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Insights into the Cross-Immunity Mechanism within Effector Families of Bacteria Type VI Secretion System from the Structure of StTae4-EcTai4 Complex

机译:从StTae4-EcTai4复合体的结构了解细菌类型VI分泌系统的效应器家族中的交叉免疫机制。

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摘要

The Gram-negative bacteria type VI secretion system (T6SS) has been found to play an important role in interbacterial competition, biofilm formation and many other virulence-related processes. The bacteria harboring T6SS inject the effectors into their recipient’s cytoplasm or periplasm to kill them and meanwhile, to avoid inhibiting itself, the cognate immunity proteins were produced to acts as the effector inhibitor. Tae4 (type VI amidase effector 4) and Tai4 (type VI amidase immunity 4) are newly identified T6SS effector-immunity (EI) pairs. We have recently solved the structures of StTae4-Tai4 and EcTae4-Tai4 complexes from the human pathogens Salmonella typhimurium and Enterobacter cloacae, respectively. It is very interesting and important to discover whether there is cross-neutralization between St- and EcTai4 and whether their effector inhibition mechanism is conserved. Here, we determined the crystal structure of StTae4 in complex with EcTai4. The solution conformation study revealed it is a compact heterotetramer that consists of an EcTai4 homodimer binding two StTae4 molecules in solution, different from that in crystal. A remarkable shift can be observed in both the flexible winding loop of StTae4 and protruding loop of EcTai4 and disulfide bonds are formed to stabilize their overall conformations. The in vitro and in vivo interactions studies showed EcTai4 can efficiently rescue the cells from the toxicity of its cognate effectors StTae4, but can not neutralize the toxic activities of the effectors from other families. These findings provide clear structural evidence to support the previous observation of cross-immunity within T6SS families and provide a basis for understanding their important roles in polymicrobial environments.
机译:已发现革兰氏阴性细菌VI型分泌系统(T6SS)在细菌间竞争,生物膜形成和许多其他与毒力相关的过程中起着重要作用。携带T6SS的细菌将效应子注入受体的细胞质或周质中以杀死它们,同时,为了避免自身抑制,产生了相关的免疫蛋白作为效应子抑制剂。 Tae4(VI型酰胺酶效应物4)和Tai4(VI型酰胺酶效应物4)是新近鉴定的T6SS效应物-免疫(EI)对。我们最近从人类病原体鼠伤寒沙门氏菌和阴沟肠杆菌分别解析了StTae4-Tai4和EcTae4-Tai4复合物的结构。发现St-和EcTai4之间是否存在交叉中和作用以及它们的效应抑制机制是否保守是非常有趣和重要的。在这里,我们确定了与EcTai4复合的StTae4的晶体结构。溶液构象研究表明,它是一种紧凑的异源四聚体,由与溶液中两个StTae4分子结合的EcTai4同型二聚体组成,与晶体中的分子不同。在StTae4的柔性缠绕环和EcTai4的突出环中都可以观察到明显的变化,并且形成了二硫键以稳定它们的整体构象。体内外相互作用研究表明,EcTai4可以有效地拯救细胞,使其同源效应物StTae4免受毒性作用,但不能中和其他家族效应物的毒性作用。这些发现提供了明确的结构证据,以支持先前对T6SS家族中交叉免疫的观察,并为了解其在多微生物环境中的重要作用提供了基础。

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