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三种β-分泌酶1(BACE1)基因多态性(外显子5 C/G、内含子5 T/G和3'非翻译区T/A)与散发性阿尔茨海默病易感性的关联:一项荟萃分析。

The association of three BACE1 gene polymorphisms (exon5 C/G, intron 5 T/G and 3'UTR T/A) with sporadic Alzheimer's disease susceptibility: a meta-analysis.

作者信息

Yuan Hai, Ling Kang, Du Xunping, Ge Pingping, Wu Shaowei, Wang Xiaotong

机构信息

Department of Rehabilitation Medicine, The Second People's Hospital of Hefei City 246th Heping Road, Hefei 230011, Anhui Province, China.

Department of Neurology, The Second People's Hospital of Hefei City 246th Heping Road, Hefei 230011, Anhui Province, China.

出版信息

Int J Clin Exp Med. 2015 Aug 15;8(8):12264-74. eCollection 2015.

Abstract

Despite biological support for a role of Beta-site APP-cleaving enzyme 1 (BACE1) in sporadic Alzheimer's disease (SAD), studies about the BACE1 genetic polymorphisms in SAD are inconsistent. To explore whether the BACE1 polymorphisms confers susceptibility to SAD, the current meta-analysis was conducted to evaluate the gene-disease association in relevant studies. The serious databases were researched to identify studies. The association between BACE1 (exon5 C/G, intron 5 T/G or 3'UTR T/A) polymorphism and SAD risk was evaluated by odds ratios (ORs) together with their 95% confidence intervals (CIs). The combined results showed no significant difference in all models on the basis of all studies for BACE1 (exon5 C/G, intron 5 T/G or 3'UTR T/A) polymorphisms. When subgroup analysis was performed based on ethnicity and the epsilon 4 allele of apolipoprotein E (APOEε4) carriers status, significant associations were demonstrated (CC versus CG+GG: OR=1.37, 95% CI=1.04-1.82, P=0.03<0.05 and CC versus CG: OR=1.49, 95% CI=1.11-2.01, P=0.01<0.05) for APOEε4 carriers status. The pooled results suggest the BACE1 (exon5 C/G, intron 5 T/G or 3'UTR T/A) polymorphism could be not a risk factor for SAD. However, individuals with CC genotype have higher risk of SAD with APOEε4 carrier status, and gene-gene interaction might affect on the association. Further studies with large sample size, especially in subgroup analysis, should be done to confirm these findings.

摘要

尽管有生物学证据支持β-位点淀粉样前体蛋白裂解酶1(BACE1)在散发性阿尔茨海默病(SAD)中发挥作用,但关于SAD中BACE1基因多态性的研究结果并不一致。为了探究BACE1基因多态性是否会使个体易患SAD,本荟萃分析对相关研究中的基因与疾病关联进行了评估。通过检索主要数据库来识别相关研究。采用优势比(OR)及其95%置信区间(CI)评估BACE1(外显子5 C/G、内含子5 T/G或3'非翻译区T/A)多态性与SAD风险之间的关联。综合所有研究结果显示,BACE1(外显子5 C/G、内含子5 T/G或3'非翻译区T/A)多态性在所有模型中均无显著差异。按种族和载脂蛋白E(APOE)ε4等位基因携带者状态进行亚组分析时,发现存在显著关联(对于APOEε4携带者状态,CC与CG+GG相比:OR = 1.37,95%CI = 1.04 - 1.82,P = 0.03<0.05;CC与CG相比:OR = 1.49,95%CI = 1.11 - 2.01,P = 0.01<0.05)。汇总结果表明,BACE1(外显子5 C/G、内含子5 T/G或3'非翻译区T/A)多态性可能不是SAD的危险因素。然而,CC基因型个体在APOEε4携带者状态下患SAD的风险更高,并且基因-基因相互作用可能会影响这种关联。需要进行更大样本量的进一步研究,尤其是亚组分析,以证实这些发现。

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