Synthesis and characterisation of the carboxylate linked osmium clusters [{Os3H(CO)10}2(CO2CH2CO2)], [{Os3H(CO)10}2(CO2C2H4CO2)], [{Os3H(CO)10}2(C4O4)] and [{Os3H(CO)10}2(C4O4){Co2(CO)6}]

Reactions between the activated cluster [Os₃(CO)₁₀(NCMe)₂] and malonic acid, succinic acid and dicarboxylic acetylene, respectively, lead to the formation of the linked cluster complexes [{Os₃H(CO)₁₀}₂(CO₂CH₂CO₂)] (1), [{Os₃H(CO)₁₀}₂(CO₂C₂H₄CO₂)] (2), and [{Os₃H(CO)₁₀}₂(C₄O₄)] (3) in good yield. Cluster 3 was subsequently treated with [Co₂(CO)₈] and this results in the addition of a “Co₂(CO)₆” group giving [{Os₃H(CO)₁₀}₂(C₂O₄){Co₂(CO)₆}] (4). The X-ray crystal structures are reported for 2–4. In each structure the two triangular triosmium units are linked by the carboxylate groups and within each complex the carboxylate groups are chelating and bridge two osmium atoms.     

95Mo NMR spectra of MoO2(C8H7N2S)2 and X-ray crystal structure of Mo2O4(C8H7N2S)2(C3H7NO)2

The facile preparation of MoO₂(C₈H₇N₂S)₂ is given and its complex behaviour in dimethylformamide, as revealed by ⁹⁵Mo NMR spectroscopy, discussed. The X-ray crystal structure of one of the products obtained from this dimethylformamide solution is briefly described. This structure indicates that the Mo(VI) has been reduced to Mo(V) and is based on the [Mo₂O₄]²⁺ core.     

Two new scorpionates vanadium haloperoxidases model complexes: synthesis and structure of VO(O2)(pzH)(HB(pz)3) and VO(O2)(pzH)(B(pz)4) (pzH = pyrazole(C3H4N2))

Using vanadate, poly(1H-pyrazol-1-yl)borate and pyrazole as starting materials, two new neutral peroxovanadium(V) complexes with poly(1H-pyrazol-1-yl)borate, VO(O(2))(pzH)(HB(pz)(3))(1) and VO(O(2))(pzH)(B(pz)(4))(2), were synthesized successfully. Both complexes were characterized by elemental analysis, IR, UV-vis and NMR spectra. And the structure of complex 1 was determined by X-ray diffraction, which is somewhat relevant for haloperoxidase enzymes. Cytotoxic effects also are discussed on 3T3 cell proliferation. In the concentration range (0.1-100mumol), both complexes have an inhibiting cellular proliferation effect. When the cells cultivated with the complexes at high dose, the toxicity effect of both complexes is more and more predominant.     

95Mo NMR studies of complexes containing the Mo2O52+ core and crystal structure of Mo2O5[SC6H4NHCH2C5H4N]2(C3H7NO)3

The crystal structure of Mo₂O₅[SC₆H₄NHCH₂C₅H₄N]₂(C₃N₇NO)₃ is reported and seen to consist of a single oxo-bridged species with each Mo atom bonded to cis dioxo groups and the nitrogen atoms and thiolate group of the tridentate ligand. ⁹⁵Mo NMR spectra of this and three related complexes are presented and attempts made to interpret them in terms of their crystal structures.     

Investigations of the {ReO} core: A '2+2' complex from bidentate and potentially trident ligands: [ReO(η-HOC(6)H(4)-2-CH(2)NC(6)H(4)S)(η-SC(5)H(4)N)(PPh(3))

The reaction of [ReOCl(3)(PPh(3))(2)] with N-(2-hydroxybenzyl)-2-mercaptoaniline (H(3)hbma) (2) and 2-mercaptopyridine in hot CHCl yields [ReO(η(2)-HOC(6)H(4)-2-CH(2)NC(6)H(4)S)(η(2)-SC(5)H(4)N)(PPh(3))] (3). The structure of 3 consists of distorted octahedral Re(V) monomers. The coordination geometry at the rhenium is defined by a terminal oxo-group, the nitrogen and sulfur donors of the chelating mercaptopyridine, the nitrogen and sulfur donors of a bidentate (Hhbma)(2-) ligand, and the phosphorus of the PPh(3) group. The -C(6)H(4)OH arm of (Hhbma)(2-) is pendant, and the coordinated nitrogen of this ligand is present as a deprotonated amido nitrogen.     

Synthesis,structure, reactivity and electrochemistry of a new molybdenum(0) dithiocarbamato complex, [Et4N][Mo(CO)4(S2CNEt2)]

