共 48 条
Foxf1 siRNA Delivery to Hepatic Stellate Cells by DBTC Lipoplex Formulations Ameliorates Fibrosis in Livers of Bile Duct Ligated Mice
被引:18
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Brensel, Malte
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Univ Rostock, Med Ctr, Inst Expt Surg, D-18057 Rostock, Germany Univ Rostock, Med Ctr, Inst Expt Surg, D-18057 Rostock, Germany

Genz, Berit
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Univ Rostock, Med Ctr, Inst Expt Surg, D-18057 Rostock, Germany Univ Rostock, Med Ctr, Inst Expt Surg, D-18057 Rostock, Germany

Roth, Kira
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Univ Rostock, Med Ctr, Inst Expt Surg, D-18057 Rostock, Germany Univ Rostock, Med Ctr, Inst Expt Surg, D-18057 Rostock, Germany

Thomas, Maria
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机构:
Dr Margarete Fischer Bosch Inst Clin Pharmacol, D-70376 Stuttgart, Germany
Univ Tubingen, Tubingen, Germany Univ Rostock, Med Ctr, Inst Expt Surg, D-18057 Rostock, Germany

Fehring, Volker
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Silence Therapeut GmbH, D-13125 Berlin, Germany Univ Rostock, Med Ctr, Inst Expt Surg, D-18057 Rostock, Germany

Schaeper, Ute
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Silence Therapeut GmbH, D-13125 Berlin, Germany Univ Rostock, Med Ctr, Inst Expt Surg, D-18057 Rostock, Germany

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机构:
[1] Univ Rostock, Med Ctr, Inst Expt Surg, D-18057 Rostock, Germany
[2] Dr Margarete Fischer Bosch Inst Clin Pharmacol, D-70376 Stuttgart, Germany
[3] Univ Tubingen, Tubingen, Germany
[4] Silence Therapeut GmbH, D-13125 Berlin, Germany
关键词:
Cholestasis;
chronic liver disease;
intravital microscopy;
lipoplex;
mouse;
silencing;
GROWTH-FACTOR RECEPTOR;
RNA INTERFERENCE;
IN-VIVO;
ACTIVATION;
MIGRATION;
LUNG;
HAPLOINSUFFICIENCY;
CONTRACTION;
HEPATOCYTES;
INHIBITION;
D O I:
10.2174/1566523215666150126114634
中图分类号:
Q3 [遗传学];
学科分类号:
071007 ;
090102 ;
摘要:
Activation of hepatic stellate cells (HSCs) is a key event in pathogenesis of liver fibrosis and represents an orchestral interplay of inhibiting and activating transcription factors like forkhead box f1 (Foxf1), being described to stimulate pro-fibrogenic genes in HSCs. Here, we evaluated a lipidbased liver-specific delivery system (DBTC) suitable to transfer Foxf1 siRNA specifically to HSCs and examined its antifibrotic potential on primary HSCs and LX-2 cells as well as in a murine model of bile duct ligation (BDL)-induced secondary cholestasis. Foxf1 silencing reduced proliferation capacity and attenuated contractility of HSCs. Systemic administration of DBTC-lipoplexes in mice was sufficient to specifically silence genes expressed in different liver cell types. Using intravital and immunofluorescence microscopy we confirmed the specific delivery of Cy3-labeled DBTC to the liver, and particularly to HSCs. Repeated treatment with DBTC-lipoplexes resulted in siRNA-mediated silencing of Foxf1 early after BDL and finally attenuated progression of the fibrotic process. Decreased HSC activation in-effect ameliorated liver injury as shown by substantial reduction of necrotic area and deposition of extracellular matrix. Our findings suggest that Foxf1 may serve as a target gene to disrupt progression of liver fibrosis and DBTC might provide a potentially feasible and effective tool for HSC-specific delivery of therapeutic RNA.
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收藏
页码:215 / 227
页数:13
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