Division, King's College London, London, UK.

出版信息

Xenobiotica. 2006 Sep;36(9):739-49. doi: 10.1080/00498250600738637.

Abstract

p-Hydroxybenzoate ester (paraben) preservatives are used in numerous orally administered products. The recognized route of metabolism for parabens is hydrolysis to p-hydroxybenzoic acid followed by conjugation and excretion. However, in the presence of alcohols, a presystemic transesterification pathway not previously reported for the human intestine can occur. Using human intestinal (Caco-2) cells, it was observed that hydrolysis of parabens to p-hydroxybenzoic acid is reduced markedly by ethanol concentrations that can occur in the human intestine, 0.25-0.5% (v/v). Ethanol concentrations of 1.0-2.5% (v/v) were optimal for transesterification to ethylparaben in Caco-2 cell homogenates. The kinetics of the transesterification reaction with regard to ethanol concentration (0-20%), time, pH (3-9), protein concentration (1-5 mg ml-1) and substrate concentration (6.25-200 microM) as well as the effects of different alcohols were studied. The Km and Vmax values for transesterification with ethanol for methyl, propyl, butyl, heptyl and octyl parabens were 449.7, 165.7, 86.1, 24.2 and 45.9 microM and 114.4, 37.5, 19.5, 7.5 and 7.6 micromol h-1 mg-1 Caco-2 cell protein, respectively. The Vmax values for transesterification of methylparaben with ethanol, propan-1-ol, butan-1-ol were 114.4, 5.1 and 4.9 micromol h-1 mg-1, respectively. Collectively, the kinetic data demonstrate that the enzyme responsible for the transesterification reaction has a preference for short-chain esters and represents the first report of transesterification in human intestinal cells. An implication of this mechanism is that alcohol-containing in vitro biosystems or protocols for the study of parabens disposition could generate transesterified artefacts. The clinical or toxicological implication is that, following co-ingestion of ester compounds with ethanol, transesterification could provide the basis for a previously unrecognized drug-alcohol interaction.

摘要

对羟基苯甲酸酯(尼泊金酯)防腐剂被用于众多口服产品中。尼泊金酯公认的代谢途径是水解为对羟基苯甲酸,随后进行结合反应并排出体外。然而,在有醇类存在的情况下,会出现一种此前未报道过的人体肠道内的首过性酯交换途径。利用人肠道(Caco-2)细胞观察到,人体肠道中可能出现的乙醇浓度(0.25 - 0.5%,v/v)会显著降低尼泊金酯水解为对羟基苯甲酸的过程。在Caco-2细胞匀浆中,乙醇浓度为1.0 - 2.5%(v/v)时最有利于酯交换生成对羟基苯甲酸乙酯。研究了酯交换反应关于乙醇浓度(0 - 20%)、时间、pH(3 - 9)、蛋白质浓度(1 - 5 mg/ml)和底物浓度(6.25 - 200 μM)的动力学,以及不同醇类的影响。用乙醇进行酯交换反应时,对羟基苯甲酸甲酯、丙酯、丁酯、庚酯和辛酯的Km和Vmax值分别为449.7、165.7、86.1、24.2和45.9 μM以及114.4、37.5、19.5、7.5和7.6 μmol h-1 mg-1 Caco-2细胞蛋白。对羟基苯甲酸甲酯与乙醇、丙醇-1、丁醇-1进行酯交换反应的Vmax值分别为114.4、5.1和4.9 μmol h-1 mg-1。总体而言,动力学数据表明负责酯交换反应的酶对短链酯有偏好,这是人体肠道细胞中酯交换反应的首次报道。这一机制的一个影响是,含醇的体外生物系统或用于研究尼泊金酯处置的方案可能会产生酯交换假象。临床或毒理学方面的影响是,酯类化合物与乙醇共同摄入后,酯交换可能为一种此前未被认识的药物-酒精相互作用提供基础。

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