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Neuroblastoma RAS viral oncogene homolog (N-RAS) deficiency aggravates liver injury and fibrosis

Authors :
Kang, Zheng
Fengjie, Hao
Medrano García, Sandra
Chaobo, Chen
Morán Blanco, Laura
Peligros Gómez, María Isabel
Bañares Cañizares, Rafael
Vaquero Martín, Francisco Javier
Gómez Del Moral Martín-Consuegra, Manuel María
Regueiro González-Barros, José Ramón
Martínez Naves, Eduardo
Gallego Durán, Rocío
Maya, Douglas
Ampuero, Javier
Romero Gómez, Manuel
Gilbert Ramos, Albert
Guixé Muntet, Sergi
Fernández Iglesias, Anabel
Gracia Sancho, Jordi
Coll, Mar
Graupera, Isabel
Ginès, Pere
Pericàs, Juan M.
Ramos Molina, Bruno
Herranz, José María
Ávila, Matías A.
Nevzorova, Yulia
Fernández Malavé, Edgar Gonzalo
Cubero Palero, Francisco Javier
Kang, Zheng
Fengjie, Hao
Medrano García, Sandra
Chaobo, Chen
Morán Blanco, Laura
Peligros Gómez, María Isabel
Bañares Cañizares, Rafael
Vaquero Martín, Francisco Javier
Gómez Del Moral Martín-Consuegra, Manuel María
Regueiro González-Barros, José Ramón
Martínez Naves, Eduardo
Gallego Durán, Rocío
Maya, Douglas
Ampuero, Javier
Romero Gómez, Manuel
Gilbert Ramos, Albert
Guixé Muntet, Sergi
Fernández Iglesias, Anabel
Gracia Sancho, Jordi
Coll, Mar
Graupera, Isabel
Ginès, Pere
Pericàs, Juan M.
Ramos Molina, Bruno
Herranz, José María
Ávila, Matías A.
Nevzorova, Yulia
Fernández Malavé, Edgar Gonzalo
Cubero Palero, Francisco Javier
Publication Year :
2024

Abstract

Progressive hepatic damage and fibrosis are major features of chronic liver diseases of different etiology, yet the underlying molecular mechanisms remain to be fully defined. N-RAS, a member of the RAS family of small guanine nucleotide-binding proteins also encompassing the highly homologous H-RAS and K-RAS isoforms, was previously reported to modulate cell death and renal fibrosis; however, its role in liver damage and fibrogenesis remains unknown. Here, we approached this question by using N-RAS deficient (N-RAS-/-) mice and two experimental models of liver injury and fibrosis, namely carbon tetrachloride (CCl4) intoxication and bile duct ligation (BDL). In wild-type (N-RAS+/+) mice both hepatotoxic procedures augmented N-RAS expression in the liver. Compared to N-RAS+/+ counterparts, N-RAS-/- mice subjected to either CCl4 or BDL showed exacerbated liver injury and fibrosis, which was associated with enhanced hepatic stellate cell (HSC) activation and leukocyte infiltration in the damaged liver. At the molecular level, after CCl4 or BDL, N-RAS-/- livers exhibited augmented expression of necroptotic death markers along with JNK1/2 hyperactivation. In line with this, N-RAS ablation in a human hepatocytic cell line resulted in enhanced activation of JNK and necroptosis mediators in response to cell death stimuli. Of note, loss of hepatic N-RAS expression was characteristic of chronic liver disease patients with fibrosis. Collectively, our study unveils a novel role for N-RAS as a negative controller of the progression of liver injury and fibrogenesis, by critically downregulating signaling pathways leading to hepatocyte necroptosis. Furthermore, it suggests that N-RAS may be of potential clinical value as prognostic biomarker of progressive fibrotic liver damage, or as a novel therapeutic target for the treatment of chronic liver disease.<br />Ministerio de Ciencia e Innovación<br />Unión Europea<br />Comunidad de Madrid<br />Depto. de Inmunología, Oftalmología y ORL<br />Fac. de Medicina<br />TRUE<br />pub

Details

Database :
OAIster
Notes :
application/pdf, 2041-4889, English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1429626259
Document Type :
Electronic Resource

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