Investigations on organo‐tin compounds. III. The biocidal properties of organo‐tin compounds

Kerk, G. J. M. Der Van; Luijten, J. G. A.

doi:10.1002/jctb.5010040607

Cited by 156 publications

(28 citation statements)

References 5 publications

(1 reference statement)

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“…For alkylorganostannanes, toxicity varies depending on the alkyl group. In general an increase in the alkyl chain length gives a decrease in toxicity [1,2,23,24]. The particular pattern for methyl, ethyl, propyl, and butyl varies with test organism.…”

Section: Resultsmentioning

confidence: 99%

Organotin Polyethers as Biomaterials

Carraher

Roner

2009

Materials

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Organotin polyethers are easily synthesized employing interfacial polymerization systems involving the reaction of hydroxyl-containing Lewis bases and organotin halides. A wide variety of organotin-containing polymeric products have been synthesized including those derived from natural and synthetic polymers such as lignin, xylan, cellulose, dextran, and poly(vinyl alcohol). Others have been synthesized employing known drug diols such as dicumarol, DES, and dienestrol and a wide variety of synthetic diols. Included in these materials are the first water soluble organotin polymers. The organotin polyethers exhibit a wide range of biological activities. Some selectively inhibit a number of unwanted bacteria, including Staph. MRSA, and unwanted yeasts such as Candida albicans. Some also inhibit a variety of viruses including those responsible for herpes infections and smallpox. Others show good inhibition of a wide variety of cancer cell lines including cell lines associated with ovarian, colon, lung, prostrate, pancreatic and breast cancer. The synthesis, structural characterization, and biological characterization of these materials is described in this review.

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Section: Resultsmentioning

confidence: 99%

Organotin Polyethers as Biomaterials

Carraher

Roner

2009

Materials

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“…[5] Thus, the limitations of platinum chemotherapeutic metallopharmaceuticals lead to development towards non-platinum chemotherapeutics aiming to increase the proficiency of such medications. [9][10][11] For instance, the initial biocidal properties of triorganotin compounds like tripropyltin, triphenyltin and tributyltin were studied by Van der Kerk and Luijten [12] during 1954, and these compounds were further known to battle the parasite that roots for schistosomiasis in human beings. [9][10][11] For instance, the initial biocidal properties of triorganotin compounds like tripropyltin, triphenyltin and tributyltin were studied by Van der Kerk and Luijten [12] during 1954, and these compounds were further known to battle the parasite that roots for schistosomiasis in human beings.…”

Section: Introductionmentioning

confidence: 99%

“…[6][7][8] Of these, organotins have been emerging as impending biologically active metallopharmaceuticals. [9][10][11] For instance, the initial biocidal properties of triorganotin compounds like tripropyltin, triphenyltin and tributyltin were studied by Van der Kerk and Luijten [12] during 1954, and these compounds were further known to battle the parasite that roots for schistosomiasis in human beings. [13,14] Besides, the crucial role of organotin compounds as potent antitumorogenic agents both in vitro and in vivo has also been established.…”

Section: Introductionmentioning

confidence: 99%

Binuclear diphenyltin(IV)dithiocarbamate complexes bearing functionalized linkers: Synthesis, spectral characterization, DFT and in vitro anticancer activity

Pillai

Patel

Buch

et al. 2018

Applied Organom Chemis

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A new series of diphenyltin(IV)dithiocarbamate complexes of the type [(Ph2Sn)2‐μ2‐bis{(κ2S,S‐S2CN(R)CH2CONHC6H4)2SO2}] {R = Cy (1), iPr (2), nBu (3)} and [(Ph2Sn)2‐μ2‐bis{(κ2S,S‐S2CN(R)CH2CONH)2C6H4}] {R = Cy (4), iPr (5)} has been efficiently synthesized and characterized by the relevant spectroscopic (1H, 13C, 1H DOSY, 119Sn NMR, ESI MS, UV–visible absorption, IR) and thermogravimetric methods. Density functional theory level calculations have been carried out to reinforce the experimental data. Compounds have been screened for their in vitro anticancer ability against a malignant human tumor HepG2 (hepatoma) cell line by MTT assay. Remarkably, the anticancer activities of binuclear organotin(IV)dithiocarbamate complexes 1–5 are evidently boosted as high as 22‐fold in 1 (3.32 ± 0.14 μM), 44‐fold in 2 (1.77 ± 0.11 μM), 37‐fold in 3 (2.02 ± 0.47 μM), 8 fold in 4 (8.72 ± 0.19 μM) and 29‐fold in 5 (2.60 ± 0.67 μM), compared with the reference drug cisplatin (75.67 ± 0.51 μM). Morphological proofs like shrinking of cells specifies the induction of apoptosis as part of the mechanism of action of these compounds, which is further reinforced by the individual staining of the cells by acridine orange/ethidium bromide.

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“…Significance of the X group in R 3 SnX derivatives has been reported to have minor effects on the biological activity of the compounds [2,9] unless X itself is biologically active or can assist the transport of the molecule to the active site. It has also been shown to be significant if the X group is chelated to the tin atom.…”

Section: Introductionmentioning

confidence: 99%

“…It was not until the 1950s that their toxicities were studied systematically [2,3]. The toxicity of organotins has been found to be a function of the number of organic groups attached to the tin atom, as well as to the nature of the organic group.…”

Section: Introductionmentioning

confidence: 99%