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Ryu, Ja-Hyoung
Supramolecular Nanomaterials Lab.
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Folic Acid-Functionalized β-Cyclodextrin for Delivery of Organelle-Targeted Peptide Chemotherapeutics in Cancer

Author(s)
Ok, Hae WonJin, SeongeonPark, GaeunJana, BatakrishnaRyu, Ja-Hyoung
Issued Date
2024-07
DOI
10.1021/acs.molpharmaceut.4c00400
URI
https://scholarworks.unist.ac.kr/handle/201301/83519
Citation
MOLECULAR PHARMACEUTICS
Abstract
Recent emphasis on the design of drug delivery systems typically involves the effective transport of a pharmaceutical substance to the disease site with the desired therapeutic efficacy and minimal cytotoxicity. Organelle-targeted peptides have become an integral part of designing an important class of prodrug/prodrug assemblies for new supramolecular therapeutics owing to their favorable biocompatibility, synthetic ease, tunability of their aggregation behavior, and desired functionalization for site-specificity. However, it is still limited due to the low selectivity. We designed a folic acid-functionalized beta-cyclodextrin (FA-CD) as a delivery platform for specific and selective delivery of organelle-targeted (such as microtubule, lysosome, and mitochondria) peptide chemotherapeutics to the folate receptor (FR) overexpressing cancer cell lines. Low toxicity was found for the FA-CD and organelle-targeted peptide inclusion complex in FR-negative normal cells, but superior inhibition of tumor growth with no in vivo toxicity was found for the inclusion complex in the xenograft tumor model.
Publisher
AMER CHEMICAL SOC
ISSN
1543-8384
Keyword (Author)
peptide amphiphilesself-assemblyorganelle targetingcancertherapyhost-guest interaction
Keyword
STAR POLYMERPRODRUGSCELLSNANOPARTICLESMITOCHONDRIACOMBINATIONINHIBITIONCHEMISTRYTHERAPYDESIGN

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