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Serotonin receptor 5-HT <sub>2A</sub> as a potential target for HCC immunotherapy

Rong En Tay, Charmaine Min Ho, Nicholas Da Zhi Ang, Hui Chien Tay, Daniel Z Lopez, Quan Na, Yi Wen Tan, Ser Mei Koh, Kim Peng Tan, Wendy Lee, Jackwee Lim, Maichan Lau, Han Chong Toh, Olaf Rötzschke, Laurent Rénia

2025Journal for ImmunoTherapy of Cancer11 citationsDOIOpen Access PDF

Abstract

Background While recent clinical trials of combination immunotherapies for hepatocellular carcinoma (HCC) have shown promising clinical efficacy and survival improvements breakthroughs, there is still much room for further improvement. A key limiting factor for HCC immunotherapy is the intrinsic immunosuppression within the liver microenvironment, resulting in suboptimal priming of tumor-specific CD8 cytotoxic T cells and thus immune evasion by the tumor. Hence, identifying new key molecular pathways suppressing T-cell responses within the liver is critical for the rational design of more effective combination immunotherapies for HCC. Methods We identified the 5-HT 2A serotonin receptor as a potential target for HCC immunotherapy in a chemical screening approach and validated that targeting 5-HT 2A signaling could be a viable approach for HCC immunotherapy via in vitro and in vivo studies. Results Disruption of 5-HT 2A signaling using either a selective antagonist small molecule, ketanserin, or by knockout of its coding gene Htr2a augments the cytotoxic effector phenotype of mouse CD8 T cells activated in vitro with immunosuppressive liver non-parenchymal cells. Ketanserin treatment of in vitro activated human CD8 T cells also increased expression of the cytotoxic effector molecules granzyme B and perforin. Abrogation of 5-HT 2A signaling was associated with increased expression of cytotoxicity-related genes such as granzyme B and reduced expression of transcription factors downstream of MAP kinase signaling. In vivo, systemic ketanserin treatment significantly prolonged survival of HCC tumor-bearing mice and was non-inferior to α-programmed death ligand 1 (PD-L1)+α-vascular endothelial growth factor A (VEGFA) combination antibody treatment. Combining ketanserin with αPD-L1+αVEGFA antibodies also significantly prolonged survival relative to control-treated mice while preserving the occurrence of complete tumor regression observed with αPD-L1+αVEGFA treatment alone. Conclusions Together, our data describe a role for 5-HT 2A as a negative regulator of the cytotoxic effector phenotype in CD8 T cells and highlight the therapeutic potential of targeting 5-HT 2A for HCC immunotherapy.

Topics & Concepts

Immunotherapy5-HT receptorMedicineReceptorSerotoninCancer researchInternal medicineCancerCancer, Stress, Anesthesia, and Immune ResponseCancer Immunotherapy and BiomarkersVagus Nerve Stimulation Research
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