2012
DOI: 10.1016/j.jconrel.2012.03.009
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Molecular binding of self-assembling peptide EAK16-II with anticancer agent EPT and its implication in cancer cell inhibition

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Cited by 41 publications
(39 citation statements)
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“…For instance, an 8-fold diluted complex showed stronger emission than the complex at original concentration, which could be due to inner filter effect demonstrated in previous study. 24 According to a previous study, the electrostatic interaction between protonated EPT and negatively charged glutamic acid was the major driving force that stabilized EPT in EAK16-II-based system, whereby each glutamic acid could bind one protonated EPT molecule. 24 When preparing the complex, the molar ratio of EPT to glutamic acid is 1:2.6, 1:2.5, 1:2.5 and 1:2.3 for EAR16-II, EAR8-II, EAR-IIa and ELR8-IIa systems, respectively.…”
Section: Characterization Of Peptide-ept Complexesmentioning
confidence: 97%
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“…For instance, an 8-fold diluted complex showed stronger emission than the complex at original concentration, which could be due to inner filter effect demonstrated in previous study. 24 According to a previous study, the electrostatic interaction between protonated EPT and negatively charged glutamic acid was the major driving force that stabilized EPT in EAK16-II-based system, whereby each glutamic acid could bind one protonated EPT molecule. 24 When preparing the complex, the molar ratio of EPT to glutamic acid is 1:2.6, 1:2.5, 1:2.5 and 1:2.3 for EAR16-II, EAR8-II, EAR-IIa and ELR8-IIa systems, respectively.…”
Section: Characterization Of Peptide-ept Complexesmentioning
confidence: 97%
“…22,24 The UV-adsorption of EPT at 295 nm was fitted linearly as a function of EPT concentration (1 × 10 -3 -1 × 10 -2 mg/mL) to obtain a calibration curve. The EPT standard sample was prepared by dissolving EPT in a mixture of 95% DMSO with 5% water.…”
Section: Ept Loading Capacity Measurementmentioning
confidence: 99%
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“…The in vitro experiments also demonstrated that the encapsulated anticancer drug ellipticine in the self-assembled nanofibers in protonated stage is more efficient than in the crystalline stage for cancer therapy. These EAK peptide self-assembled nanostructures and the two encapsulation methods could also be used for some other anticancer agents in drug delivery for cancer therapy [119].…”
Section: Anticancer Drug Deliverymentioning
confidence: 99%