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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >DNA damage responses and p53 in the aging process
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DNA damage responses and p53 in the aging process

机译:老化过程中的DNA损伤响应和P53

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The genome is constantly attacked by genotoxic insults. DNA damage has long been established as a cause of cancer development through its mutagenic consequences. Conversely, radiation therapy and chemotherapy induce DNA damage to drive cells into apoptosis or senescence as outcomes of the DNA damage response (DDR). More recently, DNA damage has been recognized as a causal factor for the aging process. The role of DNA damage in aging and age-related diseases is illustrated by numerous congenital progeroid syndromes that are caused by mutations in genome maintenance pathways. During the past 2 decades, understanding how DDR drives cancer development and contributes to the aging process has progressed rapidly. It turns out that the DDR factor p53 takes center stage during tumor development and also plays an important role in the aging process. Studies in metazoan models ranging from Caenorhabditis elegans to mammals have revealed cell-autonomous and systemic DDR mechanisms that orchestrate adaptive responses that augment maintenance of the aging organism amid gradually accumulating DNA damage.
机译:基因组不断受到遗传毒性损伤的攻击。通过其致突变后果,DNA损伤长期以来是癌症发展的原因。相反,放射治疗和化疗诱导DNA损伤,使细胞作为DNA损伤反应(DDR)的结果转化为凋亡或衰老。最近,DNA损伤已被认为是老化过程的因果因素。 DNA损伤在衰老和年龄相关疾病中的作用是由基因组维持途径中的突变引起的许多先天性突变综合征。在过去的二十年中,了解DDR如何推动癌症的发展,并为老龄化进程做出贡献迅速发展。事实证明,DDR因子P53在肿瘤发育期间采用中心阶段,并且在老化过程中也发挥着重要作用。甲壳虫杆菌的Metazoan模型对哺乳动物的研究揭示了细胞 - 自主和系统性DDR机制,其协调了在逐渐积累DNA损伤中增加了衰老生物的适应性反应。

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