Affiliation:
1. Department of Chemistry City University of Hong Kong 83 Tat Chee Ave, Kowloon Tong Hong Kong SAR P. R. China
2. City University of Hong Kong Shenzhen Research Institute Shenzhen P. R. China
3. School of Pharmaceutical Sciences Health Science Center Shenzhen University Shenzhen 518055 P. R. China
Abstract
AbstractAlthough multitargeted PtIV anticancer prodrugs have shown significant activities in reducing drug resistance, the types of bioactive ligands and drugs that can be conjugated to the Pt center remain limited to O‐donors. Herein, we report the synthesis of PtIV complexes bearing axial pyridines via ligand exchange reactions. Unexpectedly, the axial pyridines are quickly released after reduction, indicating their potential to be utilized as axial leaving groups. We further expand our synthetic approach to obtaining two multitargeted PtIV prodrugs containing bioactive pyridinyl ligands: a PARP inhibitor and an EGFR tyrosine kinase inhibitor; these conjugates exhibit great potential for overcoming drug resistance, and the latter conjugate inhibits the growth of Pt‐resistant tumor in vivo. This research adds to the array of synthetic methods for accessing PtIV prodrugs and significantly increases the types of bioactive axial ligands that can be conjugated to a PtIV center.
Funder
National Natural Science Foundation of China
Subject
General Chemistry,Catalysis
Cited by
16 articles.
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