先天性淋巴细胞
先天免疫系统
免疫
免疫学
生物
细胞生物学
免疫系统
作者
Wei Yang,Sílvia Pires,Seun Oguntunmibi,Gretchen E. Diehl,Brian T. Edelson,Randy Longman
出处
期刊:Journal of Immunology
[American Association of Immunologists]
日期:2024-05-01
卷期号:212 (1_Supplement): 0393_5158-0393_5158
标识
DOI:10.4049/jimmunol.212.supp.0393.5158
摘要
Abstract A central feature of intestinal mucosal immune system is the ability enable antigen specific tolerance to the gut bacteria. Genetic variants in TNFSF15 (which encodes protein TL1A) are linked to inflammatory bowel disease and have implicated roles for TL1A in regulating both T cell and innate lymphoid cells (ILC), but how these cellular pathways coordinate a response to limit intestinal inflammation is not completely understood. Deletion of TL1A receptor Tnfrsf25 (also called DR3), we demonstrate that TL1A signaling is required for efficient generation of RORγt+Foxp3+ intestinal iTregs at steady state. To investigate if this response resulted from DR3 deletion in T cells or the potential role for DR3 signaling in ILCs to regulate iTregs indirectly, we generated antigen specific transgenic T cells to H. Hepaticus (Hh) with DR3 deletion. Our results reveal that TL1A signaling is dispensable on T cells but required on ILC3s to regulate the balance between intestinal iTreg and inflammatory Th17 cells. RNA sequencing of ILC3s revealed the induction of Bhlhe40 in response to TL1A stimulation. Using conditional deletion models, we defined Bhlhe40 as a transcriptional regulator of ILC3 expression of Tnfsf4 (OX40L) and the subsequent requirement for ILC3-specific Bhlhe40 and Tnfsf4 in promoting Hh-specific Treg induction. These data reveal a novel function for TL1A and downstream transcription factor Bhlhe40 in enabling ILC3 coordination of gut commensal T cell immunity.
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