Durable anticancer immunity from intratumoral administration of IL-23, IL-36γ, and OX40L mRNAs

细胞因子 免疫 趋化因子 CD8型 生物 肿瘤微环境 细胞毒性T细胞 免疫学 T细胞 免疫疗法 癌症研究 免疫系统 体外 生物化学
作者
Susannah L. Hewitt,Ailin Bai,D. R. Shackleton Bailey,Kana Ichikawa,John Zielinski,Russell Karp,Ameya Apte,Kristen Arnold,Sima J. Zacharek,Maria S. Iliou,Khushbu Bhatt,Maija K. Garnaas,Faith Musenge,Ashley N. Davis,Nikhil Khatwani,Stephen Su,Graham MacLean,Samuel J. Farlow,Kristine Burke,Joshua P. Frederick
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science (AAAS)]
卷期号:11 (477) 被引量:213
标识
DOI:10.1126/scitranslmed.aat9143
摘要

Many solid cancers contain dysfunctional immune microenvironments. Immune system modulators that initiate responses to foreign pathogens could be promising candidates for reigniting productive responses toward tumors. Interleukin-1 (IL-1) and IL-12 cytokine family members cooperate at barrier tissues after microbial invasion, in human inflammatory diseases, and in antitumoral immunity. IL-36γ, in classic alarmin fashion, acts in damaged tissues, whereas IL-23 centrally coordinates immune responses to danger signals. In this study, direct intratumoral delivery of messenger RNAs (mRNAs) encoding these cytokines produced robust anticancer responses in a broad range of tumor microenvironments. The addition of mRNA encoding the T cell costimulator OX40L increased complete response rates in treated and untreated distal tumors compared to the cytokine mRNAs alone. Mice exhibiting complete responses were subsequently protected from tumor rechallenge. Treatments with these mRNA mixtures induced downstream cytokine and chemokine expression, and also activated multiple dendritic cell (DC) and T cell types. Consistent with this, efficacy was dependent on Batf3-dependent cross-presenting DCs and cytotoxic CD8+ T cells. IL-23/IL-36γ/OX40L triplet mRNA mixture triggered substantial immune cell recruitment into tumors, enabling effective tumor destruction irrespective of previous tumoral immune infiltrates. Last, combining triplet mRNA with checkpoint blockade led to efficacy in models otherwise resistant to systemic immune checkpoint inhibition. Human cell studies showed similar cytokine responses to the individual components of this mRNA mixture, suggesting translatability of immunomodulatory activity to human patients.
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