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SMAD inhibition attenuates epithelial to mesenchymal transition by primary keratinocytes in vitro

Epithelial to mesenchymal transition (EMT) is a process whereby epithelial cells undergo transition to a mesenchymal phenotype and contribute directly to fibrotic disease. Recent studies support a role for EMT in cutaneous fibrotic diseases including scleroderma and hypertrophic scarring, although t...

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Published in:	Experimental dermatology 2014-07, Vol.23 (7), p.497-503
Main Authors:	O'Kane, Donal, Jackson, Megan V., Kissenpfennig, Adrien, Spence, Shaun, Damkat-Thomas, Lindsay, Tolland, Julia P., Smyth, Anita E., Denton, Christopher P., Stuart Elborn, J., McAuley, Daniel F., O'Kane, Cecilia M.
Format:	Article
Language:	English
Subjects:	Benzamides - chemistry Collagen - metabolism Cytokines - metabolism Dioxoles - chemistry Down-Regulation Epidermis - cytology epithelial to mesenchymal transition Epithelial-Mesenchymal Transition Fibronectins - metabolism Fibrosis - metabolism Humans keratinocyte Keratinocytes - cytology Matrix Metalloproteinases - metabolism p38 Mitogen-Activated Protein Kinases - metabolism Recombinant Proteins - metabolism Signal Transduction Smad Proteins - antagonists & inhibitors Smad Proteins - metabolism Transforming Growth Factor beta - metabolism transforming growth factor-β Tumor Necrosis Factor-alpha - metabolism tumor necrosis factor-α Vimentin - metabolism
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cited_by	cdi_FETCH-LOGICAL-c3632-9ada9c941664aec278f9894c73258d897e4d6aba39b17466135c189080a29bc3
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container_title	Experimental dermatology
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creator	O'Kane, Donal Jackson, Megan V. Kissenpfennig, Adrien Spence, Shaun Damkat-Thomas, Lindsay Tolland, Julia P. Smyth, Anita E. Denton, Christopher P. Stuart Elborn, J. McAuley, Daniel F. O'Kane, Cecilia M.
description	Epithelial to mesenchymal transition (EMT) is a process whereby epithelial cells undergo transition to a mesenchymal phenotype and contribute directly to fibrotic disease. Recent studies support a role for EMT in cutaneous fibrotic diseases including scleroderma and hypertrophic scarring, although there is limited data on the cytokines and signalling mechanisms regulating cutaneous EMT. We investigated the ability of TGF‐β and TNF‐α, both overexpressed in cutaneous scleroderma and central mediators of EMT in other epithelial cell types, to induce EMT in primary keratinocytes and studied the signalling mechanisms regulating this process. TGF‐β induced EMT in normal human epidermal keratinocytes (NHEK cells), and this process was enhanced by TNF‐α. EMT was characterised by changes in morphology, proteome (down‐regulation of E‐cadherin and Zo‐1 and up‐regulation of vimentin and fibronectin), MMP secretion and COL1α1 mRNA expression. TGF‐β and TNF‐α in combination activated SMAD and p38 signalling in NHEK cells. P38 inhibition with SB203580 partially attenuated EMT, whereas SMAD inhibition using SB431542 significantly inhibited EMT and also reversed established EMT. These data highlight the retained plasticity of adult keratinocytes and support further studies of EMT in clinically relevant in vivo models of cutaneous fibrosis and investigation of SMAD inhibition as a potential therapeutic intervention.
