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Pharmacogenetic landscape of Metabolic Syndrome components drug response in Tunisia and comparison with worldwide populations

机译:突尼斯代谢综合症成分药物反应的药理学概况及与全球人群的比较

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摘要

Genetic variation is an important determinant affecting either drug response or susceptibility to adverse drug reactions. Several studies have highlighted the importance of ethnicity in influencing drug response variability that should be considered during drug development. Our objective is to characterize the genetic variability of some pharmacogenes involved in the response to drugs used for the treatment of Metabolic Syndrome (MetS) in Tunisia and to compare our results to the worldwide populations. A set of 135 Tunisians was genotyped using the Affymetrix Chip 6.0 genotyping array. Variants located in 24 Very Important Pharmacogenes (VIP) involved in MetS drug response were extracted from the genotyping data. Analysis of variant distribution in Tunisian population compared to 20 worldwide populations publicly available was performed using R software packages. Common variants between Tunisians and the 20 investigated populations were extracted from genotyping data. Multidimensional screening showed that Tunisian population is clustered with North African and European populations. The greatest divergence was observed with the African and Asian population. In addition, we performed Inter-ethnic comparison based on the genotype frequencies of five VIP biomarkers. The genotype frequencies of the biomarkers rs3846662, rs1045642, rs7294 and rs12255372 located respectively in HMGCR, ABCB1, VKORC1 and TCF7L2 are similar between Tunisian, Tuscan (TSI) and European (CEU). The genotype frequency of the variant rs776746 located in CYP3A5 gene is similar between Tunisian and African populations and different from CEU and TSI. The present study shows that the genetic make up of the Tunisian population is relatively complex in regard to pharmacogenes and reflects previous historical events. It is important to consider this ethnic difference in drug prescription in order to optimize drug response to avoid serious adverse drug reactions. Taking into account similarities with other neighboring populations, our study has an impact not only on the Tunisian population but also on North African population which are underrepresented in pharmacogenomic studies.
机译:遗传变异是影响药物反应或药物不良反应易感性的重要决定因素。几项研究强调了种族在影响药物开发过程中应考虑的药物反应差异方面的重要性。我们的目标是表征与突尼斯代谢综合征(MetS)所用药物反应相关的某些药理基因的遗传变异性,并将我们的结果与全球人群进行比较。使用Affymetrix Chip 6.0基因分型阵列对135名突尼斯人进行基因分型。从基因分型数据中提取了参与MetS药物反应的24种非常重要的药物原(VIP)中的变体。使用R软件包对突尼斯人口与全球20个公众可获得的变异进行了分析。突尼斯人和20个调查人群之间的常见变异是从基因分型数据中提取的。多维筛选显示,突尼斯人口与北非和欧洲人口聚集在一起。非洲和亚洲人口之间的差异最大。此外,我们基于5个VIP生物标记物的基因型频率进行了种族间比较。分别位于HMGCR,ABCB1,VKORC1和TCF7L2中的生物标记rs3846662,rs1045642,rs7294和rs12255372的基因型频率在突尼斯,托斯卡纳(TSI)和欧洲(CEU)之间相似。 CYP3A5基因中的rs776746变体的基因型频率在突尼斯和非洲人群之间相似,并且与CEU和TSI不同。本研究表明,就药物基因而言,突尼斯人口的遗传构成相对复杂,并反映了以前的历史事件。重要的是要考虑药物处方中的种族差异,以便优化药物反应以避免严重的药物不良反应。考虑到与其他邻近人群的相似性,我们的研究不仅对突尼斯人口有影响,而且对药物基因组学研究中代表性不足的北非人口也有影响。

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