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藏族人群胆固醇代谢途径多态性位点与胆结石的关联研究

Association Study Between Polymorphic Loci in Cholesterol Metabolism Pathway and Gallstone in the Tibetan Population.

作者信息

Ma Lifeng, Chen Hui, Zhang Zhiying, Liu Lijun, Zhao Yiduo, Li Yansong, Zhao Zhipeng, Chen Haitao, Kang Longli

机构信息

Key Laboratory for Molecular Genetic Mechanisms and Intervention Research on High Altitude Disease of Tibet Autonomous Region, Xianyang, China.

Key Laboratory of High Altitude Environment and Genes Related to Diseases of Tibet Autonomous Region, School of Medicine, Xizang Minzu University, Xianyang, China.

出版信息

Front Genet. 2022 May 16;13:902553. doi: 10.3389/fgene.2022.902553. eCollection 2022.

Abstract

The incidence of gallstones in the Tibetan population is increasing rapidly. Previous studies indicated that genetic variation located in the cholesterol metabolism pathway may be associated with the incidence of gallstones. By recruiting 132 Tibetan gallstone patients and 52 normal Tibetan controls, we performed next-generation sequencing for 508 genes in the cholesterol metabolism pathway. Additionally, by integrating the sequence data of 41 normal Tibetan subjects in the public database, we finally obtained 93 normal Tibetan controls. Single nucleotide polymorphisms (SNPs) calling were performed by using the GATK pipeline. The quality control criteria for SNPs were: missing rate <0.05; minor allele frequency (MAF) > 0.01; and value >0.001 in the Hardy-Weinberg Equilibrium (HWE) test. To eliminate the influence of population heterogeneity, Principal Component Analysis (PCA) was carried out by using the smartpca software. Association analyses were performed by Plink software. Multiple tests were adjusted by the false discovery rate (FDR) method. A total of 2,401 SNPs were obtained by analyzing 508 genes, and 2,011 SNPs left after quality control. After adjusting the eigen vectors, we found that 10 SNPs (SNV05997, rs80145081, rs80005560, rs79074685, rs748546375, rs201880593, rs142559357, rs750769471, rs869789 and rs4072341) were significantly associated with gallstone. Subsequently, by comparing the case group with our control group and the public database control group separately, we further found that the SNP rs869789 was consistently significantly associated with gallstone ( = 9.04 × 10 in cases vs. our controls and 5.73 × 10 in cases vs. public controls, respectively). By systematically analyzed SNPs in the cholesterol metabolism pathway, we identified one polymorphic locus rs869789 significantly associated with the pathogenesis of gallstone in the Tibetan population. This study will provide clue for further mechanism study of gallstone in the Tibetan population.

摘要

藏族人群胆结石的发病率正在迅速上升。先前的研究表明,胆固醇代谢途径中的基因变异可能与胆结石的发病率有关。通过招募132名藏族胆结石患者和52名正常藏族对照,我们对胆固醇代谢途径中的508个基因进行了二代测序。此外,通过整合公共数据库中41名正常藏族受试者的序列数据,我们最终获得了93名正常藏族对照。使用GATK流程进行单核苷酸多态性(SNP)的检测。SNP的质量控制标准为:缺失率<0.05;次要等位基因频率(MAF)>0.01;在哈迪-温伯格平衡(HWE)检验中的 值>0.001。为了消除人群异质性的影响,使用smartpca软件进行主成分分析(PCA)。使用Plink软件进行关联分析。通过错误发现率(FDR)方法对多重检验进行校正。通过分析508个基因共获得2401个SNP,质量控制后剩下2011个SNP。调整特征向量后,我们发现10个SNP(SNV05997、rs80145081、rs80005560、rs79074685、rs748546375、rs201880593、rs142559357、rs750769471、rs869789和rs4072341)与胆结石显著相关。随后,通过分别将病例组与我们的对照组以及公共数据库对照组进行比较,我们进一步发现SNP rs869789与胆结石始终显著相关(病例组与我们的对照组相比 = 9.04×10,病例组与公共对照组相比 = 5.73×10)。通过系统分析胆固醇代谢途径中的SNP,我们在藏族人群中鉴定出一个与胆结石发病机制显著相关的多态性位点rs869789。本研究将为进一步研究藏族人群胆结石的发病机制提供线索。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9bf5/9149373/7bce1beb9c6a/fgene-13-902553-g001.jpg

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