Effects of trialkyllead compounds on mitochondrial energy conservation

The effects of triethyllead acetate and tri-n-butyllead acetate on rat liver mitochondrial ATPase, succinate-driven ATP synthase and mitochondrial membrane potential have been compared with those of the equivalent organotin compounds. ATP synthase I₅₀ values were approximately four times the ATPase I₅₀ values for organotin compounds but the reverse pattern of activity is observed with trialkyllead compounds, which are 5-10 times more effective inhibitors of ATP synthase than of ATPase activity. The primary effects of trialkyltins are as inhibitors of the ATPase complex with relatively minor effects on mitochondrial membrane potential ($PS). In contrast, trialkylleads are potent uncoupling agents, which accounts for their potent inhibition of ATP synthesis. The uncoupling action of trialkylleads and trialkyltins is independent of chloride concentration and is unlikely to be due to Cl^?/OH^? exchange.     

Determination of organotin compounds (OTC) at low levels in seawater by solid-phase extraction (SPE) and gas chromatography-pulsed flame photometric detection (GC-PFPD)

In this work, a simple, sensitive and affordable analytical method for the simultaneous determination of nine organotin compounds (butyltins, phenyltins and methyltins) in seawater using solid-phase extraction (SPE) and gas chromatography-pulsed flame photometric detection was developed and validated. The performance of three different SPE cartridges (Envi C₁₈, Oasis HLB and Oasis MCX) and three elution solvents of different polarity (hexane, methanol and acetonitrile) was evaluated. The extraction parameters, such as solvent volume, presence of complexing and ion-pairing reagents, sample volume and pH and breakthrough volume, were also investigated. Tributyltin, as the organotin compound of special interest, was efficiently extracted using any of the cartridges and solvents tested. However, the simultaneous extraction of all nine organotin compounds was the most efficient using reversed-phase Envi C₁₈ cartridge and 0.1% (w/v) tropolone in methanol as eluent. The optimised method resulted in good recovery, precision and linearity for all compounds, particularly for tri- and disubstituted species. Method detection limits ranged from 0.22 to 1.27 ng(Sn) L^?1 for butyltins, 0.37 to 4.91 ng(Sn) L^?1 for phenyltins and 0.45 to 1.16 ng(Sn) L^?1 for methyltins. The accuracy of butyltins determination was further verified by the comparison with purchased derivatised standards. The developed method was successfully applied to the environmental samples.     

Emission studies of pyrene solutions

Emission spectra of pyrene in hexane have been obtained over a temperature range (from 130 to 260 K) that has not been explored before for concentrations ranging from 10^?4 mole/? to 2 × 10^?2 mole/?. A conventional and new approximation which does not depend on the experimental set-up response functions has been used for evaluating pyrene excimer association energy W_DM and other pyrene parameters. In both methods W_DM agrees quite satisfactorlly, at all concentrations used, with that reported in the literature and obtained by other techniques. However, both approximation fail to yield the right values of the rate parameters at concentrations ? 2 g/?. This set the upper limit of sample solubility to be at C = 2g/? for our range of temperature. Furthermore, the new approximation can probably be used at higher concentration (for higher range of temperature) and even may be used for other organic molecules. There was also no difference in the ratio of the excimer (I_D) to monomer (I_M) quantum yields when an intense laser beam was used as a source of excitation rather than a super-pressure Hg-lamp. This suggested that the concentrations we used might not be large enough. As a result, the laser beam would not create enough density of excited molecules to affect the ratio of I_D/I_M.     

