MRC Centre for Molecular Bacteriology and Infection, Department of Life Sciences, Imperial College London, London, United Kingdom.
Division of Cancer Biology, The Institute of Cancer Research London, London, United Kingdom.
PLoS Pathog. 2018 Oct 26;14(10):e1007406. doi: 10.1371/journal.ppat.1007406. eCollection 2018 Oct.
Infection with Citrobacter rodentium triggers robust tissue damage repair responses, manifested by secretion of IL-22, in the absence of which mice succumbed to the infection. Of the main hallmarks of C. rodentium infection are colonic crypt hyperplasia (CCH) and dysbiosis. In order to colonize the host and compete with the gut microbiota, C. rodentium employs a type III secretion system (T3SS) that injects effectors into colonic intestinal epithelial cells (IECs). Once injected, the effectors subvert processes involved in innate immune responses, cellular metabolism and oxygenation of the mucosa. Importantly, the identity of the effector/s triggering the tissue repair response is/are unknown. Here we report that the effector EspO ,an orthologue of OspE found in Shigella spp, affects proliferation of IECs 8 and 14 days post C. rodentium infection as well as secretion of IL-22 from colonic explants. While we observed no differences in the recruitment of group 3 innate lymphoid cells (ILC3s) and T cells, which are the main sources of IL-22 at the early and late stages of C. rodentium infection respectively, infection with ΔespO was characterized by diminished recruitment of sub-mucosal neutrophils, which coincided with lower abundance of Mmp9 and chemokines (e.g. S100a8/9) in IECs. Moreover, mice infected with ΔespO triggered significantly lesser nutritional immunity (e.g. calprotectin, Lcn2) and expression of antimicrobial peptides (Reg3β, Reg3γ) compared to mice infected with WT C. rodentium. This overlapped with a decrease in STAT3 phosphorylation in IECs. Importantly, while the reduced CCH and abundance of antimicrobial proteins during ΔespO infection did not affect C. rodentium colonization or the composition of commensal Proteobacteria, they had a subtle consequence on Firmicutes subpopulations. EspO is the first bacterial virulence factor that affects neutrophil recruitment and secretion of IL-22, as well as expression of antimicrobial and nutritional immunity proteins in IECs.
柠檬酸杆菌感染会引发强烈的组织损伤修复反应,表现为白细胞介素 22(IL-22)的分泌,而缺乏这种反应的小鼠则会死于感染。柠檬酸杆菌感染的主要特征包括结肠隐窝增生(CCH)和菌群失调。为了在宿主中定植并与肠道微生物群竞争,柠檬酸杆菌利用一种 III 型分泌系统(T3SS)将效应物注入结肠肠上皮细胞(IECs)。一旦注入,这些效应物颠覆了先天免疫反应、细胞代谢和粘膜氧合过程。重要的是,触发组织修复反应的效应物的身份尚不清楚。在这里,我们报告说效应物 EspO,一种与志贺氏菌属中发现的 OspE 同源的蛋白,会影响柠檬酸杆菌感染后第 8 天和第 14 天 IEC 的增殖以及结肠外植体中白细胞介素 22 的分泌。虽然我们没有观察到 3 组固有淋巴细胞(ILC3s)和 T 细胞募集的差异,它们分别是柠檬酸杆菌感染早期和晚期 IL-22 的主要来源,但感染 ΔespO 的特征是粘膜下中性粒细胞募集减少,同时 IECs 中的 Mmp9 和趋化因子(如 S100a8/9)丰度降低。此外,与感染 WT 柠檬酸杆菌的小鼠相比,感染 ΔespO 的小鼠触发的营养免疫(如钙卫蛋白、Lcn2)和抗菌肽(Reg3β、Reg3γ)的表达显著减少。这与 IECs 中 STAT3 磷酸化的减少相吻合。重要的是,虽然在 ΔespO 感染期间 CCH 减少和抗菌蛋白丰度降低不会影响柠檬酸杆菌的定植或共生变形杆菌的组成,但它们对厚壁菌门亚群有微妙的影响。EspO 是第一个影响中性粒细胞募集和白细胞介素 22 分泌以及 IECs 中抗菌和营养免疫蛋白表达的细菌毒力因子。
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