Literature DB >> 30820699

Optimization of Chitosan-α-casein Nanoparticles for Improved Gene Delivery: Characterization, Stability, and Transfection Efficiency.

João Panão Costa1,2, Sofia Carvalho1, Sandra Jesus1,2, Edna Soares1,2, Ana Patrícia Marques1,2, Olga Borges3,4.   

Abstract

Among non-viral vectors, the cationic polymer chitosan has gained attention as a gene delivery system. We hypothesized that the addition of casein into the nanoparticle's structure would facilitate a proper gene transfer. The work herein presented aimed to optimize the production method of chitosan-casein nanoparticles (ChiCas NPs) and to test their ability as a gene delivery system. ChiCas NPs formulation optimization was carried out by analyzing several characteristics such as NP size, zeta potential, and chitosan and casein incorporation efficacy. The best formulation developed presented small and homogenous particle size (around 335 nm) and positive zeta potential (≈ + 38 mV), and showed to be stable for 34 weeks both, at 4°C and 20°C. The particles were further used to entrap or to adsorb DNA and form NPs-DNA complexes. In vitro transfection studies, carried out in COS-7 cells, suggested a low transfection efficiency of the different NPs:DNA ratios tested, comparatively to the positive control. Nonetheless, we could observe that the complexes with larger sizes presented better transfection results than those with smaller diameters. To conclude, ChiCas NPs have great technological potential since the preparation process is very simple, and the DNA incorporation efficacy is very high and shows to be physically very stable. The NPs:DNA ratio still needs to be optimized with the aim of achieving better transfection results and being able to anticipate a high gene expression on DNA-based vaccination studies.

Keywords:  DNA vaccine; chitosan nanoparticles; gene delivery system; glucan; α-casein

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Year:  2019        PMID: 30820699     DOI: 10.1208/s12249-019-1342-y

Source DB:  PubMed          Journal:  AAPS PharmSciTech        ISSN: 1530-9932            Impact factor:   3.246


  2 in total

1.  Engineering Human Circulating Monocytes/Macrophages by Systemic Deliverable Gene Editing.

Authors:  So Yoon Lee; Javier Fierro; Jake Dipasquale; Anthony Bastian; An M Tran; Deawoo Hong; Brandon Chin; Paul J Nguyen-Lee; Sarah Mazal; Jamil Espinal; Tima Thomas; Huanyu Dou
Journal:  Front Immunol       Date:  2022-05-18       Impact factor: 8.786

2.  Cytoplasmic Trafficking of Nanoparticles Delivers Plasmid DNA for Macrophage Gene-editing.

Authors:  So Yoon Lee; Javier Fierro; An M Tran; Daewoo Hong; Jamil Espinal; Huanyu Dou
Journal:  Curr Gene Ther       Date:  2021       Impact factor: 4.676

  2 in total

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