Lowered Expression of Tumor Suppressor Candidate MYO1C Stimulates Cell Proliferation, Suppresses Cell Adhesion and Activates AKT

Myosin-1C (MYO1C) is a tumor suppressor candidate located in a region of recurrent losses distal to TP53. Myo1c can tightly and specifically bind to PIP2, the substrate of Phosphoinositide 3-kinase (PI3K), and to Rictor, suggesting a role for MYO1C in the PI3K pathway. This study was designed to exa...

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Autores principales: Visuttijai, Kittichate, Pettersson, Jennifer, Mehrbani Azar, Yashar, van den Bout, Iman, Örndal, Charlotte, Marcickiewicz, Janusz, Nilsson, Staffan, Hörnquist, Michael, Olsson, Björn, Ejeskär, Katarina, Behboudi, Afrouz
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5055341/
https://www.ncbi.nlm.nih.gov/pubmed/27716847
http://dx.doi.org/10.1371/journal.pone.0164063
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author Visuttijai, Kittichate
Pettersson, Jennifer
Mehrbani Azar, Yashar
van den Bout, Iman
Örndal, Charlotte
Marcickiewicz, Janusz
Nilsson, Staffan
Hörnquist, Michael
Olsson, Björn
Ejeskär, Katarina
Behboudi, Afrouz
author_facet Visuttijai, Kittichate
Pettersson, Jennifer
Mehrbani Azar, Yashar
van den Bout, Iman
Örndal, Charlotte
Marcickiewicz, Janusz
Nilsson, Staffan
Hörnquist, Michael
Olsson, Björn
Ejeskär, Katarina
Behboudi, Afrouz
author_sort Visuttijai, Kittichate
collection PubMed
description Myosin-1C (MYO1C) is a tumor suppressor candidate located in a region of recurrent losses distal to TP53. Myo1c can tightly and specifically bind to PIP2, the substrate of Phosphoinositide 3-kinase (PI3K), and to Rictor, suggesting a role for MYO1C in the PI3K pathway. This study was designed to examine MYO1C expression status in a panel of well-stratified endometrial carcinomas as well as to assess the biological significance of MYO1C as a tumor suppressor in vitro. We found a significant correlation between the tumor stage and lowered expression of MYO1C in endometrial carcinoma samples. In cell transfection experiments, we found a negative correlation between MYO1C expression and cell proliferation, and MYO1C silencing resulted in diminished cell migration and adhesion. Cells expressing excess of MYO1C had low basal level of phosphorylated protein kinase B (PKB, a.k.a. AKT) and cells with knocked down MYO1C expression showed a quicker phosphorylated AKT (pAKT) response in reaction to serum stimulation. Taken together the present study gives further evidence for tumor suppressor activity of MYO1C and suggests MYO1C mediates its tumor suppressor function through inhibition of PI3K pathway and its involvement in loss of contact inhibition.
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spelling pubmed-50553412016-10-27 Lowered Expression of Tumor Suppressor Candidate MYO1C Stimulates Cell Proliferation, Suppresses Cell Adhesion and Activates AKT Visuttijai, Kittichate Pettersson, Jennifer Mehrbani Azar, Yashar van den Bout, Iman Örndal, Charlotte Marcickiewicz, Janusz Nilsson, Staffan Hörnquist, Michael Olsson, Björn Ejeskär, Katarina Behboudi, Afrouz PLoS One Research Article Myosin-1C (MYO1C) is a tumor suppressor candidate located in a region of recurrent losses distal to TP53. Myo1c can tightly and specifically bind to PIP2, the substrate of Phosphoinositide 3-kinase (PI3K), and to Rictor, suggesting a role for MYO1C in the PI3K pathway. This study was designed to examine MYO1C expression status in a panel of well-stratified endometrial carcinomas as well as to assess the biological significance of MYO1C as a tumor suppressor in vitro. We found a significant correlation between the tumor stage and lowered expression of MYO1C in endometrial carcinoma samples. In cell transfection experiments, we found a negative correlation between MYO1C expression and cell proliferation, and MYO1C silencing resulted in diminished cell migration and adhesion. Cells expressing excess of MYO1C had low basal level of phosphorylated protein kinase B (PKB, a.k.a. AKT) and cells with knocked down MYO1C expression showed a quicker phosphorylated AKT (pAKT) response in reaction to serum stimulation. Taken together the present study gives further evidence for tumor suppressor activity of MYO1C and suggests MYO1C mediates its tumor suppressor function through inhibition of PI3K pathway and its involvement in loss of contact inhibition. Public Library of Science 2016-10-07 /pmc/articles/PMC5055341/ /pubmed/27716847 http://dx.doi.org/10.1371/journal.pone.0164063 Text en © 2016 Visuttijai et al http://creativecommons.org/licenses/by/4.0/ 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 author and source are credited.
spellingShingle Research Article
Visuttijai, Kittichate
Pettersson, Jennifer
Mehrbani Azar, Yashar
van den Bout, Iman
Örndal, Charlotte
Marcickiewicz, Janusz
Nilsson, Staffan
Hörnquist, Michael
Olsson, Björn
Ejeskär, Katarina
Behboudi, Afrouz
Lowered Expression of Tumor Suppressor Candidate MYO1C Stimulates Cell Proliferation, Suppresses Cell Adhesion and Activates AKT
title Lowered Expression of Tumor Suppressor Candidate MYO1C Stimulates Cell Proliferation, Suppresses Cell Adhesion and Activates AKT
title_full Lowered Expression of Tumor Suppressor Candidate MYO1C Stimulates Cell Proliferation, Suppresses Cell Adhesion and Activates AKT
title_fullStr Lowered Expression of Tumor Suppressor Candidate MYO1C Stimulates Cell Proliferation, Suppresses Cell Adhesion and Activates AKT
title_full_unstemmed Lowered Expression of Tumor Suppressor Candidate MYO1C Stimulates Cell Proliferation, Suppresses Cell Adhesion and Activates AKT
title_short Lowered Expression of Tumor Suppressor Candidate MYO1C Stimulates Cell Proliferation, Suppresses Cell Adhesion and Activates AKT
title_sort lowered expression of tumor suppressor candidate myo1c stimulates cell proliferation, suppresses cell adhesion and activates akt
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5055341/
https://www.ncbi.nlm.nih.gov/pubmed/27716847
http://dx.doi.org/10.1371/journal.pone.0164063
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