QSAR for the Organophosphate-Induced Inhibition and ‚Aging‚ of the Enzyme Neuropathy Target Esterase (NTE)

Abstract

QSAR was devised for the neuropathy potency of various organophosphate (OP) compounds. The neuropathy-target-esterase (NTE) inhibition data were either obtained from the literature for a number of OP compounds or were determined experimentally for methamidophos, acephate, coumaphos and EPN. Aging Index that determined whether or not an OP would age NTE, correlated with molecular depth (MD) and the index density dipole-moment (density? Ω) (Eq. (1)). The t_1/2 values that represented the time (min) during which 50% of the OP-inhibited brain NTE undergoes ?aging‘, correlated with the topological indices Dif₃ and 1/Dif₄ (Eq. (2)). Log₁₀I₅₀ for AChE that determined the OP concentration causing 50% inhibition in AChE activity, correlated with E_bond and Charge^?1 (Eq. 3)). Log₁₀I₅₀ for NTE correlated with 1 HS² and H-Bonding (Eq. (4)). The (Log₁₀I₅₀NTE)/(Log₁₀I₅₀AChE) ratio that determined an OPs neuropathy potential relative to its cholinergic toxicity potential, correlated with log P and Log₁₀Polarity (Eq. (6)). Equation (3) accurately predicted AChE inhibition by methamidophos, coumaphos and EPN, but not by acephate. Equations (1), (2), (4)–(6), accurately predicted their respective biological indices. Therefore, it is proposed that the QSAR models developed in this study may accurately predict the neuropathy potential of OP compounds. The only exception is Eq. (3) that did not accurately predict the acephate-induced inhibition of AChE, possibly because acephate and other OPs inhibit the enzyme by distinct mechanisms.     

Chemical equilibria and sequential extractive spectrophotometric determination of selenium(IV) and (VI) using the chromogenic reagent 4,4′-dichlorodithizone

The chromogenic reagent 4,4′-dichloro(3-mercapto-1,5-diphenylformazan), Cl₂H₂D _Z , forms a yellow–red-coloured complex with selenium(IV). The produced complex species was extracted quantitatively into n-hexane, and its absorbance was measured at 416?nm. The chemical composition of the extracted selenium(IV)-Cl₂H₂D _Z chelate and the molar absorptivity at 416?nm were found to be [SeO (Cl₂HD _Z )₂] and 9?×?10⁴?L?mol^?1?cm^?1, respectively. The values of the extraction constants (K _D, K _ex, β) enable a convenient application of the proposed system for the liquid–liquid extraction procedure and sequential spectrophotometric determination of traces of inorganic selenium(IV) and/or selenium(VI) after reduction of the later to selenium(IV) with HCl (6?M). Beer's law and Ringbom's plots were obeyed in the concentration range 0.01–20 and 0.5–19?µg?mL^?1 of selenium(IV), respectively, with a relative standard deviation of 2.2%. The proposed method has been successfully applied to the determination of selenium(IV) or (VI) and total inorganic selenium(IV) and (VI) in tap and freshwater samples.     

Structural and antimicrobial studies of potassium hydrotris(2-mercaptobenzathiazolyl)borate and its organotin(IV) derivatives

Potassium hydrotris(2-mercaptobenzathiazolyl)borate (KL) was formed by the solid state reaction of potassium borohydride and 2-mercaptobenzathiazoline. This ligand was reacted with R _n SnCl_4?n (R =?methyl, butyl and phenyl, n =?2 and 3) in dichloromethane and four different neutral organotin(IV) complexes were obtained. All compounds were characterized by elemental analyses, FT-IR and multinuclear NMR (¹H, ¹³C, ¹¹ B and ¹¹⁹Sn) spectroscopy. Spectroscopic data indicate the six-coordinated nature of tin in its di and triorganotin(IV) complexes.

To check the toxic potential of the ligand and its organotin(IV) complexes, selected bacterial (E. coli, S. epidemidis and S. dysenteriae) and fungal (A. niger, C. albicanes and A. flaves) species were screened. The results were compared with standard drugs kinamycine and miconazole for bacterial and fungal activity, respectively. The toxicity of the organotin(IV) complexes depends on the number and nature of organic groups attached to the tin atom; triorganotin(IV) complexes exhibit better inhibition than diorganotin(IV) complexes. All compounds were also screened on the cyanobacterial strains (Aulosira fertillissma, Anabaena variabilis, Anabaena species and Nostoc muscorum). Results show that the compounds inhibit the growth of organisms at very low concentration.     

