首页> 外文期刊>MBio >Distinct Roles of the Repeat-Containing Regions and Effector Domains of the Vibrio vulnificus Multifunctional-Autoprocessing Repeats-in-Toxin (MARTX) Toxin
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Distinct Roles of the Repeat-Containing Regions and Effector Domains of the Vibrio vulnificus Multifunctional-Autoprocessing Repeats-in-Toxin (MARTX) Toxin

机译:多功能自动加工毒素重复序列( italic> vulnificus vulnificus )的重复区和效应域的不同作用

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ABSTRACT Vibrio vulnificus is a seafood-borne pathogen that destroys the intestinal epithelium, leading to rapid bacterial dissemination and death. The most important virulence factor is the multifunctional-autoprocessing repeats-in-toxin (MARTX) toxin comprised of effector domains in the center region flanked by long repeat-containing regions which are well conserved among MARTX toxins and predicted to translocate effector domains. Here, we examined the role of the repeat-containing regions using a modified V.?vulnificus MARTX (MARTX_(Vv)) toxin generated by replacing all the internal effector domains with β-lactamase (Bla). Bla activity was detected in secretions from the bacterium and also in the cytosol of intoxicated epithelial cells. The modified MARTX_(Vv)toxin without effector domains retained its necrotic activity but lost its cell-rounding activity. Further, deletion of the carboxyl-terminal repeat-containing region blocked toxin secretion from the bacterium. Deletion of the amino-terminal repeat-containing region had no effect on secretion but completely abolished translocation and necrosis. Neither secretion nor translocation was affected by enzymatically inactivating the cysteine protease domain of the toxin. These data demonstrate that the amino-terminal and carboxyl-terminal repeat-containing regions of the MARTX_(Vv)toxin are necessary and sufficient for the delivery of effector domains and epithelial cell lysis in vitro but that effector domains are required for other cytopathic functions. Furthermore, Ca~(2+)-dependent secretion of the modified MARTX_(Vv)toxin suggests that nonclassical RTX-like repeats found in the carboxyl-terminal repeat-containing region are functionally similar to classical RTX repeats found in other RTX proteins. IMPORTANCE Up to 95% of deaths from seafood-borne infections in the United States are due solely to one pathogen, V.?vulnificus . Among its various virulence factors, the MARTX_(Vv)toxin has been characterized as a critical exotoxin for successful pathogenesis of V.?vulnificus in mouse infection models. Similarly to MARTX toxins of other pathogens, MARTX_(Vv)toxin is comprised of repeat-containing regions, central effector domains, and an autoprocessing cysteine protease domain. Yet how each of these regions contributes to essential activities of the toxins has not been fully identified for any of MARTX toxins. Using modified MARTX_(Vv)toxin fused with β-lactamase as a reporter enzyme, the portion(s) responsible for toxin secretion from bacteria, effector domain translocation into host cells, rapid host cell rounding, and necrotic host cell death was identified. The results are relevant for understanding how MARTX_(Vv)toxin serves as both a necrotic pore-forming toxin and an effector delivery platform.
机译:摘要创伤弧菌是海鲜传播的病原体,会破坏肠道上皮,导致细菌迅速传播并死亡。最重要的毒力因子是多功能自动加工毒素重复序列(MARTX)毒素,该毒素由位于中央区域的效应子结构域构成,两侧是长的重复序列区域,这些区域在MARTX毒素之间高度保守,并预计会转移效应子结构域。在这里,我们使用经修饰的V.?vulnificus MARTX(MARTX_(Vv))毒素检查了包含重复区域的作用,该毒素通过用β-内酰胺酶(Bla)取代所有内部效应子域而产生。在细菌分泌物中以及在中毒的上皮细胞的细胞质中都检测到了Bla活性。没有效应子域的修饰的MARTX_(Vv)毒素保留了其坏死活性,但失去了其细胞周围活性。此外,缺失含羧基末端重复序列的区域可阻止细菌分泌毒素。含有氨基末端重复序列的区域的缺失对分泌没有影响,但是完全消除了易位和坏死。酶的灭活毒素的半胱氨酸蛋白酶结构域都不会影响分泌和转运。这些数据证明,MARTX_(Vv)毒素的含氨基末端和羧基末端重复的区域对于在体外递送效应子结构域和上皮细胞裂解是必需的,并且是足够的,但是效应子结构域对于其他细胞病变功能是必需的。此外,修饰的MARTX_(Vv)毒素的Ca〜(2+)依赖性分泌表明,在含羧基末端重复序列的区域发现的非经典RTX样重复序列在功能上类似于在其他RTX蛋白中发现的经典RTX重复序列。重要信息在美国,高达95%的由海鲜传播的死亡均是由一种病原体V.?vulnificus造成的。在其各种毒力因子中,MARTX_(Vv)毒素已被表征为在小鼠感染模型中成功感染V.?vulnificus的关键外毒素。与其他病原体的MARTX毒素相似,MARTX_(Vv)毒素由包含重复区域,中枢效应域和自加工半胱氨酸蛋白酶域组成。然而,对于任何MARTX毒素,尚未完全确定这些区域中的每一个如何对毒素的基本活性作出贡献。使用与β-内酰胺酶融合的修饰的MARTX_(Vv)毒素作为报告酶,鉴定了负责细菌中毒素分泌,效应子结构域转移到宿主细胞,宿主细胞快速圆化和坏死宿主细胞死亡的部分。该结果与了解MARTX_(Vv)毒素如何同时充当坏死的造孔毒素和效应物递送平台有关。

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