Ligand substitution reactions afford oxaliplatin-based platinum(IV) complexes bearing axial alkoxido ligands

被引:0
|
作者
Xu, Zoufeng [1 ]
Lin, Long [1 ]
Fu, Binbin [1 ]
Huang, Fu-Ping [2 ]
Zhou, Qiyuan [3 ]
Zhu, Guangyu [3 ]
Wang, Zhigang [1 ]
机构
[1] Shenzhen Univ, Med Sch, Int Canc Ctr, Sch Pharm, Shenzhen 518055, Guangdong, Peoples R China
[2] Guangxi Normal Univ, Sch Chem & Pharmaceut Sci, State Key Lab Chem & Mol Engn Med Resources, Guilin 541006, Guangxi, Peoples R China
[3] City Univ Hong Kong, Dept Chem, Kowloon Tong, 83 Tat Chee Ave, Hong Kong 999077, Peoples R China
关键词
HALOACETATO LIGANDS; HYDROGEN-PEROXIDE; CISPLATIN; PRODRUGS; HYDROLYSIS; GENERATION; STABILITY; OXIDATION; DELIVERY; CANCER;
D O I
10.1039/d3qi01562
中图分类号
O61 [无机化学];
学科分类号
070301 ; 081704 ;
摘要
The application of new synthetic methods in the area of platinum(iv) anticancer prodrugs greatly increases the availability of accessible chemical entities that can be conjugated to the platinum(iv) center. These new axial ligands not only endow platinum(iv) complexes with unique properties but also inspire new concepts in platinum(iv)-based prodrug design and development. Herein, oxaliplatin-based platinum(iv) complexes are synthesized with axial alkoxido ligands via a ligand substitution reaction. In the presence of base, alcohol molecules can spontaneously replace the labile axial trifluoroacetato ligand and transform into new alkoxido ligands in platinum(iv) complexes. Further investigations indicate that compared with carboxylato ligands, the axial alkoxido ligands more greatly improve the hydrolytic and reductive stability of platinum(iv) complexes. Cytotoxicity studies suggest that alkoxido platinum(iv) complexes exert less activity against cancer cells than that of their carboxylated platinum(iv) analogues under similar cellular platinum accumulation levels, which could be attributed to their improved stability. This research provides a new strategy to synthesize alkoxido platinum(iv) complexes, which are expected to have significant applications as platinum(iv)-based anticancer prodrugs.
引用
收藏
页码:6058 / 6066
页数:9
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