Emricasan Ameliorates Portal Hypertension and Liver Fibrosis in Cirrhotic Rats Through a Hepatocyte‐Mediated Paracrine Mechanism

In cirrhosis, liver microvascular dysfunction is a key factor increasing hepatic vascular resistance to portal blood flow, which leads to portal hypertension. De‐regulated inflammatory and pro‐apoptotic processes due to chronic injury play important roles in the dysfunction of liver sinusoidal cells...

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Autores principales: Gracia‐Sancho, Jordi, Manicardi, Nicolò, Ortega‐Ribera, Martí, Maeso‐Díaz, Raquel, Guixé‐Muntet, Sergi, Fernández‐Iglesias, Anabel, Hide, Diana, García‐Calderó, Héctor, Boyer‐Díaz, Zoe, Contreras, Patricia C., Spada, Alfred, Bosch, Jaime
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6601324/
https://www.ncbi.nlm.nih.gov/pubmed/31304452
http://dx.doi.org/10.1002/hep4.1360
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author Gracia‐Sancho, Jordi
Manicardi, Nicolò
Ortega‐Ribera, Martí
Maeso‐Díaz, Raquel
Guixé‐Muntet, Sergi
Fernández‐Iglesias, Anabel
Hide, Diana
García‐Calderó, Héctor
Boyer‐Díaz, Zoe
Contreras, Patricia C.
Spada, Alfred
Bosch, Jaime
author_facet Gracia‐Sancho, Jordi
Manicardi, Nicolò
Ortega‐Ribera, Martí
Maeso‐Díaz, Raquel
Guixé‐Muntet, Sergi
Fernández‐Iglesias, Anabel
Hide, Diana
García‐Calderó, Héctor
Boyer‐Díaz, Zoe
Contreras, Patricia C.
Spada, Alfred
Bosch, Jaime
author_sort Gracia‐Sancho, Jordi
collection PubMed
description In cirrhosis, liver microvascular dysfunction is a key factor increasing hepatic vascular resistance to portal blood flow, which leads to portal hypertension. De‐regulated inflammatory and pro‐apoptotic processes due to chronic injury play important roles in the dysfunction of liver sinusoidal cells. The present study aimed at characterizing the effects of the pan‐caspase inhibitor emricasan on systemic and hepatic hemodynamics, hepatic cells phenotype, and underlying mechanisms in preclinical models of advanced chronic liver disease. We investigated the effects of 7‐day emricasan on hepatic and systemic hemodynamics, liver function, hepatic microcirculatory function, inflammation, fibrosis, hepatic cells phenotype, and paracrine interactions in rats with advanced cirrhosis due to chronic CCl(4) administration. The hepato‐protective effects of emricasan were additionally investigated in cells isolated from human cirrhotic livers. Cirrhotic rats receiving emricasan showed significantly lower portal pressure than vehicle‐treated animals with no changes in portal blood flow, indicating improved vascular resistance. Hemodynamic improvement was associated with significantly better liver function, reduced hepatic inflammation, improved phenotype of hepatocytes, liver sinusoidal endothelial cells, hepatic stellate cells and macrophages, and reduced fibrosis. In vitro experiments demonstrated that emricasan exerted its benefits directly improving hepatocytes’ expression of specific markers and synthetic capacity, and ameliorated nonparenchymal cells through a paracrine mechanism mediated by small extracellular vesicles released by hepatocytes. Conclusion: This study demonstrates that emricasan improves liver sinusoidal microvascular dysfunction in cirrhosis, which leads to marked amelioration in fibrosis, portal hypertension and liver function, and therefore encourages its clinical evaluation in the treatment of advanced chronic liver disease.
