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细菌蛋白的低复杂度区域的保守性依赖于菌株的致病性和蛋白的亚细胞定位。

The Conservation of Low Complexity Regions in Bacterial Proteins Depends on the Pathogenicity of the Strain and Subcellular Location of the Protein.

机构信息

Institute of Organismic and Molecular Evolution, Faculty of Biology, Johannes Gutenberg University, 55128 Mainz, Germany.

出版信息

Genes (Basel). 2021 Mar 22;12(3):451. doi: 10.3390/genes12030451.

Abstract

Low complexity regions (LCRs) in proteins are characterized by amino acid frequencies that differ from the average. These regions evolve faster and tend to be less conserved between homologs than globular domains. They are not common in bacteria, as compared to their prevalence in eukaryotes. Studying their conservation could help provide hypotheses about their function. To obtain the appropriate evolutionary focus for this rapidly evolving feature, here we study the conservation of LCRs in bacterial strains and compare their high variability to the closeness of the strains. For this, we selected 20 taxonomically diverse bacterial species and obtained the completely sequenced proteomes of two strains per species. We calculated all orthologous pairs for each of the 20 strain pairs. Per orthologous pair, we computed the conservation of two types of LCRs: compositionally biased regions (CBRs) and homorepeats (polyX). Our results show that, in bacteria, Q-rich CBRs are the most conserved, while A-rich CBRs and polyA are the most variable. LCRs have generally higher conservation when comparing pathogenic strains. However, this result depends on protein subcellular location: LCRs accumulate in extracellular and outer membrane proteins, with conservation increased in the extracellular proteins of pathogens, and decreased for polyX in the outer membrane proteins of pathogens. We conclude that these dependencies support the functional importance of LCRs in host-pathogen interactions.

摘要

蛋白质中的低复杂度区域(LCRs)的特点是其氨基酸频率与平均值不同。这些区域的进化速度较快,与同源物相比,它们在球状结构域之间的保守性较低。与真核生物相比,它们在细菌中并不常见。研究它们的保守性可以帮助提供关于它们功能的假设。为了获得这个快速进化特征的适当进化焦点,我们在这里研究了细菌菌株中 LCRs 的保守性,并将其高变异性与菌株的亲缘关系进行了比较。为此,我们选择了 20 种具有不同分类学特征的细菌物种,并获得了每个物种的两种菌株的完全测序蛋白质组。我们为 20 对菌株中的每一对计算了所有的直系同源对。对于每个直系同源对,我们计算了两种类型的 LCR 的保守性:组成偏向区域(CBRs)和同源重复(polyX)。我们的结果表明,在细菌中,富含 Q 的 CBRs 是最保守的,而富含 A 的 CBRs 和 polyA 是最可变的。在比较致病菌株时,LCRs 的一般保守性更高。然而,这个结果取决于蛋白质的亚细胞位置:LCRs 在细胞外和外膜蛋白中积累,病原体的细胞外蛋白的保守性增加,而病原体的外膜蛋白中的 polyX 减少。我们得出结论,这些依赖性支持 LCRs 在宿主-病原体相互作用中的功能重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec84/8004648/6ed54dd9c808/genes-12-00451-g001.jpg

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