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样本量和群体历史对观测到的突变谱的影响:以人类和黑猩猩群体为例。

The Impact of Sample Size and Population History on Observed Mutational Spectra: A Case Study in Human and Chimpanzee Populations.

机构信息

Center for Evolution and Medicine, Arizona State University, Tempe, AZ, USA.

School of Life Sciences, Center for Evolution and Medicine, Arizona State University, Tempe, AZ, USA.

出版信息

Genome Biol Evol. 2023 Mar 3;15(3). doi: 10.1093/gbe/evad019.

Abstract

Recent studies have highlighted variation in the mutational spectra among human populations as well as closely related hominoids-yet little remains known about the genetic and nongenetic factors driving these rate changes across the genome. Pinpointing the root causes of these differences is an important endeavor that requires careful comparative analyses of population-specific mutational landscapes at both broad and fine genomic scales. However, several factors can confound such analyses. Although previous studies have shown that technical artifacts, such as sequencing errors and batch effects, can contribute to observed mutational shifts, other potentially confounding parameters have received less attention thus far. Using population genetic simulations of human and chimpanzee populations as an illustrative example, we here show that the sample size required for robust inference of mutational spectra depends on the population-specific demographic history. As a consequence, the power to detect rate changes is high in certain hominoid populations while, for others, currently available sample sizes preclude analyses at fine genomic scales.

摘要

最近的研究强调了人类群体以及密切相关的同源物种之间突变谱的差异——但对于驱动这些基因组范围内速率变化的遗传和非遗传因素知之甚少。确定这些差异的根本原因是一项重要的努力,需要在广泛和精细的基因组尺度上仔细比较分析特定人群的突变景观。然而,有几个因素会使这些分析变得复杂。尽管先前的研究表明,技术伪影,如测序错误和批次效应,可能导致观察到的突变转移,但到目前为止,其他潜在的混杂参数受到的关注较少。我们使用人类和黑猩猩种群的群体遗传模拟作为说明性示例,这里表明,稳健推断突变谱所需的样本量取决于特定人群的人口统计学历史。因此,在某些同源物种群体中,检测速率变化的能力很高,而对于其他群体,目前可用的样本量则排除了精细基因组尺度的分析。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ff7e/9989333/f2f620f4ca5d/evad019f1.jpg

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