Antitumor adaptive immunity remains intact following inhibition of autophagy and antimalarial treatment
Hanna Starobinets, … , Matthew Krummel, Jayanta Debnath
Hanna Starobinets, … , Matthew Krummel, Jayanta Debnath
Published October 24, 2016
Citation Information: J Clin Invest. 2016;126(12):4417-4429. https://doi.org/10.1172/JCI85705.
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Research Article Immunology Oncology Article has an altmetric score of 32

Antitumor adaptive immunity remains intact following inhibition of autophagy and antimalarial treatment

Abstract

The rising success of cancer immunotherapy has produced immense interest in defining the clinical contexts that may benefit from this therapeutic approach. To this end, there is a need to ascertain how the therapeutic modulation of intrinsic cancer cell programs influences the anticancer immune response. For example, the role of autophagy as a tumor cell survival and metabolic fitness pathway is being therapeutically targeted in ongoing clinical trials that combine cancer therapies with antimalarial drugs for the treatment of a broad spectrum of cancers, many of which will likely benefit from immunotherapy. However, our current understanding of the interplay between autophagy and the immune response remains incomplete. Here, we have evaluated how autophagy inhibition impacts the antitumor immune response in immune-competent mouse models of melanoma and mammary cancer. We observed equivalent levels of T cell infiltration and function within autophagy-competent and -deficient tumors, even upon treatment with the anthracycline chemotherapeutic doxorubicin. Similarly, we found equivalent T cell responses upon systemic treatment of tumor-bearing mice with antimalarial drugs. Our findings demonstrate that antitumor adaptive immunity is not adversely impaired by autophagy inhibition in these models, allowing for the future possibility of combining autophagy inhibitors with immunotherapy in certain clinical contexts.

Authors

Hanna Starobinets, Jordan Ye, Miranda Broz, Kevin Barry, Juliet Goldsmith, Timothy Marsh, Fanya Rostker, Matthew Krummel, Jayanta Debnath

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Figure 6

Antimalarial-treated tumors exhibit equivalent T cell responses.

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Antimalarial-treated tumors exhibit equivalent T cell responses. Subcuta...
Subcutaneous B16 melanomas were raised in GREAT reporter mice and orthotopic 4T1 mammary tumors in WT BALB/c mice. Primary tumors were allowed to form for 7–10 days and were subsequently treated daily with chloroquine, quinacrine, or vehicle control by i.p. injection. (A) Primary tumor growth of B16 (n = 5 per cohort) and 4T1 tumors (Vehicle, n = 9; Chloroquine, n = 9; Quinacrine, n = 8) as assessed by caliper measurements of tumor area. Error bars represent SD, and arrows indicate treatment days. (B) Autophagy deficiency was confirmed in resected B16 tumors by immunofluorescence for P62, and accumulation of P62 aggregates was quantified. Error bars represent SD; ***P < 0.001 using unpaired t test. (C) Infiltration and functional phenotype of CD4+ and CD8+ T cell populations were measured by flow cytometry in vehicle- and chloroquine-treated B16 tumors. Data points represent distinct tumors from individual mice; bars represent mean values with 2-way ANOVA not significant. (D) Infiltration and activation of CD4+ and CD8+ T cell populations were measured by flow cytometry in vehicle-, chloroquine-, and quinacrine-treated 4T1 tumors. Data points represent distinct tumors from individual mice, and bars represent mean values with 2-way ANOVA not significant.