| Literature DB >> 30650375 |
Oxana Dmitrieva-Posocco1, Amiran Dzutsev2, David F Posocco3, Vivianty Hou3, Wuxing Yuan2, Vishal Thovarai4, Ilgiz A Mufazalov5, Matthias Gunzer6, Igor P Shilovskiy7, Musa R Khaitov7, Giorgio Trinchieri2, Ari Waisman5, Sergei I Grivennikov8.
Abstract
Chronic inflammation drives the progression of colorectal cancer (CRC). Increased expression of interleukin (IL)-17A is associated with poor prognosis, and IL-17A blockade curbs tumor progression in preclinical models of CRC. Here we examined the impact of IL-1 signaling, a key regulator of the IL-17 pathway, in different cell types within the CRC microenvironment. Genetic deletion of the IL-1 receptor (IL-1R1) in epithelial cells alleviated tumorigenesis in the APC model of CRC, demonstrating a cell-autonomous role for IL-1 signaling in early tumor seed outgrowth. T cell specific ablation of IL-1R1 decreased tumor-elicited inflammation dependent on IL-17 and IL-22, thereby reducing CRC progression. The pro-tumorigenic roles of IL-1 were counteracted by its effects on myeloid cells, particularly neutrophils, where IL-1R1 ablation resulted in bacterial invasion into tumors, heightened inflammation and aggressive CRC progression. Thus, IL-1 signaling elicits cell-type-specific responses, which, in aggregate, set the inflammatory tone of the tumor microenvironment and determine the propensity for disease progression.Entities:
Keywords: Cytokine; Interleukin 1; cell type specific signaling; colorectal cancer; microbiota; tumor elicited inflammation; tumor microenvironment
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Year: 2019 PMID: 30650375 PMCID: PMC6490968 DOI: 10.1016/j.immuni.2018.11.015
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 43.474