首页> 外文期刊>Mechanisms of Ageing and Development >Lack of association between human longevity and polymorphisms of IL-1 cluster, IL-6, IL-10 and TNF-alpha genes in Finnish nonagenarians.
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Lack of association between human longevity and polymorphisms of IL-1 cluster, IL-6, IL-10 and TNF-alpha genes in Finnish nonagenarians.

机译:人类寿命与芬兰非agenarians中的IL-1簇,IL-6,IL-10和TNF-α基因多态性之间缺乏关联。

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摘要

There has been increasing interest in research on genetic basis of longevity. Aging is accompanied by immune deterioration and dysregulation of cytokines. Increased IL-6 concentration in vivo and enhanced IL-6, IL-1beta, and TNF-alpha production in vitro have been reported in healthy elderly people. Cytokine gene polymorphisms have been demonstrated to be associated with cytokine production both in vivo and in vitro, and with some diseases. Thus, gene polymorphisms of cytokine may play a role in longevity by modulating an individual's responses to life-threatening disorders. Cytokine gene polymorphisms at IL1A-889, IL1B+3953, IL1B-511, IL1RN VNTR, IL6-174, IL10-1082, and TNFA-308 were genotyped in 250 Finnish nonagenarians (52 men and 198 women) and in 400 healthy blood donors (18-60 years) as controls. No statistically significant differences were found in the genotype distributions, allelic frequencies and A2+ carrier status of IL-1alpha, IL-1beta, IL-1RA, IL-6, IL-10, and TNF-alpha genes between nonagenarians and younger controls within Finnish population, nor between male and female nonagenarians. No differences emerged between nonagenarians and younger controls by comparing different IL-1 gene cluster haplotypes. Thus, there is no evidence of an association of IL-1 complex, IL-6, IL-10, and TNF-alpha gene polymorphisms with longevity, alone or in combination.
机译:人们对基于寿命的遗传基础的研究越来越感兴趣。衰老伴随着免疫恶化和细胞因子的失调。在健康的老年人中,体内IL-6浓度增加,体外IL-6,IL-1beta和TNF-α产生增加。已经证明细胞因子基因多态性与体内和体外细胞因子的产生以及某些疾病有关。因此,细胞因子的基因多态性可能通过调节个体对危及生命的疾病的反应而在长寿中发挥作用。在250名芬兰非老年患者(52名男性和198名女性)和400名健康献血者中对IL1A-889,IL1B + 3953,IL1B-511,IL1RN VNTR,IL6-174,IL10-1082和TNFA-308的细胞因子基因多态性进行了基因分型。 (18-60岁)作为对照。在非芬兰人和较年轻的对照组中,IL-1α,IL-1β,IL-1RA,IL-6,IL-10和TNF-α基因的基因型分布,等位基因频率和A2 +携带者状态在统计学上无显着差异人口,非男性和女性之间也没有关系。通过比较不同的IL-1基因簇单倍型,非agenarians和较年轻的对照组之间没有差异。因此,没有证据表明单独或组合使用IL-1复合物,IL-6,IL-10和TNF-α基因多态性可以延年益寿。

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