| Literature DB >> 31753697 |
Abiodun Anifowose1, Zhengnan Yuan1, Xiaoxiao Yang2, Zhixiang Pan1, Yueqin Zheng1, Zhongwei Zhang1, Binghe Wang3.
Abstract
Previously, we reported a class of MDM2-MDM4 dimerization inhibitors that upregulate p53 and showed potent anticancer activity in animal models. However, water solubility hinders their further development. Herein we describe our effort to develop a prodrug approach that overcomes the solubility problem. The prodrug of BW-AQ-238, a potent anthraquinone analog, was made by esterification of the hydroxyl group with various natural amino acids. Cytotoxicity of these compounds toward Hela and EU-1 cells, their aqueous solubility, and the release kinetics of these prodrugs in buffer and in the presence of hydrolytic enzymes were studied. The results demonstrate that the amino acid prodrug approach significantly improved the water solubility while maintaining the potency of the parent drug.Entities:
Keywords: Amino acid prodrug; Anthraquinone; Anticancer agent; Esterase; Kallikrein
Year: 2019 PMID: 31753697 PMCID: PMC6942214 DOI: 10.1016/j.bmcl.2019.126786
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823