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Single nucleotide polymorphisms linked to mitochondrial uncoupling protein genes UCP2 and UCP3 affect mitochondrial metabolism and healthy aging in female nonagenarians

机译:与线粒体解偶联蛋白基因UCP2和UCP3相关联的单核苷酸多态性影响女性非原虫的线粒体代谢和健康衰老

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摘要

Energy expenditure decreases with age, but in the oldest-old, energy demand for maintenance of body functions increases with declining health. Uncoupling proteins have profound impact on mitochondrial metabolic processes; therefore, we focused attention on mitochondrial uncoupling protein genes. Alongside resting metabolic rate (RMR), two SNPs in the promoter region of UCP2 were associated with healthy aging. These SNPs mark potential binding sites for several transcription factors; thus, they may affect expression of the gene. A third SNP in the 3'-UTR of UCP3 interacted with RMR. This UCP3 SNP is known to impact UCP3 expression in tissue culture cells, and it has been associated with body weight and mitochondrial energy metabolism. The significant main effects of the UCP2 SNPs and the interaction effect of the UCP3 SNP were also observed after controlling for fat-free mass (FFM) and physical-activity related energy consumption. The association of UCP2/3 with healthy aging was not found in males. Thus, our study provides evidence that the genetic risk factors for healthy aging differ in males and females, as expected from the differences in the phenotypes associated with healthy aging between the two sexes. It also has implications for how mitochondrial function changes during aging.
机译:能量消耗随着年龄的增长而减少,但在最老的人群中,维持身体功能所需的能量随健康状况的下降而增加。解偶联蛋白对线粒体代谢过程有深远的影响。因此,我们将注意力集中在线粒体解偶联蛋白基因上。除了静息代谢率(RMR)外,UCP2启动子区域中的两个SNP与健康衰老相关。这些SNP标记了几个转录因子的潜在结合位点。因此,它们可能影响基因的表达。 UCP3的3'-UTR中的第三个SNP与RMR相互作用。已知该UCP3 SNP影响组织培养细胞中UCP3的表达,并且与体重和线粒体能量代谢有关。在控制了无脂肪质量(FFM)和与运动有关的能量消耗之后,还观察到了UCP2 SNP的重要主要作用和UCP3 SNP的相互作用。在男性中未发现UCP2 / 3与健康衰老的关系。因此,我们的研究提供了证据,表明男性和女性的健康衰老的遗传风险因素有所不同,这是由两性与健康衰老相关的表型差异所预期的。它也对衰老过程中线粒体功能的变化有影响。

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