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Signatures of diversifying selection and convergence acting on passerine Toll-like receptor 4 in an evolutionary context

机译:在进化环境中对雀狼收缩受体4作用的多样化选择和收敛的签名

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摘要

Positive selection acting on Toll-like receptors (TLRs) has been recently investigated to reveal evolutionary mechanisms of host-pathogen molecular co-adaptation. Much of this research, however, has focused mainly on the identification of sites predicted to be under positive selection, bringing little insight into the functional differences and similarities among species and a limited understanding of convergent evolution in the innate immune molecules. In this study, we provide evidence of phenotypic variability in the avian TLR4 ligand-binding region (LBR), the direct interface between host and pathogen molecular structures. We show that 55 passerine species vary substantially in the distribution of electrostatic potential on the surface of the receptor, and based on these distinct patterns, we identified four species clusters. Seven of the 34 evolutionarily nonconservative and positively selected residues correspond topologically to sites previously identified as being important for lipopolysaccharide, lipid IVa or MD-2 binding. Five of these positions codetermine the identity of the charge clusters. Groups of species that host-related communities of pathogens were predicted to cluster based on their TLR4 LBR charge. Despite some evidence for convergence among taxa, there were no clear associations between the TLR4 LBR charge distribution and any of the general ecological characteristics compared (migration, latitudinal distribution and diet). Closely related species, however, mostly belonged to the same surface charge cluster indicating that phylogenetic constraints are key determinants shaping TLR4 adaptive evolution. Our results suggest that host innate immune evolution is consistent with Fahrenholz's rule on the cospeciation of hosts and their parasites.
机译:最近研究了作用于Toll样受体(TLR)的阳性选择以揭示宿主病原分子共适应的进化机制。然而,这项研究的大部分主要集中在预测在正面选择的网站的识别上,这几乎没有于物种之间的功能差异和相似性,以及对先天免疫分子的收敛演变的有限理解。在这项研究中,我们提供了禽TLR4配体结合区(LBR)的表型变异性的证据,宿主和病原体分子结构之间的直接界面。我们表明,55个旁角物种基本上变化在受体表面上的静电电位分布,并基于这些明显的图案,我们确定了四种种类的簇。 34中的七种进化不含非任业性和正面选择的残留物对应于先前鉴定为脂多糖,脂质IVA或MD-2结合重要的网站。这些位置中的五个代码术委员会的指定电荷簇的标识。基于他们的TLR4 LBR充电预测宿主相关群体群体的物种组。尽管存在纳税群体的趋同证据,但TLR4 LBR电荷分布与任何一般生态特征之间没有明确的协会(迁移,延迟分布和饮食)。然而,密切相关的物种主要属于具有相同的表面电荷簇,表明系统发育约束是塑造TLR4自适应演化的关键决定因素。我们的结果表明,主机天生的免疫演变与Fahrenholz关于宿主和寄生虫的核化的规则一致。

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