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Monochalcoplatin: An Actively Transported, Quickly Reducible, and Highly Potent Pt IV Anticancer Prodrug
Author(s) -
Ma Lili,
Wang Na,
Ma Rong,
Li Cai,
Xu Zoufeng,
Tse ManKit,
Zhu Guangyu
Publication year - 2018
Publication title -
angewandte chemie
Language(s) - English
Resource type - Journals
eISSN - 1521-3757
pISSN - 0044-8249
DOI - 10.1002/ange.201804314
Subject(s) - prodrug , lipophilicity , cisplatin , chemistry , cytotoxicity , in vivo , in vitro , cytotoxic t cell , apoptosis , cancer cell , combinatorial chemistry , pharmacology , stereochemistry , biochemistry , cancer , chemotherapy , biology , genetics , microbiology and biotechnology
Recently, Pt IV prodrugs have attracted much attention as the next generation of platinum‐based antineoplastic drug candidates. Here we report the discovery and evaluation of monochalcoplatin, a monocarboxylated Pt IV prodrug that is among the most cytotoxic Pt IV prodrugs to date. Compared with its dicarboxylated counterpart chalcoplatin, monochalcoplatin accumulates astonishingly effectively and rapidly in cancer cells, which is not ascribed to its lipophilicity. The prodrug is quickly reduced, causes DNA damage, and induces apoptosis, resulting in superior cytotoxicity with IC 50 values in the nanomolar range in both cisplatin‐sensitive and ‐resistant cells; these IC 50 values are up to 422‐fold higher than that of cisplatin. A detailed mechanistic study reveals that monochalcoplatin actively enters cells through a transporter‐mediated process. Moreover, monochalcoplatin shows significant antitumor activity in an in vivo colorectal tumor model. Our study implies a practical strategy for the design of more effective Pt IV prodrugs to conquer drug resistance by tuning both cellular uptake pathways and activation processes.