AZD4635 Targets cAMP/CREB Axis to Salvage PARPi-Induced Immune Evasion and Enhance Antitumor Efficacy in Ovarian Cancer
Botao Pan, Xiujuan Yang, Xuanji Wang, Jiahao Fang, Qingqing Liu, Ning Zou, Chenglai Xia, Huiling Shang

TL;DR
Combining PARP inhibitors with A2AR antagonists improves ovarian cancer treatment by enhancing immune response and reducing tumor growth.
Contribution
A novel combination therapy targeting the cAMP/CREB axis to overcome PARPi-induced immune evasion in ovarian cancer.
Findings
Combining PARPi with AZD4635 enhances antitumor activity by inhibiting cAMP/CREB pathway activation.
The combination therapy reduces immunosuppressive cells and increases cytotoxic T cells in the tumor microenvironment.
Single-cell RNA sequencing reveals immune heterogeneity and distinct functional subpopulations of immune cells.
Abstract
Background/Objectives: Poly(ADP-ribose) polymerase inhibitors (PARPis) have significantly transformed the treatment landscape for ovarian cancer; however, their clinical efficacy is often limited by poor response rates and the emergence of resistance. Recent studies have revealed that in ovarian cancer cells resistant to PARPi, the expression levels of adenosine receptors are upregulated. Accumulation of adenosine activates adenosine A2A receptor (A2AR) on immune cells, leading to immune suppression and immune escape. We hypothesize that this is a key factor limiting the efficacy of PARPi and driving the development of resistance. Therefore, the rational combination of PARPi with A2AR antagonists (A2ARas) may represent a highly promising anticancer strategy. Methods: To assess the effects of the PARPi AG14361 and the A2ARa AZD4635 on ovarian cancer growth and the immune…
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Taxonomy
TopicsAdenosine and Purinergic Signaling · PARP inhibition in cancer therapy · Cancer Mechanisms and Therapy
