Triply Triggered Doxorubicin Release From Supramolecular Nanocontainers

Loh, Xian Jun; Barrio, Jesús del; Toh, Pearl Pei Chern; Lee, Tung‐Chun; Jiao, Dezhi; Rauwald, Urs; Appel, Eric A.; Scherman, Oren A.

doi:10.1021/bm201588m

Cited by 171 publications

(118 citation statements)

References 42 publications

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“…[42][43][44][45] For instance, Lee and Scherman et al have demonstrated the release of cancer drugs from hierarchical nanocarriers can be controlled by three orthogonal, biologically relevant triggers (pH, temperature and a specific molecular cue) that can result in disassembly of the micelles, releasing doxorubicin. 46 This controlled release reduces toxicity to other areas of the body. A wide range of stimuli-responsive polymeric structures have been designed, governed by hydrophobic interactions, which can selectively release molecules in response to certain stimuli.…”

Section: Self-assembled Nanomachinesmentioning

confidence: 99%

Artificial molecular and nanostructures for advanced nanomachinery

et al. 2018

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Section: Self-assembled Nanomachinesmentioning

confidence: 99%

Artificial molecular and nanostructures for advanced nanomachinery

et al. 2018

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“…The macrocyclic host, cucurbit [7]uril (CB [7]) was chosen as the model. Cucurbit[n]urils (CB[n]s) are a family of water-soluble macrocyclic hosts, which have a hydrophobic cavity capable of the binding of one or two guest molecules depending on the size of di®erent CB[n]s. [22][23][24] CB [7] possesses good solubility in water and strong a±nity for one guest molecule. [25][26][27][28][29][30][31] The authors employed CB [7] to bind with the positive charge and hydrophobic component on "-poly-l-lysine hydrochlorides to construct the polypseudorotaxane for antibacterial regulation.…”

Section: Responsive Antibacterial Materialsmentioning

confidence: 99%

Latest Advances in Antibacterial Materials

Loh

2017

J. Mol. Eng. Mater.

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This paper will update readers on the latest work in the area of antibacterial polymeric systems. There is extensive literature on existing systems. This complexity con¯nes us to the latest antibacterial materials which possess (1) responsive antibacterial activity on their own; (2) antibio¯lm formation and (3) formation of antibacterial polymeric¯lms. The objective of this review is to provide an overview of the antibacterial synthetic polymer¯eld. In this paper, I will analyze the early promise of this technology as well as highlight potential challenges that adopters could face. The primary focus will be the application of materials to the medical industry and to show how these materials can be tailored to create responsive, customized bactericidal materials.

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“…The final product was dialyzed against deionized water through dialysis tube (M w cutoff: 8000-14,000 g mol 21 ) for 1 week to remove the unreacted mPEG (see Supporting Information Fig. S5).…”

Section: Synthesis Of 4-adamantane Carboxylate Benzaldehydementioning

confidence: 99%

pH‐ and β‐cyclodextrin‐responsive micelles based on polyaspartamide derivatives as drug carrier

Sun

Zhang

et al. 2015

J. Polym. Sci. Part A: Polym. Chem.

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A novel kind of graft polymer poly(aspartic acid)-ethanediamine-g-adamantane/methyloxy polyethylene glycol (Pasp-EDA-g-Ad/mPEG) was designed and synthesized for drug delivery in this study. The chemical structure of the prepared polymer was confirmed by proton NMR. The obtained polymer can self-assemble into micelles which were stable under a physiological environment and displayed pH-and bcyclodextrin (b-CD)-responsive behaviors because of the acidlabile benzoic imine linkage and hydrophobic adamantine groups in the side chains of the polymer. The doxorubicin (Dox)-loaded micelles showed a slow release under physiological conditions and a rapid release after exposure to weakly acidic or b-CD environment. The in vitro cytotoxicity results suggested that the polymer was good at biocompatibility and could remain Dox biologically active. Hence, the Pasp-EDA-gAd/mPEG micelles may be applied as promising controlled drug delivery system for hydrophobic antitumor drugs. V C 2015

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Triply Triggered Doxorubicin Release From Supramolecular Nanocontainers

Cited by 171 publications

References 42 publications

Artificial molecular and nanostructures for advanced nanomachinery

Artificial molecular and nanostructures for advanced nanomachinery

Latest Advances in Antibacterial Materials

pH‐ and β‐cyclodextrin‐responsive micelles based on polyaspartamide derivatives as drug carrier

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