RIP2在肺炎链球菌感染的凋亡细胞efferocysis过程中促进CD4+ T细胞IFN-γ的产生

Victoria Eugenia Niño-Castaño, Letícia de Aquino Penteado, Ludmilla Silva-Pereira, Júlia Miranda Ribeiro Bazzano, Allan Botinhon Orlando, Ana Carolina Guerta Salina, Naiara Naiana Dejani, Vânia L D Bonato, C Henrique Serezani, Alexandra Ivo Medeiros
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引用次数: 4

摘要

在efferocytosis过程中,专业和非专业吞噬细胞对凋亡细胞的清除对保持组织稳态至关重要。树突状细胞摄取凋亡细胞产生调节性T细胞并诱导对自身抗原的免疫耐受。相反,摄入受感染的凋亡细胞可促进TLR4/ myd88依赖性骨髓源性树突状细胞(bmdc)的激活,并触发Th17细胞分化。在这项研究中,我们评估了C57BL/6小鼠来源的BMDCs感染的肺炎链球菌感染的凋亡细胞efferocysis对CD4+ T细胞亚群分化和扩增的影响,以及TLR2/4和受体相互作用蛋白2 (receptor-interacting protein 2, RIP2)受体在efferocysis过程中识别细胞内病原体的作用。我们证明了bmdc介导的肺链球菌感染的凋亡细胞的efferocysis诱导Th1细胞分化和扩增。虽然BMDCs中TLR2/4和RIP2的缺乏不会影响Th1细胞在efferocytosis期间的分化,但RIP2的缺乏会降低CD4 T细胞在扩增期产生的IFN-γ。这些发现表明,rip2介导的IL-1β产生在肺炎链球菌感染的凋亡细胞的efferocysis过程中部分支持th1介导的IFN-γ产生微环境。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
RIP2 Contributes to Expanded CD4+ T Cell IFN-γ Production during Efferocytosis of Streptococcus pneumoniae-Infected Apoptotic Cells.

Apoptotic cell clearance by professional and nonprofessional phagocytes in the process of efferocytosis is critical to preserve tissue homeostasis. Uptake of apoptotic cells by dendritic cells generates regulatory T cells and induces immunologic tolerance against self-antigens. In contrast, ingestion of infected apoptotic cells promotes activation of TLR4/MyD88-dependent bone marrow-derived dendritic cells (BMDCs) and triggers Th17 cell differentiation. In this study, we evaluated the impact of Streptococcus pneumoniae-infected apoptotic cell efferocytosis by BMDCs derived from C57BL/6 mice on differentiation and expansion of CD4+ T cell subsets, as well as the role of TLR2/4 and receptor-interacting protein 2 (RIP2) receptors in recognizing intracellular pathogens during efferocytosis. We demonstrated that BMDC-mediated efferocytosis of S. pneumoniae-infected apoptotic cells induced Th1 cell differentiation and expansion. Although TLR2/4 and RIP2 deficiency in BMDCs did not affect Th1 cell differentiation during efferocytosis, the absence of RIP2 decreased IFN-γ production by CD4 T cells during the expansion phase. These findings suggest that RIP2-mediated IL-1β production during efferocytosis of S. pneumoniae-infected apoptotic cells partially supports a Th1-mediated IFN-γ production microenvironment.

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