What question did this study set out to answer?

This research aims to clarify the mechanism of action and immunological effects of PDE10A inhibition in cancer treatment.

March 7, 2026

Abstract A034: Targeting phosphodiesterase 10A by ADT-030 normalizes the tumor immune microenvironment by inhibiting RAS-MAPK signaling in both cancer cells and myeloid-derived suppressor cells

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This research aims to clarify the mechanism of action and immunological effects of PDE10A inhibition in cancer treatment.
Administered ADT-030, a PDE10A inhibitor, in various murine tumor models.
Conducted immune profiling in the 4T1 breast cancer model to evaluate immune cell changes.
Evaluated effects of ADT-030 on tumor growth and immune responses, including tumor-associated neutrophils and CD8+ T cells.
ADT-030 demonstrated strong cytotoxicity against multiple murine tumor cell lines.
The drug was effective in reducing tumor growth in syngeneic mouse models, dependent on host immunity.
Comprehensive immune profiling revealed a reduction in tumor-associated neutrophils and restoration of CD8+ T cell function.

Abstract

Abstract Phosphodiesterase 10A (PDE10A), a cyclic nucleotide-degrading enzyme, is overexpressed in various human cancers. While PDE10A inhibition using small-molecule inhibitors or gene silencing suppresses tumor growth in xenograft models, its precise mechanism of action and immunological impact remain unclear. Here, we report that ADT-030, a novel PDE10A inhibitor, exhibits potent cytotoxicity against a broad range of murine tumor cell lines through suppression of RAS/MAPK signaling in both cancer cells and myeloid-derived suppressor cells (MDSCs). ADT-030 is orally bioavailable and effectively suppresses tumor growth in multiple syngeneic mouse models. Notably, its efficacy is significantly diminished in immunodeficient mice or upon CD8+ T cell depletion, highlighting a critical dependence on host immunity. The immunopotentiating effects of ADT-030 are further evidenced by its synergy with anti-PD-1 therapy, its ability to induce immunogenic tumor cell death and promote dendritic cell (DC) maturation in vitro, and its reliance on cDC1 to elicit antitumor effects in vivo. Comprehensive immune profiling in the 4T1 triple-negative breast cancer model, both in orthotopic and metastatic settings, revealed that ADT-030 selectively reduces tumor-associated neutrophils while restoring the presence and function of CD8+ T cells. These findings highlight PDE10A inhibition as a multi-faceted strategy that not only disrupts tumor-intrinsic oncogenic signaling but also reshapes the tumor immune microenvironment to unleash antitumor immunity. Citation Format: Md Gazi, Ogacheko Okoko, Yan Ye, Xin Wang, Khalda Fadlalla, Adam Keeton, Yulia Maxuitenko, Xi Chen, Huidong Shi, Gary Piazza, Gang Zhou. Targeting phosphodiesterase 10A by ADT-030 normalizes the tumor immune microenvironment by inhibiting RAS-MAPK signaling in both cancer cells and myeloid-derived suppressor cells abstract. In: Proceedings of the AACR Special Conference in Cancer Research: RAS Oncogenesis and Therapeutics; 2026 Mar 5-8; Los Angeles, CA. Philadelphia (PA): AACR; Cancer Res 2026;86 (5Suppl₁): Abstract nr A034.

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Abstract A034: Targeting phosphodiesterase 10A by ADT-030 normalizes the tumor immune microenvironment by inhibiting RAS-MAPK signaling in both cancer cells and myeloid-derived suppressor cells

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