microRNA-29 negatively regulates EMT regulator N-myc interactor in breast cancer

BACKGROUND: N-Myc Interactor is an inducible protein whose expression is compromised in advanced stage breast cancer. Downregulation of NMI, a gatekeeper of epithelial phenotype, in breast tumors promotes mesenchymal, invasive and metastatic phenotype of the cancer cells. Thus the mechanisms that re...

Descripción completa

Detalles Bibliográficos
Autores principales: Rostas, Jack W, Pruitt, Hawley C, Metge, Brandon J, Mitra, Aparna, Bailey, Sarah K, Bae, Sejong, Singh, Karan P, Devine, Daniel J, Dyess, Donna L, Richards, William O, Tucker, J Allan, Shevde, Lalita A, Samant, Rajeev S
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2014
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4169820/
https://www.ncbi.nlm.nih.gov/pubmed/25174825
http://dx.doi.org/10.1186/1476-4598-13-200
_version_ 1782335767929946112
author Rostas, Jack W
Pruitt, Hawley C
Metge, Brandon J
Mitra, Aparna
Bailey, Sarah K
Bae, Sejong
Singh, Karan P
Devine, Daniel J
Dyess, Donna L
Richards, William O
Tucker, J Allan
Shevde, Lalita A
Samant, Rajeev S
author_facet Rostas, Jack W
Pruitt, Hawley C
Metge, Brandon J
Mitra, Aparna
Bailey, Sarah K
Bae, Sejong
Singh, Karan P
Devine, Daniel J
Dyess, Donna L
Richards, William O
Tucker, J Allan
Shevde, Lalita A
Samant, Rajeev S
author_sort Rostas, Jack W
collection PubMed
description BACKGROUND: N-Myc Interactor is an inducible protein whose expression is compromised in advanced stage breast cancer. Downregulation of NMI, a gatekeeper of epithelial phenotype, in breast tumors promotes mesenchymal, invasive and metastatic phenotype of the cancer cells. Thus the mechanisms that regulate expression of NMI are of potential interest for understanding the etiology of breast tumor progression and metastasis. METHOD: Web based prediction algorithms were used to identify miRNAs that potentially target the NMI transcript. Luciferase reporter assays and western blot analysis were used to confirm the ability of miR-29 to target NMI. Quantitive-RT-PCRs were used to examine levels of miR29 and NMI from cell line and patient specimen derived RNA. The functional impact of miR-29 on EMT phenotype was evaluated using transwell migration as well as monitoring 3D matrigel growth morphology. Anti-miRs were used to examine effects of reducing miR-29 levels from cells. Western blots were used to examine changes in GSK3β phosphorylation status. The impact on molecular attributes of EMT was evaluated using immunocytochemistry, qRT-PCRs as well as Western blot analyses. RESULTS: Invasive, mesenchymal-like breast cancer cell lines showed increased levels of miR-29. Introduction of miR-29 into breast cancer cells (with robust level of NMI) resulted in decreased NMI expression and increased invasion, whereas treatment of cells with high miR-29 and low NMI levels with miR-29 antagonists increased NMI expression and decreased invasion. Assessment of 2D and 3D growth morphologies revealed an EMT promoting effect of miR-29. Analysis of mRNA of NMI and miR-29 from patient derived breast cancer tumors showed a strong, inverse relationship between the expression of NMI and the miR-29. Our studies also revealed that in the absence of NMI, miR-29 expression is upregulated due to unrestricted Wnt/β-catenin signaling resulting from inactivation of GSK3β. CONCLUSION: Aberrant miR-29 expression may account for reduced NMI expression in breast tumors and mesenchymal phenotype of cancer cells that promotes invasive growth. Reduction in NMI levels has a feed-forward impact on miR-29 levels.
format Online
Article
Text
id pubmed-4169820
