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Cytotoxic effects of halogenated tin phosphinoyldithioformate complexes against several cancer cell lines.

Michaela BalogováShubham SharmaPaulina CherekSigurjón N ÓlafssonSigrídur JónsdóttirHelga M ÖgmundsdóttirKrishna K Damodaran
Published in: Dalton transactions (Cambridge, England : 2003) (2022)
Organotin complexes are studied as promising alternatives to the anticancer drug cisplatin. We report two monoorganotin(IV) complexes based on a dibenzyl phosphinoyldithioformate (H-DBPTF) ligand, containing either bromide (Sn-DBPTF-1) or chloride (Sn-DBPTF-2) anions. The complexes were characterized by standard analytical techniques and the structural details of these complexes were elucidated by single crystal X-ray diffraction. Sn-DBPTF-1 was cytotoxic at IC 50 <10 μg mL -1 against cancer cell lines A549 (lung cancer), Aspc-1 (pancreatic cancer), OVCAR-3 (ovarian cancer), T-47D (breast cancer) and HCT116 (colon cancer), and breast epithelial stem cell line D492. The non-tumorigenic breast epithelial cell line MCF-10 was less sensitive at IC 50 = 22 μg mL -1 . Sn-DBPTF-2 had limited cytotoxic effect at IC 50 13-37 μg mL -1 . Sn-DBPTF-1 induced apoptosis and double-strand DNA breaks. Cell cycle arrest in G2 occurred in HCT116 and accumulation in G1 in Aspc-1. The results indicate that the basic effect of Sn-DBPTF-1 is to induce DNA damage, leading to apoptosis and cell cycle arrest depending on the cell line.
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