Butyrate Protects against Diet-Induced NASH and Liver Fibrosis and Suppresses Specific Non-Canonical TGF-β Signaling Pathways in Human Hepatic Stellate Cells

In obesity-associated non-alcoholic steatohepatitis (NASH), persistent hepatocellular damage and inflammation are key drivers of fibrosis, which is the main determinant of NASH-associated mortality. The short-chain fatty acid butyrate can exert metabolic improvements and anti-inflammatory activities...

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Autores principales: Gart, Eveline, van Duyvenvoorde, Wim, Toet, Karin, Caspers, Martien P. M., Verschuren, Lars, Nielsen, Mette Juul, Leeming, Diana Julie, Souto Lima, Everton, Menke, Aswin, Hanemaaijer, Roeland, Keijer, Jaap, Salic, Kanita, Kleemann, Robert, Morrison, Martine C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8698820/
https://www.ncbi.nlm.nih.gov/pubmed/34944770
http://dx.doi.org/10.3390/biomedicines9121954
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author Gart, Eveline
van Duyvenvoorde, Wim
Toet, Karin
Caspers, Martien P. M.
Verschuren, Lars
Nielsen, Mette Juul
Leeming, Diana Julie
Souto Lima, Everton
Menke, Aswin
Hanemaaijer, Roeland
Keijer, Jaap
Salic, Kanita
Kleemann, Robert
Morrison, Martine C.
author_facet Gart, Eveline
van Duyvenvoorde, Wim
Toet, Karin
Caspers, Martien P. M.
Verschuren, Lars
Nielsen, Mette Juul
Leeming, Diana Julie
Souto Lima, Everton
Menke, Aswin
Hanemaaijer, Roeland
Keijer, Jaap
Salic, Kanita
Kleemann, Robert
Morrison, Martine C.
author_sort Gart, Eveline
collection PubMed
description In obesity-associated non-alcoholic steatohepatitis (NASH), persistent hepatocellular damage and inflammation are key drivers of fibrosis, which is the main determinant of NASH-associated mortality. The short-chain fatty acid butyrate can exert metabolic improvements and anti-inflammatory activities in NASH. However, its effects on NASH-associated liver fibrosis remain unclear. Putative antifibrotic effects of butyrate were studied in Ldlr-/-.Leiden mice fed an obesogenic diet (HFD) containing 2.5% (w/w) butyrate for 38 weeks and compared with a HFD-control group. Antifibrotic mechanisms of butyrate were further investigated in TGF-β-stimulated primary human hepatic stellate cells (HSC). HFD-fed mice developed obesity, insulin resistance, increased plasma leptin levels, adipose tissue inflammation, gut permeability, dysbiosis, and NASH-associated fibrosis. Butyrate corrected hyperinsulinemia, lowered plasma leptin levels, and attenuated adipose tissue inflammation, without affecting gut permeability or microbiota composition. Butyrate lowered plasma ALT and CK-18M30 levels and attenuated hepatic steatosis and inflammation. Butyrate inhibited fibrosis development as demonstrated by decreased hepatic collagen content and Sirius-red-positive area. In TGF-β-stimulated HSC, butyrate dose-dependently reduced collagen deposition and decreased procollagen1α1 and PAI1 protein expression. Transcriptomic analysis and subsequent pathway and upstream regulator analysis revealed deactivation of specific non-canonical TGF-β signaling pathways Rho-like GTPases and PI3K/AKT and other important pro-fibrotic regulators (e.g., YAP/TAZ, MYC) by butyrate, providing a potential rationale for its antifibrotic effects. In conclusion, butyrate protects against obesity development, insulin resistance-associated NASH, and liver fibrosis. These antifibrotic effects are at least partly attributable to a direct effect of butyrate on collagen production in hepatic stellate cells, involving inhibition of non-canonical TGF-β signaling pathways.