Synthesis,molecular characterisation,and in vivo study of platinum(IV) coordination compounds against B16 mouse melanoma tumours

A novel platinum(IV) coordination compound with 6-mercaptopurine (6-Hmp) has been synthesised and characterised by IR and NMR spectroscopy. Spectroscopic parameters indicate the presence of two chelate (S-6, N-7) monodeprotonated ligands and two chloride ions in the coordination sphere of [PtCl₂(6-mp)₂] · H₂O (I). Two Pt(IV) coordination compounds, [PtCl₂(6-mp)₂] · H₂O (I) and [PtCl₄(dbtp)₂] (II), were used in the in vivo test against B16 mouse melanoma tumours. Cytotoxic activity of compound II against the tumour cells was found to be high (LC₁₀ = 2.6 μM, LC₅₀ = 17.0 μM, LC₉₀ = 58.0 μM) compared to that of cisplatin.     

Synthesis and insecticidal activity of anthranilic diamides with hydrazone substructure

A series of anthranilic diamides with a hydrazone substructure was synthesised and characterised using ¹HNMR, ¹³C NMR, IR and elemental analyses. The in vitro insecticidal activity of all the compounds was tested against Plutella xylostella. The results showed the synthesised compounds to possess good insecticidal activity. The LC₅₀ values of compounds VIIg, VIIl, VIIm, VIIn exhibited excellent insecticidal activities, with the LC₅₀ affording 7.92 mg L^?1, 12.01 mg L^?1, 0.62 mg L^?1 and 10.71 mg L^?1, respectively. These may prove to be useful as potential insecticidal agents.     

Synthesis,spectroscopic characterization (IR, 1H, 13C and 119Sn NMR,electrospray mass spectrometry) and toxicity of new organotin(IV) complexes with N,N′,O‐ and N,N′,S‐scorpionate ligands

New organotin(IV) derivatives containing the anionic ligands bis(3,5‐dimethylpyrazol‐1‐yl)dithioacetate [LCS₂]⁻ and bis(3,5‐dimethylpyrazol‐1‐yl)acetate [LCO₂]⁻ have been synthesized from reaction between (CH₃)₂SnCl₂ and lithium salts of the ligands. Mononuclear complexes of the type {[LCX₂](CH₃)₂SnCl} (X = S or O) have been obtained and fully characterized by elemental analyses and FT‐IR in the solid state and by NMR (¹H, ¹³C and ¹¹⁹Sn) spectroscopy, conductivity measurements and electrospray ionization mass spectrometry in solution. The acute toxicity of new organotin(IV) derivatives on rat was studied, comparing their effect with those of dimethyltin chloride (CH₃)₂SnCl₂. The comparison of LD₅₀ of organotin(IV) complexes and (CH₃)₂SnCl₂ administered intraperitoneally, as a single dose, evaluated in vivo on rats, showed that toxicity decreases as follows: (CH₃)₂SnCl₂ > LCO₂ > LCS₂. The effect of these organotin(IV) complexes on DNA was evaluated in vitro and in vivo on rats treated with different doses of these compounds (1/20 LD₅₀ and 1/100 LD₅₀). The lymphocyte DNA status was assessed by the comet assay, a rapid and sensitive single‐cell electrophoresis technique, used to detect primary DNA damage in individual cells. After 36 h from the start of treatment the two new organotin(IV) derivatives induced a significant rise in comet assay parameters, indicating an increasing presence of damaged DNA. Copyright © 2005 John Wiley & Sons, Ltd.     

