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MicroRNA-Driven Developmental Remodeling in the Brain Distinguishes Humans from Other Primates

机译:脑中MicroRNA驱动的发育重塑使人类与其他灵长类动物区分开来。

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While multiple studies have reported the accelerated evolution of brain gene expression in the human lineage, the mechanisms underlying such changes are unknown. Here, we address this issue from a developmental perspective, by analyzing mRNA and microRNA (miRNA) expression in two brain regions within macaques, chimpanzees, and humans throughout their lifespan. We find that constitutive gene expression divergence (species differences independent of age) is comparable between humans and chimpanzees. However, humans display a 3–5 times faster evolutionary rate in divergence of developmental patterns, compared to chimpanzees. Such accelerated evolution of human brain developmental patterns (i) cannot be explained by life-history changes among species, (ii) is twice as pronounced in the prefrontal cortex than the cerebellum, (iii) preferentially affects neuron-related genes, and (iv) unlike constitutive divergence does not depend on cis-regulatory changes, but might be driven by human-specific changes in expression of trans-acting regulators. We show that developmental profiles of miRNAs, as well as their target genes, show the fastest rates of human-specific evolutionary change, and using a combination of computational and experimental methods, we identify miR-92a, miR-454, and miR-320b as possible regulators of human-specific neural development. Our results suggest that different mechanisms underlie adaptive and neutral transcriptome divergence, and that changes in the expression of a few key regulators may have been a major driving force behind rapid evolution of the human brain.
机译:尽管多项研究报告了人类谱系中脑基因表达的加速进化,但这种变化的潜在机制尚不清楚。在这里,我们通过分析猕猴,黑猩猩和人类一生中两个大脑区域的mRNA和microRNA(miRNA)表达,从发展的角度解决了这个问题。我们发现人类和黑猩猩之间的组成型基因表达差异(物种差异与年龄无关)是可比的。但是,与黑猩猩相比,人类在发育方式差异上的进化速度快3至5倍。人类大脑发育模式的这种加速进化(i)不能用物种之间的生活史变化来解释;(ii)在前额叶皮层中的表达是小脑的两倍;(iii)优先影响神经元相关基因,并且(iv )与组成型差异不同,它不依赖于顺式调节变化,而可能是由人类特异的反式调节因子表达驱动的。我们显示,miRNA及其靶基因的发育概况显示出人类特异性进化变化的最快速度,并且结合使用计算机和实验方法,我们确定了miR-92a,miR-454和miR-320b作为人类特定神经发育的可能调节剂。我们的结果表明,不同的机制是适应性转录组和中性转录组差异的基础,并且一些关键调控因子的表达变化可能是人类大脑快速进化的主要驱动力。

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