Deficient Pms2, ERCC1, Ku86, CcOI in Field Defects During Progression to Colon Cancer

In carcinogenesis, the "field defect" is recognized clinically because of the high propensity of survivors of certain cancers to develop other malignancies of the same tissue type, often in a nearby location. Such field defects have been indicated in colon cancer. The molecular abnormaliti...

Descripción completa

Detalles Bibliográficos
Autores principales: Nguyen, Huy, Loustaunau, Cristy, Facista, Alexander, Ramsey, Lois, Hassounah, Nadia, Taylor, Hilary, Krouse, Robert, Payne, Claire M., Tsikitis, V. Liana, Goldschmid, Steve, Banerjee, Bhaskar, Perini, Rafael F., Bernstein, Carol
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MyJove Corporation 2010
Materias:
Cellular Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3149991/
https://www.ncbi.nlm.nih.gov/pubmed/20689513
http://dx.doi.org/10.3791/1931
_version_ 1782209499303510016
author Nguyen, Huy
Loustaunau, Cristy
Facista, Alexander
Ramsey, Lois
Hassounah, Nadia
Taylor, Hilary
Krouse, Robert
Payne, Claire M.
Tsikitis, V. Liana
Goldschmid, Steve
Banerjee, Bhaskar
Perini, Rafael F.
Bernstein, Carol
author_facet Nguyen, Huy
Loustaunau, Cristy
Facista, Alexander
Ramsey, Lois
Hassounah, Nadia
Taylor, Hilary
Krouse, Robert
Payne, Claire M.
Tsikitis, V. Liana
Goldschmid, Steve
Banerjee, Bhaskar
Perini, Rafael F.
Bernstein, Carol
author_sort Nguyen, Huy
collection PubMed
description In carcinogenesis, the "field defect" is recognized clinically because of the high propensity of survivors of certain cancers to develop other malignancies of the same tissue type, often in a nearby location. Such field defects have been indicated in colon cancer. The molecular abnormalities that are responsible for a field defect in the colon should be detectable at high frequency in the histologically normal tissue surrounding a colonic adenocarcinoma or surrounding an adenoma with advanced neoplasia (well on the way to a colon cancer), but at low frequency in the colonic mucosa from patients without colonic neoplasia. Using immunohistochemistry, entire crypts within 10 cm on each side of colonic adenocarcinomas or advanced colonic neoplasias were found to be frequently reduced or absent in expression for two DNA repair proteins, Pms2 and/or ERCC1. Pms2 is a dual role protein, active in DNA mismatch repair as well as needed in apoptosis of cells with excess DNA damage. ERCC1 is active in DNA nucleotide excision repair. The reduced or absent expression of both ERCC1 and Pms2 would create cells with both increased ability to survive (apoptosis resistance) and increased level of mutability. The reduced or absent expression of both ERCC1 and Pms2 is likely an early step in progression to colon cancer. DNA repair gene Ku86 (active in DNA non-homologous end joining) and Cytochrome c Oxidase Subunit I (involved in apoptosis) had each been reported to be decreased in expression in mucosal areas close to colon cancers. However, immunohistochemical evaluation of their levels of expression showed only low to modest frequencies of crypts to be deficient in their expression in a field defect surrounding colon cancer or surrounding advanced colonic neoplasia. We show, here, our method of evaluation of crypts for expression of ERCC1, Pms2, Ku86 and CcOI. We show that frequency of entire crypts deficient for Pms2 and ERCC1 is often as great as 70% to 95% in 20 cm long areas surrounding a colonic neoplasia, while frequency of crypts deficient in Ku86 has a median value of 2% and frequency of crypts deficient in CcOI has a median value of 16% in these areas. The entire colon is 150 cm long (about 5 feet) and has about 10 million crypts in its mucosal layer. The defect in Pms2 and ERCC1 surrounding a colon cancer thus may include 1 million crypts. It is from a defective crypt that colon cancer arises.
format Online
Article
Text
id pubmed-3149991
institution National Center for Biotechnology Information
language English
publishDate 2010
publisher MyJove Corporation
record_format MEDLINE/PubMed
