Detalle Publicación

Oral methylthioadenosine administration attenuates fibrosis and chronic liver disease progression in Mdr2-/- mice

Autores: Latasa Sada, María Ujué; Gil Puig, Maria del Carmen; García Fernández de Barrena, Maite; Rodríguez Ortigosa, Carlos Manuel; Bañales Asurmendi, Jesús; Urtasun Alonso, Raquel; Goñi Irigoyen, Saioa; Méndez, Miriam; Arcelus Echávarri, Sara; Juanarena Ancho, Nerea; Recio, Juan A.; Lotersztajn, Sophie; Prieto Valtueña, Jesús María; Berasain Lasarte, María del Carmen; Corrales Izquierdo, Fernando José; Lecanda Cordero, Jon; Ávila Zaragoza, Matías Antonio
Título de la revista: PLoS One
ISSN: 1932-6203
Volumen: 5
Número: 12
Páginas: e15690
Fecha de publicación: 2010
Resumen:
Background: Inflammation and fibrogenesis are directly related to chronic liver disease progression, including hepatocellular carcinoma (HCC) development. Currently there are few therapeutic options available to inhibit liver fibrosis. We have evaluated the hepatoprotective and anti-fibrotic potential of orally-administered 59-methylthioadenosine (MTA) in Mdr2(-/-) mice, a clinically relevant model of sclerosing cholangitis and spontaneous biliary fibrosis, followed at later stages by HCC development. Methodology: MTA was administered daily by gavage to wild type and Mdr2(-/-) mice for three weeks. MTA anti-inflammatory and anti-fibrotic effects and potential mechanisms of action were examined in the liver of Mdr2(-/-) mice with ongoing fibrogenesis and in cultured liver fibrogenic cells (myofibroblasts). Principal Findings: MTA treatment reduced hepatomegaly and liver injury. alpha-Smooth muscle actin immunoreactivity and collagen deposition were also significantly decreased. Inflammatory infiltrate, the expression of the cytokines IL6 and Mcp-1, pro-fibrogenic factors like TGF beta 2 and tenascin-C, as well as pro-fibrogenic intracellular signalling pathways were reduced by MTA in vivo. MTA inhibited the activation and proliferation of isolated myofibroblasts and down-regulated cyclin D1 gene expression at the transcriptional level. The expression of JunD, a key transcription factor in liver fibrogenesis, was also reduced by MTA in activated myofibroblasts. Conclusions/Significance: Oral MTA administration was well tolerated and proved its efficacy in reducing liver inflammation and fibrosis. MTA may have multiple molecular and cellular targets. These include the inhibition of inflammatory and profibrogenic cytokines, as well as the attenuation of myofibroblast activation and proliferation. Downregulation of JunD and cyclin D1 expression in myofibroblasts may be important regarding the mechanism of action of MTA. This compound could be a good candidate to be tested for the treatment of (biliary) liver fibrosis.
Enlace DADUN: http://hdl.handle.net/10171/20237
DOI: https://doi.org/10.1371/journal.pone.0015690
Impacto:
Google Scholar