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对氧磷酶1是一种长寿基因:一项荟萃分析的结果。

PON1 is a longevity gene: results of a meta-analysis.

作者信息

Lescai Francesco, Marchegiani Francesca, Franceschi Claudio

机构信息

CIG-Centre L. Galvani for Biophysics, Bioinformatics and Biocomplexity, Alma Mater Studiorum Università di Bologna, Bologna, Italy.

出版信息

Ageing Res Rev. 2009 Oct;8(4):277-84. doi: 10.1016/j.arr.2009.04.001. Epub 2009 Apr 17.

Abstract

Paraoxonase 1 (PON1) is one of the most studied genes regarding cardiovascular risk, oxidative stress and inflammation. Several lines of evidence suggests that PON1 promotes an atheroprotective effect. Patients carrying PON1 codon 192 QQ genotype display a higher risk of cardiovascular events, the major cause of mortality in the elderly: it can be predicted that gene variants increasing the risk of mortality will be under-represented in long-living individuals. We first reported that PON1 R allele (R+) carriers are significantly more represented in Italian centenarians; subsequently this topic has been addressed by many other groups, and here we report a meta-analysis on 11 studies in different populations selected by a review of the literature available in PubMed and testing the effect of the Q192R polymorphism on human ageing. QUORUM guidelines for meta-analysis have been followed, and a total number of 5962 subjects have been included: 2795 young controls (<65 years of age) and 3167 old subjects (>65 years of age). The Mantel-Haenszel weighting for pooling in presence of a fixed effects model has been applied. The meta-analysis of R carriers showed a significant result with an overall OR of 1.16 (1.04-1.30, 95% CI, p=0.006). The meta-analysis of QR genotype also showed a significant result, with an overall OR of 1.14 (1.02-1.27, 95% CI, p=0.016). The results show that PON1 gene variants at codon 192 impact on the probability of attaining longevity, and that subjects carrying RR and QR genotypes (R+ carriers) are favoured in reaching extreme ages. These results likely represent the counterpart of the effects observed on cardiovascular diseases (CVD), as centenarians and nonagenarians escaped or delayed the onset of the major age-related diseases, including CVD.

摘要

对氧磷酶1(PON1)是在心血管风险、氧化应激和炎症方面研究最多的基因之一。多项证据表明,PON1具有抗动脉粥样硬化作用。携带PON1密码子192 QQ基因型的患者发生心血管事件的风险更高,而心血管事件是老年人死亡的主要原因:可以预测,增加死亡风险的基因变异在长寿个体中的比例会较低。我们首次报道,PON1 R等位基因(R+)携带者在意大利百岁老人中所占比例显著更高;随后,许多其他研究团队也探讨了这一话题,在此我们对11项不同人群的研究进行荟萃分析,这些研究是通过检索PubMed上的文献并检测Q192R多态性对人类衰老的影响来选取的。我们遵循了荟萃分析的QUORUM指南,共纳入5962名受试者:2795名年轻对照组(年龄<65岁)和3167名老年受试者(年龄>65岁)。采用固定效应模型下的Mantel-Haenszel加权法进行合并分析。R携带者的荟萃分析结果显著,总体比值比为1.16(1.04 - 1.30,95%置信区间,p = 0.006)。QR基因型的荟萃分析结果也显著,总体比值比为1.14(1.02 - 1.27,95%置信区间,p = 0.016)。结果表明,密码子192处的PON1基因变异会影响达到长寿的概率,携带RR和QR基因型(R+携带者)的受试者更有可能活到极高年龄。这些结果可能与在心血管疾病(CVD)中观察到的效应相对应,因为百岁老人和九旬老人避免或推迟了包括CVD在内的主要年龄相关疾病的发病。

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