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Gene Expression Programs of Human Smooth Muscle Cells: Tissue-Specific Differentiation and Prognostic Significance in Breast Cancers

Smooth muscle is present in a wide variety of anatomical locations, such as blood vessels, various visceral organs, and hair follicles. Contraction of smooth muscle is central to functions as diverse as peristalsis, urination, respiration, and the maintenance of vascular tone. Despite the varied phy...

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Autores principales: Chi, Jen-Tsan, Rodriguez, Edwin H, Wang, Zhen, Nuyten, Dimitry S. A, Mukherjee, Sayan, van de Rijn, Matt, van de Vijver, Marc J., Hastie, Trevor, Brown, Patrick O
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2007
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1994710/
https://www.ncbi.nlm.nih.gov/pubmed/17907811
http://dx.doi.org/10.1371/journal.pgen.0030164
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author Chi, Jen-Tsan
Rodriguez, Edwin H
Wang, Zhen
Nuyten, Dimitry S. A
Mukherjee, Sayan
van de Rijn, Matt
van de Vijver, Marc J.
Hastie, Trevor
Brown, Patrick O
author_facet Chi, Jen-Tsan
Rodriguez, Edwin H
Wang, Zhen
Nuyten, Dimitry S. A
Mukherjee, Sayan
van de Rijn, Matt
van de Vijver, Marc J.
Hastie, Trevor
Brown, Patrick O
author_sort Chi, Jen-Tsan
collection PubMed
description Smooth muscle is present in a wide variety of anatomical locations, such as blood vessels, various visceral organs, and hair follicles. Contraction of smooth muscle is central to functions as diverse as peristalsis, urination, respiration, and the maintenance of vascular tone. Despite the varied physiological roles of smooth muscle cells (SMCs), we possess only a limited knowledge of the heterogeneity underlying their functional and anatomic specializations. As a step toward understanding the intrinsic differences between SMCs from different anatomical locations, we used DNA microarrays to profile global gene expression patterns in 36 SMC samples from various tissues after propagation under defined conditions in cell culture. Significant variations were found between the cells isolated from blood vessels, bronchi, and visceral organs. Furthermore, pervasive differences were noted within the visceral organ subgroups that appear to reflect the distinct molecular pathways essential for organogenesis as well as those involved in organ-specific contractile and physiological properties. Finally, we sought to understand how this diversity may contribute to SMC-involving pathology. We found that a gene expression signature of the responses of vascular SMCs to serum exposure is associated with a significantly poorer prognosis in human cancers, potentially linking vascular injury response to tumor progression.
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spelling pubmed-19947102007-09-27 Gene Expression Programs of Human Smooth Muscle Cells: Tissue-Specific Differentiation and Prognostic Significance in Breast Cancers Chi, Jen-Tsan Rodriguez, Edwin H Wang, Zhen Nuyten, Dimitry S. A Mukherjee, Sayan van de Rijn, Matt van de Vijver, Marc J. Hastie, Trevor Brown, Patrick O PLoS Genet Research Article Smooth muscle is present in a wide variety of anatomical locations, such as blood vessels, various visceral organs, and hair follicles. Contraction of smooth muscle is central to functions as diverse as peristalsis, urination, respiration, and the maintenance of vascular tone. Despite the varied physiological roles of smooth muscle cells (SMCs), we possess only a limited knowledge of the heterogeneity underlying their functional and anatomic specializations. As a step toward understanding the intrinsic differences between SMCs from different anatomical locations, we used DNA microarrays to profile global gene expression patterns in 36 SMC samples from various tissues after propagation under defined conditions in cell culture. Significant variations were found between the cells isolated from blood vessels, bronchi, and visceral organs. Furthermore, pervasive differences were noted within the visceral organ subgroups that appear to reflect the distinct molecular pathways essential for organogenesis as well as those involved in organ-specific contractile and physiological properties. Finally, we sought to understand how this diversity may contribute to SMC-involving pathology. We found that a gene expression signature of the responses of vascular SMCs to serum exposure is associated with a significantly poorer prognosis in human cancers, potentially linking vascular injury response to tumor progression. Public Library of Science 2007-09 2007-09-28 /pmc/articles/PMC1994710/ /pubmed/17907811 http://dx.doi.org/10.1371/journal.pgen.0030164 Text en Copyright: © 2007 Chi et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Chi, Jen-Tsan
Rodriguez, Edwin H
Wang, Zhen
Nuyten, Dimitry S. A
Mukherjee, Sayan
van de Rijn, Matt
van de Vijver, Marc J.
Hastie, Trevor
Brown, Patrick O
Gene Expression Programs of Human Smooth Muscle Cells: Tissue-Specific Differentiation and Prognostic Significance in Breast Cancers
title Gene Expression Programs of Human Smooth Muscle Cells: Tissue-Specific Differentiation and Prognostic Significance in Breast Cancers
title_full Gene Expression Programs of Human Smooth Muscle Cells: Tissue-Specific Differentiation and Prognostic Significance in Breast Cancers
title_fullStr Gene Expression Programs of Human Smooth Muscle Cells: Tissue-Specific Differentiation and Prognostic Significance in Breast Cancers
title_full_unstemmed Gene Expression Programs of Human Smooth Muscle Cells: Tissue-Specific Differentiation and Prognostic Significance in Breast Cancers
title_short Gene Expression Programs of Human Smooth Muscle Cells: Tissue-Specific Differentiation and Prognostic Significance in Breast Cancers
title_sort gene expression programs of human smooth muscle cells: tissue-specific differentiation and prognostic significance in breast cancers
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1994710/
https://www.ncbi.nlm.nih.gov/pubmed/17907811
http://dx.doi.org/10.1371/journal.pgen.0030164
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