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Secretion signal recognition by YscN, the Yersinia type III secretion ATPase

机译:耶尔森氏菌III型分泌ATPase YscN识别分泌信号

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Yersinia type III machines secrete protein substrates across the bacterial envelope. Secretion signals of some substrates have been identified; however, the mechanisms whereby these signals interact with type III machines are not known. Here we show that fusion of YopR, an early secretion substrate, to the IN terminus of dihydrofolate reductase (DHFR) or other tightly folded proteins generates impassable hybrids that cannot travel the type III pathway. YopR hybrids capture YscN, the ATPase that provides energy for type III transport reactions, in the bacterial cytoplasm. Eleven IN-terminal residues function as the YopR secretion signal, which is required for both binding to YscN and blocking the type III pathway. When expressed during type III machine assembly, YopR-DHFR blocks all secretion. Delayed expression of YopR-DHFR, when yersiniae have already engaged the type III pathway, blocks secretion of early (YscP) but not of late (effector Yops) substrates. These observations support a model whereby type III machines are programmed to secrete a sequence of proteins that can be disrupted when an impassable early substrate interacts with the YscN ATPase and blocks the transport of late substrates.
机译:III型耶尔森氏菌机器在整个细菌包膜中分泌蛋白质底物。已经鉴定出某些底物的分泌信号。但是,这些信号与III型机器相互作用的机制尚不清楚。在这里,我们表明,早期分泌底物YopR与二氢叶酸还原酶(DHFR)或其他紧密折叠的蛋白质的IN末端融合产生无法通过III型途径的不可逾越的杂种。 YopR杂种捕获细菌细胞质中的YscN(一种为III型转运反应提供能量的ATPase)。 11个IN末端残基充当YopR分泌信号,这是与YscN结合并阻断III型途径所必需的。当在III型机器组装过程中表达时,YopR-DHFR会阻止所有分泌。当耶尔森氏菌已经参与了III型途径时,YopR-DHFR的延迟表达会阻断早期(YscP)而不是晚期(有效Yops)底物的分泌。这些观察结果支持一个模型,通过该模型可以对III型机器进行编程,以分泌一系列蛋白质,这些蛋白质在无法逾越的早期底物与YscN ATPase相互作用并阻止晚期底物的运输时会被破坏。

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