| Literature DB >> 26035636 |
Shiying Luo1, Ying Gu2, Yuannian Zhang1, Pei Guo1, Jean Felix Mukerabigwi1, Min Liu1, Shaojun Lei1, Yu Cao1, Hongxuan He3, Xueying Huang1.
Abstract
A major challenge of combinatorial therapy is the unification of the pharmacokinetics and cellular uptake of various drug molecules with precise control of the dosage thereby maximizing the combined effects. To realize ratiometric delivery and synchronized release of different drugs from a single carrier, a novel approach was designed in this study to load dual drugs onto the macromolecular carrier with different molar ratio by covalently preconjugating dual drugs through peptide linkers to form drug conjugates. In contrast to loading individual types of drugs separately, these drug conjugates enable the loading of dual drugs onto the same carrier in a precisely controllable manner to reverse multidrug resistance (MDR) of human hepatoma (HepG2) cells. As a proof of concept, the synthesis and characterization of xyloglucan-mitomycin C/doxorubicin (XG-MMC/DOX) conjugates were demonstrated. This approach enabled MMC and DOX to be conjugated to the same polymeric carrier with precise control of drug dosage. The cytotoxicity and combinatorial effects were significantly improved compared to the cocktail mixtures of XG-MMC and XG-DOX as well as the individual conjugate of the mixture. Moreover, the results also showed that there was an optimum ratio of dual drugs showing the best cytotoxicity effect and greatest synergy among other tested polymeric conjugate formulations.Entities:
Keywords: combinational therapy; drug delivery; polymeric conjugates; ratiometric drug loading; reversion of multidrug resistance
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Year: 2015 PMID: 26035636 DOI: 10.1021/mp500867g
Source DB: PubMed Journal: Mol Pharm ISSN: 1543-8384 Impact factor: 4.939