IL-1R signaling drives enteric glia-macrophage interactions in colorectal cancer.
Lies van BaarleVeronica De SimoneLinda SchneiderSneha SanthoshSaeed AbdurahimanFrancesca BiscuReiner SchneiderLisa ZanolettiRenata Siqueira de MelloSara VerbandtZedong HuMichelle StakenborgBo-Jun KeNathalie StakenborgRaquel Salvador LaureanoBalbina García-ReyesJonas HennMarieta TomaMaxime VanmechelenGuy E BoeckxstaensFrederik De SmetAbhishek Dinkarnath GargSales IbizaSabine TejparSven WehnerGianluca MatteoliPublished in: Nature communications (2024)
Enteric glia have been recently recognized as key components of the colonic tumor microenvironment indicating their potential role in colorectal cancer pathogenesis. Although enteric glia modulate immune responses in other intestinal diseases, their interaction with the colorectal cancer immune cell compartment remains unclear. Through a combination of single-cell and bulk RNA-sequencing, both in murine models and patients, here we find that enteric glia acquire an immunomodulatory phenotype by bi-directional communication with tumor-infiltrating monocytes. The latter direct a reactive enteric glial cell phenotypic and functional switch via glial IL-1R signaling. In turn, tumor glia promote monocyte differentiation towards pro-tumorigenic SPP1 + tumor-associated macrophages by IL-6 release. Enteric glia cell abundancy correlates with worse disease outcomes in preclinical models and colorectal cancer patients. Thereby, our study reveals a neuroimmune interaction between enteric glia and tumor-associated macrophages in the colorectal tumor microenvironment, providing insights into colorectal cancer pathogenesis.
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