MTG16 is a tumor suppressor in colitis-associated carcinoma
Elizabeth M. McDonough, Caitlyn W. Barrett, Bobak Parang, Mukul K. Mittal, J. Joshua Smith, Amber M. Bradley, Yash A. Choksi, Lori A. Coburn, Sarah P. Short, Joshua J. Thompson, Baolin Zhang, Shenika V. Poindexter, Melissa A. Fischer, Xi Chen, Jiang Li, Frank L. Revetta, Rishi Naik, M. Kay Washington, Michael J. Rosen, Scott W. Hiebert, Keith T. Wilson, Christopher S. Williams
Elizabeth M. McDonough, Caitlyn W. Barrett, Bobak Parang, Mukul K. Mittal, J. Joshua Smith, Amber M. Bradley, Yash A. Choksi, Lori A. Coburn, Sarah P. Short, Joshua J. Thompson, Baolin Zhang, Shenika V. Poindexter, Melissa A. Fischer, Xi Chen, Jiang Li, Frank L. Revetta, Rishi Naik, M. Kay Washington, Michael J. Rosen, Scott W. Hiebert, Keith T. Wilson, Christopher S. Williams
View: Text | PDF
Research Article Gastroenterology Genetics Inflammation Oncology

MTG16 is a tumor suppressor in colitis-associated carcinoma

Abstract

MTG16 is a member of the myeloid translocation gene (MTG) family of transcriptional corepressors. While MTGs were originally identified in chromosomal translocations in acute myeloid leukemia, recent studies have uncovered a role in intestinal biology. For example, Mtg16–/– mice have increased intestinal proliferation and are more sensitive to intestinal injury in colitis models. MTG16 is also underexpressed in patients with moderate/severe ulcerative colitis. Based on these findings, we postulated that MTG16 might protect against colitis-associated carcinogenesis. MTG16 was downregulated at the protein and RNA levels in patients with inflammatory bowel disease and in those with colitis-associated carcinoma. Mtg16–/– mice subjected to inflammatory carcinogenesis modeling exhibited worse colitis and increased tumor multiplicity and size. Loss of MTG16 also increased severity of dysplasia, apoptosis, proliferation, DNA damage, and WNT signaling. Moreover, transplantation of WT marrow into Mtg16–/– mice failed to rescue the Mtg16–/– protumorigenic phenotypes, indicating an epithelium-specific role for MTG16. While MTG dysfunction is widely appreciated in hematopoietic malignancies, the role of this gene family in epithelial homeostasis, and in colon cancer, was unrealized. This report identifies MTG16 as an important modulator of colitis and tumor development in inflammatory carcinogenesis.

Authors

Elizabeth M. McDonough, Caitlyn W. Barrett, Bobak Parang, Mukul K. Mittal, J. Joshua Smith, Amber M. Bradley, Yash A. Choksi, Lori A. Coburn, Sarah P. Short, Joshua J. Thompson, Baolin Zhang, Shenika V. Poindexter, Melissa A. Fischer, Xi Chen, Jiang Li, Frank L. Revetta, Rishi Naik, M. Kay Washington, Michael J. Rosen, Scott W. Hiebert, Keith T. Wilson, Christopher S. Williams

×

Figure 9

MTG16 expression is reduced in human colorectal cancer (CRC) and ulcerative colitis (UC) samples.

Options: View larger image (or click on image) Download as PowerPoint
MTG16 expression is reduced in human colorectal cancer (CRC) and ulcerat...
(A) Analysis of the combined Moffitt Cancer Center (MCC) and Vanderbilt Medical Center colon tumor expression array data set (10 normal samples, 6 adenomas, 33 stage I, 76 stage 2, 82 stage 3, and 59 stage 4, for a combined total of 250 CRC samples). (B) MTG16 mRNA levels in the indicated CRC stage from TCGA datasets (n = 41 normal samples, 75 stage I, 174 stage II, 126 stage III, 64 stage IV). (C) MTG16 mRNA in situ hybridization was performed on the Vanderbilt CRC tissue microarray (left) and quantified (right). (D) Box-and-whisker plot (line, median; +, mean; hinges, 25th and 75th percentile; whiskers, 10th to 90th percentile) demonstrating MTG16 staining extent (intensity and fraction of biopsy at that intensity) in cores from normal (n = 8), grade I (n = 27), grade II (n = 119), and grade III (n = 51) from human CRC. (E) Box-and-whisker plot (line, median; +, mean; hinges, 25th and 75th percentile; whiskers, 10th to 90th percentile) demonstrating MTG16 staining extent in cores from normal, non-UC patients (normal [Nrml], n = 9), control, noncancer UC patients (control [Ctrl], n = 10), uninvolved UC tissue adjacent to dysplasia (UI, n = 39), dysplastic (Dysp, n = 30), colitis-associated carcinoma (CAC, n = 28), and metastatic (Met, n = 8) tissue from patients with UC. One-way ANOVA and Newman-Keuls post-test were used to compare multiple groups such as those seen with MTG16 protein index in the human CAC array. For expression array and TCGA analysis, Wilcoxon rank-sum test with continuity correction was applied. *P < 0.05, **P < 0.01, ***P < 0.001, ****P < 0.0001 for all categories compared with normal tissue; θP < 0.05 between uninvolved UC and metastatic UC; θθθP < 0.001 between grade I and grade III.