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药物基因组学新兴技术:快速 SNP 检测、分子动力学模拟和 QSAR 分析方法,验证人类 ABC 转运蛋白 ABCB1(P-糖蛋白/MDR1)的临床重要遗传变异。

Emerging new technologies in Pharmacogenomics: rapid SNP detection, molecular dynamic simulation, and QSAR analysis methods to validate clinically important genetic variants of human ABC Transporter ABCB1 (P-gp/MDR1).

机构信息

Graduate School of Bioscience and Biotechnology, Tokyo Institute of Technology, Yokohama, 225-8501, Japan.

出版信息

Pharmacol Ther. 2010 Apr;126(1):69-81. doi: 10.1016/j.pharmthera.2010.01.005. Epub 2010 Feb 4.

DOI:10.1016/j.pharmthera.2010.01.005
PMID:20138191
Abstract

Pharmacogenomics, the study of the influence of genetic factors on drug action, is increasingly important for predicting pharmacokinetics profiles and/or adverse reactions to drugs. Drug transporters as well as drug-metabolism play pivotal roles in determining the pharmacokinetic profiles of drugs and, by extension, their overall pharmacological effects. There are an increasing number of reports addressing genetic polymorphisms of drug transporters. A key requirement for the development of individualized medicine or personalized therapy is the ability to rapidly and conveniently test patients for genetic polymorphisms and/or mutations. We have recently developed a rapid and cost-effective method for single nucleotide polymorphism (SNP) detection, named Smart Amplification Process 2 (SmartAmp2), which enables us to detect genetic polymorphisms or mutations in 30 to 45min under isothermal conditions without DNA isolation and PCR amplification. Furthermore, high-speed functional screening, quantitative structure-activity relationship (QSAR) analysis, and molecular dynamic (MD) simulation methods have been developed to study the substrate specificity of ABC transporters and to evaluate the effect of genetic polymorphisms on their function and substrate specificity. These methods would provide powerful and practical tools for screening synthetic and natural compounds, and the deduced data can be applied to the molecular design of new drugs. This review addresses such new methods for validating genetic polymorphisms of human ABC transporter ABCB1 (P-gp/MDR1) which is critically involved in the pharmacokinetics of drugs.

摘要

药物基因组学是研究遗传因素对药物作用的影响,对于预测药物代谢动力学特征和/或药物不良反应越来越重要。药物转运体以及药物代谢在决定药物代谢动力学特征及其整体药理作用方面起着关键作用。越来越多的报告涉及药物转运体的遗传多态性。开发个体化医学或个性化治疗的关键要求是能够快速方便地对患者进行遗传多态性和/或突变检测。我们最近开发了一种快速且具有成本效益的单核苷酸多态性(SNP)检测方法,称为 Smart Amplification Process 2(SmartAmp2),该方法使我们能够在无需 DNA 分离和 PCR 扩增的情况下,在 30 至 45 分钟内实现等温条件下的遗传多态性或突变检测。此外,还开发了高速功能筛选、定量构效关系(QSAR)分析和分子动力学(MD)模拟方法,以研究 ABC 转运体的底物特异性,并评估遗传多态性对其功能和底物特异性的影响。这些方法将为筛选合成和天然化合物提供强大而实用的工具,并且推断出的数据可应用于新药的分子设计。本文综述了这些新方法在验证人类 ABC 转运体 ABCB1(P-糖蛋白/MDR1)的遗传多态性方面的应用,该多态性对药物的药代动力学至关重要。

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