3.8 Article

Inhalable Dual-Targeted Hybrid Lipid Nanocore-Protein Shell Composites for Combined Delivery of Genistein and All-Trans Retinoic Acid to Lung Cancer Cells

Journal

ACS BIOMATERIALS SCIENCE & ENGINEERING
Volume 6, Issue 1, Pages 71-87

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsbiomaterials.8b01374

Keywords

hybrid lipid protein nanoparticles; all-trans retinoic acid; genistein; dual targeting; inhalable nanocomposites; lung cancer

Funding

  1. Science and Technology Development Fund (STDF), Ministry of Scientific Research, Egypt [5731]

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Localized pulmonary delivery of anticancer agents to lungs has proven to be pioneering approach for lung cancer therapy. Hybrid lipid nanocore-protein shell nanoparticles (HLPNPs) coloaded with all-trans retinoic acid (ATRA) and genistein (GNS) were prepared via sequential solvent evaporation followed by nanoprecipitation of zein shell onto the lipid core. The outer protein shell of HLPNPs provided additional drug reservoir for encapsulation of ATRA/stearyl amine ion pair and enabled dual tumor-targeting with biotin and ATRA. Enhanced uptake and cytotoxic activity of HLPNPs against A549 lung cancer cells was confirmed. To improve their deep lung deposition, dual-targeted drug-loaded HLPNP nanocomposites were fabricated. The nanocomposites prepared using mannitol/HP beta CD/leucine demonstrated favorable aerosolization (MMAD = 2.47 mu m and FPF = 70.81%). In vivo, the inhalable nanocomposites were superior to aerosolized or i.v. nanoparticle suspension against lung carcinoma bearing mice. Overall, inhalable dual-targeted HLPNPs nanocomposites provided localized codelivery of GNS and ATRA for lung cancer therapy.

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