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Is Alpha-1 Antichymotrypsin Gene Polymorphism a Risk Factor for Primary Intracerebral Hemorrhage? A Case-Control Study and Meta-Analysis

机译:Alpha-1抗胰凝乳蛋白酶基因多态性是原发性脑出血的危险因素吗?病例对照研究和荟萃分析

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摘要

BACKGROUND Alpha-1 antichymotrypsin (ACT) signal peptide A/T polymorphism has been suggested to play a role in various brain diseases with arterial wall pathology. We conducted a case-control study and a meta-analysis to evaluate the association between this polymorphism and risk of primary intracerebral hemorrhage. MATERIAL AND METHODS A total of 188 patients and 200 age- and sex-matched healthy controls were enrolled in our case-control study. The ACT polymorphism was genotyped by PCR-LDR. Further meta-analysis was conducted by searching literature from PUBMED, EMBASE, and Chinese National Knowledge Infrastructure databases until December 2014, then combining data using STATA10.0. RESULTS Similar genotype distribution was detected between PICH patients and healthy controls (p=0.523). Further analysis based on hypertension and location of hemorrhage did not observe significant association. Multiple logistic regression analysis also failed to identify ACT polymorphism as an independent risk factor for PICH. With regard to meta-analysis, a total of 6 case-control studies including 932 PICH patients and 1140 controls were enrolled. Pooled ORs failed to detect a significant association of ACT signal peptide A/T polymorphism with PICH (dominant model: OR=1.03, 95%CI=0.72–1.46; recessive model: OR=1.08, 95%CI=0.88–1.32). Subgroup analysis based on hypertension revealed no association in hypertensive PICH or in normotensive PICH. CONCLUSIONS Our case-control study in a Chinese population did not detect a significant association between ACT signal peptide A/T polymorphism and PICH. Moreover, meta-analysis combining data from relevant studies failed to provide evidence for the association. Further well-designed studies with larger sample sizes are warranted to verify our findings.
机译:背景技术已经提出α-1抗胰凝乳蛋白酶(ACT)信号肽A / T多态性在各种具有动脉壁病理的脑疾病中起作用。我们进行了一项病例对照研究和一项荟萃分析,以评估这种多态性与原发性脑出血风险之间的关联。材料与方法我们的病例对照研究共纳入188名患者以及200名年龄和性别相匹配的健康对照。通过PCR-LDR对ACT多态性进行基因分型。直到2014年12月,才从PUBMED,EMBASE和中国国家知识基础设施数据库中检索文献,然后使用STATA10.0合并数据,从而进行进一步的荟萃分析。结果在PICH患者和健康对照之间检测到相似的基因型分布(p = 0.523)。基于高血压和出血部位的进一步分析未发现显着相关性。多元逻辑回归分析也未能将ACT多态性确定为PICH的独立危险因素。关于荟萃分析,共纳入了6个病例对照研究,包括932名PICH患者和1140名对照。合并的OR未能检测到ACT信号肽A / T多态性与PICH的显着相关性(显性模型:OR = 1.03,95%CI = 0.72-1.46;隐性模型:OR = 1.08,95%CI = 0.88-1.32)。基于高血压的亚组分析显示,高血压PICH或血压正常PICH中无关联。结论我们在中国人群中进行的病例对照研究未发现ACT信号肽A / T多态性与PICH之间存在显着关联。此外,荟萃分析结合了相关研究的数据未能为关联提供证据。有必要进行更大样本量的精心设计的研究,以验证我们的发现。

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