The effect of antifibrotic drugs in rat precision-cut fibrotic liver slices.

The effect of antifibrotic drugs in rat precision-cut fibrotic liver slices.

Two important signaling pathways in liver fibrosis are the PDGF- and TGFβ pathway and compounds inhibiting these pathways are currently developed as antifibrotic drugs. Testing antifibrotic drugs requires large numbers of animal experiments with high discomfort. Therefore, a method to study these dr...

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Main Authors: Inge M Westra, Dorenda Oosterhuis, Geny M M Groothuis, Peter Olinga
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3995767?pdf=render
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spelling doaj-b71651fb584e4b05980e273a07652e892020-11-25T01:59:46ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0194e9546210.1371/journal.pone.0095462The effect of antifibrotic drugs in rat precision-cut fibrotic liver slices.Inge M WestraDorenda OosterhuisGeny M M GroothuisPeter OlingaTwo important signaling pathways in liver fibrosis are the PDGF- and TGFβ pathway and compounds inhibiting these pathways are currently developed as antifibrotic drugs. Testing antifibrotic drugs requires large numbers of animal experiments with high discomfort. Therefore, a method to study these drugs ex vivo was developed using precision-cut liver slices from fibrotic rat livers (fPCLS), representing an ex vivo model with a multicellular fibrotic environment. We characterized the fibrotic process in fPCLS from rat livers after 3 weeks of bile duct ligation (BDL) during incubation and tested compounds predominantly inhibiting the TGFβ pathway (perindopril, valproic acid, rosmarinic acid, tetrandrine and pirfenidone) and PDGF pathway (imatinib, sorafenib and sunitinib). Gene expression of heat shock protein 47 (Hsp47), α smooth muscle actin (αSma) and pro-collagen 1A1 (Pcol1A1) and protein expression of collagens were determined. During 48 hours of incubation, the fibrosis process continued in control fPCLS as judged by the increased gene expression of the three fibrosis markers, and the protein expression of collagen 1, mature fibrillar collagen and total collagen. Most PDGF-inhibitors and TGFβ-inhibitors significantly inhibited the increase in gene expression of Hsp47, αSma and Pcol1A1. Protein expression of collagen 1 was significantly reduced by all PDGF-inhibitors and TGFβ-inhibitors, while total collagen was decreased by rosmarinic acid and tetrandrine only. However, fibrillar collagen expression was not changed by any of the drugs. In conclusion, rat fPCLS can be used as a functional ex vivo model of established liver fibrosis to test antifibrotic compounds inhibiting the PDGF- and TGFβ signalling pathway.http://europepmc.org/articles/PMC3995767?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Inge M Westra
Dorenda Oosterhuis
Geny M M Groothuis
Peter Olinga
spellingShingle Inge M Westra
Dorenda Oosterhuis
Geny M M Groothuis
Peter Olinga
The effect of antifibrotic drugs in rat precision-cut fibrotic liver slices.
PLoS ONE
author_facet Inge M Westra
Dorenda Oosterhuis
Geny M M Groothuis
Peter Olinga
author_sort Inge M Westra
title The effect of antifibrotic drugs in rat precision-cut fibrotic liver slices.
title_short The effect of antifibrotic drugs in rat precision-cut fibrotic liver slices.
title_full The effect of antifibrotic drugs in rat precision-cut fibrotic liver slices.
title_fullStr The effect of antifibrotic drugs in rat precision-cut fibrotic liver slices.
title_full_unstemmed The effect of antifibrotic drugs in rat precision-cut fibrotic liver slices.
title_sort effect of antifibrotic drugs in rat precision-cut fibrotic liver slices.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Two important signaling pathways in liver fibrosis are the PDGF- and TGFβ pathway and compounds inhibiting these pathways are currently developed as antifibrotic drugs. Testing antifibrotic drugs requires large numbers of animal experiments with high discomfort. Therefore, a method to study these drugs ex vivo was developed using precision-cut liver slices from fibrotic rat livers (fPCLS), representing an ex vivo model with a multicellular fibrotic environment. We characterized the fibrotic process in fPCLS from rat livers after 3 weeks of bile duct ligation (BDL) during incubation and tested compounds predominantly inhibiting the TGFβ pathway (perindopril, valproic acid, rosmarinic acid, tetrandrine and pirfenidone) and PDGF pathway (imatinib, sorafenib and sunitinib). Gene expression of heat shock protein 47 (Hsp47), α smooth muscle actin (αSma) and pro-collagen 1A1 (Pcol1A1) and protein expression of collagens were determined. During 48 hours of incubation, the fibrosis process continued in control fPCLS as judged by the increased gene expression of the three fibrosis markers, and the protein expression of collagen 1, mature fibrillar collagen and total collagen. Most PDGF-inhibitors and TGFβ-inhibitors significantly inhibited the increase in gene expression of Hsp47, αSma and Pcol1A1. Protein expression of collagen 1 was significantly reduced by all PDGF-inhibitors and TGFβ-inhibitors, while total collagen was decreased by rosmarinic acid and tetrandrine only. However, fibrillar collagen expression was not changed by any of the drugs. In conclusion, rat fPCLS can be used as a functional ex vivo model of established liver fibrosis to test antifibrotic compounds inhibiting the PDGF- and TGFβ signalling pathway.
url http://europepmc.org/articles/PMC3995767?pdf=render
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