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药物遗传学与人类遗传多态性。

Pharmacogenetics and human genetic polymorphisms.

机构信息

Institute of Cellular Medicine, Newcastle University Medical School, UK.

出版信息

Biochem J. 2010 Aug 1;429(3):435-49. doi: 10.1042/BJ20100522.

DOI:10.1042/BJ20100522
PMID:20626352
Abstract

The term pharmacogenetics was first used in the late 1950s and can be defined as the study of genetic factors affecting drug response. Prior to formal use of this term, there was already clinical data available in relation to variable patient responses to the drugs isoniazid, primaquine and succinylcholine. The subject area developed rapidly, particularly with regard to genetic factors affecting drug disposition. There is now comprehensive understanding of the molecular basis for variable drug metabolism by the cytochromes P450 and also for variable glucuronidation, acetylation and methylation of certain drugs. Some of this knowledge has already been translated to the clinic. The molecular basis of variation in drug targets, such as receptors and enzymes, is generally less well understood, although there is consistent evidence that polymorphisms in the genes encoding the beta-adrenergic receptors and the enzyme vitamin K epoxide reductase is of clinical importance. The genetic basis of rare idiosyncratic adverse drug reactions had also been examined. Susceptibility to reactions affecting skin and liver appears to be determined in part by the HLA (human leucocyte antigen) genotype, whereas reactions affecting the heart and muscle may be determined by polymorphisms in genes encoding ion channels and transporters respectively. Genome-wide association studies are increasingly being used to study drug response and susceptibility to adverse drug reactions, resulting in identification of some novel pharmacogenetic associations.

摘要

“药物遗传学”一词最早于 20 世纪 50 年代末使用,可以定义为研究影响药物反应的遗传因素。在正式使用这个术语之前,已经有临床数据表明患者对异烟肼、伯氨喹和琥珀酰胆碱等药物的反应存在差异。该主题领域发展迅速,特别是在影响药物处置的遗传因素方面。现在,人们对细胞色素 P450 影响药物代谢的分子基础以及某些药物的可变葡糖苷酸化、乙酰化和甲基化有了全面的了解。其中一些知识已经应用于临床。药物靶点(如受体和酶)变异的分子基础一般理解得较少,但有一致的证据表明,β-肾上腺素能受体和维生素 K 环氧化物还原酶编码基因的多态性具有临床重要性。罕见的特发性药物不良反应的遗传基础也已经过研究。皮肤和肝脏反应的易感性部分由 HLA(人类白细胞抗原)基因型决定,而影响心脏和肌肉的反应可能分别由编码离子通道和转运体的基因的多态性决定。全基因组关联研究越来越多地用于研究药物反应和对不良反应的易感性,从而确定了一些新的药物遗传学相关性。

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