Issue 36, 2019

Kinetic stability-driven cytotoxicity of small-molecule prodrug nanoassemblies

Abstract

Nanoassemblies (NAs) of small-molecule lipophilic prodrugs have been widely investigated for efficient drug delivery in cancer therapy, but their kinetic stability has not attracted sufficient attention in the past studies. Herein, we reported that kinetic stability has a great influence on the drug release from the NAs of lipophilic prodrugs in physiologically relevant media. Based on the co-assembled FRET nanosystems of two lipophilic fluorescent prodrugs, we demonstrated that NAs constructed by lipophilic prodrugs containing shorter alkyl chains or those with higher unsaturated degrees displayed poorer kinetic stability, which further resulted in remarkably faster drug release in mouse plasma and various tissue homogenates. More importantly, these kinetically unstable NAs also induced rapid intracellular drug release, resulting in much more potent cytotoxicity. These findings highlight the crucial role of kinetic stability in determining the drug release from the NAs of lipophilic prodrugs, which would effectively guide their rational designs for cancer therapy.

Graphical abstract: Kinetic stability-driven cytotoxicity of small-molecule prodrug nanoassemblies

Supplementary files

Article information

Article type
Paper
Submitted
24 Jun 2019
Accepted
14 Aug 2019
First published
15 Aug 2019

J. Mater. Chem. B, 2019,7, 5563-5572

Kinetic stability-driven cytotoxicity of small-molecule prodrug nanoassemblies

Y. Li, Y. Chen, Y. Huang, W. Wu, Y. Liu, J. Zhang, M. Huang and M. Gou, J. Mater. Chem. B, 2019, 7, 5563 DOI: 10.1039/C9TB01270B

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