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脊椎动物胰岛素/TOR 信号转导通路的比较基因组学:选择性压力的网络级分析。

Comparative genomics of the vertebrate insulin/TOR signal transduction pathway: a network-level analysis of selective pressures.

机构信息

Departament de Genètica, Facultat de Biologia, Universitat de Barcelona, Barcelona, Spain.

出版信息

Genome Biol Evol. 2011;3:87-101. doi: 10.1093/gbe/evq084. Epub 2010 Dec 13.

Abstract

Complexity of biological function relies on large networks of interacting molecules. However, the evolutionary properties of these networks are not fully understood. It has been shown that selective pressures depend on the position of genes in the network. We have previously shown that in the Drosophila insulin/target of rapamycin (TOR) signal transduction pathway there is a correlation between the pathway position and the strength of purifying selection, with the downstream genes being most constrained. In this study, we investigated the evolutionary dynamics of this well-characterized pathway in vertebrates. More specifically, we determined the impact of natural selection on the evolution of 72 genes of this pathway. We found that in vertebrates there is a similar gradient of selective constraint in the insulin/TOR pathway to that found in Drosophila. This feature is neither the result of a polarity in the impact of positive selection nor of a series of factors affecting selective constraint levels (gene expression level and breadth, codon bias, protein length, and connectivity). We also found that pathway genes encoding physically interacting proteins tend to evolve under similar selective constraints. The results indicate that the architecture of the vertebrate insulin/TOR pathway constrains the molecular evolution of its components. Therefore, the polarity detected in Drosophila is neither specific nor incidental of this genus. Hence, although the underlying biological mechanisms remain unclear, these may be similar in both vertebrates and Drosophila.

摘要

生物功能的复杂性依赖于相互作用的分子的大型网络。然而,这些网络的进化特性还不完全清楚。已经表明,选择压力取决于基因在网络中的位置。我们之前已经表明,在果蝇胰岛素/雷帕霉素靶蛋白 (TOR) 信号转导途径中,途径位置与纯化选择的强度之间存在相关性,下游基因受到的约束最大。在这项研究中,我们研究了脊椎动物中这种特征良好的途径的进化动态。更具体地说,我们确定了自然选择对该途径的 72 个基因进化的影响。我们发现,在脊椎动物中,胰岛素/TOR 途径中的选择约束梯度与在果蝇中发现的相似。这一特征既不是正选择影响的极性的结果,也不是一系列影响选择约束水平的因素(基因表达水平和广度、密码子偏倚、蛋白质长度和连接性)的结果。我们还发现,编码物理相互作用蛋白的途径基因往往在相似的选择约束下进化。研究结果表明,脊椎动物胰岛素/TOR 途径的结构限制了其成分的分子进化。因此,在果蝇中检测到的极性既不是该属特有的,也不是偶然的。因此,尽管潜在的生物学机制尚不清楚,但这些机制在脊椎动物和果蝇中可能是相似的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/80a0/3030423/69bdec184ef8/gbeevq084f01_ht.jpg

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