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-41698202014-09-22 microRNA-29 negatively regulates EMT regulator N-myc interactor in breast cancer Rostas, Jack W Pruitt, Hawley C Metge, Brandon J Mitra, Aparna Bailey, Sarah K Bae, Sejong Singh, Karan P Devine, Daniel J Dyess, Donna L Richards, William O Tucker, J Allan Shevde, Lalita A Samant, Rajeev S Mol Cancer Research BACKGROUND: N-Myc Interactor is an inducible protein whose expression is compromised in advanced stage breast cancer. Downregulation of NMI, a gatekeeper of epithelial phenotype, in breast tumors promotes mesenchymal, invasive and metastatic phenotype of the cancer cells. Thus the mechanisms that regulate expression of NMI are of potential interest for understanding the etiology of breast tumor progression and metastasis. METHOD: Web based prediction algorithms were used to identify miRNAs that potentially target the NMI transcript. Luciferase reporter assays and western blot analysis were used to confirm the ability of miR-29 to target NMI. Quantitive-RT-PCRs were used to examine levels of miR29 and NMI from cell line and patient specimen derived RNA. The functional impact of miR-29 on EMT phenotype was evaluated using transwell migration as well as monitoring 3D matrigel growth morphology. Anti-miRs were used to examine effects of reducing miR-29 levels from cells. Western blots were used to examine changes in GSK3β phosphorylation status. The impact on molecular attributes of EMT was evaluated using immunocytochemistry, qRT-PCRs as well as Western blot analyses. RESULTS: Invasive, mesenchymal-like breast cancer cell lines showed increased levels of miR-29. Introduction of miR-29 into breast cancer cells (with robust level of NMI) resulted in decreased NMI expression and increased invasion, whereas treatment of cells with high miR-29 and low NMI levels with miR-29 antagonists increased NMI expression and decreased invasion. Assessment of 2D and 3D growth morphologies revealed an EMT promoting effect of miR-29. Analysis of mRNA of NMI and miR-29 from patient derived breast cancer tumors showed a strong, inverse relationship between the expression of NMI and the miR-29. Our studies also revealed that in the absence of NMI, miR-29 expression is upregulated due to unrestricted Wnt/β-catenin signaling resulting from inactivation of GSK3β. CONCLUSION: Aberrant miR-29 expression may account for reduced NMI expression in breast tumors and mesenchymal phenotype of cancer cells that promotes invasive growth. Reduction in NMI levels has a feed-forward impact on miR-29 levels. BioMed Central 2014-08-29 /pmc/articles/PMC4169820/ /pubmed/25174825 http://dx.doi.org/10.1186/1476-4598-13-200 Text en © Rostas et al.; licensee BioMed Central Ltd. 2014 This article is published under license to BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Rostas, Jack W
Pruitt, Hawley C
Metge, Brandon J
Mitra, Aparna
Bailey, Sarah K
Bae, Sejong
Singh, Karan P
Devine, Daniel J
Dyess, Donna L
Richards, William O
Tucker, J Allan
Shevde, Lalita A
Samant, Rajeev S
microRNA-29 negatively regulates EMT regulator N-myc interactor in breast cancer
title microRNA-29 negatively regulates EMT regulator N-myc interactor in breast cancer
title_full microRNA-29 negatively regulates EMT regulator N-myc interactor in breast cancer
title_fullStr microRNA-29 negatively regulates EMT regulator N-myc interactor in breast cancer
title_full_unstemmed microRNA-29 negatively regulates EMT regulator N-myc interactor in breast cancer
title_short microRNA-29 negatively regulates EMT regulator N-myc interactor in breast cancer
title_sort microrna-29 negatively regulates emt regulator n-myc interactor in breast cancer
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4169820/
https://www.ncbi.nlm.nih.gov/pubmed/25174825
http://dx.doi.org/10.1186/1476-4598-13-200
work_keys_str_mv AT rostasjackw microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT pruitthawleyc microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT metgebrandonj microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT mitraaparna microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT baileysarahk microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT baesejong microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT singhkaranp microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT devinedanielj microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT dyessdonnal microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT richardswilliamo microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT tuckerjallan microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT shevdelalitaa microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer
AT samantrajeevs microrna29negativelyregulatesemtregulatornmycinteractorinbreastcancer

Ejemplares similares