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二硫键环在自转运蛋白分泌中的大小和构象限制。

Size and conformation limits to secretion of disulfide-bonded loops in autotransporter proteins.

机构信息

School of Immunity and Infection, University of Birmingham, Birmingham B15 2TT, United Kingdom.

School of Cancer Sciences, University of Birmingham, Birmingham B15 2TT, United Kingdom.

出版信息

J Biol Chem. 2011 Dec 9;286(49):42283-42291. doi: 10.1074/jbc.M111.306118. Epub 2011 Oct 17.

Abstract

Autotransporters are a superfamily of virulence factors typified by a channel-forming C terminus that facilitates translocation of the functional N-terminal passenger domain across the outer membrane of Gram-negative bacteria. This final step in the secretion of autotransporters requires a translocation-competent conformation for the passenger domain that differs markedly from the structure of the fully folded secreted protein. The nature of the translocation-competent conformation remains controversial, in particular whether the passenger domain can adopt secondary structural motifs, such as disulfide-bonded segments, while maintaining a secretion-competent state. Here, we used the endogenous and closely spaced cysteine residues of the plasmid-encoded toxin (Pet) from enteroaggregative Escherichia coli to investigate the effect of disulfide bond-induced folding on translocation of an autotransporter passenger domain. We reveal that rigid structural elements within disulfide-bonded segments are resistant to autotransporter-mediated secretion. We define the size limit of disulfide-bonded segments tolerated by the autotransporter system demonstrating that, when present, cysteine pairs are intrinsically closely spaced to prevent congestion of the translocator pore by large disulfide-bonded regions. These latter data strongly support the hairpin mode of autotransporter biogenesis.

摘要

自动转运蛋白是一类毒力因子的超家族,其特征是具有一个形成通道的 C 端,该 C 端有助于功能性 N 端载体域穿过革兰氏阴性菌的外膜进行易位。自动转运蛋白分泌的最后一步需要载体域具有易位能力的构象,该构象与完全折叠的分泌蛋白的结构明显不同。易位能力构象的性质仍然存在争议,特别是载体域是否可以在保持分泌能力状态的同时采用二级结构模体,如二硫键结合的片段。在这里,我们使用肠聚集性大肠杆菌中质粒编码毒素(Pet)的内源性和紧密间隔的半胱氨酸残基来研究二硫键诱导折叠对自动转运蛋白载体域易位的影响。我们揭示了二硫键结合片段内的刚性结构元件抵抗自动转运蛋白介导的分泌。我们定义了自动转运蛋白系统可耐受的二硫键结合片段的大小限制,证明了当存在时,半胱氨酸对本质上是紧密间隔的,以防止大的二硫键结合区域堵塞转运子孔。这些后一组数据强烈支持自动转运蛋白生物发生的发夹模式。

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本文引用的文献

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