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转录、结构和类器官在人类和大猩猩的整个生命周期中跨越时间进行转化。

Transcription, structure, and organoids translate time across the lifespan of humans and great apes.

作者信息

Charvet Christine J, Ofori Kwadwo, Falcone Carmen, Rigby Dames Brier A

机构信息

Department of Anatomy, Physiology and Pharmacology, College of Veterinary Medicine, Auburn University, 1130 Wire Road, Auburn, 36832, AL, USA.

Department of Biology, Delaware State University, 1200 N. Dupont Highway, Dover, DE, 19901, USA.

出版信息

PNAS Nexus. 2023 Jul 20;2(8):pgad230. doi: 10.1093/pnasnexus/pgad230. eCollection 2023 Aug.

Abstract

How the neural structures supporting human cognition developed and arose in evolution is an enduring question of interest. Yet, we still lack appropriate procedures to align ages across primates, and this lacuna has hindered progress in understanding the evolution of biological programs. We generated a dataset of unprecedented size consisting of 573 time points from abrupt and gradual changes in behavior, anatomy, and transcription across human and 8 nonhuman primate species. We included time points from diverse human populations to capture within-species variation in the generation of cross-species age alignments. We also extracted corresponding ages from organoids. The identification of corresponding ages across the lifespan of 8 primate species, including apes (e.g., orangutans, gorillas) and monkeys (i.e., marmosets, macaques), reveals that some biological pathways are extended in humans compared with some nonhuman primates. Notably, the human lifespan is unusually extended relative to studied nonhuman primates demonstrating that very old age is a phase of life in humans that does not map to other studied primate species. More generally, our work prompts a reevaluation in the choice of a model system to understand aging given very old age in humans is a period of life without a clear counterpart in great apes.

摘要

支持人类认知的神经结构在进化过程中是如何发展和出现的,这是一个长期以来备受关注的问题。然而,我们仍然缺乏合适的程序来校准灵长类动物的年龄,而这一空白阻碍了我们在理解生物程序进化方面取得进展。我们生成了一个规模空前的数据集,包含来自人类和8种非人类灵长类动物行为、解剖结构及转录方面的突然和渐进变化的573个时间点。我们纳入了不同人类群体的时间点,以捕捉跨物种年龄校准过程中的种内变异。我们还从类器官中提取了相应的年龄。对包括猿类(如猩猩、大猩猩)和猴类(如狨猴、猕猴)在内的8种灵长类动物整个生命周期中相应年龄的识别表明,与一些非人类灵长类动物相比,人类的一些生物途径有所延长。值得注意的是,相对于所研究的非人类灵长类动物,人类的寿命异常延长,这表明高龄是人类生命中的一个阶段,在其他所研究的灵长类物种中并无对应。更普遍地说,鉴于人类的高龄阶段在大猩猩中没有明确的对应阶段,我们的工作促使人们重新评估用于理解衰老的模型系统的选择。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a29d/10406161/e65af7714c5d/pgad230f1.jpg

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