Improving combination therapies: targeting A2B-adenosine receptor to modulate metabolic tumor microenvironment and immunosuppression-Reference-Cited by-同舟云学术

Improving combination therapies: targeting A2B-adenosine receptor to modulate metabolic tumor microenvironment and immunosuppression

Published:2023-05-17 Issue:11 Volume:115 Page:1404-1419
ISSN:0027-8874
Container-title:JNCI: Journal of the National Cancer Institute
language:en
Short-container-title:

Author:

Evans Jason V¹²,Suman Shankar¹,Goruganthu Mounika Uttam L¹,Tchekneva Elena E¹,Guan Shuxiao¹,Arasada Rajeswara Rao¹³,Antonucci Anneliese¹,Piao Longzhu¹,Ilgisonis Irina⁴,Bobko Andrey A⁵⁶,Driesschaert Benoit⁵⁷,Uzhachenko Roman V⁸⁹,Hoyd Rebecca¹,Samouilov Alexandre¹,Amann Joseph¹,Wu Ruohan¹,Wei Lai¹,Pallerla Aaditya¹,Ryzhov Sergey V¹⁰,Feoktistov Igor¹¹,Park Kyungho P¹¹,Kikuchi Takefumi¹²,Castro Julio¹³,Ivanova Alla V⁸¹⁴,Kanagasabai Thanigaivelan⁸¹⁴,Owen Dwight H¹,Spakowicz Daniel J¹,Zweier Jay L¹,Carbone David P¹,Novitskiy Sergey V¹⁵,Khramtsov Valery V⁵⁶,Shanker Anil⁸¹⁴¹⁶¹⁷¹⁸^ORCID,Dikov Mikhail M¹

Affiliation:

1. Department of Internal Medicine, The James Comprehensive Cancer Center, The Ohio State University , Columbus, OH, USA

2. Department of Pathology, Anatomy, and Laboratory Medicine, School of Medicine, West Virginia University , Morgantown, WV, USA

3. Pfizer Inc , New York, NY, USA

4. N.V. Sklifosovsky Institute of Clinical Medicine, I.M. Sechenov First Moscow State Medical University , Moscow, Russia

5. In Vivo Multifunctional Magnetic Resonance Center, West Virginia University , Morgantown, WV, USA

6. Department of Biochemistry, West Virginia University , Morgantown, WV, USA

7. Department of Pharmaceutical Sciences, School of Pharmacy, West Virginia University , Morgantown, WV, USA

8. Department of Biochemistry, Cancer Biology, Neuroscience and Pharmacology, School of Medicine, Meharry Medical College , Nashville, TN, USA

9. Department of Pathology, The Ohio State University Wexner Medical Center , Columbus, OH, USA

10. Center for Molecular Medicine, Maine Medical Center Research Institute , Scarborough, ME, USA

11. Division of Clinical Pharmacology, Department of Medicine, Vanderbilt University , Nashville, TN, USA

12. Division of Gastroenterology, Department of Internal Medicine, Sapporo Shirakabadai Hospital , Sapporo, Japan

13. Palobiofarma SL , Barcelona, Spain

14. School of Graduate Studies, Meharry Medical College , Nashville, TN, USA

15. Division of Allergy, Pulmonary, and Critical Care Medicine, Department of Medicine, Vanderbilt University , Nashville, TN, USA

16. Vanderbilt-Ingram Cancer Center, Vanderbilt University , Nashville, TN, USA

17. V , Nashville, TN, USA

18. anderbilt Institute for Infection, Immunology and Inflammation, Vanderbilt University , Nashville, TN, USA

Abstract

Abstract Background We investigated the role of A2B-adenosine receptor in regulating immunosuppressive metabolic stress in the tumor microenvironment. Novel A2B-adenosine receptor antagonist PBF-1129 was tested for antitumor activity in mice and evaluated for safety and immunologic efficacy in a phase I clinical trial of patients with non-small cell lung cancer. Methods The antitumor efficacy of A2B-adenosine receptor antagonists and their impact on the metabolic and immune tumor microenvironment were evaluated in lung, melanoma, colon, breast, and epidermal growth factor receptor–inducible transgenic cancer models. Employing electron paramagnetic resonance, we assessed changes in tumor microenvironment metabolic parameters, including pO2, pH, and inorganic phosphate, during tumor growth and evaluated the immunologic effects of PBF-1129, including its pharmacokinetics, safety, and toxicity, in patients with non-small cell lung cancer. Results Levels of metabolic stress correlated with tumor growth, metastasis, and immunosuppression. Tumor interstitial inorganic phosphate emerged as a correlative and cumulative measure of tumor microenvironment stress and immunosuppression. A2B-adenosine receptor inhibition alleviated metabolic stress, downregulated expression of adenosine-generating ectonucleotidases, increased expression of adenosine deaminase, decreased tumor growth and metastasis, increased interferon γ production, and enhanced the efficacy of antitumor therapies following combination regimens in animal models (anti–programmed cell death 1 protein vs anti–programmed cell death 1 protein plus PBF-1129 treatment hazard ratio = 11.74 [95% confidence interval = 3.35 to 41.13], n = 10, P < .001, 2-sided F test). In patients with non-small cell lung cancer, PBF-1129 was well tolerated, with no dose-limiting toxicities; demonstrated pharmacologic efficacy; modulated the adenosine generation system; and improved antitumor immunity. Conclusions Data identify A2B-adenosine receptor as a valuable therapeutic target to modify metabolic and immune tumor microenvironment to reduce immunosuppression, enhance the efficacy of immunotherapies, and support clinical application of PBF-1129 in combination therapies.

Funder

National Institutes of Health

Meharry Clinical and Translational Research Center Pilot

OSU K12 Training Grant for Clinical Investigators

Publisher

Oxford University Press (OUP)

Subject

Cancer Research,Oncology

Link

https://academic.oup.com/jnci/advance-article-pdf/doi/10.1093/jnci/djad091/51275693/djad091.pdf

Reference60 articles.

1. Changing perspective on oncometabolites: from metabolic signature of cancer to tumorigenic and immunosuppressive agents;Corrado;Oncotarget,2016