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首页> 外文期刊>Philosophical Transactions of the Royal Society of London, Series B. Biological Sciences >The mitochondrial genome, paternal age and telomere length in humans
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The mitochondrial genome, paternal age and telomere length in humans

机译:人类的线粒体基因组,父母年龄和端粒长度

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摘要

Telomere length (TL) in humans is highly heritable and undergoes progressive age-dependent shortening in somatic cells. By contrast, sperm donated by older men display comparatively long telomeres, presumably because in the male germline, telomeres become longer with age. This puzzling phenomenon might explain why TL in the offspring correlates positively with paternal age. The present communication proposes that mitochondrial DNA polymorphisms and heteroplasmy cause variation in the production of reactive oxygen species, which, in turn, mediate age-dependent selection of germ stem cells with long telomeres and hence sperm with long telomeres. These long telomeres are then inherited by the offspring. The effect of paternal age on the offspring TL might be an evolutionarily driven mechanism that helps regulate TL across the human population.
机译:人体中的端粒长度(TL)是高度遗传的,在体细胞中依赖于逐步缩短。 相比之下,老年男性捐赠的精子显示相对长的端粒,可能是因为在雄性种系中,端粒随着年龄的增长而变长。 这种令人费解的现象可以解释原因在后代中的TL与父亲年龄的相关性相关。 目前的通信提出了线粒体DNA多态性和异质性导致反应性氧物种的产生变化,反过来,又介导年龄依赖于长端粒的生殖干细胞选择,并具有长端粒的精子。 这些长端粒体然后由后代继承。 父亲年龄对后代TL的影响可能是一种进化驱动的机制,有助于调节人群的TL。

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