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脊椎动物PEPT1和PEPT2基因的比较分析

Comparative analysis of vertebrate PEPT1 and PEPT2 genes.

作者信息

Wang Minghui, Zhang Xiangzhe, Zhao Hongbo, Wang Qishan, Pan Yuchun

机构信息

School of Agriculture and Biology, Department of Animal Sciences, Shanghai Jiao Tong University, 200240, Shanghai, People's Republic of China.

出版信息

Genetica. 2010 Jun;138(6):587-99. doi: 10.1007/s10709-009-9431-6. Epub 2009 Dec 20.

Abstract

The plasma membrane transport proteins belong to SoLute Carrier 15 (SLC15) family and two members of this family have been characterized extensively in higher vertebrates, namely PEPT1 and PEPT2. Despite many efforts have made to define a pharmacophore model for efficient binding and transporting of substrates, there is not a comprehensive study performed to elucidate the evolutionary mechanisms among the SLC15 family members and to statistically evaluate sequence conservation and functional divergence between members. In this study, we compared and contrasted the rates and patterns of molecular evolution of 2 PEPT genes. Phylogenetic tree assembly with all available vertebrate PEPTs suggests that the PEPTs originated by duplications and diverged from a common protein at the base of the eukaryotic tree. Topological structure demonstrates both members share the similar hydrophobic domains (TMDs), which have been constrained by purifying selection. Although both genes show qualitatively similar patterns, their rates of evolution differ significantly due to an increased rate of synonymous substitutions in the structural domains in one copy, suggesting substantial differences in functional constraint on each gene. Site-specific profiles were established by posterior probability analysis revealing significantly divergent regions mainly locate at the hydrophobic region between predicted transmembrane domains 9 and 10 of the proteins. Thus, these results provide the evidence that several amino acid residues with reduced selective constraints are largely responsible for functional divergence between the paralogous PEPTs. These findings may provide a starting point for further experimental verifications.

摘要

质膜转运蛋白属于溶质载体15(SLC15)家族,该家族的两个成员在高等脊椎动物中已得到广泛研究,即PEPT1和PEPT2。尽管已经做出很多努力来定义一个用于底物高效结合和转运的药效团模型,但尚未进行全面研究以阐明SLC15家族成员之间的进化机制,也未对成员之间的序列保守性和功能差异进行统计学评估。在本研究中,我们比较并对比了2个PEPT基因的分子进化速率和模式。用所有可用的脊椎动物PEPT构建的系统发育树表明,PEPTs起源于基因复制,并在真核生物树的基部从一个共同的蛋白质分化而来。拓扑结构显示两个成员都具有相似的疏水域(跨膜结构域,TMDs),这些结构域受到纯化选择的限制。尽管两个基因显示出定性相似的模式,但由于其中一个拷贝的结构域中同义替换率增加,它们的进化速率存在显著差异,这表明每个基因在功能限制上存在实质性差异。通过后验概率分析建立了位点特异性图谱,揭示出显著不同的区域主要位于蛋白质预测跨膜结构域9和10之间的疏水区域。因此,这些结果提供了证据,表明几个选择性限制降低的氨基酸残基在很大程度上导致了旁系同源PEPTs之间的功能差异。这些发现可能为进一步的实验验证提供一个起点。

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