Lipid-derived nanoparticles for immunostimulatory RNA adjuvant delivery

Nguyen, David N.; Mahon, Kerry P.; Chikh, Ghania; Kim, Phillip; Chung, Hattie; Vicari, Alain; Love, Kevin T.; Goldberg, Michael S.; Chen, Steve; Krieg, Arthur Μ.; Chen, Jianzhu; Langer, Robert; Anderson, Daniel G.

doi:10.1073/pnas.1121423109

Cited by 89 publications

(61 citation statements)

References 57 publications

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“…Lipidoid is a lipid-like material consisting of an amine-containing head group and hydrocarbon tails, which is synthesized via epoxide ring-opening by amine substrate [77]. Study on cynomolgus monkeys showed that iv.…”

Section: Lipidoid Nanoparticlesmentioning

confidence: 99%

Nanocarriers for Delivery of siRNA and Co-Delivery of siRNA and Other Therapeutic Agents

Zhao

Feng

2015

Nanomedicine (Lond.)

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A major problem in cancer treatment is the multidrug resistance. siRNA inhibitors have great advantages to solve the problem, if the bottleneck of their delivery could be well addressed by the various nanocarriers. Moreover, co-delivery of siRNA together with the various anticancer agents in one nanocarrier may maximize their additive or synergistic effect. This review provides a comprehensive summary on the state-of-the-art of the nanocarriers, which may include prodrugs, micelles, liposomes, dendrimers, nanohydrogels, solid lipid nanoparticles, nanoparticles of biodegradable polymers and nucleic acid nanocarriers for delivery of siRNA and co-delivery of siRNA together with anticancer agents with focus on synthesis of the nanocarrier materials, design and characterization, in vitro and in vivo evaluation, and prospect and challenges of nanocarriers.

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Section: Lipidoid Nanoparticlesmentioning

confidence: 99%

Nanocarriers for Delivery of siRNA and Co-Delivery of siRNA and Other Therapeutic Agents

Zhao

Feng

2015

Nanomedicine (Lond.)

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“…Efforts have primarily focused on constructs for immunostimulation (IS) and include complexing oligonucleotides with albumin (15), gold nanoparticles with two-component external coronas consisting of IS-oligonucleotides together with protein antigens (16), gold nanoparticle-IS-oligonucleotide conjugates (17), IS-oligonucleotides conjugated to polymeric nanoparticles (18), and IS-oligonucleotides in complex with lipids (19). Although these studies have uncovered the promise of nanomaterials for immunomodulation, it is still unclear what the dominant structural factors are.…”

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confidence: 99%

Immunomodulatory spherical nucleic acids

Radovic‐Moreno

Chernyak

Mader

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

215

233

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Immunomodulatory nucleic acids have extraordinary promise for treating disease, yet clinical progress has been limited by a lack of tools to safely increase activity in patients. Immunomodulatory nucleic acids act by agonizing or antagonizing endosomal toll-like receptors (TLR3, TLR7/8, and TLR9), proteins involved in innate immune signaling. Immunomodulatory spherical nucleic acids (SNAs) that stimulate (immunostimulatory, IS-SNA) or regulate (immunoregulatory, IR-SNA) immunity by engaging TLRs have been designed, synthesized, and characterized. Compared with free oligonucleotides, IS-SNAs exhibit up to 80-fold increases in potency, 700-fold higher antibody titers, 400-fold higher cellular responses to a model antigen, and improved treatment of mice with lymphomas. IR-SNAs exhibit up to eightfold increases in potency and 30% greater reduction in fibrosis score in mice with nonalcoholic steatohepatitis (NASH). Given the clinical potential of SNAs due to their potency, defined chemical nature, and good tolerability, SNAs are attractive new modalities for developing immunotherapies.

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“…Unmodified naked siRNAs are degraded rapidly by nuclease in the circulation and removed efficiently through renal clearance (34,35). In addition, activation of nonspecific innate immune stimulation of short RNA sequences could be a significant problem with repetitive and high-dose therapeutic application of siRNAs (5,6). Therefore, to achieve optimal in vivo siRNA delivery and specific silencing, it is imperative to develop modified siRNA or strategies that allow protection of siRNAs from nuclease degradation and facilitate cellular uptake for efficient gene silencing without significant immunogenicity.…”

Section: Discussionmentioning

confidence: 99%

“…Naked nucleic acid molecules, including synthetic siRNA, are degraded easily by ubiquitous nucleases either in the circulation or inside cells, and they are unable to enter cells through passive diffusion mechanisms because of the large molecular weight and polycationic nature of the chemical structure (4). In addition, the nonspecific innate immune-stimulatory function of siRNA could be a serious problem, especially for repetitive and high-dose therapeutic applications (5,6). In the last decade, various approaches have been developed to overcome these issues.…”

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confidence: 99%

Self-assembled Micelle Interfering RNA for Effective and Safe Targeting of Dysregulated Genes in Pulmonary Fibrosis

Yoon¹,

Park

Lee

et al. 2016

Journal of Biological Chemistry

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The siRNA silencing approach has long been used as a method to regulate the expression of specific target genes in vitro and in vivo. However, the effectiveness of delivery and the nonspecific immune-stimulatory function of siRNA are the limiting factors for therapeutic applications of siRNAs. To overcome these limitations, we developed self-assembled micelle inhibitory RNA (SAMiRNA) nanoparticles made of individually biconjugated siRNAs with a hydrophilic polymer and lipid on their ends and characterized their stability, immune-stimulatory function, and in vivo silencing efficacy. SAMiRNAs form very stable nanoparticles with no significant degradation in size distribution and polydispersity index over 1 year. Overnight incubation of SAMiRNAs (3 M) on murine peripheral blood mononuclear cells did not cause any significant elaboration of innate immune cytokines such as TNF-␣, IL-12, or IL-6, whereas unmodified siRNAs or liposomes or liposome complexes significantly stimulated the expression of these cytokines. Last, the in vivo silencing efficacy of SAMiRNAs was evaluated by targeting amphiregulin and connective tissue growth factor in bleomycin or TGF-␤ transgenic animal models of pulmonary fibrosis. Intratracheal or intravenous delivery two or three times of amphiregulin or connective tissue growth factor SAMiRNAs significantly reduced the bleomycin-or TGF-␤-stimulated collagen accumulation in the lung and substantially restored the lung function of TGF-␤ transgenic mice. This study demonstrates that SAMiRNA nanoparticle is a less toxic, stable siRNA silencing platform for efficient in vivo targeting of genes implicated in the pathogenesis of pulmonary fibrosis.

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Lipid-derived nanoparticles for immunostimulatory RNA adjuvant delivery

Cited by 89 publications

References 57 publications

Nanocarriers for Delivery of siRNA and Co-Delivery of siRNA and Other Therapeutic Agents

Nanocarriers for Delivery of siRNA and Co-Delivery of siRNA and Other Therapeutic Agents

Immunomodulatory spherical nucleic acids

Self-assembled Micelle Interfering RNA for Effective and Safe Targeting of Dysregulated Genes in Pulmonary Fibrosis

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