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尼古丁的遗传决定代谢及其临床意义。

Genetically determined metabolism of nicotine and its clinical significance.

作者信息

Delijewski Marcin, Bartoń Aleksandra, Delijewska Paulina, Balwierz Radosław, Jakubiak Grzegorz, Kośmider Leon, Pawlas Natalia

机构信息

Department of Pharmacology, School of Medicine with the Division of Dentistry in Zabrze, Medical University of Silesia, Katowice, Poland.

Department of Nuclear Medicine and Endocrine Oncology, Maria Sklodowska-Curie Memorial Cancer Center and Institute of Oncology, Gliwice Branch, Gliwice, Poland.

出版信息

Acta Biochim Pol. 2019 Oct 4;66(4):375-381. doi: 10.18388/abp.2019_2645.

Abstract

Enzymes of the cytochrome P-450 (CYP 450) which belong to the family of oxidase enzymes, are present in cells of all organisms and play a major role in the first phase of xenobiotic metabolism. There are several isoenzymes of CYP 450 that show differences in the speed of metabolism: poor-, extensive- and ultra-rapid. Nicotine undergoes biotransformation in the liver mainly by the CYP2A6 isoform of CYP 450. There are many polymorphic isoforms of CYP2A6 affecting the metabolism of nicotine. There are also several CYP2A6 activity inhibitors and inducers among commonly used drugs. The ability of CYP2A6 isozymes to activate certain procancerogenic substances present in cigarette smoke makes their polymorphism more significant. Moreover, some isoforms may have also influence on the risk of lung cancer development by affecting the enzymatic activation of tobacco-specific nitrosamines. Metabolism of nicotine, mainly through CYP2A6, has also many clinical implications, such as efficacy and safety of the nicotine replacement therapy (NRT) or occurrence of several diseases. In summary, type of the nicotine metabolism may be a potential predictor of the clinical outcomes in patients with cardiovascular disease, addicted to nicotine and in those using NRT. The purpose of this work is to summarize current knowledge on variation in genetically determined metabolism of nicotine and its clinical significance.

摘要

细胞色素P-450(CYP 450)酶属于氧化酶家族,存在于所有生物体的细胞中,在异源生物代谢的第一阶段发挥主要作用。CYP 450有几种同工酶,它们在代谢速度上存在差异:代谢缓慢型、代谢广泛型和超快速型。尼古丁在肝脏中主要通过CYP 450的CYP2A6同工型进行生物转化。CYP2A6有许多影响尼古丁代谢的多态性同工型。常用药物中也有几种CYP2A6活性抑制剂和诱导剂。CYP2A6同工酶激活香烟烟雾中某些致癌物质的能力使其多态性更为显著。此外,一些同工型可能还会通过影响烟草特异性亚硝胺的酶促激活作用,对肺癌发生风险产生影响。尼古丁的代谢主要通过CYP2A6进行,这也具有许多临床意义,如尼古丁替代疗法(NRT)的疗效和安全性或多种疾病的发生。总之,尼古丁代谢类型可能是心血管疾病患者、尼古丁成瘾者以及使用NRT者临床结局的一个潜在预测指标。这项工作的目的是总结目前关于尼古丁遗传决定代谢的变异及其临床意义的知识。

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