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Novel Molecular Markers of Malignancy in Histologically Normal and Benign Breast

To detect the molecular changes of malignancy in histologically normal breast (HNB) tissues, we recently developed a novel 117-gene-malignancy-signature. Here we report validation of our leading malignancy-risk-genes, topoisomerase-2-alpha (TOP2A), minichromosome-maintenance-protein-2 (MCM2) and “bu...

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Autores principales: Nasir, Aejaz, Chen, Dung-Tsa, Gruidl, Mike, Henderson-Jackson, Evita B., Venkataramu, Chinnambally, McCarthy, Susan M., McBride, Heyoung L., Harris, Eleanor, Khakpour, Nazanin, Yeatman, Timothy J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: SAGE-Hindawi Access to Research 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3140260/
https://www.ncbi.nlm.nih.gov/pubmed/21785684
http://dx.doi.org/10.4061/2011/489064
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author Nasir, Aejaz
Chen, Dung-Tsa
Gruidl, Mike
Henderson-Jackson, Evita B.
Venkataramu, Chinnambally
McCarthy, Susan M.
McBride, Heyoung L.
Harris, Eleanor
Khakpour, Nazanin
Yeatman, Timothy J.
author_facet Nasir, Aejaz
Chen, Dung-Tsa
Gruidl, Mike
Henderson-Jackson, Evita B.
Venkataramu, Chinnambally
McCarthy, Susan M.
McBride, Heyoung L.
Harris, Eleanor
Khakpour, Nazanin
Yeatman, Timothy J.
author_sort Nasir, Aejaz
collection PubMed
description To detect the molecular changes of malignancy in histologically normal breast (HNB) tissues, we recently developed a novel 117-gene-malignancy-signature. Here we report validation of our leading malignancy-risk-genes, topoisomerase-2-alpha (TOP2A), minichromosome-maintenance-protein-2 (MCM2) and “budding-uninhibited-by-benzimidazoles-1-homolog-beta” (BUB1B) at the protein level. Using our 117-gene malignancy-signature, we classified 18 fresh-frozen HNB tissues from 18 adult female breast cancer patients into HNB-tissues with low-grade (HNB-LGMA; N = 9) and high-grade molecular abnormality (HNB-HGMA; N = 9). Archival sections of additional HNB tissues from these patients, and invasive ductal carcinoma (IDC) tissues from six other patients were immunostained for these biomarkers. TOP2A/MCM2 expression was assessed as staining index (%) and BUB1B expression as H-scores (0–300). Increasing TOP2A, MCM2, and BUB1B protein expression from HNB-LGMA to HNB-HGMA tissues to IDCs validated our microarray-based molecular classification of HNB tissues by immunohistochemistry. We also demonstrated an increasing expression of TOP2A protein on an independent test set of HNB/benign/reductionmammoplasties, atypical-ductal-hyperplasia with and without synchronous breast cancer, DCIS and IDC tissues using a custom tissue microarray (TMA). In conclusion, TOP2A, MCM2, and BUB1B proteins are potential molecular biomarkers of malignancy in histologically normal and benign breast tissues. Larger-scale clinical validation studies are needed to further evaluate the clinical utility of these molecular biomarkers.
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spelling pubmed-31402602011-07-22 Novel Molecular Markers of Malignancy in Histologically Normal and Benign Breast Nasir, Aejaz Chen, Dung-Tsa Gruidl, Mike Henderson-Jackson, Evita B. Venkataramu, Chinnambally McCarthy, Susan M. McBride, Heyoung L. Harris, Eleanor Khakpour, Nazanin Yeatman, Timothy J. Patholog Res Int Research Article To detect the molecular changes of malignancy in histologically normal breast (HNB) tissues, we recently developed a novel 117-gene-malignancy-signature. Here we report validation of our leading malignancy-risk-genes, topoisomerase-2-alpha (TOP2A), minichromosome-maintenance-protein-2 (MCM2) and “budding-uninhibited-by-benzimidazoles-1-homolog-beta” (BUB1B) at the protein level. Using our 117-gene malignancy-signature, we classified 18 fresh-frozen HNB tissues from 18 adult female breast cancer patients into HNB-tissues with low-grade (HNB-LGMA; N = 9) and high-grade molecular abnormality (HNB-HGMA; N = 9). Archival sections of additional HNB tissues from these patients, and invasive ductal carcinoma (IDC) tissues from six other patients were immunostained for these biomarkers. TOP2A/MCM2 expression was assessed as staining index (%) and BUB1B expression as H-scores (0–300). Increasing TOP2A, MCM2, and BUB1B protein expression from HNB-LGMA to HNB-HGMA tissues to IDCs validated our microarray-based molecular classification of HNB tissues by immunohistochemistry. We also demonstrated an increasing expression of TOP2A protein on an independent test set of HNB/benign/reductionmammoplasties, atypical-ductal-hyperplasia with and without synchronous breast cancer, DCIS and IDC tissues using a custom tissue microarray (TMA). In conclusion, TOP2A, MCM2, and BUB1B proteins are potential molecular biomarkers of malignancy in histologically normal and benign breast tissues. Larger-scale clinical validation studies are needed to further evaluate the clinical utility of these molecular biomarkers. SAGE-Hindawi Access to Research 2011-07-10 /pmc/articles/PMC3140260/ /pubmed/21785684 http://dx.doi.org/10.4061/2011/489064 Text en Copyright © 2011 Aejaz Nasir et al. https://creativecommons.org/licenses/by/3.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Nasir, Aejaz
Chen, Dung-Tsa
Gruidl, Mike
Henderson-Jackson, Evita B.
Venkataramu, Chinnambally
McCarthy, Susan M.
McBride, Heyoung L.
Harris, Eleanor
Khakpour, Nazanin
Yeatman, Timothy J.
Novel Molecular Markers of Malignancy in Histologically Normal and Benign Breast
title Novel Molecular Markers of Malignancy in Histologically Normal and Benign Breast
title_full Novel Molecular Markers of Malignancy in Histologically Normal and Benign Breast
title_fullStr Novel Molecular Markers of Malignancy in Histologically Normal and Benign Breast
title_full_unstemmed Novel Molecular Markers of Malignancy in Histologically Normal and Benign Breast
title_short Novel Molecular Markers of Malignancy in Histologically Normal and Benign Breast
title_sort novel molecular markers of malignancy in histologically normal and benign breast
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3140260/
https://www.ncbi.nlm.nih.gov/pubmed/21785684
http://dx.doi.org/10.4061/2011/489064
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