Gut microbiota modulates adoptive cell therapy via CD8α dendritic cells and IL-12
Mireia Uribe-Herranz, … , Carl H. June, Andrea Facciabene
Mireia Uribe-Herranz, … , Carl H. June, Andrea Facciabene
Published February 22, 2018
Citation Information: JCI Insight. 2018;3(4):e94952. https://doi.org/10.1172/jci.insight.94952.
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Research Article Immunology Microbiology

Gut microbiota modulates adoptive cell therapy via CD8α dendritic cells and IL-12

Abstract

Adoptive T cell therapy (ACT) is a promising new modality for malignancies. Here, we report that adoptive T cell efficacy in tumor-bearing mice is significantly affected by differences in the native composition of the gut microbiome or treatment with antibiotics, or by heterologous fecal transfer. Depletion of bacteria with vancomycin decreased the rate of tumor growth in mice from The Jackson Laboratory receiving ACT, whereas treatment with neomycin and metronidazole had no effect, indicating the role of specific bacteria in host response. Vancomycin treatment induced an increase in systemic CD8α+ DCs, which sustained systemic adoptively transferred antitumor T cells in an IL-12–dependent manner. In subjects undergoing allogeneic hematopoietic cell transplantation, we found that oral vancomycin also increased IL-12 levels. Collectively, our findings demonstrate an important role played by the gut microbiota in the antitumor effectiveness of ACT and suggest potentially new avenues to improve response to ACT by altering the gut microbiota.

Authors

Mireia Uribe-Herranz, Kyle Bittinger, Stavros Rafail, Sonia Guedan, Stefano Pierini, Ceylan Tanes, Alex Ganetsky, Mark A. Morgan, Saar Gill, Janos L. Tanyi, Frederic D. Bushman, Carl H. June, Andrea Facciabene

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Figure 7

Vancomycin treatment increases the number of systemic CD8α+ DC.

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Vancomycin treatment increases the number of systemic CD8α+ DC. Jackson ...
Jackson mice were treated for 10 days with antibiotics. (A) Phenotype analysis of splenic DC population by flow cytometry, CD8α+ DC subset shown (CD11chighCD8+B220CD11b). (B) Il12a RNA expression of purified CD11c+ DC (pooled by group). (C) Mouse IL-12p70 protein serum levels. (D) Human IL-12p70 serum levels on patients undergoing the same therapy, allogeneic hematopoietic cell transplantation, and treated with vancomycin. (E) E749–57 IFN-γ ELISPOT of purified CD11c+ DCs from not treated (control), treated with Neo/Met or vancomycin (± the addition of 1 μg/ml of blocking monoclonal antibody IL-12p70) mice and incubated with T cells from immunized mice. Mouse data is representative of 3 independent experiments with 4–9 mice per group. Each dot represents a mouse; means ± SEM are shown. A multiple t test analysis was performed. *P < 0.05, ***P < 0.001.