Enhanced In Vivo Tumor Detection by Active Tumor Cell Targeting Using Multiple Tumor Receptor-Binding Peptides Presented on Genetically Engineered Human Ferritin Nanoparticles

Authors
Kwon, Koo ChulKo, Ho KyungLee, JiyunLee, Eun JungKim, KwangmeyungLee, Jeewon
Issue Date
2016-08-17
Publisher
WILEY-V C H VERLAG GMBH
Citation
SMALL, v.12, no.31, pp.4241 - 4253
Abstract
Human ferritin heavy-chain nanoparticle (hFTH) is genetically engineered to present tumor receptor-binding peptides (affibody and/or RGD-derived cyclic peptides, named 4CRGD here) on its surface. The affibody and 4CRGD specifically and strongly binds to human epidermal growth factor receptor I (EGFR) and human integrin alpha v beta 3, respectively, which are overexpressed on various tumor cells. Through in vitro culture of EGFR-overexpressing adenocarcinoma (MDA-MB-468) and integrin-overexpressing glioblastoma cells (U87MG), it is clarified that specific interactions between receptors on tumor cells and receptor-binding peptides on engineered hFTH is critical in active tumor cell targeting. After labeling with the near-infrared fluorescence dye (Cy5.5) and intravenouse injection into MDA-MB-468 or U87MG tumor-bearing mice, the recombinant hFTHs presenting either peptide or both of affibody and 4CRGD are successfully delivered to and retained in the tumor for a prolonged period of time. In particular, the recombinant hFTH presenting both affibody and 4CRGD notably enhances in vivo detection of U87MG tumors that express heterogeneous receptors, integrin and EGFR, compared to the other recombinant hFTHs presenting either affibody or 4CRGD only. Like affibody and 4CRGD used in this study, other multiple tumor receptor-binding peptides can be also genetically introduced to the hFTH surface for actively targeting of in vivo tumors with heterogenous receptors.
Keywords
PROTEIN NANOPARTICLES; SURFACE MODIFICATION; HIGH-AFFINITY; H-CHAIN; DELIVERY; EXPRESSION; MOLECULES; AGENTS; TRANSFERRIN; REMOVAL; PROTEIN NANOPARTICLES; SURFACE MODIFICATION; HIGH-AFFINITY; H-CHAIN; DELIVERY; EXPRESSION; MOLECULES; AGENTS; TRANSFERRIN; REMOVAL
ISSN
1613-6810
URI
https://pubs.kist.re.kr/handle/201004/123782
DOI
10.1002/smll.201600917
Appears in Collections:
KIST Article > 2016
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