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元分析证实,5-羟色胺转运体基因中的一个功能性多态性(5-HTTLPR)使欧洲人群易患双相情感障碍。

Meta-analysis confirms a functional polymorphism (5-HTTLPR) in the serotonin transporter gene conferring risk of bipolar disorder in European populations.

机构信息

Department of Psychiatry, The First Affiliated Hospital of Kunming Medical University, Kunming, China.

出版信息

Neurosci Lett. 2013 Aug 9;549:191-6. doi: 10.1016/j.neulet.2013.05.065. Epub 2013 Jun 10.

DOI:10.1016/j.neulet.2013.05.065
PMID:23756178
Abstract

The serotonin transporter (5-HTT) is a candidate risk gene for bipolar disorder, and a functional polymorphism of 44-bp insertion/deletion (5-HTTLPR) located in the promoter region of this gene has been investigated for the association with the illness extensively among worldwide populations, but overall results were inconsistent and its role in the disorder remains unclear. The present study attempts to find its potential association with bipolar disorder using meta-analyzes that maximize the statistical power. We applied meta-analysis techniques by combining all available case-control studies of 5-HTTLPR and bipolar disorder in samples of European ancestry (with a total of 3778 cases and 4997 controls), and we assessed the evidence for allelic associations, heterogeneity among different studies, influence of each single study, and potential publication bias. The short allele (S allele) of 5-HTTLPR showed a significant association with bipolar disorder in our meta-analysis (odds ratio=1.10, p-value=0.005), suggesting it is likely a risk polymorphism for the illness, and the observed OR is consistent with other susceptibility loci identified through recent large-scale genetic association studies on bipolar disorder, which could be regarded simply as a small but detectable effects.

摘要

5-羟色胺转运体(5-HTT)是双相情感障碍的候选风险基因,该基因启动子区域的 44bp 插入/缺失(5-HTTLPR)功能多态性已在世界范围内广泛研究与该疾病的相关性,但总体结果不一致,其在该疾病中的作用仍不清楚。本研究试图通过最大限度地提高统计效力的荟萃分析来发现其与双相情感障碍的潜在关联。我们应用荟萃分析技术,结合了欧洲血统样本中所有可用的 5-HTTLPR 和双相情感障碍的病例对照研究(共有 3778 例病例和 4997 例对照),并评估了等位基因关联、不同研究之间的异质性、单个研究的影响以及潜在的发表偏倚的证据。5-HTTLPR 的短等位基因(S 等位基因)在我们的荟萃分析中与双相情感障碍显著相关(优势比=1.10,p 值=0.005),表明它可能是该疾病的风险多态性,观察到的 OR 与最近通过大规模遗传关联研究确定的其他易感性基因座一致,这可能被视为一个小但可检测的影响。

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