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果蝇衰老的遗传分析。

A genetic analysis of senescence in Drosophila.

作者信息

Hughes K A, Charlesworth B

机构信息

Committee on Evolutionary Biology, University of Chicago, Illinois 60637.

出版信息

Nature. 1994 Jan 6;367(6458):64-6. doi: 10.1038/367064a0.

Abstract

Two attractive theories for the evolution of senescence are based on the principle that the force of natural selection decreases with age. The theories differ in the type of age-specific gene action that they assume. Antagonistic pleiotropy postulates that pleiotropic genes with positive effects early in life and negative effects of comparable magnitude late in life are favoured by selection, whereas genes with the reverse pattern of action are selected against. Mutation accumulation assumes that deleterious mutant alleles with age-specific effects will equilibrate at a lower frequency if their effects are expressed early rather than late in life. Explicit models demonstrate that both mechanisms can lead to the evolution of senescent life histories under reasonable conditions. Antagonistic pleiotropy has gained considerable empirical support, but the evidence in support of mutation accumulation is more sparse. Here we report that the genetic variability of mortality in male Drosophila melanogaster increases greatly at very late ages, as predicted by the mutation accumulation hypothesis. The rate of increase in mortality with age exhibits substantial genetic and environmental variability. This result provides a possible explanation for recent observations of non-increasing mortality rates in very old flies.

摘要

衰老进化的两种引人关注的理论基于这样一个原则

自然选择的力量会随着年龄增长而减弱。这两种理论在它们所假定的年龄特异性基因作用类型上有所不同。拮抗多效性假说认为,那些在生命早期具有正向作用而在生命后期具有同等程度负向作用的多效基因会受到自然选择的青睐,而具有相反作用模式的基因则会被淘汰。突变积累假说认为,如果具有年龄特异性效应的有害突变等位基因在生命早期而非后期表达,那么它们将以较低的频率达到平衡。明确的模型表明,在合理的条件下,这两种机制都能导致衰老生命史的进化。拮抗多效性已经获得了相当多的实证支持,但支持突变积累的证据则较为稀少。在此我们报告,正如突变积累假说所预测的那样,雄性黑腹果蝇在非常老龄时死亡率的遗传变异性会大幅增加。死亡率随年龄增长的速率表现出显著的遗传和环境变异性。这一结果为近期观察到的老龄果蝇死亡率不增加的现象提供了一种可能的解释。

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