Effects of β4 integrin expression on microRNA patterns in breast cancer

Effects of β4 integrin expression on microRNA patterns in breast cancer

Summary The integrin α6β4 is defined as an adhesion receptor for laminins. Referred to as ‘β4’, this integrin plays a key role in the progression of various carcinomas through its ability to orchestrate key signal transduction events and promote cell motility. To identify novel downstream effectors...

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Main Authors: Kristin D. Gerson, V. S. R. Krishna Maddula, Bruce E. Seligmann, Jeffrey R. Shearstone, Ashraf Khan, Arthur M. Mercurio
Format: Article
Language:English
Published: The Company of Biologists 2012-05-01
Series:Biology Open
Subjects:
Integrin β4
MicroRNA
Breast cancer
Cell motility
Online Access:http://bio.biologists.org/content/1/7/658
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spelling doaj-80f77a2981b643adb2d9ed3fff2c42fe2021-06-02T18:57:23ZengThe Company of BiologistsBiology Open2046-63902012-05-011765866610.1242/bio.2012162820121628Effects of β4 integrin expression on microRNA patterns in breast cancerKristin D. Gerson0V. S. R. Krishna Maddula1Bruce E. Seligmann2Jeffrey R. Shearstone3Ashraf Khan4Arthur M. Mercurio5 Department of Cancer Biology, University of Massachusetts Medical School, 364 Plantation Street, Worcester, MA 01605, USA HTG Molecular Diagnostics, Inc.3430 E. Global Loop, Tucson, AZ 85706, USA HTG Molecular Diagnostics, Inc.3430 E. Global Loop, Tucson, AZ 85706, USA Department of Cancer Biology, University of Massachusetts Medical School, 364 Plantation Street, Worcester, MA 01605, USA Department of Pathology, University of Massachusetts Medical School, Worcester, MA 01605, USA Department of Cancer Biology, University of Massachusetts Medical School, 364 Plantation Street, Worcester, MA 01605, USA Summary The integrin α6β4 is defined as an adhesion receptor for laminins. Referred to as ‘β4’, this integrin plays a key role in the progression of various carcinomas through its ability to orchestrate key signal transduction events and promote cell motility. To identify novel downstream effectors of β4 function in breast cancer, microRNAs (miRNAs) were examined because of their extensive links to tumorigenesis and their ability to regulate gene expression globally. Two breast carcinoma cell lines and a collection of invasive breast carcinomas with varying β4 expression were used to assess the effect of this integrin on miRNA expression. A novel miRNA microarray analysis termed quantitative Nuclease Protection Assay (qNPA) revealed that β4 expression can significantly alter miRNA expression and identified two miRNA families, miR-25/32/92abc/363/363-3p/367 and miR-99ab/100, that are consistently downregulated by expression of this integrin. Analysis of published Affymetrix GeneChip data identified 54 common targets of miR-92ab and miR-99ab/100 within the subset of β4-regulated mRNAs, revealing several genes known to be key components of β4-regulated signaling cascades and effectors of cell motility. Gene ontology classification identified an enrichment in genes associated with cell migration within this population. Finally, gene set enrichment analysis of all β4-regulated mRNAs revealed an enrichment in targets belonging to distinct miRNA families, including miR-92ab and others identified by our initial array analyses. The results obtained in this study provide the first example of an integrin globally impacting miRNA expression and provide evidence that select miRNA families collectively target genes important in executing β4-mediated cell motility.http://bio.biologists.org/content/1/7/658Integrin β4MicroRNABreast cancerCell motility
collection DOAJ
language English
format Article
sources DOAJ
author Kristin D. Gerson
V. S. R. Krishna Maddula
Bruce E. Seligmann
Jeffrey R. Shearstone
Ashraf Khan
Arthur M. Mercurio
spellingShingle Kristin D. Gerson
V. S. R. Krishna Maddula
Bruce E. Seligmann
Jeffrey R. Shearstone
Ashraf Khan
Arthur M. Mercurio
Effects of β4 integrin expression on microRNA patterns in breast cancer
Biology Open
Integrin β4
MicroRNA
Breast cancer
Cell motility
author_facet Kristin D. Gerson
V. S. R. Krishna Maddula
Bruce E. Seligmann
Jeffrey R. Shearstone
Ashraf Khan
Arthur M. Mercurio
author_sort Kristin D. Gerson
title Effects of β4 integrin expression on microRNA patterns in breast cancer
title_short Effects of β4 integrin expression on microRNA patterns in breast cancer
title_full Effects of β4 integrin expression on microRNA patterns in breast cancer
title_fullStr Effects of β4 integrin expression on microRNA patterns in breast cancer
title_full_unstemmed Effects of β4 integrin expression on microRNA patterns in breast cancer
title_sort effects of β4 integrin expression on microrna patterns in breast cancer
publisher The Company of Biologists
series Biology Open
issn 2046-6390
publishDate 2012-05-01
description Summary The integrin α6β4 is defined as an adhesion receptor for laminins. Referred to as ‘β4’, this integrin plays a key role in the progression of various carcinomas through its ability to orchestrate key signal transduction events and promote cell motility. To identify novel downstream effectors of β4 function in breast cancer, microRNAs (miRNAs) were examined because of their extensive links to tumorigenesis and their ability to regulate gene expression globally. Two breast carcinoma cell lines and a collection of invasive breast carcinomas with varying β4 expression were used to assess the effect of this integrin on miRNA expression. A novel miRNA microarray analysis termed quantitative Nuclease Protection Assay (qNPA) revealed that β4 expression can significantly alter miRNA expression and identified two miRNA families, miR-25/32/92abc/363/363-3p/367 and miR-99ab/100, that are consistently downregulated by expression of this integrin. Analysis of published Affymetrix GeneChip data identified 54 common targets of miR-92ab and miR-99ab/100 within the subset of β4-regulated mRNAs, revealing several genes known to be key components of β4-regulated signaling cascades and effectors of cell motility. Gene ontology classification identified an enrichment in genes associated with cell migration within this population. Finally, gene set enrichment analysis of all β4-regulated mRNAs revealed an enrichment in targets belonging to distinct miRNA families, including miR-92ab and others identified by our initial array analyses. The results obtained in this study provide the first example of an integrin globally impacting miRNA expression and provide evidence that select miRNA families collectively target genes important in executing β4-mediated cell motility.
topic Integrin β4
MicroRNA
Breast cancer
Cell motility
url http://bio.biologists.org/content/1/7/658
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