Non-viral systemic delivery of Fas siRNA suppresses cyclophosphamide-induced diabetes in NOD mice

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A membrane receptor, Fas (CD95), and its ligand FasL have been considered as key players in diabetes pathogenesis. They are known to mediate interactions between beta cells and cytotoxic T cells, which results in apoptotic cell death. We hypothesized that the interruption of Fas-FasL interactions by suppressing Fas expression in beta cells would affect the development of diabetes. The effect of Fas-silencing siRNA (Fas siRNA) on diabetes development was evaluated in a cyclophosphamide (CY)-accelerated diabetes animal model after intravenous administration using a polymeric carrier, polyethylenimine (PEI). The systemic non-viral delivery of Fas siRNA showed significant delay in diabetes incidence up to 40 days, while the control mice treated with naked Fas siRNA, scrambled dsRNA, or PBS were afflicted with diabetes within 20 days. The retardation of diabetes incidence after the treatment of Fas siRNA may be due to the delayed progression of the pancreatic insulitis. In this study, the potential use of a non-viral carrier based siRNA gene therapy for the prevention of type-1 diabetes is demonstrated. (C) 2009 Elsevier B.V. All rights reserved.
Publisher
Elsevier Science Bv
Issue Date
2010-04
Language
English
Article Type
Article
Keywords

BETA-CELL DESTRUCTION; CHRONIC AUTOIMMUNE-DISEASE; IN-VIVO; T-CELLS; GENE-EXPRESSION; POLYETHYLENIMINE; MECHANISMS; COMPLEXES; DNA; PHARMACOKINETICS

Citation

JOURNAL OF CONTROLLED RELEASE, v.143, no.1, pp.88 - 94

ISSN
0168-3659
DOI
10.1016/j.jconrel.2009.12.005
URI
http://hdl.handle.net/10203/93453
Appears in Collection
BS-Journal Papers(저널논문)
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