Characterisation of colonic dysplasia-like epithelial atypia in murine colitis

Sarron Randall-Demllo; Ruchira Fernando; Terry Brain; Sukhwinder Singh Sohal; Anthony L Cook; Nuri Guven; Dale Kunde; Kevin Spring; Rajaraman Eri

doi:10.3748/wjg.v22.i37.8334

Characterisation of colonic dysplasia-like epithelial atypia in murine colitis

World J Gastroenterol. 2016 Oct 7;22(37):8334-8348. doi: 10.3748/wjg.v22.i37.8334.

Authors

Sarron Randall-Demllo¹, Ruchira Fernando¹, Terry Brain¹, Sukhwinder Singh Sohal¹, Anthony L Cook¹, Nuri Guven¹, Dale Kunde¹, Kevin Spring¹, Rajaraman Eri¹

Affiliation

¹ Sarron Randall-Demllo, Sukhwinder Singh Sohal, Dale Kunde, Rajaraman Eri, School of Health Sciences, University of Tasmania, Launceston, Launceston TAS 7250, Australia.

Abstract

Aim: To determine if exacerbation of pre-existing chronic colitis in Winnie (Muc2 mutant) mice induces colonic dysplasia.

Methods: Winnie mice and C57BL6 as a genotype control, were administered 1% w/v dextran sulphate sodium (DSS) orally, followed by drinking water alone in week-long cycles for a total of three cycles. After the third cycle, mice were killed and colonic tissue collected for histological and immunohistochemical evaluation. Inflammation and severity of dysplasia in the colonic mucosa were assessed in H&E sections of the colon. Epithelial cell proliferation was assessed using Ki67 and aberrant β-catenin signalling assessed with enzyme-based immunohistochemistry. Extracted RNA from colonic segments was used for the analysis of gene expression using real-time quantitative PCR. Finally, the distribution of Cxcl5 was visualised using immunohistochemistry.

Results: Compared to controls, Winnie mice exposed to three cycles of DSS displayed inflammation mostly confined to the distal-mid colon with extensive mucosal hyperplasia and regenerative atypia resembling epithelial dysplasia. Dysplasia-like changes were observed in 100% of Winnie mice exposed to DSS, with 55% of these animals displaying changes similar to high-grade dysplasia, whereas high-grade changes were absent in wild-type mice. Occasional penetration of the muscularis mucosae by atypical crypts was observed in 27% of Winnie mice after DSS. Atypical crypts however displayed no evidence of oncogenic nuclear β-catenin accumulation, regardless of histological severity. Expression of Cav1, Trp53 was differentially regulated in the distal colon of Winnie relative to wild-type mice. Expression of Myc and Ccl5 was increased by DSS treatment in Winnie only. Furthermore, increased Ccl5 expression correlated with increased complexity in abnormal crypts. While no overall difference in Cxcl5 mucosal expression was observed between treatment groups, epithelial Cxcl5 protein appeared to be diminished in the atypical epithelium.

Conclusion: Alterations to the expression of Cav1, Ccl5, Myc and Trp53 in the chronically inflamed Winnie colon may influence the transition to dysplasia.

Keywords: Colitis; Colon; Dextran sulphate sodium; Dysplasia; Mice; Mucin-2.

MeSH terms

Animals
Body Weight
Chemokine CXCL5 / metabolism
Colitis / pathology*
Colitis, Ulcerative / metabolism
Colon / pathology*
Colonic Neoplasms / pathology*
Dextran Sulfate
Female
Gene Expression Regulation
Genotype
Inflammation / metabolism
Intestinal Mucosa / pathology*
Ki-67 Antigen / metabolism
Male
Mice
Mice, Inbred C57BL
Mutation
RNA / metabolism
Signal Transduction
beta Catenin / metabolism

Substances

CTNNB1 protein, mouse
Chemokine CXCL5
Cxcl5 protein, mouse
Ki-67 Antigen
beta Catenin
RNA
Dextran Sulfate