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Self-identity reprogrammed by a single residue switch in a cell surface receptor of a social bacterium

机译:通过社交细菌细胞表面受体中的单个残基开关对自我身份进行重新编程

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摘要

The ability to recognize close kin confers survival benefits on single-celled microbes that live in complex and changing environments. Microbial kinship detection relies on perceptible cues that reflect relatedness between individuals, although the mechanisms underlying recognition in natural populations remain poorly understood. In myxobacteria, cells identify related individuals through a polymorphic cell surface receptor, TraA. Recognition of compatible receptors leads to outer membrane exchange among clonemates and fitness consequences. Here, we investigated how a single receptor creates a diversity in recognition across myxobacterial populations. We first show that TraA requires its partner protein TraB to function in cell–cell adhesion. Recognition is shown to be traA allele-specific, where polymorphisms within TraA dictate binding selectivity. We reveal the malleability of TraA recognition, and seemingly minor changes to its variable region reprogram recognition outcomes. Strikingly, we identify a single residue (A/P205) as a molecular switch for TraA recognition. Substitutions at this position change the specificity of a diverse panel of environmental TraA receptors. In addition, we engineered a receptor with unique specificity by simply creating an A205P substitution, suggesting that modest changes in TraA can lead to diversification of new recognition groups in nature. We hypothesize that the malleable property of TraA has allowed it to evolve and create social barriers between myxobacterial populations and in turn avoid adverse interactions with relatives.
机译:识别近亲的能力赋予生活在复杂多变的环境中的单细胞微生物以生存优势。微生物亲缘关系检测依靠反映个体之间相关性的可感知线索,尽管对自然种群识别的基本机制仍然知之甚少。在黏细菌中,细胞通过多态性细胞表面受体TraA识别相关个体。相容受体的识别导致克隆人之间的外膜交换和适应性后果。在这里,我们研究了单个受体如何在粘菌群体中创造识别多样性。我们首先表明TraA需要其伴侣蛋白TraB在细胞间粘附中发挥作用。识别显示是traA等位基因特异的,其中TraA内的多态性决定了结合的选择性。我们揭示了TraA识别的可塑性,以及其可变区重新编程识别结果的细微变化。令人惊讶的是,我们将一个残基(A / P205)识别为TraA识别的分子开关。在该位置的取代改变了环境TraA受体的多样性。此外,我们通过简单地创建A205P取代来设计具有独特特异性的受体,这表明TraA的适度变化可导致自然界中新识别基团的多样化。我们假设TraA的可塑性使它得以发展,并在黏细菌种群之间建立了社会障碍,从而避免了与亲属的不利相互作用。

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