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首页> 外文期刊>The Plant Cell >Intrinsic disorder in pathogen effectors: protein flexibility as an evolutionary hallmark in a molecular arms race.
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Intrinsic disorder in pathogen effectors: protein flexibility as an evolutionary hallmark in a molecular arms race.

机译:病原体效应物的内在障碍:蛋白质柔韧性是分子军备竞赛中的进化标志。

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Effector proteins represent a refined mechanism of bacterial pathogens to overcome plants' innate immune systems. These modular proteins often manipulate host physiology by directly interfering with immune signaling of plant cells. Even if host cells have developed efficient strategies to perceive the presence of pathogenic microbes and to recognize intracellular effector activity, it remains an open question why only few effectors are recognized directly by plant resistance proteins. Based on in-silico genome-wide surveys and a reevaluation of published structural data, we estimated that bacterial effectors of phytopathogens are highly enriched in long-disordered regions (>50 residues). These structurally flexible segments have no secondary structure under physiological conditions but can fold in a stimulus-dependent manner (e.g., during protein-protein interactions). The high abundance of intrinsic disorder in effectors strongly suggests positive evolutionary selection of this structural feature and highlights the dynamic nature of these proteins. We postulate that such structural flexibility may be essential for (1) effector translocation, (2) evasion of the innate immune system, and (3) host function mimicry. The study of these dynamical regions will greatly complement current structural approaches to understand the molecular mechanisms of these proteins and may help in the prediction of new effectors.
机译:效应蛋白代表细菌病原体克服植物先天免疫系统的精细机制。这些模块蛋白通常通过直接干扰植物细胞的免疫信号传导来操纵宿主生理。即使宿主细胞已开发出有效的策略来感知病原微生物的存在并识别细胞内效应子的活性,但为什么只有很少的效应子被植物抗性蛋白直接识别仍然是一个悬而未决的问题。根据计算机全基因组范围内的调查和对已发表结构数据的重新评估,我们估计植物病原体的细菌效应子在长期无序的区域(> 50个残基)中高度富集。这些结构上柔性的片段在生理条件下没有二级结构,但是可以以刺激依赖性方式折叠(例如在蛋白质-蛋白质相互作用期间)。效应子中大量内在失调强烈暗示了该结构特征的积极进化选择,并突出了这些蛋白质的动态性质。我们假定这种结构的灵活性可能对于(1)效应子易位,(2)逃避先天免疫系统和(3)宿主功能模仿至关重要。这些动力学区域的研究将大大补充当前的结构方法,以了解这些蛋白质的分子机制,并可能有助于预测新的效应子。

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