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首页> 外文期刊>Journal of Cell Science >Lamins are rapamycin targets that impact human longevity: A study in centenarians
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Lamins are rapamycin targets that impact human longevity: A study in centenarians

机译:薄层蛋白是雷帕霉素的靶标,可影响人类寿命:百岁老人的一项研究

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The dynamic organisation of the cell nucleus is profoundly modified during growth, development and senescence as a result of changes in chromatin arrangement and gene transcription. A plethora of data suggests that the nuclear lamina is a key player in chromatin dynamics and argues in favour of a major involvement of prelamin A in fundamental mechanisms regulating cellular senescence andorganism ageing. As the best model to analyse the role of prelamin A in normal ageing, we used cells from centenarian subjects. We show that prelamin A is accumulated in fibroblasts from centenarians owing to downregulation of its specific endoprotease ZMPSTE24, whereas other nuclear envelope constituents are mostly unaffected and cells do not enter senescence. Accumulation of prelamin A in nuclei of cells from centenarians elicits loss of heterochromatin, as well as recruitment of the inactive form of 53BP1, associated with rapid response to oxidative stress. These effects, including the prelamin-A-mediated increase of nuclear 53BP1, can be reproduced by rapamycin treatment of cells from younger individuals. These data identify prelamin A and 53BP1 as new targets of rapamycin that are associated with human longevity. We propose that the reported mechanisms safeguard healthy ageing in humans through adaptation of the nuclear environment to stress stimuli.
机译:由于染色质排列和基因转录的变化,细胞核的动态组织在生长,发育和衰老过程中被深刻地修饰。大量数据表明,核纤层蛋白是染色质动力学的关键因素,并主张在细胞调节衰老和生物衰老的基本机制中主要参与prelaminA。作为分析Prelamin A在正常衰老中作用的最佳模型,我们使用了百岁老人的细胞。我们显示,prelamin A由于其特定的内切蛋白酶ZMPSTE24的下调而在百岁老人的成纤维细胞中积累,而其他核被膜成分大多不受影响,并且细胞不会进入衰老状态。百岁老人细胞核中前醇溶蛋白A的积累会导致异染色质的丧失,并招募失活形式的53BP1,这与对氧化应激的快速反应有关。这些作用,包括prelamin-A介导的核53BP1的增加,可以通过雷帕霉素处理年轻个体的细胞来再现。这些数据确定了prelamin A和53BP1是雷帕霉素的新靶点,与人类寿命有关。我们建议所报道的机制通过适应压力刺激的核环境来维护人类的健康衰老。

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