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Deciphering the Role of Rapidly Evolving Conserved Elements in Primate Brain Development and Exploring Their Potential Involvement in Alzheimers Disease

机译:破译快速进化的保守元素在灵长类动物大脑发育中的作用并探索它们在阿尔茨海默病中的潜在参与

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摘要

Although previous studies have identified human-specific accelerated regions as playing a key role in the recent evolution of the human brain, the characteristics and cellular functions of rapidly evolving conserved elements (RECEs) in ancestral primate lineages remain largely unexplored. Here, based on large-scale primate genome assemblies, we identify 888 RECEs that have been highly conserved in primates that exhibit significantly accelerated substitution rates in the ancestor of the Simiiformes. This primate lineage exhibits remarkable morphological innovations, including an expanded brain mass. Integrative multiomic analyses reveal that RECEs harbor sequences with potential cis-regulatory functions that are activated in the adult human brain. Importantly, genes linked to RECEs exhibit pronounced expression trajectories in the adult brain relative to the fetal stage. Furthermore, we observed an increase in the chromatin accessibility of RECEs in oligodendrocytes from individuals with Alzheimer's disease (AD) compared to that of a control group, indicating that these RECEs may contribute to brain aging and AD. Our findings serve to expand our knowledge of the genetic underpinnings of brain function during primate evolution.
机译:尽管以前的研究已经确定人类特异性加速区域在人类大脑的近期进化中起着关键作用,但祖先灵长类动物谱系中快速进化的保守元件 (RECE) 的特征和细胞功能在很大程度上仍未得到探索。在这里,基于大规模灵长类动物基因组组装,我们鉴定了 888 个 RECEs,这些 RECE 在灵长类动物中高度保守,它们在 Simiiformes 的祖先中表现出显着加速的替换率。这种灵长类动物谱系表现出显着的形态创新,包括扩大的脑质量。综合多组学分析显示,RECE 包含具有潜在顺式调节功能的序列,这些功能在成人人脑中被激活。重要的是,与 RECE 相关的基因在成人大脑中相对于胎儿阶段表现出明显的表达轨迹。此外,我们观察到与对照组相比,阿尔茨海默病 (AD) 个体少突胶质细胞中 RECE 的染色质可及性增加,表明这些 RECE 可能导致大脑衰老和 AD。我们的发现有助于扩展我们对灵长类动物进化过程中大脑功能的遗传基础的了解。

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