Desorption behavior of a surfactant in a linear low‐density polyethylene blend at elevated temperatures

The desorption behavior of a surfactant in a linear low‐density polyethylene (LLDPE) blend at elevated temperatures of 50, 70, and 80 °C was studied with Fourier transform infrared spectroscopy. The composition of the LLDPE blend was 70:30 LLDPE/low‐density polyethylene. Three different specimens (II, III, and IV) were prepared with various compositions of a small molecular penetrant, sorbitan palmitate (SPAN‐40), and a migration controller, poly(ethylene acrylic acid) (EAA), in the LLDPE blend. The calculated diffusion coefficient (D) of SPAN‐40 in specimens II, III, and IV, between 50 and 80 °C, varied from 1.74 × 10^?11 to 6.79 × 10^?11 cm²/s, from 1.10 × 10^?11 to 5.75 × 10^?11 cm²/s, and from 0.58 × 10^?11 to 4.75 × 10^?11 cm²/s, respectively. In addition, the calculated activation energies (E_D) of specimens II, III, and IV, from the plotting of ln D versus 1/T between 50 and 80 °C, were 42.9, 52.7, and 65.6 kJ/mol, respectively. These values were different from those obtained between 25 and 50 °C and were believed to have been influenced by the interference of Tinuvin (a UV stabilizer) at elevated temperatures higher than 50 °C. Although the desorption rate of SPAN‐40 increased with the temperature and decreased with the EAA content, the observed spectral behavior did not depend on the temperature and time. For all specimens stored over 50 °C, the peak at 1739 cm^?1 decreased in a few days and subsequently increased with a peak shift toward 1730 cm^?1. This arose from the carbonyl stretching vibration of Tinuvin, possibly because of oxidation or degradation at elevated temperatures. In addition, the incorporation of EAA into the LLDPE blend suppressed the desorption rate of SPAN‐40 and retarded the appearance of the 1730 cm^?1 peak. © 2004 Wiley Periodicals, Inc. J Polym Sci Part B: Polym Phys 42: 1114–1126, 2004     

Cytotoxicity and 2D-QSAR study of some heterocyclic compounds

Herein we have studied the cytotoxicity and quantitative structure–activity relationship (QSAR) of heterocyclic compounds containing cyclic urea and thiourea nuclei. A set of 22 hydantoin and thiohydantoin related heterocyclic compounds were investigated with respect to their LC₅₀ values (Log of LC₅₀) against brine shrimp lethality bioassay in order to derive the 2D-QSAR models using MLR, PLS and ANN methods. The best predictive models by MLR, PLS and ANN methods gave highly significant square correlation coefficient (R²) values of 0.83, 0.81 and 0.91 respectively. The model also exhibited good predictive power confirmed by the high value of cross validated correlation coefficient Q² (0.74).     

Structure and in vitro antifungal activity of [2,6‐bis(dimethylaminomethyl)phenyl]diphenyltin(IV) compounds

A set of seven [2,6‐bis(dimethylaminomethyl)phenyl]diphenyltin(IV) ({[(CH₃)₂NCH₂]₂(C₆H₃)}­(C₆H₅)₂Sn⁺X^?) ionic organotin(IV) compounds (X = Br, NO₃, CN, SCN, SeCN, BF₄ and PF₆) has been prepared and characterized by electrospray ionization mass spectrometry, ¹H NMR spectroscopy in CDCl₃,¹¹⁹Sn NMR in CDCl₃ and DMSO‐d₆ solution, as well as by ¹³C and ¹¹⁹Sn CP/MAS NMR spectroscopy and X‐ray diffraction techniques in the solid state. The in vitro antifungal activity of these water‐soluble ionic organotin(IV) compounds was compared with starting compounds and the antifungal drugs currently in clinical use. Copyright © 2002 John Wiley & Sons, Ltd.     

