Adenosine receptors on the immuno-oncology expressway: TIME, perspectives, and translation
Biswanath Majumder, Santanu Datta

TL;DR
This review explores how adenosine receptors influence cancer immunity and how targeting them could improve cancer treatments like immune checkpoint inhibitors and CAR-T therapies.
Contribution
The paper provides a comprehensive overview of adenosine receptor signaling in tumor immunity and highlights novel therapeutic strategies involving these pathways.
Findings
Adenosine receptors like A2AR and A2BR are key players in immune suppression within the tumor microenvironment.
Inhibiting adenosine signaling could restore anti-tumor immunity and enhance the effectiveness of existing therapies.
Emerging clinical trials and biomarkers suggest promising avenues for combining adenosine inhibitors with other cancer treatments.
Abstract
A decade since immune checkpoint inhibitors made a stride in the clinical landscape of oncology, there has been a substantial focus on understanding the response heterogeneity following these therapies. Insights gained from clinical data identified the primary and secondary resistance mechanisms that escape the upfront therapy pressure. Beyond PD-1 and CTLA-4, new checkpoints averting this pressure are under clinical development. Adenosinergic pathways are actively engaged in oncogenic signaling. The main protagonists, CD73, A2AR, and A2BR, span diverse immune subsets of lymphoid and myeloid lineages and have emerged as alternative checkpoints. This review discusses the latest update on immune regulation dynamics of adenosine receptor signaling and their complex interplay with hypoxia in a heterogeneous tumor immune microenvironment (TIME). In this spectrum, we also review the…
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Taxonomy
TopicsAdenosine and Purinergic Signaling · Cancer Immunotherapy and Biomarkers · Phagocytosis and Immune Regulation
