2009
DOI: 10.1007/s10637-009-9300-2
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In vitro cytotoxic evaluation of novel dichlorodiorgano[N-(2-pyridylmethylene)arylamine]tin(IV) derivatives in human tumor cell lines

Abstract: The present report overviews the studies on diorganotin(IV) complexes of N-(2-pyridylmethylene)arylamine, R(2)SnCl(2).L (R = Me (1), Et (2), Bu (3) or Ph (4)) as cytotoxic agents. This family of complexes was designed to include highly electron-donating N;Nchelating ligand to afford octahedral R(2)SnCl(2).L complexes of relatively high hydrolytic stability, with the aim to retain ligand binding throughout the biological activity for achieving controlled processes and allowing mechanistic evaluation. It is obse… Show more

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Cited by 11 publications
(13 citation statements)
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“…They exhibit hydrogen bonding interactions with the active site of amino acids of the aforementioned enzymes. The higher activity was attributed to the presence of the azo group nitrogen atoms in the molecules of triphenyltin (IV) complexes [27]. As a continuation of our previous work in this area, we report some new triphenyltin(IV) complexes, Ph 3 SnL 1 − 4 H (1-4), of related systems where the ligand skeletal framework has been modified (Scheme 1) in an attempt to improve the dissolution properties and thereby influence cytotoxicity.…”
Section: Introductionmentioning
confidence: 78%
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“…They exhibit hydrogen bonding interactions with the active site of amino acids of the aforementioned enzymes. The higher activity was attributed to the presence of the azo group nitrogen atoms in the molecules of triphenyltin (IV) complexes [27]. As a continuation of our previous work in this area, we report some new triphenyltin(IV) complexes, Ph 3 SnL 1 − 4 H (1-4), of related systems where the ligand skeletal framework has been modified (Scheme 1) in an attempt to improve the dissolution properties and thereby influence cytotoxicity.…”
Section: Introductionmentioning
confidence: 78%
“…The in vitro cytotoxicity testing of triphenyltin(IV) complexes 1-5 was performed using the SRB test for estimation of cell viability. Experimental protocols for 6 and 7 have been reported [27] and the cytotoxic results are included here for convenience of discussion. The cell lines WIDR colon carcinoma, M19 MEL melanoma, A498 renal cell carcinoma, IGROV ovarian carcinoma and H226 non-small-cell lung cancer belong to the currently used anticancer screening panel of the NCI, USA [34].…”
Section: Experimental Protocol and Cytotoxicity Testsmentioning
confidence: 99%
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“…Over the years, much attention has been focused on developing cisplatin analogues. Currently, cisplatin, carboplatin and oxaplatin are widely used anticancer drugs, and are especially effective against testicular and ovarian carcinomas, bladder tumors and tumors of the head and neck (9). It is generally believed that the ultimate target of this type of drug is DNA (10).…”
Section: Introductionmentioning
confidence: 99%