Litcius/Paper detail

Microbiome-derived inosine modulates response to checkpoint inhibitor immunotherapy

Lukas F. Mager, Regula Burkhard, Nicola Pett, Noah C.A. Cooke, Kirsty Brown, Hena R. Ramay, Seungil Paik, John Stagg, Ryan A. Groves, Marco Gallo, Ian A. Lewis, Markus B. Geuking, Kathy D. McCoy

2020Science1,343 citationsDOI

Abstract

Inosine modulates antitumor immunity Checkpoint blockade immunotherapy harnesses the immune system to kill cancer cells and has been used with great success to treat certain tumors, but not all cancer patients respond. The efficacy of checkpoint blockade immunotherapy has been shown to depend on the presence of distinct, beneficial bacteria residing in the gut of patients, but how the microbiome mediates such beneficial effects is unclear. Mager et al. found that specific bacteria produce a metabolite called inosine that enhances the effect of checkpoint blockade immunotherapy (see the Perspective by Shaikh and Sears). In mouse models, inosine, together with proinflammatory stimuli and immunotherapy, strongly enhanced the antitumor capacities of T cells in multiple tumor types, including colorectal cancer, bladder cancer, and melanoma. Science , this issue p. 1481 ; see also p. 1427

Topics & Concepts

InosineImmunotherapyMicrobiomeComputational biologyChemistryBiologyImmunologyImmune systemBioinformaticsBiochemistryAdenosineCancer Immunotherapy and BiomarkersAdenosine and Purinergic SignalingImmune Cell Function and Interaction