Self-Assembling Micelle-like Nanoparticles with Detachable Envelopes for Enhanced Delivery of Nucleic Acid Therapeutics
- Authors
- Battogtokh, Gantumur; Ko, Young Tag
- Issue Date
- Mar-2014
- Publisher
- AMER CHEMICAL SOC
- Keywords
- self-assembling nanoparticles; nucleic acid therapeutics; polyethylenimine; phospholipid; deshielding; micelle-like nanoparticle
- Citation
- MOLECULAR PHARMACEUTICS, v.11, no.3, pp.904 - 912
- Journal Title
- MOLECULAR PHARMACEUTICS
- Volume
- 11
- Number
- 3
- Start Page
- 904
- End Page
- 912
- URI
- https://scholarworks.bwise.kr/gachon/handle/2020.sw.gachon/12811
- DOI
- 10.1021/mp400579h
- ISSN
- 1543-8384
- Abstract
- In spite of the great potential of nucleic acids as therapeutic agents, the clinical application of nucleic acid therapeutics requires the development of effective systemic delivery strategies. In an effort to develop effective nucleic acid delivery systems suitable for clinical application, we previously reported a self-assembling micelle-like nanoparticle that was based on phospholipid polyethylenimine conjugates, i.e., "micelle-like nanoparticles" (MNPs). In this study, we aimed to improve the system by enhancing the efficiency of intracellular delivery of the payload via pH-responsive detachment of the monolayer envelope and release of the nucleic acid therapeutics upon reaching the target tissues with an acidic pH, e.g., tumors. The acid-cleavable phospholipid polyethylenimine conjugate was synthesized via hydrazone bond, and acid-cleavable MNPs were then prepared and characterized as before. We evaluated the acid-cleavable MNP construct for in vitro and in vivo nucleic acid delivery efficiency using cultured tumor cells and tumor-bearing mice. The acid-cleavable nanocarrier showed an enhanced cellular delivery at pH 6.5 as compared to pH 7.4, whereas the noncleavable nanocarrier did not show any differences. Tail vein injections also led to enhanced intracellular uptake of the acid-cleavable nanocarrier compared to the noncleavable nanocarrier into tumor cells of tumor-bearing mice although no significant difference was observed in total tumor accumulation.
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