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PPARδ inhibition blocks the induction and function of tumor-induced IL-10 + regulatory B cells and enhances cancer immunotherapy.

Chen ChenJianan MaChenchen PiWei HuangTao ZhangCong FuWentao LiuYong-Guang Yang
Published in: Cell discovery (2023)
IL-10 + regulatory B cells (Bregs) play a significant role in cancer immunotherapy and their presence is an indicator of negative outcome. We found that PPARδ is significantly upregulated in tumor-induced IL-10 + Bregs with a phenotype of CD19 + CD24 hi IgD lo/- CD38 lo or CD19 + CD24 hi IgD lo/- CD38 hi in both mice and humans, and the level of PPARδ expression was correlated with their potential to produce IL-10 and to inhibit T cell activation. Genetic inactivation of PPARδ in B cells impaired the development and function of IL-10 + B cells, and treatment with PPARδ inhibitor diminished the induction of IL-10 + Bregs by tumor and CD40 engagement. Importantly, immunotherapy with anti-CD40 or anti-PD1 antibody achieved a markedly improved outcome in tumor-bearing mice with PPARδ deficiency in B cells or treated with PPARδ inhibitor. This study shows that PPARδ is required for the development and function of IL-10 + Bregs, providing a new and effective target for selectively blocking Bregs and improving antitumor immunotherapy.
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