spelling pubmed-31499912011-08-15 Deficient Pms2, ERCC1, Ku86, CcOI in Field Defects During Progression to Colon Cancer Nguyen, Huy Loustaunau, Cristy Facista, Alexander Ramsey, Lois Hassounah, Nadia Taylor, Hilary Krouse, Robert Payne, Claire M. Tsikitis, V. Liana Goldschmid, Steve Banerjee, Bhaskar Perini, Rafael F. Bernstein, Carol J Vis Exp Cellular Biology In carcinogenesis, the "field defect" is recognized clinically because of the high propensity of survivors of certain cancers to develop other malignancies of the same tissue type, often in a nearby location. Such field defects have been indicated in colon cancer. The molecular abnormalities that are responsible for a field defect in the colon should be detectable at high frequency in the histologically normal tissue surrounding a colonic adenocarcinoma or surrounding an adenoma with advanced neoplasia (well on the way to a colon cancer), but at low frequency in the colonic mucosa from patients without colonic neoplasia. Using immunohistochemistry, entire crypts within 10 cm on each side of colonic adenocarcinomas or advanced colonic neoplasias were found to be frequently reduced or absent in expression for two DNA repair proteins, Pms2 and/or ERCC1. Pms2 is a dual role protein, active in DNA mismatch repair as well as needed in apoptosis of cells with excess DNA damage. ERCC1 is active in DNA nucleotide excision repair. The reduced or absent expression of both ERCC1 and Pms2 would create cells with both increased ability to survive (apoptosis resistance) and increased level of mutability. The reduced or absent expression of both ERCC1 and Pms2 is likely an early step in progression to colon cancer. DNA repair gene Ku86 (active in DNA non-homologous end joining) and Cytochrome c Oxidase Subunit I (involved in apoptosis) had each been reported to be decreased in expression in mucosal areas close to colon cancers. However, immunohistochemical evaluation of their levels of expression showed only low to modest frequencies of crypts to be deficient in their expression in a field defect surrounding colon cancer or surrounding advanced colonic neoplasia. We show, here, our method of evaluation of crypts for expression of ERCC1, Pms2, Ku86 and CcOI. We show that frequency of entire crypts deficient for Pms2 and ERCC1 is often as great as 70% to 95% in 20 cm long areas surrounding a colonic neoplasia, while frequency of crypts deficient in Ku86 has a median value of 2% and frequency of crypts deficient in CcOI has a median value of 16% in these areas. The entire colon is 150 cm long (about 5 feet) and has about 10 million crypts in its mucosal layer. The defect in Pms2 and ERCC1 surrounding a colon cancer thus may include 1 million crypts. It is from a defective crypt that colon cancer arises. MyJove Corporation 2010-07-28 /pmc/articles/PMC3149991/ /pubmed/20689513 http://dx.doi.org/10.3791/1931 Text en Copyright © 2010, Journal of Visualized Experiments http://creativecommons.org/licenses/by-nc-nd/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs 3.0 Unported License. To view a copy of this license, visithttp://creativecommons.org/licenses/by-nc-nd/3.0/
spellingShingle Cellular Biology
Nguyen, Huy
Loustaunau, Cristy
Facista, Alexander
Ramsey, Lois
Hassounah, Nadia
Taylor, Hilary
Krouse, Robert
Payne, Claire M.
Tsikitis, V. Liana
Goldschmid, Steve
Banerjee, Bhaskar
Perini, Rafael F.
Bernstein, Carol
Deficient Pms2, ERCC1, Ku86, CcOI in Field Defects During Progression to Colon Cancer
title Deficient Pms2, ERCC1, Ku86, CcOI in Field Defects During Progression to Colon Cancer
title_full Deficient Pms2, ERCC1, Ku86, CcOI in Field Defects During Progression to Colon Cancer
title_fullStr Deficient Pms2, ERCC1, Ku86, CcOI in Field Defects During Progression to Colon Cancer
title_full_unstemmed Deficient Pms2, ERCC1, Ku86, CcOI in Field Defects During Progression to Colon Cancer
title_short Deficient Pms2, ERCC1, Ku86, CcOI in Field Defects During Progression to Colon Cancer
title_sort deficient pms2, ercc1, ku86, ccoi in field defects during progression to colon cancer
topic Cellular Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3149991/
https://www.ncbi.nlm.nih.gov/pubmed/20689513
http://dx.doi.org/10.3791/1931
work_keys_str_mv AT nguyenhuy deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT loustaunaucristy deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT facistaalexander deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT ramseylois deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT hassounahnadia deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT taylorhilary deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT krouserobert deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT payneclairem deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT tsikitisvliana deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT goldschmidsteve deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT banerjeebhaskar deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT perinirafaelf deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer
AT bernsteincarol deficientpms2ercc1ku86ccoiinfielddefectsduringprogressiontocoloncancer

Ejemplares similares