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小肠结肠炎耶尔森菌yopE基因中的一个同义突变影响YopE III型分泌信号的功能。

A synonymous mutation in Yersinia enterocolitica yopE affects the function of the YopE type III secretion signal.

作者信息

Ramamurthi Kumaran S, Schneewind Olaf

机构信息

Department of Microbiology, University of Chicago, 920 East 58th St., Chicago, IL 60637, USA.

出版信息

J Bacteriol. 2005 Jan;187(2):707-15. doi: 10.1128/JB.187.2.707-715.2005.

Abstract

Yersinia spp. inject virulence proteins called Yops into the cytosol of target eukaryotic cells in an effort to evade phagocytic killing via a dedicated protein-sorting pathway termed type III secretion. Previous studies have proposed that, unlike other protein translocation mechanisms, Yops are not recognized as substrates for secretion via a solely proteinaceous signal. Rather, at least some of this information may be encoded within yop mRNA. Herein, we report that the first seven codons of yopE, when fused to the reporter protein neomycin phosphotransferase (Npt), are sufficient for the secretion of YopE1-7-Npt when type III secretion is induced in vitro. Systematic mutagenesis of yopE codons 1 to 7 reveals that, like yopQ, codons 2, 3, 5, and 7 are sensitive to mutagenesis, thereby defining the first empirical similarity between the secretion signals of two type III secreted substrates. Like that of yopQ, the secretion signal of yopE exhibits a bipartite nature. This is manifested by the ability of codons 8 to 15 to suppress point mutations in the minimal secretion signal that change the amino acid specificities of particular codons or that induce alterations in the reading frame. Further, we have identified a single nucleotide position in codon 3 that, when mutated, conserves the predicted amino acid sequence of the YopE1-7-Npt but abrogates secretion of the reporter protein. When introduced into the context of the full-length yopE gene, the single-nucleotide mutation reduces the type III injection of YopE into HeLa cells, even though the predicted amino acid sequence remains the same. Thus, yopE mRNA appears to encode a property that mediates the type III injection of YopE.

摘要

耶尔森氏菌属通过一种称为III型分泌的专门蛋白质分选途径,将名为Yops的毒力蛋白注入靶真核细胞的细胞质中,以逃避吞噬细胞的杀伤作用。先前的研究表明,与其他蛋白质转运机制不同,Yops并非仅通过蛋白质信号被识别为分泌底物。相反,至少部分此类信息可能编码在yop mRNA中。在此,我们报告,当在体外诱导III型分泌时,yopE的前七个密码子与报告蛋白新霉素磷酸转移酶(Npt)融合后,足以实现YopE1-7-Npt的分泌。对yopE第1至7位密码子进行系统诱变后发现,与yopQ一样,第2、3、5和7位密码子对诱变敏感,从而确定了两种III型分泌底物分泌信号之间的首个经验性相似之处。与yopQ的分泌信号一样,yopE的分泌信号也具有二分性。这表现为第8至15位密码子能够抑制最小分泌信号中的点突变,这些点突变会改变特定密码子的氨基酸特异性或诱导阅读框改变。此外,我们在第3位密码子中确定了一个单核苷酸位置,该位置发生突变时,YopE1-7-Npt的预测氨基酸序列得以保留,但报告蛋白的分泌却被消除。当将该单核苷酸突变引入全长yopE基因的背景中时,尽管预测的氨基酸序列保持不变,但该突变会减少YopE向HeLa细胞的III型注入。因此,yopE mRNA似乎编码了一种介导YopE的III型注入的特性。

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