Targeting CCl4‐induced liver fibrosis by RNA interference–mediated inhibition of cyclin E1 in mice

Autor:	R Sonntag, Ute Haas, Christian Trautwein, Thomas Longerich, Linda Hammerich, JM Bangen, Frank Tacke, Christian Liedtke, D Lambertz, Twan Lammers, Maike Baues
Rok vydání:	2017
Předmět:	0301 basic medicine Liver injury Small interfering RNA Cyclin E Hepatology Biology Cell cycle medicine.disease Cell biology 03 medical and health sciences Cyclin E1 030104 developmental biology RNA interference medicine Cancer research Hepatic stellate cell Leukocyte proliferation
Zdroj:	Hepatology. 66:1242-1257
ISSN:	1527-3350 0270-9139
Popis:	Initiation and progression of liver fibrosis requires proliferation and activation of resting hepatic stellate cells (HSCs). Cyclin E1 (CcnE1) is the regulatory subunit of the cyclin-dependent kinase 2 (Cdk2) and controls cell cycle re-entry. We have recently shown that genetic inactivation of CcnE1 prevents activation, proliferation, and survival of HSCs and protects from liver fibrogenesis. The aim of the present study was to translate these findings into preclinical applications using an RNA interference (RNAi)-based approach. CcnE1-siRNA (small interfering RNA) efficiently inhibited CcnE1 gene expression in murine and human HSC cell lines and in primary HSCs, resulting in diminished proliferation and increased cell death. In C57BL/6 wild-type (WT) mice, delivery of stabilized siRNA using a liposome-based carrier targeted approximately 95% of HSCs, 70% of hepatocytes, and 40% of CD45+ cells after single injection. Acute CCl4 -mediated liver injury in WT mice induced endogenous CcnE1 expression and proliferation of surviving hepatocytes and nonparenchymal cells, including CD45+ leukocytes. Pretreatment with CcnE1-siRNA reverted CcnE1 induction to baseline levels of healthy mice, which was associated with reduced liver injury, diminished proliferation of hepatocytes and leukocytes, and attenuated overall inflammatory response. For induction of liver fibrosis, WT mice were challenged with CCl4 for 4-6 weeks. Co-treatment with CcnE1-siRNA once a week was sufficient to continuously block CcnE1 expression and cell-cycle activity of hepatocytes and nonparenchymal cells, resulting in significantly ameliorated liver fibrosis and inflammation. Importantly, CcnE1-siRNA also prevented progression of liver fibrosis if applied after onset of chronic liver injury. Conclusion Therapeutic targeting of CcnE1 in vivo using RNAi is feasible and has high antifibrotic activity. (Hepatology 2017;66:1242-1257).
Databáze:	OpenAIRE
Externí odkaz:	https://explore.openaire.eu/search/publication?articleId=doi_________::dcb597fd4d3334a5175d0c71c98e0c7c https://doi.org/10.1002/hep.29275 Zobrazit plný text záznamu Plný text