Systemic short chain fatty acids limit antitumor effect of CTLA-4 blockade in hosts with cancer

Author:

Coutzac CléliaORCID,Jouniaux Jean-Mehdi,Paci AngeloORCID,Schmidt Julien,Mallardo DomenicoORCID,Seck Atmane,Asvatourian Vahe,Cassard LydieORCID,Saulnier Patrick,Lacroix Ludovic,Woerther Paul-Louis,Vozy Aurore,Naigeon Marie,Nebot-Bral Laetitia,Desbois MélanieORCID,Simeone Ester,Mateus Christine,Boselli Lisa,Grivel Jonathan,Soularue Emilie,Lepage PatriciaORCID,Carbonnel Franck,Ascierto Paolo AntonioORCID,Robert CarolineORCID,Chaput NathalieORCID

Abstract

AbstractGut microbiota composition influences the clinical benefit of immune checkpoints in patients with advanced cancer but mechanisms underlying this relationship remain unclear. Molecular mechanism whereby gut microbiota influences immune responses is mainly assigned to gut microbial metabolites. Short-chain fatty acids (SCFA) are produced in large amounts in the colon through bacterial fermentation of dietary fiber. We evaluate in mice and in patients treated with anti-CTLA-4 blocking mAbs whether SCFA levels is related to clinical outcome. High blood butyrate and propionate levels are associated with resistance to CTLA-4 blockade and higher proportion of Treg cells. In mice, butyrate restrains anti-CTLA-4-induced up-regulation of CD80/CD86 on dendritic cells and ICOS on T cells, accumulation of tumor-specific T cells and memory T cells. In patients, high blood butyrate levels moderate ipilimumab-induced accumulation of memory and ICOS + CD4 + T cells and IL-2 impregnation. Altogether, these results suggest that SCFA limits anti-CTLA-4 activity.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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