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首页> 外文期刊>Pharmacogenetics and genomics >Pharmacogenomics in Papua New Guineans: unique profiles and implications for enhancing drug efficacy while improving drug safety
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Pharmacogenomics in Papua New Guineans: unique profiles and implications for enhancing drug efficacy while improving drug safety

机译:巴布亚新几内亚的药物替代科学:独特的概况和用于提高药物疗效的含义,同时提高药物安全性

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摘要

Papua New Guinea (PNG) can be roughly divided into highland, coastal and island peoples with significant mitochondrial DNA differentiation reflecting early and recent distinct migrations from Africa and East Asia, respectively. Infectious diseases such as tuberculosis, malaria and HIV severely impact on the health of its peoples for which drug therapy is the major treatment and pharmacogenetics has clinical relevance for many of these drugs. Although there is generally little information about known single nucleotide polymorphisms in the population, in some instances, their frequencies have been shown to be higher than anywhere worldwide. For example, CYP2B6*6 is over 50%, and CYP2C19*2 and *3 are over 40 and 25%, respectively. Conversely, CYP2A6*9, 2B6*2, *3, *4 and *18, and 2C8*3 appear to be much lower than in Whites. CYP2D6 known variants are unclear, and for phase II enzymes, only UGT2B7 and UGT1A9 data are available, with variant frequencies either slightly lower than or similar to Whites. Although almost all PNG people tested are rapid acetylators, but which variant(s) define this phenotype is not known. For HLA-B*13:01, HLA-B*35:05 and HLA-C*04:01, the frequencies show some regioselectivity, but the clinical implications with respect to adverse drug reactions are not known. There are minimal phenotype data for the CYPs and nothing is known about drug transporter or receptor genetics. Determination of genetic variants that are rare in Whites or Asians but common in PNG people is a topic of both scientific and clinical importance, and further research needs to be carried out. Optimizing the safety and efficacy of infectious disease drug therapy through pharmacogenetic studies that have translation potential is a priority.
机译:巴布亚新几内亚(PNG)可以大致分为高地,沿海和岛民族,分别具有显着的线粒体DNA差异化,反映了非洲和东亚最近的截图。结核病,疟疾和艾滋病毒的传染病严重影响其各国人民的健康,其中药物治疗是主要的治疗和药物遗传学,对许多这些药物具有临床相关性。尽管在某些情况下,群体中已知的单核苷酸多态性的知名信息通常很少,但它们的频率已被证明高于全球的任何地方。例如,CYP2B6 * 6超过50%,CYP2C19 * 2和* 3分别超过40%和25%。相反,CYP2A6 * 9,2B6 * 2,* 3,* 4和* 18和2C8 * 3似乎远低于白人。 CYP2D6已知的变体尚不清楚,对于II次酶,只有UGT2B7和UGT1A9数据可用,变体频率略低于或类似于WHITES。尽管几乎所有测试的PNG人都是快速乙酰剂,但是哪种变体定义这种表型是不知道的。对于HLA-B * 13:01,HLA-B * 35:05和HLA-C * 04:01,频率显示出一些区域选择性,但是对不良药物反应的临床意义是未知的。 CYPS存在最小的表型数据,没有任何关于药物转运蛋白或受体遗传学的表型数据。测定白人或亚洲人罕见的遗传变异,但在PNG人中常见是科学和临床重要性的主题,需要进行进一步的研究。通过具有翻译潜力的药物发生研究优化传染病药物治疗的安全性和功效是优先级。

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