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spelling pubmed-86988202021-12-24 Butyrate Protects against Diet-Induced NASH and Liver Fibrosis and Suppresses Specific Non-Canonical TGF-β Signaling Pathways in Human Hepatic Stellate Cells Gart, Eveline van Duyvenvoorde, Wim Toet, Karin Caspers, Martien P. M. Verschuren, Lars Nielsen, Mette Juul Leeming, Diana Julie Souto Lima, Everton Menke, Aswin Hanemaaijer, Roeland Keijer, Jaap Salic, Kanita Kleemann, Robert Morrison, Martine C. Biomedicines Article In obesity-associated non-alcoholic steatohepatitis (NASH), persistent hepatocellular damage and inflammation are key drivers of fibrosis, which is the main determinant of NASH-associated mortality. The short-chain fatty acid butyrate can exert metabolic improvements and anti-inflammatory activities in NASH. However, its effects on NASH-associated liver fibrosis remain unclear. Putative antifibrotic effects of butyrate were studied in Ldlr-/-.Leiden mice fed an obesogenic diet (HFD) containing 2.5% (w/w) butyrate for 38 weeks and compared with a HFD-control group. Antifibrotic mechanisms of butyrate were further investigated in TGF-β-stimulated primary human hepatic stellate cells (HSC). HFD-fed mice developed obesity, insulin resistance, increased plasma leptin levels, adipose tissue inflammation, gut permeability, dysbiosis, and NASH-associated fibrosis. Butyrate corrected hyperinsulinemia, lowered plasma leptin levels, and attenuated adipose tissue inflammation, without affecting gut permeability or microbiota composition. Butyrate lowered plasma ALT and CK-18M30 levels and attenuated hepatic steatosis and inflammation. Butyrate inhibited fibrosis development as demonstrated by decreased hepatic collagen content and Sirius-red-positive area. In TGF-β-stimulated HSC, butyrate dose-dependently reduced collagen deposition and decreased procollagen1α1 and PAI1 protein expression. Transcriptomic analysis and subsequent pathway and upstream regulator analysis revealed deactivation of specific non-canonical TGF-β signaling pathways Rho-like GTPases and PI3K/AKT and other important pro-fibrotic regulators (e.g., YAP/TAZ, MYC) by butyrate, providing a potential rationale for its antifibrotic effects. In conclusion, butyrate protects against obesity development, insulin resistance-associated NASH, and liver fibrosis. These antifibrotic effects are at least partly attributable to a direct effect of butyrate on collagen production in hepatic stellate cells, involving inhibition of non-canonical TGF-β signaling pathways. MDPI 2021-12-20 /pmc/articles/PMC8698820/ /pubmed/34944770 http://dx.doi.org/10.3390/biomedicines9121954 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Gart, Eveline
van Duyvenvoorde, Wim
Toet, Karin
Caspers, Martien P. M.
Verschuren, Lars
Nielsen, Mette Juul
Leeming, Diana Julie
Souto Lima, Everton
Menke, Aswin
Hanemaaijer, Roeland
Keijer, Jaap
Salic, Kanita
Kleemann, Robert
Morrison, Martine C.
Butyrate Protects against Diet-Induced NASH and Liver Fibrosis and Suppresses Specific Non-Canonical TGF-β Signaling Pathways in Human Hepatic Stellate Cells
title Butyrate Protects against Diet-Induced NASH and Liver Fibrosis and Suppresses Specific Non-Canonical TGF-β Signaling Pathways in Human Hepatic Stellate Cells
title_full Butyrate Protects against Diet-Induced NASH and Liver Fibrosis and Suppresses Specific Non-Canonical TGF-β Signaling Pathways in Human Hepatic Stellate Cells
title_fullStr Butyrate Protects against Diet-Induced NASH and Liver Fibrosis and Suppresses Specific Non-Canonical TGF-β Signaling Pathways in Human Hepatic Stellate Cells
title_full_unstemmed Butyrate Protects against Diet-Induced NASH and Liver Fibrosis and Suppresses Specific Non-Canonical TGF-β Signaling Pathways in Human Hepatic Stellate Cells
title_short Butyrate Protects against Diet-Induced NASH and Liver Fibrosis and Suppresses Specific Non-Canonical TGF-β Signaling Pathways in Human Hepatic Stellate Cells
title_sort butyrate protects against diet-induced nash and liver fibrosis and suppresses specific non-canonical tgf-β signaling pathways in human hepatic stellate cells
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8698820/
https://www.ncbi.nlm.nih.gov/pubmed/34944770
http://dx.doi.org/10.3390/biomedicines9121954
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