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P2X7 A1513C(rs3751143)基因多态性与结核病风险的关联:一项荟萃分析的证据

Association of P2X7 A1513C (rs3751143) gene polymorphism with risk of tuberculosis: evidence from a meta-analysis.

作者信息

Areeshi Mohammad Y, Mandal Raju K, Panda Aditya K, Haque Shafiul

机构信息

College of Nursing and Allied Health Sciences, Jazan University, Jazan, Kingdom of Saudi Arabia.

出版信息

Genet Test Mol Biomarkers. 2013 Sep;17(9):662-8. doi: 10.1089/gtmb.2013.0202. Epub 2013 Aug 15.

DOI:10.1089/gtmb.2013.0202
PMID:23947898
Abstract

AIM

Many case-control studies have been performed in the past to elucidate the association between the P2X7 receptor 1513 A>C (rs3751143) polymorphism and tuberculosis (TB) risk. However, their data interpretation was difficult due to scattered and inconsistent results that led to limited power. In this study, a quantitative summary assessment has been done through meta-analysis to appraise the association between the 1513 A>C polymorphism and TB susceptibility.

METHODOLOGY

Systematic assessment was performed for the published studies related with the association between the P2X7 1513 A>C polymorphism and TB risk retrieved from PubMed (Medline), EMBASE search. A meta-analysis was done using a statistical program to evaluate the said association. Pooled odds ratios (ORs) and 95% confidence intervals (95% CIs) were calculated for allele contrast, homozygous, heterozygous, dominant, and recessive genetic models.

RESULTS

A total of 2710 controls and 2521 TB cases were included in this meta-analysis. Meta-analysis results showed that C allele carrier status was significantly associated with increased TB risk (C vs. A: p=0.001; OR=1.382, 95% CI=1.248-1.531). Significant risk of TB was associated with the homozygous mutant CC (CC vs. AA: p=0.001; OR=1.676, 95% CI=1.251-2.247) and heterozygous AC (AC vs. AA: p=0.001; OR=1.429, 95% CI=1.260-1.621) comparisons. Similarly, dominant (CC vs. AA+AC: p=0.008; OR=1.481, 95% CI=1.109-1.978) and recessive (CC+AC vs. AA: p=0.001; OR=1.458, 95% CI=1.292-1.645) genetic models also revealed increased risk of developing TB.

CONCLUSION

We found that the P2X7 1513 A>C gene polymorphism is significantly associated with increased susceptibility to TB. Also, future well-designed epidemiological studies with stratified case-control and biological characterization may be beneficial to validate these findings.

摘要

目的

过去已开展了许多病例对照研究,以阐明P2X7受体1513 A>C(rs3751143)多态性与结核病(TB)风险之间的关联。然而,由于结果分散且不一致,导致检验效能有限,难以对这些数据进行解读。在本研究中,通过荟萃分析进行了定量汇总评估,以评价1513 A>C多态性与TB易感性之间的关联。

方法

对从PubMed(医学索引数据库)、EMBASE检索到的与P2X7 1513 A>C多态性和TB风险关联的已发表研究进行系统评估。使用统计程序进行荟萃分析,以评估上述关联。计算等位基因对比、纯合子、杂合子、显性和隐性遗传模型的合并比值比(OR)和95%置信区间(95%CI)。

结果

本荟萃分析共纳入2710例对照和2521例TB病例。荟萃分析结果显示,C等位基因携带者状态与TB风险增加显著相关(C与A相比:p=0.001;OR=1.382,95%CI=1.248-1.531)。TB的显著风险与纯合突变体CC(CC与AA相比:p=0.001;OR=1.676,95%CI=1.251-2.247)和杂合子AC(AC与AA相比:p=0.001;OR=1.429,95%CI=1.260-1.621)比较相关。同样,显性(CC与AA+AC相比:p=0.008;OR=1.481,95%CI=1.109-1.978)和隐性(CC+AC与AA相比:p=0.001;OR=1.458,95%CI=1.292-1.645)遗传模型也显示患TB的风险增加。

结论

我们发现P2X7 1513 A>C基因多态性与TB易感性增加显著相关。此外,未来设计良好的分层病例对照和生物学特征的流行病学研究可能有助于验证这些发现。

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