| Literature DB >> 33990379 |
Xi Wang1, Bo Li1, Yu Jeong Kim1, Yu-Chen Wang1, Zhe Li1, Jiaji Yu1, Samuel Zeng1, Xiaoya Ma1, In Young Choi1, Stefano Di Biase1, Drake J Smith1, Yang Zhou1, Yan-Ruide Li1, Feiyang Ma2, Jie Huang1, Nicole Clarke1, Angela To1, Laura Gong1, Alexander T Pham1, Heesung Moon1, Matteo Pellegrini2,3, Lili Yang4,5,6,7.
Abstract
Monoamine oxidase A (MAO-A) is an enzyme best known for its function in the brain, where it breaks down neurotransmitters and thereby influences mood and behavior. Small-molecule MAO inhibitors (MAOIs) have been developed and are clinically used for treating depression and other neurological disorders. However, the involvement of MAO-A in antitumor immunity has not been reported. Here, we observed induction of the Maoa gene in tumor-infiltrating immune cells. Maoa knockout mice exhibited enhanced antitumor T cell immunity and suppressed tumor growth. MAOI treatment significantly suppressed tumor growth in preclinical mouse syngeneic and human xenograft tumor models in a T cell-dependent manner. Combining MAOI and anti-PD-1 treatments generated synergistic tumor suppression effects. Clinical data correlation studies associated intratumoral MAOA expression with T cell dysfunction and decreased patient survival in a broad range of cancers. We further demonstrated that MAO-A restrains antitumor T cell immunity through controlling intratumoral T cell autocrine serotonin signaling. Together, these data identify MAO-A as an immune checkpoint and support repurposing MAOI antidepressants for cancer immunotherapy.Entities:
Mesh:
Substances:
Year: 2021 PMID: 33990379 DOI: 10.1126/sciimmunol.abh2383
Source DB: PubMed Journal: Sci Immunol ISSN: 2470-9468