Tumor-associated endothelial cells display GSTP1 and RARβ2 promoter methylation in human prostate cancer

BACKGROUND: A functional blood supply is essential for tumor growth and proliferation. However, the mechanism of blood vessel recruitment to the tumor is still poorly understood. Ideally, a thorough molecular assessment of blood vessel cells would be critical in our comprehension of this process. Ye...

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Autores principales: Grover, Amelia C, Tangrea, Michael A, Woodson, Karen G, Wallis, Benjamin S, Hanson, Jeffrey C, Chuaqui, Rodrigo F, Gillespie, John W, Erickson, Heidi S, Bonner, Robert F, Pohida, Thomas J, Emmert-Buck, Michael R, Libutti, Steven K
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2006
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1420331/
https://www.ncbi.nlm.nih.gov/pubmed/16512911
http://dx.doi.org/10.1186/1479-5876-4-13
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author Grover, Amelia C
Tangrea, Michael A
Woodson, Karen G
Wallis, Benjamin S
Hanson, Jeffrey C
Chuaqui, Rodrigo F
Gillespie, John W
Erickson, Heidi S
Bonner, Robert F
Pohida, Thomas J
Emmert-Buck, Michael R
Libutti, Steven K
author_facet Grover, Amelia C
Tangrea, Michael A
Woodson, Karen G
Wallis, Benjamin S
Hanson, Jeffrey C
Chuaqui, Rodrigo F
Gillespie, John W
Erickson, Heidi S
Bonner, Robert F
Pohida, Thomas J
Emmert-Buck, Michael R
Libutti, Steven K
author_sort Grover, Amelia C
collection PubMed
description BACKGROUND: A functional blood supply is essential for tumor growth and proliferation. However, the mechanism of blood vessel recruitment to the tumor is still poorly understood. Ideally, a thorough molecular assessment of blood vessel cells would be critical in our comprehension of this process. Yet, to date, there is little known about the molecular makeup of the endothelial cells of tumor-associated blood vessels, due in part to the difficulty of isolating a pure population of endothelial cells from the heterogeneous tissue environment. METHODS: Here we describe the use of a recently developed technique, Expression Microdissection, to isolate endothelial cells from the tumor microenvironment. The methylation status of the dissected samples was evaluated for GSTP1 and RARβ2 promoters via the QMS-PCR method. RESULTS: Comparing GSTP1 and RARβ2 promoter methylation data, we show that 100% and 88% methylation is detected, respectively, in the tumor areas, both in epithelium and endothelium. Little to no methylation is observed in non-tumor tissue areas. CONCLUSION: We applied an accurate microdissection technique to isolate endothelial cells from tissues, enabling DNA analysis such as promoter methylation status. The observations suggest that epigenetic alterations may play a role in determining the phenotype of tumor-associated vasculature.
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spelling pubmed-14203312006-03-30 Tumor-associated endothelial cells display GSTP1 and RARβ2 promoter methylation in human prostate cancer Grover, Amelia C Tangrea, Michael A Woodson, Karen G Wallis, Benjamin S Hanson, Jeffrey C Chuaqui, Rodrigo F Gillespie, John W Erickson, Heidi S Bonner, Robert F Pohida, Thomas J Emmert-Buck, Michael R Libutti, Steven K J Transl Med Research BACKGROUND: A functional blood supply is essential for tumor growth and proliferation. However, the mechanism of blood vessel recruitment to the tumor is still poorly understood. Ideally, a thorough molecular assessment of blood vessel cells would be critical in our comprehension of this process. Yet, to date, there is little known about the molecular makeup of the endothelial cells of tumor-associated blood vessels, due in part to the difficulty of isolating a pure population of endothelial cells from the heterogeneous tissue environment. METHODS: Here we describe the use of a recently developed technique, Expression Microdissection, to isolate endothelial cells from the tumor microenvironment. The methylation status of the dissected samples was evaluated for GSTP1 and RARβ2 promoters via the QMS-PCR method. RESULTS: Comparing GSTP1 and RARβ2 promoter methylation data, we show that 100% and 88% methylation is detected, respectively, in the tumor areas, both in epithelium and endothelium. Little to no methylation is observed in non-tumor tissue areas. CONCLUSION: We applied an accurate microdissection technique to isolate endothelial cells from tissues, enabling DNA analysis such as promoter methylation status. The observations suggest that epigenetic alterations may play a role in determining the phenotype of tumor-associated vasculature. BioMed Central 2006-03-02 /pmc/articles/PMC1420331/ /pubmed/16512911 http://dx.doi.org/10.1186/1479-5876-4-13 Text en Copyright © 2006 Grover et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Grover, Amelia C
Tangrea, Michael A
Woodson, Karen G
Wallis, Benjamin S
Hanson, Jeffrey C
Chuaqui, Rodrigo F
Gillespie, John W
Erickson, Heidi S
Bonner, Robert F
Pohida, Thomas J
Emmert-Buck, Michael R
Libutti, Steven K
Tumor-associated endothelial cells display GSTP1 and RARβ2 promoter methylation in human prostate cancer
title Tumor-associated endothelial cells display GSTP1 and RARβ2 promoter methylation in human prostate cancer
title_full Tumor-associated endothelial cells display GSTP1 and RARβ2 promoter methylation in human prostate cancer
title_fullStr Tumor-associated endothelial cells display GSTP1 and RARβ2 promoter methylation in human prostate cancer
title_full_unstemmed Tumor-associated endothelial cells display GSTP1 and RARβ2 promoter methylation in human prostate cancer
title_short Tumor-associated endothelial cells display GSTP1 and RARβ2 promoter methylation in human prostate cancer
title_sort tumor-associated endothelial cells display gstp1 and rarβ2 promoter methylation in human prostate cancer
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1420331/
https://www.ncbi.nlm.nih.gov/pubmed/16512911
http://dx.doi.org/10.1186/1479-5876-4-13
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