Chimeric Capsid Protein as a Nanocarrier for siRNA Delivery: Stability and Cellular Uptake of Encapsulated siRNA

Authors
Choi, Kyung-miChoi, Seung-HyeJeon, HyesungKim, In-SanAhn, Hyung Jun
Issue Date
2011-11
Publisher
AMER CHEMICAL SOC
Citation
ACS NANO, v.5, no.11, pp.8690 - 8699
Abstract
For the efficient cytoplasmic delivery of siRNA, we designed a chimeric capsid protein composed of a capsid shell, integrin targeting peptide, and p19 RNA binding protein. This recombinant protein assembled into a macromolecular container-like structure with capsid shell and provided a nanocarrier for siRNA delivery. Our capsid nanocarriers had dual affinity both for siRNA within the interior and Integin receptors on the exterior, and the capsid shell structure allowed the encapsulated siRNAs to be protected from the external nucleases, leading to the enhanced stability of siRNA in serum conditions. The capsid nanocarriers could complex with siRNA in a size-dependent and sequence-independent manner and showed the pH-dependent complexing/dissocation behaviors with siRNA. Moreover, RGD peptides on the exterior surface of the capsid shell enabled the capsid nanocarriers to deliver siRNA into the cytosol of the target cells. Here, we demonstrated the superior efficiency of our siRNA/capsid nanocarrier complexes in RFP gene silencing, compared to untreated cells. These results provide an alternative approach to enhancing the stability of siRNA as well as to achieving targeted siRNA delivery.
Keywords
SMALL INTERFERING RNA; GENE DELIVERY; IN-VIVO; ELECTRON CRYOMICROSCOPY; SYNTHETIC SIRNAS; MAMMALIAN-CELLS; COATED PIT; VECTORS; EFFICIENT; CYTOTOXICITY; SMALL INTERFERING RNA; GENE DELIVERY; IN-VIVO; ELECTRON CRYOMICROSCOPY; SYNTHETIC SIRNAS; MAMMALIAN-CELLS; COATED PIT; VECTORS; EFFICIENT; CYTOTOXICITY; capsid protein; siRNA delivery; nanocarrier; gene silencing; recombinant proteins
ISSN
1936-0851
URI
https://pubs.kist.re.kr/handle/201004/129846
DOI
10.1021/nn202597c
Appears in Collections:
KIST Article > 2011
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