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人类基因家族的年龄分布模式:基因本体论类别存在差异,不同亚细胞定位一致。

Age distribution patterns of human gene families: divergent for Gene Ontology categories and concordant between different subcellular localizations.

机构信息

State Key Laboratory of Genetic Engineering and MOE Key Laboratory of Contemporary Anthropology, School of Life Sciences, Fudan University, Biology Building II 113, Shanghai, 200433, China.

出版信息

Mol Genet Genomics. 2014 Apr;289(2):137-47. doi: 10.1007/s00438-013-0799-8. Epub 2013 Dec 10.

Abstract

The age distribution of gene duplication events within the human genome exhibits two waves of duplications along with an ancient component. However, because of functional constraint differences, genes in different functional categories might show dissimilar retention patterns after duplication. It is known that genes in some functional categories are highly duplicated in the early stage of vertebrate evolution. However, the correlations of the age distribution pattern of gene duplication between the different functional categories are still unknown. To investigate this issue, we developed a robust pipeline to date the gene duplication events in the human genome. We successfully estimated about three-quarters of the duplication events within the human genome, along with the age distribution pattern in each Gene Ontology (GO) slim category. We found that some GO slim categories show different distribution patterns when compared to the whole genome. Further hierarchical clustering of the GO slim functional categories enabled grouping into two main clusters. We found that human genes located in the duplicated copy number variant regions, whose duplicate genes have not been fixed in the human population, were mainly enriched in the groups with a high proportion of recently duplicated genes. Moreover, we used a phylogenetic tree-based method to date the age of duplications in three signaling-related gene superfamilies: transcription factors, protein kinases and G-protein coupled receptors. These superfamilies were expressed in different subcellular localizations. They showed a similar age distribution as the signaling-related GO slim categories. We also compared the differences between the age distributions of gene duplications in multiple subcellular localizations. We found that the distribution patterns of the major subcellular localizations were similar to that of the whole genome. This study revealed the whole picture of the evolution patterns of gene functional categories in the human genome.

摘要

人类基因组中基因复制事件的年龄分布呈现出两波复制以及一个古老的成分。然而,由于功能约束的差异,不同功能类别的基因在复制后可能表现出不同的保留模式。已知在脊椎动物进化的早期阶段,某些功能类别的基因高度重复。然而,不同功能类别之间基因复制年龄分布模式的相关性仍然未知。为了研究这个问题,我们开发了一种稳健的管道来确定人类基因组中的基因复制事件。我们成功地估计了人类基因组中约四分之三的复制事件,以及每个基因本体(GO)精简类别中的年龄分布模式。我们发现,一些 GO 精简类别与整个基因组相比显示出不同的分布模式。进一步对 GO 精简功能类别进行层次聚类,可将其分为两个主要聚类。我们发现,位于人类基因组中拷贝数变异区域的基因,其重复基因尚未在人类群体中固定,主要富集在高比例最近复制基因的组中。此外,我们使用基于系统发育树的方法来确定三个信号转导相关基因超家族(转录因子、蛋白激酶和 G 蛋白偶联受体)中重复的年龄。这些超家族在不同的亚细胞定位中表达。它们的年龄分布与信号转导相关的 GO 精简类别相似。我们还比较了多个亚细胞定位中基因复制年龄分布的差异。我们发现,主要亚细胞定位的分布模式与整个基因组相似。这项研究揭示了人类基因组中基因功能类别进化模式的全貌。

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