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相关稳定选择塑造了基因调控网络的拓扑结构。

Correlated stabilizing selection shapes the topology of gene regulatory networks.

机构信息

CNRS, IRD, UMR EGCE, Université Paris-Saclay, 91190 Gif-sur-Yvette, France.

UMR 7206 Eco-Anthropologie, CNRS, MNHN, Université Paris Cité, 75116 Paris, France.

出版信息

Genetics. 2023 May 26;224(2). doi: 10.1093/genetics/iyad065.

DOI:10.1093/genetics/iyad065
PMID:37070537
Abstract

The evolution of gene expression is constrained by the topology of gene regulatory networks, as co-expressed genes are likely to have their expressions affected together by mutations. Conversely, co-expression can also be an advantage when genes are under joint selection. Here, we assessed theoretically whether correlated selection (selection for a combination of traits) was able to affect the pattern of correlated gene expressions and the underlying gene regulatory networks. We ran individual-based simulations, applying a stabilizing correlated fitness function to three genetic architectures: a quantitative genetics (multilinear) model featuring epistasis and pleiotropy, a quantitative genetics model where each genes has an independent mutational structure, and a gene regulatory network model, mimicking the mechanisms of gene expression regulation. Simulations showed that correlated mutational effects evolved in the three genetic architectures as a response to correlated selection, but the response in gene networks was specific. The intensity of gene co-expression was mostly explained by the regulatory distance between genes (largest correlations being associated to genes directly interacting with each other), and the sign of co-expression was associated with the nature of the regulation (transcription activation or inhibition). These results concur to the idea that gene network topologies could partly reflect past selection patterns on gene expression.

摘要

基因表达的进化受到基因调控网络拓扑结构的限制,因为共表达的基因很可能会因为突变而同时受到影响。相反,当基因受到联合选择时,共表达也可能是一种优势。在这里,我们从理论上评估了相关选择(选择一组特征的组合)是否能够影响相关基因表达模式和潜在的基因调控网络。我们进行了基于个体的模拟,对三种遗传结构应用了稳定的相关适应度函数:具有上位性和多效性的数量遗传学(多线性)模型、每个基因具有独立突变结构的数量遗传学模型,以及模拟基因表达调控机制的基因调控网络模型。模拟结果表明,相关的突变效应在三种遗传结构中作为对相关选择的反应而进化,但在基因网络中的反应是特定的。基因共表达的强度主要由基因之间的调控距离解释(最大相关性与直接相互作用的基因相关联),共表达的符号与调控的性质有关(转录激活或抑制)。这些结果与基因网络拓扑结构可能部分反映过去对基因表达的选择模式的观点一致。

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