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Testing evolutionary models of senescence: traditional approaches and future directions.

机译:测试衰老的进化模型:传统方法和未来方向。

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From an evolutionary perspective, the existence of senescence is a paradox. Why has senescence not been more effectively selected against given its associated decreases in Darwinian fitness? Why does senescence exist and how has it evolved? Three major theories offer explanations: (1) the theory of mutation accumulation suggested by PB Medawar; (2) the theory of antagonistic pleiotropy suggested by GC Williams; and (3) the disposable soma theory suggested by TBL Kirkwood. These three theories differ in the underlying causes of aging that they propose but are not mutually exclusive. This paper compares the specific biological predictions of each theory and discusses the methods and results of previous empirical tests. Lifespan is found to be the most frequently used estimate of senescence in evolutionary investigations. This measurement acts as a proxy for an individual's rate of senescence, but provides no information on an individual's senescent state or "biological age" throughout life. In the future, use of alternative longitudinal measures of senescence may facilitate investigation of previously neglected aspects of evolutionary models, such as intra- and inter-individual heterogeneity in the process of aging. DNA methylation data are newly proposed to measure biological aging and are suggested to be particularly useful for such investigations.
机译:从进化的角度来看,衰老的存在是一个悖论。鉴于与之相关的达尔文健康度下降,为什么不能更有效地选择衰老呢?为什么衰老存在并且如何发展?三个主要理论提供了解释:(1)PB Medawar提出的突变积累理论; (2)威廉姆斯(GC Williams)提出的拮抗多效性理论; (3)TBL Kirkwood提出的一次性体细胞理论。这三种理论在提出的老龄化根本原因上有所不同,但并不相互排斥。本文比较了每种理论的具体生物学预测,并讨论了以前的经验测试的方法和结果。发现寿命是进化研究中最常用的衰老估计。该测量值可以代替个体的衰老率,但是在整个生命中都无法提供有关个体的衰老状态或“生物年龄”的信息。将来,使用替代性的纵向衰老测量方法可能有助于研究以前忽略的进化模型,例如衰老过程中个体间和个体间的异质性。新提出了DNA甲基化数据来测量生物衰老,并被认为对于此类研究特别有用。

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