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spelling pubmed-66013242019-07-12 Emricasan Ameliorates Portal Hypertension and Liver Fibrosis in Cirrhotic Rats Through a Hepatocyte‐Mediated Paracrine Mechanism Gracia‐Sancho, Jordi Manicardi, Nicolò Ortega‐Ribera, Martí Maeso‐Díaz, Raquel Guixé‐Muntet, Sergi Fernández‐Iglesias, Anabel Hide, Diana García‐Calderó, Héctor Boyer‐Díaz, Zoe Contreras, Patricia C. Spada, Alfred Bosch, Jaime Hepatol Commun Original Articles In cirrhosis, liver microvascular dysfunction is a key factor increasing hepatic vascular resistance to portal blood flow, which leads to portal hypertension. De‐regulated inflammatory and pro‐apoptotic processes due to chronic injury play important roles in the dysfunction of liver sinusoidal cells. The present study aimed at characterizing the effects of the pan‐caspase inhibitor emricasan on systemic and hepatic hemodynamics, hepatic cells phenotype, and underlying mechanisms in preclinical models of advanced chronic liver disease. We investigated the effects of 7‐day emricasan on hepatic and systemic hemodynamics, liver function, hepatic microcirculatory function, inflammation, fibrosis, hepatic cells phenotype, and paracrine interactions in rats with advanced cirrhosis due to chronic CCl(4) administration. The hepato‐protective effects of emricasan were additionally investigated in cells isolated from human cirrhotic livers. Cirrhotic rats receiving emricasan showed significantly lower portal pressure than vehicle‐treated animals with no changes in portal blood flow, indicating improved vascular resistance. Hemodynamic improvement was associated with significantly better liver function, reduced hepatic inflammation, improved phenotype of hepatocytes, liver sinusoidal endothelial cells, hepatic stellate cells and macrophages, and reduced fibrosis. In vitro experiments demonstrated that emricasan exerted its benefits directly improving hepatocytes’ expression of specific markers and synthetic capacity, and ameliorated nonparenchymal cells through a paracrine mechanism mediated by small extracellular vesicles released by hepatocytes. Conclusion: This study demonstrates that emricasan improves liver sinusoidal microvascular dysfunction in cirrhosis, which leads to marked amelioration in fibrosis, portal hypertension and liver function, and therefore encourages its clinical evaluation in the treatment of advanced chronic liver disease. John Wiley and Sons Inc. 2019-04-22 /pmc/articles/PMC6601324/ /pubmed/31304452 http://dx.doi.org/10.1002/hep4.1360 Text en © 2019 The Authors. Hepatology Communications published by Wiley Periodicals, Inc., on behalf of the American Association for the Study of Liver Diseases. This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc-nd/4.0/ License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Original Articles
Gracia‐Sancho, Jordi
Manicardi, Nicolò
Ortega‐Ribera, Martí
Maeso‐Díaz, Raquel
Guixé‐Muntet, Sergi
Fernández‐Iglesias, Anabel
Hide, Diana
García‐Calderó, Héctor
Boyer‐Díaz, Zoe
Contreras, Patricia C.
Spada, Alfred
Bosch, Jaime
Emricasan Ameliorates Portal Hypertension and Liver Fibrosis in Cirrhotic Rats Through a Hepatocyte‐Mediated Paracrine Mechanism
title Emricasan Ameliorates Portal Hypertension and Liver Fibrosis in Cirrhotic Rats Through a Hepatocyte‐Mediated Paracrine Mechanism
title_full Emricasan Ameliorates Portal Hypertension and Liver Fibrosis in Cirrhotic Rats Through a Hepatocyte‐Mediated Paracrine Mechanism
title_fullStr Emricasan Ameliorates Portal Hypertension and Liver Fibrosis in Cirrhotic Rats Through a Hepatocyte‐Mediated Paracrine Mechanism
title_full_unstemmed Emricasan Ameliorates Portal Hypertension and Liver Fibrosis in Cirrhotic Rats Through a Hepatocyte‐Mediated Paracrine Mechanism
title_short Emricasan Ameliorates Portal Hypertension and Liver Fibrosis in Cirrhotic Rats Through a Hepatocyte‐Mediated Paracrine Mechanism
title_sort emricasan ameliorates portal hypertension and liver fibrosis in cirrhotic rats through a hepatocyte‐mediated paracrine mechanism
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6601324/
https://www.ncbi.nlm.nih.gov/pubmed/31304452
http://dx.doi.org/10.1002/hep4.1360
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