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. 2014 Jun;33(6):1477-83.
doi: 10.3892/ijmm.2014.1708. Epub 2014 Mar 20.

Reduced hTERT protein levels are associated with DNA aneuploidy in the colonic mucosa of patients suffering from longstanding ulcerative colitis

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Reduced hTERT protein levels are associated with DNA aneuploidy in the colonic mucosa of patients suffering from longstanding ulcerative colitis

Mariann Friis-Ottessen et al. Int J Mol Med. 2014 Jun.

Abstract

Longstanding ulcerative colitis (UC) is a disease of chronic inflammation of the colon. It is associated with the development of colorectal cancer through a multistep process including increasing degrees of dysplasia and DNA-ploidy changes. However, not all UC patients will develop these characteristics even during lifelong disease, and patients may therefore be divided into progressors who develop dysplasia or cancer, and non-progressors who do not exhibit such changes. In the present study, the amount of hTERT, the catalytic subunit of the enzyme telomerase, was estimated by using peroxidase immunohistochemistry (IHC) in a set of progressor and non-progressor UC colectomies. The protein levels in the colonic mucosa of the progressors and non‑progressors were compared, and further comparisons between different categories of dysplastic development and to DNA-ploidy status within the progressors were made. Levels of hTERT were elevated in the colonic mucosa of the progressors and non-progressors when compared to non-UC control samples, but no difference was observed between the hTERT levels in the mucosa of progressors and non-progressors. The levels of hTERT associated with levels of Ki67 to a significant degree within the non-progressors. hTERT expression in lesions with DNA-aneuploidy were decreased as compared to diploid lesions, when stratified for different classes of colonic morphology. Our results indicate an association between hTERT protein expression and aneuploidy in UC-progressor colons, and also a possible protective mechanism in the association between hTERT and Ki67, against development of malignant features within the mucosa of a UC-colon.

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Figures

Figure 1
Figure 1
Immunohistochemistry (IHC) for hTERT. (A) Non-UC control sample (from full section), (B) ulcerative colitis (UC)-lesion with low hTERT levels and (C) UC-lesion with high hTERT levels. Images of UC colons are from tissue microarray (TMA)-cores. Arrows mark colonic mucosal cells positive for hTERT in low expression levels, arrowheads mark hTERT-stained leucocytes. Images are ×400 magnification.
Figure 2
Figure 2
Western blot analysis confirming the specificity of ab5181, a monoclonal antibody for hTERT expression. The antibody was specific, showing a single band at 127 kDa when tested using several cancer cell lines.
Figure 3
Figure 3
hTERT in ulcerative colitis (UC) progressors, non-progressors and non-UC controls. Protein levels of hTERT detected by immunohistochemistry (IHC) in progressors, non-progressors and non-UC controls.
Figure 4
Figure 4
hTERT in diploid and aneuploid lesions of progressors. Expression of hTERT in non-progressors and within areas with different morphologies harbouring diploid or aneuploid populations in progressors.

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