doi_str_mv	10.1111/exd.12452
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Recent studies support a role for EMT in cutaneous fibrotic diseases including scleroderma and hypertrophic scarring, although there is limited data on the cytokines and signalling mechanisms regulating cutaneous EMT. We investigated the ability of TGF‐β and TNF‐α, both overexpressed in cutaneous scleroderma and central mediators of EMT in other epithelial cell types, to induce EMT in primary keratinocytes and studied the signalling mechanisms regulating this process. TGF‐β induced EMT in normal human epidermal keratinocytes (NHEK cells), and this process was enhanced by TNF‐α. EMT was characterised by changes in morphology, proteome (down‐regulation of E‐cadherin and Zo‐1 and up‐regulation of vimentin and fibronectin), MMP secretion and COL1α1 mRNA expression. TGF‐β and TNF‐α in combination activated SMAD and p38 signalling in NHEK cells. P38 inhibition with SB203580 partially attenuated EMT, whereas SMAD inhibition using SB431542 significantly inhibited EMT and also reversed established EMT. These data highlight the retained plasticity of adult keratinocytes and support further studies of EMT in clinically relevant in vivo models of cutaneous fibrosis and investigation of SMAD inhibition as a potential therapeutic intervention.</description><identifier>ISSN: 0906-6705</identifier><identifier>EISSN: 1600-0625</identifier><identifier>DOI: 10.1111/exd.12452</identifier><identifier>PMID: 24848428</identifier><language>eng</language><publisher>Denmark: Blackwell Publishing Ltd</publisher><subject>Benzamides - chemistry ; Collagen - metabolism ; Cytokines - metabolism ; Dioxoles - chemistry ; Down-Regulation ; Epidermis - cytology ; epithelial to mesenchymal transition ; Epithelial-Mesenchymal Transition ; Fibronectins - metabolism ; Fibrosis - metabolism ; Humans ; keratinocyte ; Keratinocytes - cytology ; Matrix Metalloproteinases - metabolism ; p38 Mitogen-Activated Protein Kinases - metabolism ; Recombinant Proteins - metabolism ; Signal Transduction ; Smad Proteins - antagonists & inhibitors ; Smad Proteins - metabolism ; Transforming Growth Factor beta - metabolism ; transforming growth factor-β ; Tumor Necrosis Factor-alpha - metabolism ; tumor necrosis factor-α ; Vimentin - metabolism</subject><ispartof>Experimental dermatology, 2014-07, Vol.23 (7), p.497-503</ispartof><rights>2014 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd</rights><rights>2014 John Wiley & Sons A/S. 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P38 inhibition with SB203580 partially attenuated EMT, whereas SMAD inhibition using SB431542 significantly inhibited EMT and also reversed established EMT. These data highlight the retained plasticity of adult keratinocytes and support further studies of EMT in clinically relevant in vivo models of cutaneous fibrosis and investigation of SMAD inhibition as a potential therapeutic intervention.</description><subject>Benzamides - chemistry</subject><subject>Collagen - metabolism</subject><subject>Cytokines - metabolism</subject><subject>Dioxoles - chemistry</subject><subject>Down-Regulation</subject><subject>Epidermis - cytology</subject><subject>epithelial to mesenchymal transition</subject><subject>Epithelial-Mesenchymal Transition</subject><subject>Fibronectins - metabolism</subject><subject>Fibrosis - metabolism</subject><subject>Humans</subject><subject>keratinocyte</subject><subject>Keratinocytes - cytology</subject><subject>Matrix Metalloproteinases - metabolism</subject><subject>p38 Mitogen-Activated Protein Kinases - metabolism</subject><subject>Recombinant Proteins - metabolism</subject><subject>Signal Transduction</subject><subject>Smad Proteins - antagonists & inhibitors</subject><subject>Smad Proteins - metabolism</subject><subject>Transforming Growth Factor beta - metabolism</subject><subject>transforming