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Diverse interventions that extend mouse lifespan suppress shared age-associated epigenetic changes at critical gene regulatory regions

机译:延长小鼠寿命的多种干预措施可抑制关键基因调控区中与年龄相关的表观遗传学共同变化

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摘要

BackgroundAge-associated epigenetic changes are implicated in aging. Notably, age-associated DNA methylation changes comprise a so-called aging “clock”, a robust biomarker of aging. However, while genetic, dietary and drug interventions can extend lifespan, their impact on the epigenome is uncharacterised. To fill this knowledge gap, we defined age-associated DNA methylation changes at the whole-genome, single-nucleotide level in mouse liver and tested the impact of longevity-promoting interventions, specifically the Ames dwarf Prop1 df/df mutation, calorie restriction and rapamycin.
机译:背景与年龄相关的表观遗传变化与衰老有关。值得注意的是,与年龄相关的DNA甲基化变化包括所谓的衰老“时钟”,这是衰老的强大生物标记。然而,尽管遗传,饮食和药物干预可以延长寿命,但它们对表观基因组的影响尚不明确。为了填补这一知识空白,我们在小鼠肝脏的全基因组,单核苷酸水平上定义了与年龄相关的DNA甲基化变化,并测试了长寿干预措施的影响,特别是艾姆斯矮人Prop1 df / df 突变,卡路里限制和雷帕霉素。

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