在前瞻性研究Treviso Longeva (TRELONG)中,SIRT1启动子多态性位点rs12778366增加IL-6相关的人类死亡率。

International journal of molecular epidemiology and genetics Pub Date : 2015-09-09 eCollection Date: 2015-01-01
Diego Albani, Stefano Mazzuco, Armando Chierchia, Federica Fusco, Lucia Boeri, Rosalba Martines, Enrico Di Giorgi, Andrea Frigato, Elisabetta Durante, Livio Caberlotto, Andrea Zanardo, Marinella Siculi, Maurizio Gallucci, Gianluigi Forloni
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引用次数: 0

摘要

sirtuins (SIRT)是一个具有去乙酰化酶活性的蛋白家族,其研究已经提供了这些酶在衰老相关生理功能中的关键作用的证据。SIRT1和长寿之间的联系已经在模式生物中出现,但很少有关于人类的数据,特别是依赖于纵向研究。在这里,我们评估了SIRT1基因启动子(rs12778366)内的遗传变异是否与人类寿命相关。我们分析了在“Treviso Longeva”(TRELONG)研究中收集的586个基因组DNA (gDNA),其中包括来自意大利东北部特雷维索市70岁以上的老年人,并进行了11年的随访。采用实时聚合酶链反应(RT-PCR)等位基因鉴别法对SIRT1 rs12778366进行基因分型。通过比较85岁以上和85岁以下的人进行的横断面分析没有证据表明rs12778366与寿命之间存在关联。当我们将死亡率作为因变量进行纵向分析时,我们没有观察到rs12778366与整个人群的寿命相关(校正p值= 0.33)。然而,当我们根据白细胞介素-6 (IL-6)的循环水平对TRELONG受试者进行分层时,我们发现与TT对照组相比,rs12778366 (TC+CC)携带者的死亡风险增加(校正p值= 0.03,HR 1.47)。IL-6是残疾和死亡率的预测因子。我们的数据不支持rs12778366在人类寿命中的主要作用,但对IL-6的分层分析表明,该变体可能与老年人高循环IL-6的有害影响有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The SIRT1 promoter polymorphic site rs12778366 increases IL-6 related human mortality in the prospective study "Treviso Longeva (TRELONG)".

The SIRT1 promoter polymorphic site rs12778366 increases IL-6 related human mortality in the prospective study "Treviso Longeva (TRELONG)".

Studies on sirtuins (SIRT), a family of proteins with deacetylase activity, have provided convergent evidence of the key role of these enzymes in aging-linked physiological functions. The link between SIRT1 and longevity has emerged in model organism but few data are available in humans, in particular relying on longitudinal studies. Here, we assessed whether a genetic variant within SIRT1 gene promoter (rs12778366) was associated to human longevity. We analyzed 586 genomic DNA (gDNA) collected in the study "Treviso Longeva" (TRELONG), including elderly over 70 years of age from the municipality of Treviso, a town in the Northeast of Italy, with a 11-year follow-up. We genotyped SIRT1 rs12778366 by real-time polymerase chain reaction (RT-PCR) allelic discrimination assay. A cross-sectional analysis performed by comparing people over and under 85 years of age did not evidence association between rs12778366 and longevity. When we performed a longitudinal analysis considering mortality as dependent variable, we did not observe an association of rs12778366 with longevity in the whole population (corrected P-value = 0.33). However, when we stratified the TRELONG subjects according to circulating level of interleukin-6 (IL-6), a predictor of disability and mortality, we found that rs12778366 (TC+CC) carriers were at increased risk of mortality in comparison to the TT reference group (corrected P-value = 0.03, HR 1.47). Our data do not support a major role of rs12778366 in human longevity, but the stratified analysis on IL-6 suggests that this variant may be involved in the detrimental effect of high circulating IL-6 in the elderly.

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