Delivery of Small Interfering RNA by Peptide-Targeted Mesoporous Silica Nanoparticle-Supported Lipid Bilayers

被引:199
作者
Ashley, Carlee E. [1 ,4 ]
Carnes, Eric C. [2 ,3 ,4 ]
Epler, Katharine E. [3 ]
Padilla, David P. [3 ]
Phillips, Genevieve K. [4 ]
Castillo, Robert E. [3 ]
Wilkinson, Dan C. [3 ]
Wilkinson, Brian S. [3 ]
Burgard, Cameron A. [3 ]
Kalinich, Robin M. [5 ]
Townson, Jason L. [3 ]
Chackerian, Bryce [4 ,7 ]
Willman, Cheryl L. [4 ,6 ]
Peabody, David S. [4 ,7 ]
Wharton, Walker [4 ,6 ]
Brinker, C. Jeffrey [2 ,3 ,4 ,7 ,8 ]
机构
[1] Sandia Natl Labs, Biotechnol & Bioengn Dept, Livermore, CA 94551 USA
[2] Univ New Mexico, Dept Chem & Nucl Engn, Albuquerque, NM 87131 USA
[3] Univ New Mexico, Ctr Microengn Mat, Albuquerque, NM 87131 USA
[4] Univ New Mexico, Hlth Sci Ctr, Canc Res & Treatment Ctr, Albuquerque, NM 87131 USA
[5] Sandia Natl Labs, Ceram Proc & Inorgan Mat Dept, Albuquerque, NM 87185 USA
[6] Univ New Mexico, Hlth Sci Ctr, Dept Pathol, Albuquerque, NM 87131 USA
[7] Univ New Mexico, Hlth Sci Ctr, Dept Mol Genet & Microbiol, Albuquerque, NM 87131 USA
[8] Sandia Natl Labs, Self Assembled Mat Dept, Albuquerque, NM 87185 USA
关键词
mesoporous silica nanoparticle; supported lipid bilayer; lipid nanoparticle; targeted delivery; peptide ligand; small interfering RNA; cancer; OVERCOME DRUG-RESISTANCE; IN-VITRO; ENDOSOMAL ESCAPE; CATIONIC LIPIDS; SIRNA DELIVERY; GENE DELIVERY; CANCER-CELLS; THERAPEUTICS; NANOCARRIERS; DOXORUBICIN;
D O I
10.1021/nn204102q
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
The therapeutic potential of small interfering RNAs (siRNAs) is severely limited by the availability of delivery platforms that protect siRNA from degradation, deliver it to the target cell with high specificity and efficiency, and promote its endosomal escape and cytosolic dispersion. Here we report that mesoporous silica nanoparticle-supported lipid bilayers (or "protocells") exhibit multiple properties that overcome many of the limitations of existing delivery platforms. Protocells have a 10- to 100-fold greater capacity for siRNA than corresponding lipid nanoparticles and are markedly more stable when incubated under physiological conditions. Protocells loaded with a cocktail of siRNAs bind to cells in a manner dependent on the presence of an appropriate targeting peptide and, through an endocytic pathway followed by endosomal disruption, promote delivery of the silencing nucleotides to the cytoplasm. The expression of each of the genes targeted by the siRNAs was shown to be repressed at the protein level, resulting in a potent induction of growth arrest and apoptosis. Incubation of control cells that lack expression of the antigen recognized by the targeting peptide with siRNA-loaded protocells induced neither repression of protein expression nor apoptosis, indicating the precise specificity of cytotoxic activity. In terms of loading capacity, targeting capabilities, and potency of action, protocells provide unique attributes as a delivery platform for therapeutic oligonucleotides.
引用
收藏
页码:2174 / 2188
页数:15
相关论文
共 62 条
[1]   RNAi therapeutics: Principles, prospects and challenges [J].
Aagaard, Lars ;
Rossi, John J. .
ADVANCED DRUG DELIVERY REVIEWS, 2007, 59 (2-3) :75-86
[2]  
Ashley CE, 2011, NAT MATER, V10, P389, DOI [10.1038/NMAT2992, 10.1038/nmat2992]
[3]   Redox-Active Polymer Microcapsules for the Delivery of a Survivin-Specific siRNA in Prostate Cancer Cells [J].
Becker, Alisa L. ;
Orlotti, Nicola Ivan ;
Folini, Marco ;
Cavalieri, Francesca ;
Zelikin, Alexander N. ;
Johnston, Angus P. R. ;
Zaffaroni, Nadia ;
Caruso, Frank .
ACS NANO, 2011, 5 (02) :1335-1344
[4]   Enhanced Gene and siRNA Delivery by Polycation-Modified Mesoporous Silica Nanoparticles Loaded with Chloroquine [J].
Bhattarai, Shanta Raj ;
Muthuswamy, Elayaraja ;
Wani, Amit ;
Brichacek, Michal ;
Castaneda, Antonio L. ;
Brock, Stephanie L. ;
Oupicky, David .
PHARMACEUTICAL RESEARCH, 2010, 27 (12) :2556-2568
[5]   RNAi therapeutics: a potential new class of pharmaceutical drugs [J].
Bumcrot, David ;
Manoharan, Muthiah ;
Koteliansky, Victor ;
Sah, Dinah W. Y. .
NATURE CHEMICAL BIOLOGY, 2006, 2 (12) :711-719
[6]   Microparticles with Bimodal Nanoporosity Derived by Microemulsion Templating [J].
Carroll, Nick J. ;
Pylypenko, Svitlana ;
Atanassov, Plamen B. ;
Petsev, Dimiter N. .
LANGMUIR, 2009, 25 (23) :13540-13544
[7]   Impact of different PEGylation patterns on the long-term bio-stability of colloidal mesoporous silica nanoparticles [J].
Cauda, Valentina ;
Argyo, Christian ;
Bein, Thomas .
JOURNAL OF MATERIALS CHEMISTRY, 2010, 20 (39) :8693-8699
[8]   Colchicine-Loaded Lipid Bilayer-Coated 50 nm Mesoporous Nanoparticles Efficiently Induce Microtubule Depolymerization upon Cell Uptake [J].
Cauda, Valentina ;
Engelke, Hanna ;
Sauer, Anna ;
Arcizet, Delphine ;
Brauchle, Christoph ;
Radler, Joachim ;
Bein, Thomas .
NANO LETTERS, 2010, 10 (07) :2484-2492
[9]   Controlling the delivery kinetics from colloidal mesoporous silica nanoparticles with pH-sensitive gates [J].
Cauda, Valentina ;
Argyo, Christian ;
Schlossbauer, Axel ;
Bein, Thomas .
JOURNAL OF MATERIALS CHEMISTRY, 2010, 20 (21) :4305-4311
[10]   Bio-degradation study of colloidal mesoporous silica nanoparticles: Effect of surface functionalization with organo-silanes and poly(ethylene glycol) [J].
Cauda, Valentina ;
Schlossbauer, Axel ;
Bein, Thomas .
MICROPOROUS AND MESOPOROUS MATERIALS, 2010, 132 (1-2) :60-71