Dynamic PolyConjugates for targeted  in vivo  delivery of siRNA to hepatocytes

Rozema, David B.; Lewis, David L.; Wakefield, Darren H.; Wong, So C.; Klein, Jason J.; Roesch, P.; Bertin, Stephanie; Reppen, Tom W.; Chu, Qili; Blokhin, Andrei V.; Hagstrom, James E.; Wolff, Jon A.

doi:10.1073/pnas.0703778104

articleProceedings of the National Academy of SciencesJul 24, 2007GREEN OA

Dynamic PolyConjugates for targeted in vivo delivery of siRNA to hepatocytes

DBDavid B. Rozema DLDavid L. Lewis DHDarren H. Wakefield SCSo C. Wong JJJason J. Klein

Mirus Bio (United States) · University of Wisconsin–Madison

PubMed

Indexed incrossrefpubmed

Abstract

Achieving efficient in vivo delivery of siRNA to the appropriate target cell would be a major advance in the use of RNAi in gene function studies and as a therapeutic modality. Hepatocytes, the key parenchymal cells of the liver, are a particularly attractive target cell type for siRNA delivery given their central role in several infectious and metabolic disorders. We have developed a vehicle for the delivery of siRNA to hepatocytes both in vitro and in vivo, which we have named siRNA Dynamic PolyConjugates. Key features of the Dynamic PolyConjugate technology include a membrane-active polymer, the ability to reversibly mask the activity of this polymer until it reaches the acidic environment of endosomes, and…

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Topics & keywords

Topics

Keywords

Gene knockdown
In vivo
RNA interference
Apolipoprotein B
Cell biology
Endosome
Gene delivery
Ex vivo

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