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The intrinsic expression of NLRP3 in Th17 cells promotes their protumor activity and conversion into Tregs 被引量:1
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作者 Théo Accogli Christophe Hibos +15 位作者 Lylou Milian Mannon Geindreau Corentin Richard Etienne Humblin Romain Mary Sandy Chevrier Elise Jacquin Antoine Bernard Fanny Chalmin Catherine Paul Berhard Ryffel Lionel Apetoh Romain Boidot Mélanie Bruchard François Ghiringhelli Frédérique Vegran 《Cellular & Molecular Immunology》 2025年第5期541-556,共16页
Th17 cells can perform either regulatory or inflammatory functions depending on the cytokine microenvironment.These plastic cells can transdifferentiate into Tregs during inflammation resolution,in allogenic heart tra... Th17 cells can perform either regulatory or inflammatory functions depending on the cytokine microenvironment.These plastic cells can transdifferentiate into Tregs during inflammation resolution,in allogenic heart transplantation models,or in cancer through mechanisms that remain poorly understood.Here,we demonstrated that NLRP3 expression in Th17 cells is essential for maintaining their immunosuppressive functions through an inflammasome-independent mechanism.In the absence of NLRP3,Th17 cells produce more inflammatory cytokines(IFNγ,Granzyme B,TNFα)and exhibit reduced immunosuppressive activity toward CD8+cells.Moreover,the capacity of NLRP3-deficient Th17 cells to transdifferentiate into Treg-like cells is lost.Mechanistically,NLRP3 in Th17 cells interacts with the TGF-βreceptor,enabling SMAD3 phosphorylation and thereby facilitating the acquisition of immunosuppressive functions.Consequently,the absence of NLRP3 expression in Th17 cells from tumor-bearing mice enhances CD8+T-cell effectiveness,ultimately inhibiting tumor growth. 展开更多
关键词 Th17 cells TREGS NLRP3 Tumor microenvironment Cancer Immunology
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