Please use this identifier to cite or link to this item: https://doi.org/10.1039/d1ra05980g
Title: Conjugation with gold nanoparticles improves the stability of the KT2 peptide and maintains its anticancer properties
Authors: Maraming, Pornsuda
Daduang, Jureerut
Kah, James Chen Yong 
Keywords: Science & Technology
Physical Sciences
Chemistry, Multidisciplinary
Chemistry
ANTIMICROBIAL PEPTIDES
CELLS
DRUG
SIZE
RT2
Issue Date: 20-Dec-2021
Publisher: ROYAL SOC CHEMISTRY
Citation: Maraming, Pornsuda, Daduang, Jureerut, Kah, James Chen Yong (2021-12-20). Conjugation with gold nanoparticles improves the stability of the KT2 peptide and maintains its anticancer properties. RSC ADVANCES 12 (1) : 319-325. ScholarBank@NUS Repository. https://doi.org/10.1039/d1ra05980g
Abstract: One of the major weaknesses of therapeutic peptides is their sensitivity to degradation by proteolytic enzymes in vivo. Gold nanoparticles (GNPs) are a good carrier for therapeutic peptides to improve their stability and cellular uptake in vitro and in vivo. We conjugated the anticancer KT2 peptide as an anticancer peptide model to PEGylated GNPs (GNPs-PEG) and investigated the peptide stability, cellular uptake and ability of the GNPs-KT2-PEG conjugates to induce MDA-MB-231 human breast cancer cell death. We found that 11 nm GNPs protected the conjugated KT2 peptide from trypsin proteolysis, keeping it stable up to 0.128% trypsin, which is higher than the serum trypsin concentration (range 0.0000285 ± 0.0000125%) reported by Lake-Bakaar, G. et al., 1979. GNPs significantly enhanced the cellular uptake of KT2 peptides after conjugation. Free KT2 peptides pretreated with trypsin were not able to kill MDA-MB-231 cells due to proteolysis, while GNPs-KT2-PEG was still able to exert effective cancer cell killing after trypsin treatment at levels comparable to GNPs-KT2-PEG without enzyme pretreatment. The outcome of this study highlights the utility of conjugated anticancer peptides on nanoparticles to improve peptide stability and retain anticancer ability.
Source Title: RSC ADVANCES
URI: https://scholarbank.nus.edu.sg/handle/10635/248790
ISSN: 2046-2069
DOI: 10.1039/d1ra05980g
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