Anticancer immunotherapy by CTLA-4 blockade relies on the gut microbiota

Marie Vétizou; Jonathan M. Pitt; Romain Daillère; Patricia Lepage; Nadine Waldschmitt; Caroline Flament; Sylvie Rusakiewicz; Bertrand Routy; María P. Roberti; Connie P.M. Duong; Vichnou Poirier-Colame; Antoine Roux; Sonia Becharef; Silvia C. Formenti; Encouse B. Golden; Sascha Cording; Gérard Eberl; Andreas Schlitzer; Florent Ginhoux; Sridhar Mani; Takahiro Yamazaki; Nicolas Jacquelot; David Enot; M Bérard; Jérôme Nigou; Paule Opolon; Alexander Eggermont; Paul‐Louis Woerther; Élisabeth Chachaty; Nathalie Chaput; Caroline Robert; Christina Mateus; Guido Guido Kroemer; Didier Raoult; Ivo G. Boneca; Franck Carbonnel; Mathias Chamaillard; Laurence Zitvogel

doi:10.1126/science.aad1329

Abstract

1 min read

Gut microbes affect immunotherapy The unleashing of antitumor T cell responses has ushered in a new era of cancer treatment. Although these therapies can cause dramatic tumor regressions in some patients, many patients inexplicably see no benefit. Mice have been used in two studies to investigate what might be happening. Specific members of the gut microbiota influence the efficacy of this type of immunotherapy (see the Perspective by Snyder et al. ). Vétizou et al. found that optimal responses to anticytotoxic T lymphocyte antigen blockade required specific Bacteroides spp. Similarly, Sivan et al. discovered that Bifidobacterium spp. enhanced the efficacy of antiprogrammed cell death ligand 1 therapy. Science , this issue, p. 1079 and p. 1084 ; see also p. 1031

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