Synapse - Inhibition of breast cancer metastasis suppressor 1 promotes a mesenchymal phenotype in lung epithelial cells that express oncogenic k-rasv12and loss of p53

Inhibition of breast cancer metastasis suppressor 1 promotes a mesenchymal phenotype in lung epithelial cells that express oncogenic k-rasv12and loss of p53 Journal Article

Authors:	Hall, E. H.; Liu, Y.; Xiao, A.; Shock, L.; Brautigan, D. L.; Mayo, M. W.; Adusumilli, P. S.; Jones, D. R.
Article Title:	Inhibition of breast cancer metastasis suppressor 1 promotes a mesenchymal phenotype in lung epithelial cells that express oncogenic k-rasv12and loss of p53
Abstract:	Expression of the breast cancer metastasis suppressor 1 (BRMS1) protein is dramatically reduced in non-small cell lung cancer (NSCLC) cells and in primary human tumors. Although BRMS1 is a known suppressor of metastasis, the mechanisms through which BRMS1 functions to regulate cell migration and invasion in response to specific NSCLC driver mutations are poorly understood. To experimentally address this, we utilized immortalized human bronchial epithelial cells in which p53 was knocked down in the presence of oncogenic K-Ras V12 (HBEC3-p53KD-K-RasV12). These genetic alterations are commonly found in NSCLC and are associated with a poor prognosis. To determine the importance of BRMS1 for cytoskeletal function, cell migration and invasion in our model system we stably knocked down BRMS1. Here, we report that loss of BRMS1 in HBEC3-p53KD-K-RasV12 cells results in a dramatic increase in cell migration and invasion compared to controls that expressed BRMS1. Moreover, the loss of BRMS1 resulted in additional morphological changes including F-actin redistribution, paxillin accumulation at the leading edge of the lamellapodium, and cellular shape changes resembling mesenchymal phenotypes. Importantly, re-expression of BRMS1 restores, in part, cell migration and invasion; however it does not fully reestablish the epithelial phenotype. These finding suggests that loss of BRMS1 results in a permanent, largely irreversible, mesenchymal phenotype associated with increased cell migration and invasion. Collectively, in NSCLC cells without p53 and expression of oncogenic K-Ras our study identifies BRMS1 as a key regulator required to maintain a cellular morphology and cytoskeletal architecture consistent with an epithelial phenotype. © 2014 Hall et al.
Journal Title:	PLoS ONE
Volume:	9
Issue:	4
ISSN:	1932-6203
Publisher:	Public Library of Science
Date Published:	2014-04-24
Start Page:	e95869
Language:	English
DOI:	10.1371/journal.pone.0095869
PROVIDER:	scopus
PMCID:	PMC3999110
PUBMED:	24763730
DOI/URL:	http://www.scopus.com/inward/record.url?eid=2-s2.0-84899749702&partnerID=40&md5=2204628abbc69b7df96712fe8aa3cbc6
Notes:	PLoS ONE -- Export Date: 2 June 2014 -- CODEN: POLNC -- Source: Scopus

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MSK Authors

496 Adusumilli
417 Jones
22 Liu

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