Chemically activatable viral capsid functionalized for cancer targeting

Author:

Chen Chun-Chieh1,Xing Li1,Stark Marie1,Ou Tingwei1,Holla Prasida1,Xiao Kai2,Kamita Shizuo G3,Hammock Bruce D3,Lam Kit2,Cheng R Holland1

Affiliation:

1. Department of Molecular & Cellular Biology, University of California, 1 Shields Ave, Davis, CA 95616, USA

2. Department of Internal Medicine, University of California Davis, Sacramento, CA 95817, USA

3. Department of Entomology & Nematology, University of California, 1 Shields Ave, Davis, CA 95616, USA

Abstract

Aim: To design a theranostic capsule using the virus-like nanoparticle of the hepatitis E virus modified to display breast cancer cell targeting functional group (LXY30). Methods: Five surface-exposed residues were mutated to cysteine to allow conjugation to maleimide-linked chemical groups via thiol-selective linkages. Engineered virus-like nanoparticles were then covalently conjugated to a breast cancer recognized ligand, LXY30 and an amine-coupled near-infrared fluorescence dye. Results: LXY30-HEV VLP was checked for its binding and entry to a breast cancer cell line and for tumor targeting in vivo to breast cancer tissue in mice. The engineered virus-like nanoparticle not only targeted cancer cells, but also appeared immune silent to native hepatitis E virus antibodies due to epitope disruption at the antibody-binding site. Conclusion: These results demonstrate the production of a theranostic capsule suitable for cancer diagnostics and therapeutics based on surface modification of a highly stable virus-like nanoparticle.

Publisher

Future Medicine Ltd

Subject

Development,General Materials Science,Biomedical Engineering,Medicine (miscellaneous),Bioengineering

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