growth factor-β</subject><subject>Tumor Necrosis Factor-alpha - metabolism</subject><subject>tumor necrosis factor-α</subject><subject>Vimentin - metabolism</subject><issn>0906-6705</issn><issn>1600-0625</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2014</creationdate><recordtype>article</recordtype><recordid>eNp1kUlPHDEQhS0UBAPJgT-A-giHBu_LEQ2ERSQ5BClRLpbbXaMx9DLYHkL_-_TQA7dUHUolfe9J9QqhI4LPyFjn8FqfEcoF3UEzIjEusaTiE5phg2UpFRb76CClR4yJYkrsoX3K9dhUz5D7-e3isgjdMlQhh74rXM7QrV2GVMAq5CU0wTVF7osWEnR-ObSbNbouTXw1FKsYWheH4gmiy6Hr_bBRh654CTn2n9HuwjUJvmznIXr4evUwvynvf1zfzi_uS88ko6VxtTPecCIld-Cp0gujDfeKUaFrbRTwWrrKMVMRxaUkTHiiDdbYUVN5dohOJttV7J_XkLJtQ_LQNK6Dfp0sEVwJzqlgI3o6oT72KUVY2O0FlmC7CdSOgdq3QEf2eGu7rlqoP8j3BEfgfAL-hgaG_zvZq9-X75blpAgpw-uHwsUnKzf_sb--X9s7zPVciT8Ws3_6po8e</recordid><startdate>201407</startdate><enddate>201407</enddate><creator>O'Kane, Donal</creator><creator>Jackson, Megan V.</creator><creator>Kissenpfennig, Adrien</creator><creator>Spence, Shaun</creator><creator>Damkat-Thomas, Lindsay</creator><creator>Tolland, Julia P.</creator><creator>Smyth, Anita E.</creator><creator>Denton, Christopher P.</creator><creator>Stuart Elborn, J.</creator><creator>McAuley, Daniel F.</creator><creator>O'Kane, Cecilia M.</creator><general>Blackwell Publishing Ltd</general><scope>BSCLL</scope><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope></search><sort><creationdate>201407</creationdate><title>SMAD inhibition attenuates epithelial to mesenchymal transition by primary keratinocytes in vitro</title><author>O'Kane, Donal ; 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Recent studies support a role for EMT in cutaneous fibrotic diseases including scleroderma and hypertrophic scarring, although there is limited data on the cytokines and signalling mechanisms regulating cutaneous EMT. We investigated the ability of TGF‐β and TNF‐α, both overexpressed in cutaneous scleroderma and central mediators of EMT in other epithelial cell types, to induce EMT in primary keratinocytes and studied the signalling mechanisms regulating this process. TGF‐β induced EMT in normal human epidermal keratinocytes (NHEK cells), and this process was enhanced by TNF‐α. EMT was characterised by changes in morphology, proteome (down‐regulation of E‐cadherin and Zo‐1 and up‐regulation of vimentin and fibronectin), MMP secretion and COL1α1 mRNA expression. TGF‐β and TNF‐α in combination activated SMAD and p38 signalling in NHEK cells. P38 inhibition with SB203580 partially attenuated EMT, whereas SMAD inhibition using SB431542 significantly inhibited EMT and also reversed established EMT. These data highlight the retained plasticity of adult keratinocytes and support further studies of EMT in clinically relevant in vivo models of cutaneous fibrosis and investigation of SMAD inhibition as a potential therapeutic intervention.</abstract><cop>Denmark</cop><pub>Blackwell Publishing Ltd</pub><pmid>24848428</pmid><doi>10.1111/exd.12452</doi><tpages>7</tpages></addata></record>
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subjects	Benzamides - chemistry Collagen - metabolism Cytokines - metabolism Dioxoles - chemistry Down-Regulation Epidermis - cytology epithelial to mesenchymal transition Epithelial-Mesenchymal Transition Fibronectins - metabolism Fibrosis - metabolism Humans keratinocyte Keratinocytes - cytology Matrix Metalloproteinases - metabolism p38 Mitogen-Activated Protein Kinases - metabolism Recombinant Proteins - metabolism Signal Transduction Smad Proteins - antagonists & inhibitors Smad Proteins - metabolism Transforming Growth Factor beta - metabolism transforming growth factor-β Tumor Necrosis Factor-alpha - metabolism tumor necrosis factor-α Vimentin - metabolism
title	SMAD inhibition attenuates epithelial to mesenchymal transition by primary keratinocytes in vitro
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