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Accelerated Evolution of Genes and Neocortical Expansion in Mammalian Lineages

机译:哺乳动物谱系中基因和新皮肤膨胀的加速演变

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The sequencing of the human and many other genomes has allowed the recurrent question of what makes us human to be addressed at the molecular level. Signal phenotypic characteristics of humans and other anthropoid primates are their extended life spans and their enlarged brains relative to their body size, particularly their expanded neocortex. To address the question of which genes might have been involved in the adaptive evolution responsible for these emerging phenotypes we have examined the available comparative genomic data using bioinformatic and evolutionary genetic techniques. In particular, we focused on the evolution of the genes involved in aerobic energy metabolism. Nuclear genomes have provided evidence for positive Darwinian selection acting on these genes in primates, a result that correlates strongly with the increased demand for aerobic energy in the expanded anthropoid primate neocortex. We have also compared the evolutionary rate of mitochondrial genomes among select vertebrates with the encephalization quotient, a measure that normalizes brain to body size. We find that the mitochondrial encoded genes that are involved in accepting electrons from cytochrome c show evidence of accelerated rates of change that in primates result in a reduction of electrostatic charge.
机译:人和许多其他基因组的测序允许与我们将人类在分子水平进行解决的内容的反复问题。人类和其他人物灵长类动物的信号表型特征是它们的延长寿命和它们相对于身体尺寸的扩大的大脑,特别是它们的膨胀Neocortex。为了解决哪些基因可能参与对这些新兴表型的适应性进化中可能参与的问题,我们已经使用生物信息和进化遗传技术研究了可用的比较基因组数据。特别是,我们专注于参与有氧能量代谢的基因的演变。核基因组在灵长类动物中提供了对这些基因的积极达尔文选择的证据,这是随着在扩大的人体灵长类动物的膨胀性的人体细胞网状物中提高了对有氧能量的需求而强烈相关的结果。我们还将选择脊椎动物与侧膈网中的线粒体基因组的进化率进行了比较,这是一个衡量大脑对体型的措施。我们发现参与接受来自细胞色素C的电子的线粒体编码基因显示出加速的变化率的证据表明,在灵长造生物中导致静电电荷的降低。

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