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- W4200101441 abstract "Disulfide cross-linked nanoassemblies have attracted considerable attention as a drug delivery vehicle due to their responsiveness to the natural redox gradient in biology. Fundamentally understanding the factors that influence the drug loading capacity, encapsulation stability, and precise control of the liberation of encapsulated cargo would be profoundly beneficial to redox-responsive materials. Reported herein are block copolymer (BCP)-based self-cross-linked nanogels, which exhibit high drug loading capacity, high encapsulation stability, and controllable release kinetics. BCP nanogels show considerably higher loading capacity and better encapsulation stability than the random copolymer nanogels at micromolar glutathione concentrations. By partially substituting thiol-reactive pyridyl disulfide into the unreactive benzyl or butyl group, we observed opposite effects on the cross-linking process of BCP nanogels. We further studied the redox-responsive cytotoxicity of our drug-encapsulated nanogels in various cancer cell lines." @default.
- W4200101441 created "2021-12-31" @default.
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- W4200101441 date "2021-12-10" @default.
- W4200101441 modified "2023-10-18" @default.
- W4200101441 title "Influence of Polymer Structure and Architecture on Drug Loading and Redox-Triggered Release" @default.
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- W4200101441 doi "https://doi.org/10.1021/acs.biomac.1c01295" @default.
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