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首页> 外文期刊>Molecular Microbiology >Of linkers and autochaperones: an unambiguous nomenclature to identify common and uncommon themes for autotransporter secretion
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Of linkers and autochaperones: an unambiguous nomenclature to identify common and uncommon themes for autotransporter secretion

机译:连接子和自伴分子:明确的命名法,用于识别自动转运蛋白分泌的常见和不常见主题

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Autotransporter (AT) proteins provide a diverse array of important virulence functions to Gram-negative bacterial pathogens, and have also been adapted for protein surface display applications. The autotransporter' moniker refers to early models that depicted these proteins facilitating their own translocation across the bacterial outer membrane. Although translocation is less autonomous than originally proposed, AT protein segments upstream of the C-terminal transmembrane -barrel have nevertheless consistently been found to contribute to efficient translocation and/or folding of the N-terminal virulence region (the passenger'). However, defining the precise secretion functions of these AT regions has been complicated by the use of multiple overlapping and ambiguous terms to define AT sequence, structural, and functional features, including autochaperone', linker' and junction'. Moreover, the precise definitions and boundaries of these features vary among ATs and even among research groups, leading to an overall murky picture of the contributions of specific features to translocation. Here we propose a unified, unambiguous nomenclature for AT structural, functional and conserved sequence features, based on explicit criteria. Applied to 16 well-studied AT proteins, this nomenclature reveals new commonalities for translocation but also highlights that the autochaperone function is less closely associated with a conserved sequence element than previously believed.
机译:自转运蛋白(AT)可以为革兰氏阴性细菌病原体提供多种多样的重要毒力功能,并且还适用于蛋白质表面展示应用。自转运蛋白的绰号是指早期模型,描述了这些蛋白促进它们自身在细菌外膜上的转运。尽管易位性不如最初提出的自治,但始终发现C端跨膜桶上游的AT蛋白片段有助于N端毒力区(乘客)的有效易位和/或折叠。然而,通过使用多个重叠和不明确的术语来定义AT序列,结构和功能特征,包括自动伴侣',连接子和连接',定义这些AT区域的精确分泌功能变得复杂。此外,这些特征的精确定义和边界在AT甚至研究小组之间也各不相同,从而导致对特定特征对易位的贡献的整体印象模糊。在这里,我们基于明确的标准,为AT结构,功能和保守序列特征提出了统一,明确的命名法。应用于16种经过深入研究的AT蛋白质,该命名法揭示了易位的新共性,但同时也强调了自陪伴蛋白功能与保守序列元件的关联性比以前认为的低。

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