Synthesis,characterization, antibacterial,and cytotoxic activities of organotin(IV) complexes derived from N(4)-cyclohexylthiosemicarbazone: X-ray crystal structure of [Ph2SnCl(L)]

Reaction of organotin(IV) chloride(s) with 2-benzoylpyridine-N(4)-cyclohexylthiosemicarbazone, [HL] (1) yielded [MeSnCl₂(L)] (2), [BuSnCl₂(L)] (3), [Me₂SnCl(L)] (4), and [Ph₂SnCl(L)] (5). The ligand (1) and its organotin(IV) complexes have been characterized by CHN analyses, molar conductivity, UV-Vis, FT-IR, ¹H, ¹³C, and ¹¹⁹Sn NMR spectral studies. The molecular structure of 5 was also determined by X-ray diffraction. There are two independent molecules in the asymmetric unit and the central tin(IV) atom is six-coordinate in distorted octahedral geometry. The ligand (1) and complexes were screened for their in vitro antibacterial activities. The cytotoxic activities of 1–5 were tested against A2780 and A2780/Cp8 cancer cell lines. The compounds have better antibacterial activities than the free ligand; 2–5 are more potent cytotoxic agents than 1, while the diphenyltin(IV) 5 is more active with IC₅₀ values of 0.05 and 0.54?µmol?L^?1 against A2780 and A2780/Cp8 cell lines, respectively.     

Biological aspects of new organotin(IV) compounds of 3-maleimidopropionic acid

Four new compounds of organic mono carboxylic acid, 3-maleimidopropionic acid; with Bu₂Sn(IV)²⁺, Ph₃Sn(IV)⁺ and Cychex₃Sn(IV)⁺ having ligand to metal ratio 1:2 and 1:1 were prepared. The spectrophotometric techniques used for structure determination like ¹H-, ¹³C- and ¹¹⁹Sn-NMR, FT IR and ^119mSn Mössbauer have demonstrated that the organotin(IV) moieties establish chemical bonding with the ligand through carboxylic oxygen atom. The percent CHN analyses and MS data also corroborates the spectroscopic results. During in vitro LD₅₀, anti-fungal, anti-bacterial and anti-yeast bioassays promising results were exhibited. In vitro anti-tumour activity assays against five human tumor cell lines, MCF-7 Breast cancer-EVSA-T Breast cancer-WiDr Colon cancer-IGROV Ovarian cancer-M226 Non small cell lung cancer and anti-inflammatory screenings furnished the significant toxicities of the title complexes. In addition the triorganotin(IV) complexes were comparatively less toxic than the diorganotin(IV) complexes.     

Organotin(IV) complexes with 2-hydroxynaphthaldehyde-N(4)-ethylthiosemicarbazone: Synthesis,characterization, and in vitro antibacterial activity

Four new organotin(IV) complexes with 2-hydroxynaphthaldehyde-N(4)-ethylthiosemicarbazone [(H₂DNET), (1)] of the type [MeSnCl(DNET] (2), [BuSnCl(DNET)] (3), [PhSnCl(DNET)] (4), and [Ph₂Sn(DNET] (5) have been synthesized by the direct reaction of H₂DNET (1) with organotin(IV) chloride(s) in the presence of potassium hydroxide in absolute methanol. All the compounds were characterized by elemental analyses, molar conductivity, UV-Vis, IR, ¹H, ¹³C, and ¹¹⁹Sn NMR spectral studies. The molecular structure of ligand (1) has been confirmed by X-ray single crystal diffraction. Spectroscopic data clearly suggested that Sn(IV) center is coordinated with the ONS tridentate ligand (H₂DNET) and exhibits a five-coordinate geometry in solution. Antibacterial studies were carried out in vitro against four bacterial strains. All organotin(IV) compounds (2–5) showed good activity against various bacteria but lower activity than the reference drug (Ciprofloxacin). The results demonstrate that organic groups attached to tin(IV) moiety have significant effect on their biological activities. Among them, diphenyltin(IV) derivative 5 exhibits significantly good activity than the other organotin(IV) derivatives (2–4).     

