期刊论文详细信息
Journal of Leukocyte Biology: An Official Publication of the Reticuloendothelial Society
IL‐10 producing CD8+ CD122+ PD‐1+ regulatory T cells are expanded by dendritic cells silenced for Allograft Inflammatory Factor‐1
article
Diana M. Elizondo1  Temesgen E. Andargie1  Naomi L. Haddock1  Ricardo L. Louzada da Silva2  Tatiana Rodrigues de Moura2  Michael W. Lipscomb1 
[1] Department of Biology Howard University Washington DC USA;Laboratório de Biologia Molecular‐Hospital Universitário Universidade Federal de Sergipe‐Aracaju Sergipe Brazil
关键词: cytotoxic T cells;    dendritic cells;    programmed death‐1;    suppression;    tolerogenic;    Tregs;   
DOI  :  10.1002/JLB.1A0118-010RR
学科分类:生理学
来源: Federation of American Societies for Experimental Biology
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【 摘 要 】

Allograft Inflammatory Factor‐1 (AIF1) is a cytoplasmic scaffold protein that contains Ca2+ binding EF‐hand and PDZ interaction domains important for mediating intracellular signaling complexes in immune cells. The protein plays a dominant role in both macrophage‐ and dendritic cell (DC)‐mediated inflammatory responses. This study now reports that AIF1 expression in DC is important in directing CD8+ T cell effector responses. Silencing AIF1 expression in murine CD11c+ DC suppressed antigen‐specific CD8+ T cell activation, marked by reduced CXCR3, IFNγ and Granzyme B expression, and restrained proliferation. These primed CD8+ T cells had impaired cytotoxic killing of target cells in vitro. In turn, studies identified that AIF1 silencing in DC robustly expanded IL‐10 producing CD8+ CD122+ PD‐1+ regulatory T cells that suppressed neighboring immune effector responses through both IL‐10 and PD‐1‐dependent mechanisms. In vivo studies recapitulated bystander suppression of antigen‐responsive CD4+ T cells by the CD8+ Tregs expanded from the AIF1 silenced DC. These studies further demonstrate that AIF1 expression in DC serves as a potent governor of cognate T cell responses and present a novel target for engineering tolerogenic DC‐based immunotherapies.

【 授权许可】

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