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白细胞介素-22 诱导的细胞外排和白细胞介素-18 诱导的细胞死亡可预防和治疗轮状病毒感染。

IL-22-induced cell extrusion and IL-18-induced cell death prevent and cure rotavirus infection.

机构信息

Center for Inflammation, Immunity and Infection, Institute for Biomedical Sciences Georgia State University, Atlanta, GA 30303 USA.

Université Clermont Auvergne, INRAe, UMR 454 MEDIS, F-63000 Clermont-Ferrand, France.

出版信息

Sci Immunol. 2020 Oct 2;5(52). doi: 10.1126/sciimmunol.abd2876.

Abstract

Bacterial flagellin can elicit production of TLR5-mediated IL-22 and NLRC4-mediated IL-18 cytokines that act in concert to cure and prevent rotavirus (RV) infection. This study investigated the mechanism by which these cytokines act to impede RV. Although IL-18 and IL-22 induce each other's expression, we found that IL-18 and IL-22 both impeded RV independently of one another and did so by distinct mechanisms that involved activation of their cognate receptors in intestinal epithelial cells (IEC). IL-22 drove IEC proliferation and migration toward villus tips, which resulted in increased extrusion of highly differentiated IEC that serve as the site of RV replication. In contrast, IL-18 induced cell death of RV-infected IEC thus directly interrupting the RV replication cycle, resulting in spewing of incompetent virus into the intestinal lumen and causing a rapid drop in the number of RV-infected IEC. Together, these actions resulted in rapid and complete expulsion of RV, even in hosts with severely compromised immune systems. These results suggest that a cocktail of IL-18 and IL-22 might be a means of treating viral infections that preferentially target short-lived epithelial cells.

摘要

细菌鞭毛蛋白可引发 TLR5 介导的 IL-22 和 NLRC4 介导的 IL-18 细胞因子的产生,这些细胞因子协同作用以治愈和预防轮状病毒 (RV) 感染。本研究探讨了这些细胞因子发挥作用以阻碍 RV 的机制。尽管 IL-18 和 IL-22 相互诱导对方的表达,但我们发现 IL-18 和 IL-22 均可独立于彼此阻碍 RV,并且通过涉及在肠上皮细胞 (IEC) 中激活其同源受体的不同机制来实现。IL-22 驱动 IEC 向绒毛尖端增殖和迁移,从而增加了作为 RV 复制部位的高度分化 IEC 的排出。相比之下,IL-18 诱导 RV 感染的 IEC 死亡,从而直接中断 RV 复制周期,导致无能力的病毒喷射到肠腔中,并导致 RV 感染的 IEC 数量迅速下降。总之,这些作用导致 RV 迅速而完全的排出,即使在免疫系统严重受损的宿主中也是如此。这些结果表明,IL-18 和 IL-22 的混合物可能是治疗优先靶向寿命短的上皮细胞的病毒感染的一种手段。

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