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GM-CSF Tc17 细胞在不引起明显病理的情况下增强疫苗对致命真菌性肺炎的免疫。

GM-CSF Tc17 cells are required to bolster vaccine immunity against lethal fungal pneumonia without causing overt pathology.

机构信息

Department of Pathobiology, University of Illinois at Urbana-Champaign, Urbana, IL 61802, USA.

Veterinary Diagnostic Laboratory, University of Illinois at Urbana-Champaign, Urbana, IL 61802, USA.

出版信息

Cell Rep. 2022 Oct 25;41(4):111543. doi: 10.1016/j.celrep.2022.111543.

Abstract

GM-CSF co-expressing T17 cells instigate pathologic inflammation during autoimmune disorders, but their function in immunity to infections is unclear. Here, we demonstrate the role of GM-CSFTc17 cells for vaccine immunity against lethal fungal pneumonia and the cytokine requirements for their induction and memory homeostasis. Vaccine-induced GM-CSF Tc17 cells are necessary to bolster pulmonary fungal immunity without inflating pathology. Although GM-CSF expressing Tc17 cells preferentially elevate during the memory phase, their phenotypic attributes strongly suggest they are more like Tc17 cells than IFNγ-producing Tc1 cells. IL-1 and IL-23, but not GM-CSF, are necessary to elicit GM-CSF Tc17 cells following vaccination. IL-23 is dispensable for memory Tc17 and GM-CSF Tc17 cell maintenance, but recall responses of effector or memory Tc17 cells in the lung require it. Our study reveals the beneficial, nonpathological role of GM-CSF Tc17 cells during fungal vaccine immunity.

摘要

GM-CSF 共表达 T17 细胞在自身免疫性疾病中引发病理性炎症,但它们在抗感染免疫中的作用尚不清楚。在这里,我们证明了 GM-CSF Tc17 细胞在对抗致命真菌性肺炎的疫苗免疫中的作用,以及诱导和记忆稳态所需的细胞因子。疫苗诱导的 GM-CSF Tc17 细胞对于增强肺部真菌免疫是必要的,而不会增加病理学。尽管 GM-CSF 表达的 Tc17 细胞在记忆阶段优先升高,但它们的表型特征强烈表明它们更像是 Tc17 细胞,而不是 IFNγ 产生的 Tc1 细胞。IL-1 和 IL-23,但不是 GM-CSF,是接种疫苗后产生 GM-CSF Tc17 细胞所必需的。IL-23 对于记忆性 Tc17 和 GM-CSF Tc17 细胞的维持是可有可无的,但在肺部中效应或记忆性 Tc17 细胞的回忆反应需要它。我们的研究揭示了 GM-CSF Tc17 细胞在真菌疫苗免疫中的有益的、非病理性作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bdbc/9641983/a6f77ab958d8/nihms-1845187-f0002.jpg

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