Loss of NFKB1 results in expression of tumor necrosis factor and activation of STAT1 to promote gastric tumorigenesis in mice

Low, JT; Christie, M; Ernst, M; Dumoutier, L; Preaudet, A; Ni, Y; Griffin, MDW; Mielke, LA; Strasser, A; Putoczki, TL; O&#39;Reilly, LA

Author(s): Low, JT; Christie, M; Ernst, M; Dumoutier, L; Preaudet, A; Ni, Y; Griffin, MDW; Mielke, LA; Strasser, A; Putoczki, TL; O'Reilly, LA;
Details: Publication Year 2020-06-19,Volume 159,Issue #4,Page 1444-1458e15
Journal Title: Gastroenterology
Publication Type: Journal article
Abstract: BACKGROUND & AIMS: Activity of NFkB transcription factors and signaling via STAT are frequently altered in gastric cancer cells. Mice lacking NFKB1 (Nfkb1(-/-) mice) develop invasive gastric cancer and their gastric tissues have increased levels of cytokines, such as interleukin (IL)6, IL22, IL11, and tumor necrosis factor (TNF), as well as increased activation of signal transducer and activator of transcription 1 (STAT1). We investigated whether these cytokines were required for STAT1 activation in gastric tissues of mice and critical for gastric tumorigenesis. METHODS: We crossed Nfkb1(-/-) mice with Il6(-/-), Il22(-/-), Il11Ralpha(-/-) and Tnf(-/-) mice. Stomach tissues from compound mutant mice were analyzed by histology, immunoblotting and RNA sequencing. Lymphoid, myeloid and epithelial cells were isolated from stomachs and the levels of cytokines were determined by flow cytometric analysis. RESULTS: Nfkb1(-/-) mice developed gastritis, oxyntic atrophy, gastric dysplasia and invasive tumors, whereas Nfkb1(-/-)Stat1(-/-) mice did not, even when followed for as long as 2 years. The levels of Il6, Il11, and Il22 and Tnf mRNA were increased in the body and antrum of the stomachs from Nfkb1(-/-) mice, from 6 months of age. However, Nfkb1(-/-)Il6(-/-), Nfkb1(-/-)Il22(-/-) and Nfkb1(-/-)Il11Ralpha(-/-) mice still developed gastric tumors, although the absence of IL11 receptor (IL11R) significantly reduced development of invasive gastric tumors. Stomachs from Nfkb1(-/-)Tnf(-/-) mice exhibited significantly less gastritis and oxyntic atrophy and fewer tumors than Nfkb1(-/-) mice. This correlated with reduced activation of STAT1 and STAT3 and fewer numbers of T cells and B cells infiltrating the gastric body. Loss of STAT1 significantly reduced expression of PD-L1 on epithelial and myeloid (CD11b(+)) cells in the gastric mucosa of Nfkb1(-/-) mice, indeed to the levels observed on the corresponding cells from wild-type mice. CONCLUSIONS: In studies of gastric tumor development in knockout mice, we found that loss of NFKB1 causes increased expression of TNF in the stomach and thereby drives activation of STAT1, resulting in an inflammatory immune response and the development of gastric cancer. IL11R appears to be required for the progression of gastric tumors to the invasive stage. These findings suggest that inhibitors of TNF, and possibly also inhibitors of IL11/IL11Ralpha, might be useful in the treatment of gastric cancer.
Publisher: Elsevier
Research Division(s): Personalised Oncology; Inflammation; Blood Cells And Blood Cancer
PubMed ID: 32569771
Publisher's Version: https://doi.org/10.1053/j.gastro.2020.06.039
NHMRC Grants: NHMRC/1016701, NHMRC/1020363, NHMRC/1046010, NHMRC/1008614, NHMRC/1080498, NHMRC/466658,
Terms of Use/Rights Notice: Refer to copyright notice on published article.
Documents: Low JT etal_Gastroenterology_2020.pdf - (3.77MB, application/pdf)

Creation Date: 2020-06-25 07:59:31

Last Modified: 2021-11-10 09:36:15