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异源流感感染减轻了对二次细菌感染的易感性。

Heterotypic Influenza Infections Mitigate Susceptibility to Secondary Bacterial Infection.

机构信息

Department of Pediatrics, UPMC Children's Hospital of Pittsburgh, Pittsburgh, PA.

Department of Immunology, University of Pittsburgh, Pittsburgh, PA; and.

出版信息

J Immunol. 2022 Aug 15;209(4):760-771. doi: 10.4049/jimmunol.2200261. Epub 2022 Aug 1.

Abstract

Influenza-associated bacterial superinfections have devastating impacts on the lung and can result in increased risk of mortality. New strains of influenza circulate throughout the population yearly, promoting the establishment of immune memory. Nearly all individuals have some degree of influenza memory before adulthood. Due to this, we sought to understand the role of immune memory during bacterial superinfections. An influenza heterotypic immunity model was established using influenza A/Puerto Rico/8/34 and influenza A/X31. We report in this article that influenza-experienced mice are more resistant to secondary bacterial infection with methicillin-resistant as determined by wasting, bacterial burden, pulmonary inflammation, and lung leak, despite significant ongoing lung remodeling. Multidimensional flow cytometry and lung transcriptomics revealed significant alterations in the lung environment in influenza-experienced mice compared with naive animals. These include changes in the lung monocyte and T cell compartments, characterized by increased expansion of influenza tetramer-specific CD8 T cells. The protection that was seen in the memory-experienced mouse model is associated with the reduction in inflammatory mechanisms, making the lung less susceptible to damage and subsequent bacterial colonization. These findings provide insight into how influenza heterotypic immunity reshapes the lung environment and the immune response to a rechallenge event, which is highly relevant to the context of human infection.

摘要

流感相关细菌合并感染对肺部有严重影响,并可能增加死亡率。新的流感株每年在人群中传播,促进了免疫记忆的建立。几乎所有成年人在成年前都有一定程度的流感记忆。因此,我们试图了解免疫记忆在细菌合并感染中的作用。我们使用流感 A/Puerto Rico/8/34 和流感 A/X31 建立了流感异型免疫模型。在本文中我们报告称,与未感染过流感的小鼠相比,感染过流感的小鼠对耐甲氧西林金黄色葡萄球菌的二次细菌感染具有更强的抵抗力,表现在消瘦、细菌负荷、肺部炎症和肺漏方面,尽管肺部仍存在持续的重塑。多维流式细胞术和肺部转录组学显示,与未感染过流感的动物相比,感染过流感的小鼠肺部环境发生了显著变化。这些变化包括肺单核细胞和 T 细胞区室的变化,其特征是流感四聚体特异性 CD8 T 细胞的扩增增加。在记忆体验小鼠模型中观察到的保护作用与炎症机制的减少有关,这使肺部不易受到损伤和随后的细菌定植。这些发现为了解流感异型免疫如何重塑肺部环境和对再挑战事件的免疫反应提供了线索,这与人类感染的情况密切相关。

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