Literature DB >> 27163624

Hydrophobic interactions between polymeric carrier and palmitic acid-conjugated siRNA improve PEGylated polyplex stability and enhance in vivo pharmacokinetics and tumor gene silencing.

Samantha M Sarett1, Thomas A Werfel1, Irene Chandra1, Meredith A Jackson1, Taylor E Kavanaugh1, Madison E Hattaway1, Todd D Giorgio1, Craig L Duvall2.   

Abstract

Formation of stable, long-circulating siRNA polyplexes is a significant challenge in translation of intravenously-delivered, polymeric RNAi cancer therapies. Here, we report that siRNA hydrophobization through conjugation to palmitic acid (siPA) improves stability, in vivo pharmacokinetics, and tumor gene silencing of PEGylated nanopolyplexes (siPA-NPs) with balanced cationic and hydrophobic content in the core relative to the analogous polyplexes formed with unmodified siRNA, si-NPs. Hydrophobized siPA loaded into the NPs at a lower charge ratio (N(+):P(-)) relative to unmodified siRNA, and siPA-NPs had superior resistance to siRNA cargo unpackaging in comparison to si-NPs upon exposure to the competing polyanion heparin and serum. In vitro, siPA-NPs increased uptake in MDA-MB-231 breast cancer cells (100% positive cells vs. 60% positive cells) but exhibited equivalent silencing of the model gene luciferase relative to si-NPs. In vivo in a murine model, the circulation half-life of intravenously-injected siPA-NPs was double that of si-NPs, resulting in a >2-fold increase in siRNA biodistribution to orthotopic MDA-MB-231 mammary tumors. The increased circulation half-life of siPA-NPs was dependent upon the hydrophobic interactions of the siRNA and the NP core component and not just siRNA hydrophobization, as siPA did not contribute to improved circulation time relative to unmodified siRNA when delivered using polyplexes with a fully cationic core. Intravenous delivery of siPA-NPs also achieved significant silencing of the model gene luciferase in vivo (∼40% at 24 h after one treatment and ∼60% at 48 h after two treatments) in the murine MDA-MB-231 tumor model, while si-NPs only produced a significant silencing effect after two treatments. These data suggest that stabilization of PEGylated siRNA polyplexes through a combination of hydrophobic and electrostatic interactions between siRNA cargo and the polymeric carrier improves in vivo pharmacokinetics and tumor gene silencing relative to conventional formulations that are stabilized solely by electrostatic interactions.
Copyright © 2016 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  Breast cancer; Hydrophobicity; PEGylated polyplexes; Pharmacokinetics; RNA interference; Tumor targeting

Mesh:

Substances:

Year:  2016        PMID: 27163624      PMCID: PMC4894661          DOI: 10.1016/j.biomaterials.2016.04.017

Source DB:  PubMed          Journal:  Biomaterials        ISSN: 0142-9612            Impact factor:   12.479


  62 in total

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3.  In vivo disassembly of IV administered siRNA matrix nanoparticles at the renal filtration barrier.

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6.  Efficient in vivo delivery of siRNA to the liver by conjugation of alpha-tocopherol.

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7.  Safety and efficacy of RNAi therapy for transthyretin amyloidosis.

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9.  Cellular uptake mechanism and intracellular fate of hydrophobically modified glycol chitosan nanoparticles.

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10.  Gene-silencing potency of symmetric and asymmetric lipid-conjugated siRNAs and its correlation with dicer recognition.

Authors:  Takanori Kubo; Kazuyoshi Yanagihara; Yuichiro Sato; Yoshio Nishimura; Shinichi Kondo; Toshio Seyama
Journal:  Bioconjug Chem       Date:  2013-12-09       Impact factor: 4.774
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  17 in total

1.  Gal8 Visualization of Endosome Disruption Predicts Carrier-Mediated Biologic Drug Intracellular Bioavailability.

Authors:  Kameron V Kilchrist; Somtochukwu C Dimobi; Meredith A Jackson; Brian C Evans; Thomas A Werfel; Eric A Dailing; Sean K Bedingfield; Isom B Kelly; Craig L Duvall
Journal:  ACS Nano       Date:  2019-01-18       Impact factor: 15.881

2.  Lipophilic siRNA targets albumin in situ and promotes bioavailability, tumor penetration, and carrier-free gene silencing.

Authors:  Samantha M Sarett; Thomas A Werfel; Linus Lee; Meredith A Jackson; Kameron V Kilchrist; Dana Brantley-Sieders; Craig L Duvall
Journal:  Proc Natl Acad Sci U S A       Date:  2017-07-24       Impact factor: 11.205

3.  Anionic Polymer and Quantum Dot Excipients to Facilitate siRNA Release and Self-Reporting of Disassembly in Stimuli-Responsive Nanocarrier Formulations.

Authors:  Chad T Greco; Jason C Andrechak; Thomas H Epps; Millicent O Sullivan
Journal:  Biomacromolecules       Date:  2017-05-10       Impact factor: 6.988

Review 4.  Engineered Hydrogels for Local and Sustained Delivery of RNA-Interference Therapies.

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Journal:  Biomater Sci       Date:  2019-04-23       Impact factor: 6.843

6.  Combinatorial optimization of PEG architecture and hydrophobic content improves ternary siRNA polyplex stability, pharmacokinetics, and potency in vivo.

Authors:  Thomas A Werfel; Meredith A Jackson; Taylor E Kavanaugh; Kellye C Kirkbride; Martina Miteva; Todd D Giorgio; Craig Duvall
Journal:  J Control Release       Date:  2017-03-31       Impact factor: 9.776

7.  Zwitterionic Nanocarrier Surface Chemistry Improves siRNA Tumor Delivery and Silencing Activity Relative to Polyethylene Glycol.

Authors:  Meredith A Jackson; Thomas A Werfel; Elizabeth J Curvino; Fang Yu; Taylor E Kavanaugh; Samantha M Sarett; Mary D Dockery; Kameron V Kilchrist; Ayisha N Jackson; Todd D Giorgio; Craig L Duvall
Journal:  ACS Nano       Date:  2017-06-07       Impact factor: 15.881

8.  Dual carrier-cargo hydrophobization and charge ratio optimization improve the systemic circulation and safety of zwitterionic nano-polyplexes.

Authors:  Meredith A Jackson; Sean K Bedingfield; Fang Yu; Mitchell E Stokan; Rachel E Miles; Elizabeth J Curvino; Ella N Hoogenboezem; Rachel H Bonami; Shrusti S Patel; Peggy L Kendall; Todd D Giorgio; Craig L Duvall
Journal:  Biomaterials       Date:  2018-11-10       Impact factor: 12.479

9.  Complexation of Chol-DsiRNA in place of Chol-siRNA greatly increases the duration of mRNA suppression by polyplexes of PLL(30)-PEG(5K) in primary murine syngeneic breast tumors after i.v. administration.

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10.  Preliminary preclinical study of Chol-DsiRNA polyplexes formed with PLL[30]-PEG[5K] for the RNAi-based therapy of breast cancer.

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Journal:  Nanomedicine       Date:  2021-02-03       Impact factor: 5.307
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