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The TAL Effector AvrBs3 from Xanthomonas campestris pv. vesicatoria Contains Multiple Export Signals and Can Enter Plant Cells in the Absence of the Type III Secretion Translocon

机译:Xanthomonas campestris pv的TAL效应器AvrBs3。 vesicatoria包含多个输出信号并且可以在没有III型分泌转运蛋白的情况下进入植物细胞

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摘要

Pathogenicity of the Gram-negative plant-pathogenic bacterium Xanthomonas campestris pv. vesicatoria depends on a type III secretion (T3S) system which translocates effector proteins into plant cells. Effector protein delivery is controlled by the T3S chaperone HpaB, which presumably escorts effector proteins to the secretion apparatus. One intensively studied effector is the transcription activator-like (TAL) effector AvrBs3, which binds to promoter sequences of plant target genes and activates plant gene expression. It was previously reported that type III-dependent delivery of AvrBs3 depends on the N-terminal protein region. The signals that control T3S and translocation of AvrBs3, however, have not yet been characterized. In the present study, we show that T3S and translocation of AvrBs3 depend on the N-terminal 10 and 50 amino acids, respectively. Furthermore, we provide experimental evidence that additional signals in the N-terminal 30 amino acids and the region between amino acids 64 and 152 promote translocation of AvrBs3 in the absence of HpaB. Unexpectedly, in vivo translocation assays revealed that AvrBs3 is delivered into plant cells even in the absence of HrpF, which is the predicted channel-forming component of the T3S translocon in the plant plasma membrane. The presence of HpaB- and HrpF-independent transport routes suggests that the delivery of AvrBs3 is initiated during early stages of the infection process, presumably before the activation of HpaB or the insertion of the translocon into the plant plasma membrane.
机译:革兰氏阴性植物病原菌Xanthomonas campestris pv的致病性。 vesicatoria依赖于III型分泌(T3S)系统,该系统可将效应蛋白转运到植物细胞中。效应蛋白的传递受T3S伴侣HpaB的控制,后者可能将效应蛋白护送到分泌装置中。一种经过深入研究的效应子是转录激活子样(TAL)效应子AvrBs3,它与植物靶基因的启动子序列结合并激活植物基因的表达。以前有报道说,依赖于III型的AvrBs3传递取决于N末端蛋白区域。但是,尚未表征控制T3S和AvrBs3易位的信号。在本研究中,我们表明,AvrBs3的T3S和易位分别取决于N端10和50个氨基酸。此外,我们提供了实验证据,表明在不存在HpaB的情况下,N端30个氨基酸以及氨基酸64和152之间的区域中的其他信号会促进AvrBs3的移位。出乎意料的是,体内易位分析显示,即使不存在HrpF,AvrBs3仍被递送到植物细胞中,HrpF是植物质膜中T3S易位子的预测通道形成成分。 HpaB和HrpF无关的运输途径的存在表明,AvrBs3的传递是在感染过程的早期开始的,大概是在HpaB激活或转运子插入植物质膜之前。

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