Dual targeting of MEK and PI3K pathways attenuates established and progressive pulmonary fibrosis.

Dual targeting of MEK and PI3K pathways attenuates established and progressive pulmonary fibrosis.

Pulmonary fibrosis is often triggered by an epithelial injury resulting in the formation of fibrotic lesions in the lung, which progress to impair gas exchange and ultimately cause death. Recent clinical trials using drugs that target either inflammation or a specific molecule have failed, suggestin...

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Main Authors: Satish K Madala, Ramakrishna Edukulla, Mukta Phatak, Stephanie Schmidt, Cynthia Davidson, Thomas H Acciani, Thomas R Korfhagen, Mario Medvedovic, Timothy D Lecras, Kimberly Wagner, William D Hardie
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3903543?pdf=render
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spelling doaj-5fb8647e6d61433688aba3e7316ff4732020-11-24T22:16:54ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0191e8653610.1371/journal.pone.0086536Dual targeting of MEK and PI3K pathways attenuates established and progressive pulmonary fibrosis.Satish K MadalaRamakrishna EdukullaMukta PhatakStephanie SchmidtCynthia DavidsonThomas H AccianiThomas R KorfhagenMario MedvedovicTimothy D LecrasKimberly WagnerWilliam D HardiePulmonary fibrosis is often triggered by an epithelial injury resulting in the formation of fibrotic lesions in the lung, which progress to impair gas exchange and ultimately cause death. Recent clinical trials using drugs that target either inflammation or a specific molecule have failed, suggesting that multiple pathways and cellular processes need to be attenuated for effective reversal of established and progressive fibrosis. Although activation of MAPK and PI3K pathways have been detected in human fibrotic lung samples, the therapeutic benefits of in vivo modulation of the MAPK and PI3K pathways in combination are unknown. Overexpression of TGFα in the lung epithelium of transgenic mice results in the formation of fibrotic lesions similar to those found in human pulmonary fibrosis, and previous work from our group shows that inhibitors of either the MAPK or PI3K pathway can alter the progression of fibrosis. In this study, we sought to determine whether simultaneous inhibition of the MAPK and PI3K signaling pathways is a more effective therapeutic strategy for established and progressive pulmonary fibrosis. Our results showed that inhibiting both pathways had additive effects compared to inhibiting either pathway alone in reducing fibrotic burden, including reducing lung weight, pleural thickness, and total collagen in the lungs of TGFα mice. This study demonstrates that inhibiting MEK and PI3K in combination abolishes proliferative changes associated with fibrosis and myfibroblast accumulation and thus may serve as a therapeutic option in the treatment of human fibrotic lung disease where these pathways play a role.http://europepmc.org/articles/PMC3903543?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Satish K Madala
Ramakrishna Edukulla
Mukta Phatak
Stephanie Schmidt
Cynthia Davidson
Thomas H Acciani
Thomas R Korfhagen
Mario Medvedovic
Timothy D Lecras
Kimberly Wagner
William D Hardie
spellingShingle Satish K Madala
Ramakrishna Edukulla
Mukta Phatak
Stephanie Schmidt
Cynthia Davidson
Thomas H Acciani
Thomas R Korfhagen
Mario Medvedovic
Timothy D Lecras
Kimberly Wagner
William D Hardie
Dual targeting of MEK and PI3K pathways attenuates established and progressive pulmonary fibrosis.
PLoS ONE
author_facet Satish K Madala
Ramakrishna Edukulla
Mukta Phatak
Stephanie Schmidt
Cynthia Davidson
Thomas H Acciani
Thomas R Korfhagen
Mario Medvedovic
Timothy D Lecras
Kimberly Wagner
William D Hardie
author_sort Satish K Madala
title Dual targeting of MEK and PI3K pathways attenuates established and progressive pulmonary fibrosis.
title_short Dual targeting of MEK and PI3K pathways attenuates established and progressive pulmonary fibrosis.
title_full Dual targeting of MEK and PI3K pathways attenuates established and progressive pulmonary fibrosis.
title_fullStr Dual targeting of MEK and PI3K pathways attenuates established and progressive pulmonary fibrosis.
title_full_unstemmed Dual targeting of MEK and PI3K pathways attenuates established and progressive pulmonary fibrosis.
title_sort dual targeting of mek and pi3k pathways attenuates established and progressive pulmonary fibrosis.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Pulmonary fibrosis is often triggered by an epithelial injury resulting in the formation of fibrotic lesions in the lung, which progress to impair gas exchange and ultimately cause death. Recent clinical trials using drugs that target either inflammation or a specific molecule have failed, suggesting that multiple pathways and cellular processes need to be attenuated for effective reversal of established and progressive fibrosis. Although activation of MAPK and PI3K pathways have been detected in human fibrotic lung samples, the therapeutic benefits of in vivo modulation of the MAPK and PI3K pathways in combination are unknown. Overexpression of TGFα in the lung epithelium of transgenic mice results in the formation of fibrotic lesions similar to those found in human pulmonary fibrosis, and previous work from our group shows that inhibitors of either the MAPK or PI3K pathway can alter the progression of fibrosis. In this study, we sought to determine whether simultaneous inhibition of the MAPK and PI3K signaling pathways is a more effective therapeutic strategy for established and progressive pulmonary fibrosis. Our results showed that inhibiting both pathways had additive effects compared to inhibiting either pathway alone in reducing fibrotic burden, including reducing lung weight, pleural thickness, and total collagen in the lungs of TGFα mice. This study demonstrates that inhibiting MEK and PI3K in combination abolishes proliferative changes associated with fibrosis and myfibroblast accumulation and thus may serve as a therapeutic option in the treatment of human fibrotic lung disease where these pathways play a role.
url http://europepmc.org/articles/PMC3903543?pdf=render
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