In vitro antitumour activities of a novel 2:3 condensation product of salicylaldoxime with di-n-butyltin(IV) oxide

The antitumor activities of three novel condensation products of salicylaldoxime with di-n-butyltin(IV) oxide (compound 1), di-t-butyltin oxide (compound 2) and diphenyltin oxide (compound 3) are presented. Against MCF-7, a human mammary tumor cell line, compounds 1 and 2 are characterized by inhibition doses ID₅₀ in vitro of 67 and 49 ng cm^?3 respectively, whereas cis-platin, an antitumor drug used clinically, has an ID₅₀ of 850 ng cm^?3. Against WiDr, a colon carcinoma, they also score better than cis-platin: 215 and 121 ng cm^?3 versus 624 ng cm^?3. In contrast, the diphenyltin compound, 3, is inactive against both tumor cell lines. The results of a pre-screening performed on compound 1 by the National Cancer Institute (NCI) on a panel of 60 human tumor cell lines show that two of the selectivity parameters calculated by the NCI for that compound are statistically significant, namely D_G150 (51.9>50) and MGD_H (80.1>75). One is almost satisfactory (D_H = 72.4 = ca75). The other two, D_TGI (40.0<50) and D_LC50 (16.7<50) are not. (Abbreviations are explained in the text and in Gielen, M. and Willem, R. Anticancer Res., 1992, in press).     

Speciation of Organotin Compounds by Capillary Electrophoresis Coupled with Hydride Generation Atomic Fluorescence Spectrometry

Abstract

Capillary electrophoresis (CE) coupled with hydride generation atomic fluorescence spectrometry (HG‐AFS) was developed for the speciation analysis of organotin compounds. The four organotin cations of trimethyltin (TMT), monobutyltin (MBT), dibutyltin (DBT), and tributyltin (TBT) were completely separated by CE in a 50 cm×75 µm i.d. fused‐silica capillary at 15 kV and using a mixture of 50 mmol l^?1 H₃BO₃?50 mmol l^?1 Tris‐5% v/v methanol (pH 7.10) as electrolyte. 0.008 mmol l^?1 cetyltrimethylammonium bromide (CTAB) added to the electrolyte suppressed the adsorption of the organotin cations on the inner wall of capillary. The generated hydride species were detected on‐line with AFS. The precisions (RSD, n=5) were in the range of 1.7–3.1% for migration time and 3.8–4.7% for peak area response for the four organotin species. The detection limits ranged from 1–10 µmol l^?1 (as Sn).     

The acute toxicity of tri-n-butyltin taurocholate

The acute toxicity for tri-n-butyltin taurocholate (TBT-TA), a newly synthesized organotin steroid, was determined using Long Evans rats. The organotin compound was suspended in corn oil and administered by gavage using standard techniques. The TBT-TA exhibited a taurocholic acid toxicity at 24 h and a tributyltin toxicity at three days. The LD₅₀ values were 611 and 384 mg kg^?1 respectively. The dead rats exhibited distended stomachs, enlarged cecums, and lesions in the gastrointestinal tract. The toxicity is similar to that observed with other trialkyltin compounds.     

A Facile Method for the Synthesis of Binary Tungsten Iodides

The preparation of tungsten iodides in large quantities is a challenge because these compounds are not accessible using an easy synthesis method. A new, remarkably efficient route is based on a halide exchange reaction between WCl₆ and SiI₄. The reaction proceeds at moderate temperatures in a closed glass vessel. The new compounds W₃I₁₂ (W₃I₈?2 I₂) and W₃I₉ (W₃I₈? I₂) containing the novel [W₃I₈] cluster are formed at 120 and 150 °C, and remain stable in air. W₃I₁₂ is an excellent starting material for the synthesis of other metal‐rich tungsten iodides. At increasing temperature these trinuclear clusters undergo self‐reduction until an octahedral tungsten cluster is formed in W₆I₁₂. The synthesis, structure, and an analysis of the bonding of compounds containing this new trinuclear tungsten cluster are presented.