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本文引用的文献

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Commentary: Perspectives on alcohol-related gene and environment interplay in diverse populations.评论:不同人群中酒精相关基因与环境相互作用的观点
Am J Addict. 2017 Aug;26(5):526-531. doi: 10.1111/ajad.12584.
2
Conclusion: Special issue on genetic and alcohol use disorder research with diverse racial/ethnic groups: Key findings and potential next steps.结论:关于不同种族/族裔群体的基因与酒精使用障碍研究的特刊:主要发现及潜在的后续步骤。
Am J Addict. 2017 Aug;26(5):532-537. doi: 10.1111/ajad.12585.
3
Introduction: Special issue on genetic research of alcohol use disorder in diverse racial/ethnic populations.引言:关于不同种族/族裔人群酒精使用障碍基因研究的特刊。
Am J Addict. 2017 Aug;26(5):422-423. doi: 10.1111/ajad.12576. Epub 2017 Jul 3.
4
From sexless to sexy: Why it is time for human genetics to consider and report analyses of sex.从无性到性感:为何人类遗传学是时候考虑并报告性别分析了。
Biol Sex Differ. 2017 May 3;8:15. doi: 10.1186/s13293-017-0136-8. eCollection 2017.
5
ADH1B: From alcoholism, natural selection, and cancer to the human phenome.乙醇脱氢酶1B:从酗酒、自然选择、癌症到人类表型组
Am J Med Genet B Neuropsychiatr Genet. 2018 Mar;177(2):113-125. doi: 10.1002/ajmg.b.32523. Epub 2017 Mar 27.
6
Population diversity of the genetically determined TTR expression in human tissues and its implications in TTR amyloidosis.人类组织中由基因决定的转甲状腺素蛋白(TTR)表达的群体多样性及其在TTR淀粉样变性中的意义。
BMC Genomics. 2017 Mar 23;18(1):254. doi: 10.1186/s12864-017-3646-1.
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A genome-wide gene-by-trauma interaction study of alcohol misuse in two independent cohorts identifies PRKG1 as a risk locus.在两个独立队列中进行的一项全基因组基因-创伤相互作用研究表明,PRKG1 是酒精滥用的风险基因座。
Mol Psychiatry. 2018 Jan;23(1):154-160. doi: 10.1038/mp.2017.24. Epub 2017 Mar 7.
8
Genome-wide association study of therapeutic opioid dosing identifies a novel locus upstream of OPRM1.治疗性阿片类药物剂量的全基因组关联研究确定了OPRM1上游的一个新位点。
Mol Psychiatry. 2017 Mar;22(3):346-352. doi: 10.1038/mp.2016.257. Epub 2017 Jan 24.
9
Strategies for Enriching Variant Coverage in Candidate Disease Loci on a Multiethnic Genotyping Array.在多民族基因分型阵列上富集候选疾病位点变异覆盖度的策略
PLoS One. 2016 Dec 14;11(12):e0167758. doi: 10.1371/journal.pone.0167758. eCollection 2016.
10
Genetic factor common to schizophrenia and HIV infection is associated with risky sexual behavior: antagonistic vs. synergistic pleiotropic SNPs enriched for distinctly different biological functions.精神分裂症和HIV感染共有的遗传因素与危险性行为有关:拮抗与协同多效性单核苷酸多态性富集了截然不同的生物学功能。
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在一项关于危险性行为的全基因组基因与酒精依赖相互作用研究中确定的特定祖先和特定性别的风险等位基因。

Ancestry-specific and sex-specific risk alleles identified in a genome-wide gene-by-alcohol dependence interaction study of risky sexual behaviors.

作者信息

Polimanti Renato, Zhao Hongyu, Farrer Lindsay A, Kranzler Henry R, Gelernter Joel

机构信息

Department of Psychiatry, Yale University School of Medicine, West Haven, Connecticut.

VA CT Healthcare Center, West Haven, Connecticut.

出版信息

Am J Med Genet B Neuropsychiatr Genet. 2017 Dec;174(8):846-853. doi: 10.1002/ajmg.b.32604. Epub 2017 Oct 9.

DOI:10.1002/ajmg.b.32604
PMID:28990359
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5861711/
Abstract

We previously mapped loci for the genome-wide association studies (GWAS) and genome-wide gene-by-alcohol dependence interaction (GW-GxAD) analyses of risky sexual behaviors (RSB). This study extends those findings by analyzing the ancestry- and sex-specific AD-stratified effects on RSB. We examined the concordance of findings for the AD-stratified GWAS and the GW-GxAD analysis of RSB, with concordance defined as genome-wide significance in one analysis and at least nominal significance in the second analysis. A total of 2,173 African-American (AA) and 1,751 European-American (EA) subjects were investigated. Information regarding RSB (lifetime experiences of unprotected sex and multiple sexual partners) and DSM-IV diagnosis of lifetime AD were derived from the Semi-Structured Assessment for Drug Dependence and Alcoholism (SSADDA). In our ancestry- and sex-specific analyses, we identified four independent genome-wide significant (GWS) loci (p < 510 ) and one suggestive locus (p < 610 ). In men, we observed a GWS signal in FAM162A (rs2002594, p = 4.9610 ). In women, there was a suggestive locus in PLGRKT (rs3824435, p = 5.5210 ). In AAs, there was a GWS signal in GRK5 (rs1316543, p = 1.2510 ). In AA men, we observed an intergenic GWS signal (rs12898370, p = 4.4910 ) near LINGO1. In EA men, there was a GWS signal in CCSER1 (rs62313897; p = 7.93*10 ). The loci identified in this GWAS implicate molecular mechanisms related to psychiatric illness and personality features, suggesting that the interplay between AD and RSB is mediated by alleles associated with behavioral traits.

摘要

我们之前对危险性行为(RSB)进行了全基因组关联研究(GWAS)以及全基因组酒精依赖基因相互作用(GW-GxAD)分析,并绘制了相关基因座图谱。本研究通过分析基于祖先和性别的酒精依赖分层效应,对RSB的影响,扩展了这些研究结果。我们检验了酒精依赖分层GWAS与RSB的GW-GxAD分析结果的一致性,一致性定义为在一次分析中达到全基因组显著性,在第二次分析中至少达到名义显著性。总共对2173名非裔美国人(AA)和1751名欧裔美国人(EA)受试者进行了调查。关于RSB(无保护性行为和多个性伴侣的终生经历)以及终生酒精依赖的DSM-IV诊断信息,来自药物依赖和酒精中毒半结构化评估(SSADDA)。在我们基于祖先和性别的分析中,我们确定了四个独立的全基因组显著(GWS)基因座(p < 5×10 )和一个提示性基因座(p < 6×10 )。在男性中,我们在FAM162A中观察到一个GWS信号(rs2002594,p = 4.96×10 )。在女性中,PLGRKT中有一个提示性基因座(rs3824435,p = 5.52×10 )。在非裔美国人中,GRK5中有一个GWS信号(rs1316543,p = 1.25×10 )。在非裔美国男性中,我们在LINGO1附近观察到一个基因间GWS信号(rs12898370,p = 4.49×10 )。在欧裔美国男性中,CCSER1中有一个GWS信号(rs62313897;p = 7.93×10 )。在这项GWAS中确定的基因座涉及与精神疾病和人格特征相关的分子机制,表明酒精依赖和RSB之间的相互作用是由与行为特征相关的等位基因介导的。