Mapping of hepatic expression quantitative trait loci (eQTLs) in a Han Chinese population

汉族人群肝脏表达数量性状位点(eQTL)定位

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作者:Xiaoliang Wang ,Huamei Tang, Mujian Teng, Zhiqiang Li, Jianguo Li, Junwei Fan, Lin Zhong, Xing Sun, Junming Xu, Guoqing Chen, Dawei Chen, Zhaowen Wang, Tonghai Xing, Jinyan Zhang, Li Huang, Shuyun Wang, Xiao Peng, Shengying Qin, Yongyong Shi, Zhihai Peng

Abstract

Background: Elucidating the genetic basis underlying hepatic gene expression variability is of importance to understand the aetiology of the disease and variation in drug metabolism. To date, no genome-wide expression quantitative trait loci (eQTLs) analysis has been conducted in the Han Chinese population, the largest ethnic group in the world. Methods: We performed a genome-wide eQTL mapping in a set of Han Chinese liver tissue samples (n=64). The data were then compared with published eQTL data from a Caucasian population. We then performed correlations between these eQTLs with important pharmacogenes, and genome-wide association study (GWAS) identified single nucleotide polymorphisms (SNPs), in particular those identified in the Asian population. Results: Our analyses identified 1669 significant eQTLs (false discovery rate (FDR) < 0.05). We found that 41% of Asian eQTLs were also eQTLs in Caucasians at the genome-wide significance level (p=10⁻&sup8;). Both cis- and trans-eQTLs in the Asian population were also more likely to be eQTLs in Caucasians (p<10⁻&sup4;). Enrichment analyses revealed that trait-associated GWAS-SNPs were enriched within the eQTLs identified in our data, so were the GWAS-SNPs specifically identified in Asian populations in a separate analysis (p<0.001 for both). We also found that hepatic expression of very important pharmacogenetic (VIP) genes (n=44) and a manually curated list of major genes involved in pharmacokinetics (n=341) were both more likely to be controlled by eQTLs (p<0.002 for both). Conclusions: Our study provided, for the first time, a comprehensive hepatic eQTL analysis in a non-European population, further generating valuable data for characterising the genetic basis of human diseases and pharmacogenetic traits. Keywords: Clinical genetics; Genetics; Genome-wide; Molecular genetics.

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