RhoA promotes epidermal stem cell proliferation via PKN1-cyclin D1 signaling.

OBJECTIVE:Epidermal stem cells (ESCs) play a critical role in wound healing, but the mechanism underlying ESC proliferation is not well defined. Here, we explore the effects of RhoA on ESC proliferation and the possible underlying mechanism. METHODS:Human ESCs were enriched by rapid adhesion to coll...

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Main Authors: Fan Wang, Rixing Zhan, Liang Chen, Xia Dai, Wenping Wang, Rui Guo, Xiaoge Li, Zhe Li, Liang Wang, Shupeng Huang, Jie Shen, Shirong Li, Chuan Cao
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2017-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5319766?pdf=render
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spelling doaj-42e42bf2ebed4d8bbc8af3901bff505f2020-11-24T20:41:37ZengPublic Library of Science (PLoS)PLoS ONE1932-62032017-01-01122e017261310.1371/journal.pone.0172613RhoA promotes epidermal stem cell proliferation via PKN1-cyclin D1 signaling.Fan WangRixing ZhanLiang ChenXia DaiWenping WangRui GuoXiaoge LiZhe LiLiang WangShupeng HuangJie ShenShirong LiChuan CaoOBJECTIVE:Epidermal stem cells (ESCs) play a critical role in wound healing, but the mechanism underlying ESC proliferation is not well defined. Here, we explore the effects of RhoA on ESC proliferation and the possible underlying mechanism. METHODS:Human ESCs were enriched by rapid adhesion to collagen IV. RhoA(+/+)(G14V), RhoA(-/-)(T19N) and pGFP control plasmids were transfected into human ESCs. The effect of RhoA on cell proliferation was detected by cell proliferation and DNA synthesis assays. Induction of PKN1 activity by RhoA was determined by immunoblot analysis, and the effects of PKN1 on RhoA in terms of inducing cell proliferation and cyclin D1 expression were detected using specific siRNA targeting PKN1. The effects of U-46619 (a RhoA agonist) and C3 transferase (a RhoA antagonist) on ESC proliferation were observed in vivo. RESULTS:RhoA had a positive effect on ESC proliferation, and PKN1 activity was up-regulated by the active RhoA mutant (G14V) and suppressed by RhoA T19N. Moreover, the ability of RhoA to promote ESC proliferation and DNA synthesis was interrupted by PKN1 siRNA. Additionally, cyclin D1 protein and mRNA expression levels were up-regulated by RhoA G14V, and these effects were inhibited by siRNA-mediated knock-down of PKN1. RhoA also promoted ESC proliferation via PKN in vivo. CONCLUSION:This study shows that the effect of RhoA on ESC proliferation is mediated by activation of the PKN1-cyclin D1 pathway in vitro, suggesting that RhoA may serve as a new therapeutic target for wound healing.http://europepmc.org/articles/PMC5319766?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Fan Wang
Rixing Zhan
Liang Chen
Xia Dai
Wenping Wang
Rui Guo
Xiaoge Li
Zhe Li
Liang Wang
Shupeng Huang
Jie Shen
Shirong Li
Chuan Cao
spellingShingle Fan Wang
Rixing Zhan
Liang Chen
Xia Dai
Wenping Wang
Rui Guo
Xiaoge Li
Zhe Li
Liang Wang
Shupeng Huang
Jie Shen
Shirong Li
Chuan Cao
RhoA promotes epidermal stem cell proliferation via PKN1-cyclin D1 signaling.
PLoS ONE
author_facet Fan Wang
Rixing Zhan
Liang Chen
Xia Dai
Wenping Wang
Rui Guo
Xiaoge Li
Zhe Li
Liang Wang
Shupeng Huang
Jie Shen
Shirong Li
Chuan Cao
author_sort Fan Wang
title RhoA promotes epidermal stem cell proliferation via PKN1-cyclin D1 signaling.
title_short RhoA promotes epidermal stem cell proliferation via PKN1-cyclin D1 signaling.
title_full RhoA promotes epidermal stem cell proliferation via PKN1-cyclin D1 signaling.
title_fullStr RhoA promotes epidermal stem cell proliferation via PKN1-cyclin D1 signaling.
title_full_unstemmed RhoA promotes epidermal stem cell proliferation via PKN1-cyclin D1 signaling.
title_sort rhoa promotes epidermal stem cell proliferation via pkn1-cyclin d1 signaling.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2017-01-01
description OBJECTIVE:Epidermal stem cells (ESCs) play a critical role in wound healing, but the mechanism underlying ESC proliferation is not well defined. Here, we explore the effects of RhoA on ESC proliferation and the possible underlying mechanism. METHODS:Human ESCs were enriched by rapid adhesion to collagen IV. RhoA(+/+)(G14V), RhoA(-/-)(T19N) and pGFP control plasmids were transfected into human ESCs. The effect of RhoA on cell proliferation was detected by cell proliferation and DNA synthesis assays. Induction of PKN1 activity by RhoA was determined by immunoblot analysis, and the effects of PKN1 on RhoA in terms of inducing cell proliferation and cyclin D1 expression were detected using specific siRNA targeting PKN1. The effects of U-46619 (a RhoA agonist) and C3 transferase (a RhoA antagonist) on ESC proliferation were observed in vivo. RESULTS:RhoA had a positive effect on ESC proliferation, and PKN1 activity was up-regulated by the active RhoA mutant (G14V) and suppressed by RhoA T19N. Moreover, the ability of RhoA to promote ESC proliferation and DNA synthesis was interrupted by PKN1 siRNA. Additionally, cyclin D1 protein and mRNA expression levels were up-regulated by RhoA G14V, and these effects were inhibited by siRNA-mediated knock-down of PKN1. RhoA also promoted ESC proliferation via PKN in vivo. CONCLUSION:This study shows that the effect of RhoA on ESC proliferation is mediated by activation of the PKN1-cyclin D1 pathway in vitro, suggesting that RhoA may serve as a new therapeutic target for wound healing.
url http://europepmc.org/articles/PMC5319766?pdf=render
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