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Mutation in histone deacetylase HDA-3 leads to shortened locomotor healthspan in

机译:组蛋白脱乙酰酶HDA-3中的突变导致缩短运动锻造钢

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摘要

Some genes are essential for survival, while other genes play modulatory roles on health and survival. Genes that play modulatory roles may promote an organism’s survival and health by fine-tuning physiological processes. An unbiased search for genes that alter an organism’s ability to maintain aspects of health may uncover modulators of lifespan and healthspan. From an unbiased screen for Caenorhabditis elegans mutants that show a progressive decline in motility, we aimed to identify genes that play a modulatory role in maintenance of locomotor healthspan. Here we report the involvement of hda-3, encoding a class I histone deacetylase, as a genetic factor that contributes in the maintenance of general health and locomotion in C. elegans. We identified a missense mutation in HDA-3 as the causative mutation in one of the isolated strains that show a progressive decline in maximum velocity and travel distance. From transcriptome analysis, we found a cluster of genes on Chromosome II carrying BATH domains that were downregulated by hda-3. Furthermore, downregulation of individual bath genes leads to significant decline in motility. Our study identifies genetic factors that modulate the maintenance of locomotor healthspan and may reveal potential targets for delaying age-related locomotor decline.
机译:一些基因对于存活至关重要,而其他基因则对健康和生存率起调节作用。发挥调节作用的基因可以通过微调生理过程来促进生物体的生存和健康。对改变生物体维持健康方面的能力的基因的无偏见搜索可能揭示寿命和卫生钢的调节剂。从一个无偏见的秀丽隐杆线虫突变体,表现出逐步下降的动力,我们旨在识别在维护机车卫生钢的维护中发挥调制作用的基因。在这里,我们报告了HDA-3的介入,编码了I类组蛋白脱乙酰化酶,作为遗传因素,这些因素有助于维持C.秀丽隐杆线的一般健康和运动。我们鉴定了HDA-3中的畸形突变,作为其中一个分离的菌株中的致病性突变,其显示出最大速度和行驶距离的逐渐下降。从转录组分析中,我们发现染色体II上的基因簇携带浴室域,其通过HDA-3下调。此外,单个浴基因的下调导致运动性显着下降。我们的研究确定了调节运动卫生钢的维护的遗传因素,并可能揭示延迟年龄相关的机器人的潜在目标。

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