| Literature DB >> 24794893 |
Eliz Amar-Lewis1, Aharon Azagury1, Ramesh Chintakunta1, Riki Goldbart1, Tamar Traitel1, Jackson Prestwood2, Dalit Landesman-Milo3, Dan Peer3, Joseph Kost4.
Abstract
RNAi therapeutics is a powerful tool for treating diseases by sequence-specific targeting of genes using siRNA. Since its discovery, the need for a safe and efficient delivery system for siRNA has increased. Here, we have developed and characterized a delivery platform for siRNA based on the natural polysaccharide starch in an attempt to address unresolved delivery challenges of RNAi. Modified potato starch (Q-starch) was successfully obtained by substitution with quaternary reagent, providing Q-starch with cationic properties. The results indicate that Q-starch was able to bind siRNA by self-assembly formation of complexes. For efficient and potent gene silencing we monitored the physical characteristics of the formed nanoparticles at increasing N/P molar ratios. The minimum ratio for complete entrapment of siRNA was 2. The resulting complexes, which were characterized by a small diameter (~30 nm) and positive surface charge, were able to protect siRNA from enzymatic degradation. Q-starch/siRNA complexes efficiently induced P-glycoprotein (P-gp) gene silencing in the human ovarian adenocarcinoma cell line, NCI-ADR/Res (NAR), over expressing the targeted gene and presenting low toxicity. Additionally, Q-starch-based complexes showed high cellular uptake during a 24-hour study, which also suggested that intracellular siRNA delivery barriers governed the kinetics of siRNA transfection. In this study, we have devised a promising siRNA delivery vector based on a starch derivative for efficient and safe RNAi application.Entities:
Keywords: Drug delivery; Polysaccharide; Quaternized starch; Self-assembly complexes; Small interfering RNA
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Year: 2014 PMID: 24794893 DOI: 10.1016/j.jconrel.2014.04.031
Source DB: PubMed Journal: J Control Release ISSN: 0168-3659 Impact factor: 9.776