Targeting miR-23a in CD8+ cytotoxic T lymphocytes prevents tumor-dependent immunosuppression
Regina Lin, Ling Chen, Gang Chen, Chunyan Hu, Shan Jiang, Jose Sevilla, Ying Wan, John H. Sampson, Bo Zhu, Qi-Jing Li
Regina Lin, Ling Chen, Gang Chen, Chunyan Hu, Shan Jiang, Jose Sevilla, Ying Wan, John H. Sampson, Bo Zhu, Qi-Jing Li
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Research Article Oncology

Targeting miR-23a in CD8+ cytotoxic T lymphocytes prevents tumor-dependent immunosuppression

Abstract

CD8+ cytotoxic T lymphocytes (CTLs) have potent antitumor activity and therefore are leading candidates for use in tumor immunotherapy. The application of CTLs for clinical use has been limited by the susceptibility of ex vivo–expanded CTLs to become dysfunctional in response to immunosuppressive microenvironments. Here, we developed a microRNA-targeting (miRNA-targeting) approach that augments CTL cytotoxicity and preserves immunocompetence. Specifically, we screened for miRNAs that modulate cytotoxicity and identified miR-23a as a strong functional repressor of the transcription factor BLIMP-1, which promotes CTL cytotoxicity and effector cell differentiation. In a cohort of advanced lung cancer patients, miR-23a was upregulated in tumor-infiltrating CTLs, and expression correlated with impaired antitumor potential of patient CTLs. We determined that tumor-derived TGF-β directly suppresses CTL immune function by elevating miR-23a and downregulating BLIMP-1. Functional blocking of miR-23a in human CTLs enhanced granzyme B expression, and in mice with established tumors, immunotherapy with just a small number of tumor-specific CTLs in which miR-23a was inhibited robustly hindered tumor progression. Together, our findings provide a miRNA-based strategy that subverts the immunosuppression of CTLs that is often observed during adoptive cell transfer tumor immunotherapy and identify a TGF-β–mediated tumor immune-evasion pathway.

Authors

Regina Lin, Ling Chen, Gang Chen, Chunyan Hu, Shan Jiang, Jose Sevilla, Ying Wan, John H. Sampson, Bo Zhu, Qi-Jing Li

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Figure 9

Model of CTL immune modulation by targeting miR-23a.

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Model of CTL immune modulation by targeting miR-23a. (A) Under immune-ac...
(A) Under immune-activating conditions, TCR signaling upregulates cMYC in CTLs. Transcriptional repression of pri-miR-23a by cMYC permits accumulation of BLIMP-1, resulting in increased expression of its cytotoxic target genes, granzyme B, and IFN-γ. (B) In the tumor microenvironment, TGF-β suppresses CTL activity via 2 mechanisms — SMAD-mediated transcriptional reprogramming and miRNA-mediated post-transcriptional control. In the former, TGF-β–induced SMADs are recruited to the Gzmb and Ifng gene regulatory regions to repress the transcription of these cytotoxic mediators directly. In the latter, TGF-β antagonizes cMYC activity, thereby derepressing pri-miR-23a transcription. Elevated miR-23a levels in CTLs downregulate BLIMP-1, and consequently its downstream cytotoxic effectors.