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Adaptive Evolution of Four Microcephaly Genes and the Evolution of Brain Size in Anthropoid Primates

机译:拟南芥中四种小头基因的适应性进化和脑大小的进化

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The anatomical basis and adaptive function of the expansion in primate brain size have long been studied; however, we are only beginning to understand the genetic basis of these evolutionary changes. Genes linked to human primary microcephaly have received much attention as they have accelerated evolutionary rates along lineages leading to humans. However, these studies focus narrowly on apes, and the link between microcephaly gene evolution and brain evolution is disputed. We analyzed the molecular evolution of four genes associated with microcephaly (ASPM, CDK5RAP2, CENPJ, MCPH1) across 21 species representing all major clades of anthropoid primates. Contrary to prevailing assumptions, positive selection was not limited to or intensified along the lineage leading to humans. In fact we show that all four loci were subject to positive selection across the anthropoid primate phylogeny. We developed clearly defined hypotheses to explicitly test if selection on these loci was associated with the evolution of brain size. We found positive relationships between both CDK5RAP2 and ASPM and neonatal brain mass and somewhat weaker relationships between these genes and adult brain size. In contrast, there is no evidence linking CENPJ and MCPH1 to brain size evolution. The stronger association of ASPM and CDK5RAP2 evolution with neonatal brain size than with adult brain size is consistent with these loci having a direct effect on prenatal neuronal proliferation. These results suggest that primate brain size may have at least a partially conserved genetic basis. Our results contradict a previous study that linked adaptive evolution of ASPM to changes in relative cortex size; however, our analysis indicates that this conclusion is not robust. Our finding that the coding regions of two widely expressed loci has experienced pervasive positive selection in relation to a complex, quantitative developmental phenotype provides a notable counterexample to the commonly asserted hypothesis that cis-regulatory regions play a dominant role in phenotypic evolution.
机译:长期研究灵长类动物脑部扩张的解剖学基础和适应功能。但是,我们才刚刚开始了解这些进化变化的遗传基础。与人类原发性小头畸形相关的基因已经得到了极大的关注,因为它们沿着导致人类的世系加快了进化速度。然而,这些研究仅集中在猿类上,并且小头基因进化与大脑进化之间的联系存在争议。我们分析了与小头畸形相关的四个基因(ASPM,CDK5RAP2,CENPJ,MCPH1)在代表所有类人猿灵长类的21个物种中的分子进化。与普遍的假设相反,积极的选择并不仅限于或沿着导致人类的血统发展。实际上,我们表明,在整个拟人灵长类动物系统发育中,所有四个基因座都经历了阳性选择。我们提出了明确定义的假设,以明确测试在这些基因座上的选择是否与脑大小的进化有关。我们发现CDK5RAP2和ASPM与新生儿脑质量之间存在正相关关系,而这些基因与成人脑大小之间的关系则较弱。相比之下,没有证据表明CENPJ和MCPH1与大脑大小演变有关。 ASPM和CDK5RAP2进化与新生儿大脑大小的关联比与成人大脑大小的关联更强,这与这些位点对产前神经元增殖具有直接影响是一致的。这些结果表明灵长类动物的大脑大小可能至少具有部分保守的遗传基础。我们的结果与先前的研究相矛盾,该研究将ASPM的适应性进化与相对皮层大小的变化联系起来。但是,我们的分析表明该结论并不可靠。我们的发现,即两个广泛表达的基因座的编码区相对于复杂的,定量的发育表型经历了普遍的阳性选择,这为通常主张的顺式调控区在表型进化中起主要作用的假设提供了明显的反例。

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