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Inhibitory Effect of Oxaliplatin-loaded Engineered Milk Extracellular Vesicles on Tumor Progression

Authors
Go, GyeongyunPark, Hee JungLee, Jun HeeYun, Chul WonLee, Sang Hun
Issue Date
Feb-2022
Publisher
International Institute of Anticancer Research
Keywords
Milk extracellular vesicles; EGFR expressing tumor; GE11 peptide; drug delivery system; bio-engineered drug carrier
Citation
Anticancer Research, v.42, no.2, pp 857 - 866
Pages
10
Journal Title
Anticancer Research
Volume
42
Number
2
Start Page
857
End Page
866
URI
https://scholarworks.bwise.kr/sch/handle/2021.sw.sch/20373
DOI
10.21873/anticanres.15543
ISSN
0250-7005
1791-7530
Abstract
Background/Aim: Anti-cancer chemotherapy is an effective therapeutic approach. Milk extracellular vesicles (EVs) loaded with chemotherapeutics have a potential anticancer effect by acting as a drug delivery system. Thus, our study aimed to explore the effect of engineered milk extracellular vesicles. Materials and Methods: To treat epidermal growth factor receptor (EGFR) expressing solid tumors, we established oxaliplatin-loaded milk EV conjugated with GE11 peptide (GE11Milk EVoxal), which has a high affinity to EGFR and assessed their anti-cancer effect in vitro and in vivo. Results: Drug-loaded GE11Milk EVoxal showed significantly higher incorporation into EGFR expressing cancer cells compared with milk EV without GE11 conjugation (Milk EVoxal), leading to apoptosis of cancer cells. GE11Milk EVoxal also inhibited cell viability compared to milk EVoxal or oxaliplatin alone. In colorectal cancer xenograft murine model, GE11Milk EVoxal showed the maximum therapeutic effect on tumor progression. These findings indicate that GE11Milk EVoxal suppresses EGFR expressing cancer through GE11 peptide-mediated EGFR targeting and subsequently anti-cancer drug delivery. Conclusion: Anti-cancer drug-loaded engineered milk EVs might be a novel therapeutic approach for treating patients with EGFR expressing solid tumors.
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