The CCR6–CCL20 axis promotes regulatory T cell glycolysis and immunosuppression in tumors

Author:

Pant Ayush1ORCID,Jain Aanchal2ORCID,Chen Yiyun3ORCID,Patel Kisha1ORCID,Saleh Laura1ORCID,Tzeng Stephany4ORCID,Nitta Ryan T.5ORCID,Zhao Liang6ORCID,Wu Caren Yu-Ju.3ORCID,Bederson Maria7ORCID,Wang William Lee.5ORCID,Bergsneider Brandon Hwa-Lin.3ORCID,Choi John7ORCID,Medikonda Ravi7ORCID,Verma Rohit8ORCID,Cho Kwang Bog7ORCID,Kim Lily H.7ORCID,Kim Jennifer E.9ORCID,Yazigi Eli4ORCID,Lee Si Yeon7ORCID,Rajendran Sakthi10ORCID,Rajappa Prajwal10ORCID,Mackall Crystal L.11ORCID,Li Gordon5ORCID,Tyler Betty9ORCID,Brem Henry9ORCID,Pardoll Drew M.9ORCID,Lim Michael8ORCID,Jackson Christopher M.9ORCID

Affiliation:

1. Johns Hopkins Medicine, Balitmore, MD, United States

2. Johns Hopkins University School of Medicinehool of Medicine, United States

3. Stanford University, Stanford, United States

4. Johns Hopkins Medicine, United States

5. Stanford University, Stanford, CA, United States

6. Complete Omics (United States), Baltimore, MD, United States

7. Stanford University, United States

8. Stanford University, Palo alto, United States

9. Johns Hopkins Medicine, Baltimore, MD, United States

10. Nationwide Children's Hospital, Columbus, Ohio, United States

11. Stanford University, Stanford, California, United States

Abstract

Abstract Regulatory T cells (Tregs) are important players in the tumor microenvironment. However, the mechanisms behind their immunosuppressive effects are poorly understood. We found that CCR6–CCL20 activity in tumor-infiltrating Tregs is associated with greater glycolytic activity and ablation of Ccr6 reduced glycolysis and lactic acid production while increasing compensatory glutamine metabolism. Immunosuppressive activity towards CD8+ T cells was abrogated in Ccr6-/- Tregs due to reduction in activation-induced glycolysis. Furthermore, Ccr6-/- mice exhibited improved survival across multiple tumor models compared to wildtype mice, and Treg and CD8+ T-cell depletion abrogated the improvement. In addition, Ccr6 ablation further promoted the efficacy of anti-PD-1 therapy in a preclinical glioma model. Follow-up knockdown of Ccl20 with siRNA also demonstrated improvement in antitumor efficacy. Our results unveil CCR6 as a marker and regulator of Treg-induced immunosuppression and identify approaches to target the metabolic determinants of Treg immunosuppressive activity.

Publisher

American Association for Cancer Research (AACR)

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