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Structural and Functional Characterizations of Cancer Targeting Nanoparticles Based on Hepatitis B Virus Capsidopen access

Authors
Heo, YunseokJeong, HyeongseopYoo, YoungkiYun, Ji-HyeRyu, BumhanCha, Young-jeLee, Bo-RamJeon, Ye-EunKim, JongminJeong, SojinJo, EunjiWoo, Jae-SungLee, JeewonCho, Hyun-SooLee, Weontae
Issue Date
Sep-2021
Publisher
MDPI
Keywords
cancer therapy; cryo-EM; HBcAg; affibody; EGFR; gold ions
Citation
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES, v.22, no.17
Indexed
SCIE
SCOPUS
Journal Title
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
Volume
22
Number
17
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/144653
DOI
10.3390/ijms22179140
ISSN
1661-6596
Abstract
Cancer targeting nanoparticles have been extensively studied, but stable and applicable agents have yet to be developed. Here, we report stable nanoparticles based on hepatitis B core antigen (HBcAg) for cancer therapy. HBcAg monomers assemble into spherical capsids of 180 or 240 subunits. HBcAg was engineered to present an affibody for binding to human epidermal growth factor receptor 1 (EGFR) and to present histidine and tyrosine tags for binding to gold ions. The HBcAg engineered to present affibody and tags (HAF) bound specifically to EGFR and exterminated the EGFR-overexpressing adenocarcinomas under alternating magnetic field (AMF) after binding with gold ions. Using cryogenic electron microscopy (cryo-EM), we obtained the molecular structures of recombinant HAF and found that the overall structure of HAF was the same as that of HBcAg, except with the affibody on the spike. Therefore, HAF is viable for cancer therapy with the advantage of maintaining a stable capsid form. If the affibody in HAF is replaced with a specific sequence to bind to another targetable disease protein, the nanoparticles can be used for drug development over a wide spectrum.
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