A new molybdenum(0) dithiocarbamato complex [Et₄N] [Mo(CO)₄(S₂CNEt₂)] (1) has been synthesized by the reaction of Mo(CO)₆, NaS₂CNEt₂ and Et₄NCl in MeCN and characterized by routine elemental analysis, spectroscopy methods. The crystal and molecular structure of 1 was determined from X-ray three dimension data. 1 crystallizes in the orthorhombic, space group Pbc2₁ with a= 8.148(2), b=19.618(2), c=14.354(2) Å; V=2294 ų; Z=4; R₁=0.052, R₂=0.058 for 1308 independent reflections with I ⩾ 3σ(I). The geometry around Mo(0) atom in the anion [Mo(CO)₄(S₂CNEt₂)]^- of 1 is distorted octahedral with a small SMoS of 67.70° and a small angle of 3.6° between plane MoSS and MoC(1)C(2). Two groups of MoCO bond distances and the longer MoS bond distance observed in 1 are similar to that in the dinuclear Mo(0) complexes containing SR bridges but very different from those observed in the dithiocarbamato complexes of Mo in higher oxidation states. Different oxidizing products containing Mo in II-V oxidation states Mo(CO)₂(S₂CNEt₂)₂, MoO(S₂CNEt₂)₂, Mo₂O₃(S₂CNEt₂)₄ and Mo₂O₄(S₂CNEt₂)₂ were isolated from the oxidation of 1 with I₂ (or in the presence of traces of air). The electrochemical behavior of 1 in MeCN was investigated by cyclic voltammetry at Pt and C electrodes. The anodic peaks observed at 0.04, 0.14, 0.26 and 0.44 V versus SCE implied that 1 probably underwent oxidation in company with dissociation of dithiocarbamate and substitution of carbonyls resulting in several complexes of Mo in different oxidation states. The relationship between reactivity and structure is also discussed.     

An AB initio investigation of molecules with a disulfide bond: (HS)2, (CH3S)2 and cystine

ab initio Calculations at the Gaussian-70 STO-3G and 4-31G basis levels have been carried out for (HS)2 and (CH3S)2. Cystine was investigated at the STO-3G level. The STO-3G energy minimized geometry agrees well with experiments for (HS)2 and (CH3S)2. The barriers to internal rotation are predicted to be (at the 4.31G level): (HS)2, cis 8.5 kcal, trans 3.03 kcal; (CH3S)2, cis 18.47 kcal, trans 6.04 kcal.     

The structure of a dinuclear silver(I) complex: Ag2[S2C2(CN)2] [P(C6H5)3]4

The crystal structure of the dimeric Ag maleonitriledithiolate complex, Ag₂[S₂C₂(CN)₂] [P(C₆- H₅)₃]₄ (1), has been performed. Complex 1 crystallizes in the space group P2₁/c with a = 12.2898(77), b = 23.8325(91), c = 23.1790(118) Å, β = 101.315(43)° and Z = 4. Refinement using 3253 reflections with F_o²>3σ(F_o²) yielded R = 0.0662, R_w= 0.0669. The most interesting aspect of the structure is the strong bridging interaction of the chelating maleonitriledithiolate ligand with the second Ag center, where a Ag-S distance of 2.478 Å is observed. The residual bonding capability of the sulfur atoms in the chelating anion [Ag(S₂C₂(CN)₂)(PPh₃)₂]⁻ for [Ag(PPh₃)₂]⁺ is demonstrated.     

A bridged Mo(VI) complex containing six and five coordinate Mo: Synthesis, 95Mo N.m.r. spectroscopy and X-ray crystal structure of Mo2O5(C17H17N2O)2

The kinetics of the reaction between Carcinus maenas hemocyanin and cyanide has been studied at various KCN concentrations and a different temperatures (21° and 4°C) by following the decrease of the copper-peroxide absorption band, centered at 337 nm, of the copper still bound to the protein and the intrinsic fluorescence changes as functions of time. In all conditions used, the absorption band completely disappears and KCN concentration affects only the rate of the process. The reaction is kinetically homogeneous indicating no site-site interaction. The apparent rate constant increases with the square of cyanide concentration and the inverse of O₂ concentration. The copper still bound decreases at a rate slower than the 337 nm absorption and the process is not kinetically homogeneous. The fluorescence of the protein increases after an induction period showing an inflection point at about 50% of the total effect. A kinetic model has been proposed on the assumption that the two metal ions are removed sequentially from the active site. The experimental data are in agreement with the theoretical equations derived from the model. The equilibrium constants for the formation of the complex between the first and the second copper ion with cyanide and the rate constants of their decomposition have been calculated. The rate-limiting process for the removal of the second copper ion is the formation of the complex with cyanide.     

Crystal structures and cytotoxicity of isopropylamine Pt(II) complexes: a trinuclear squarato-bridged [Pt3(mu2-C4O4)3(H2NPri)6].3H2O and a mononuclear cis-[Pt(NO3)2(H2NPri)2

Crystals of a novel platinum(II) complex with squarato ligand, [Pt(3)(mu(2)-C(4)O(4))(3)(H(2)NPr(i))(6)].3H(2)O (1) (H(2)NPr(i)=ipa), have been isolated from the aqueous solution of cis-[Pt(H(2)O)(2)(H(2)NPr(i))(2)]SO(4) and barium squarate. Slow evaporation of methanol solution of cis-[Pt(NO(3))(2)(H(2)NPr(i))(2)] (2) resulted in crystallization of nitrato complex. The single crystal X-ray diffraction method was used to determine structures of 1 and 2. Complex 1 crystallizes in a triclinic space group P1 with a=11.17380(10)A, b=14.4535(2)A, c=14.8010(2)A, alpha=86.0901(10) degrees , beta=78.4343(11) degrees , gamma=69.1915(5) degrees , and complex 2 in a monoclinic space group P2(1)/n, with a=10.1161(2)A, b=9.9188(2)A, c=13.3766(2)A, beta=102.7360(7) degrees . The X-ray structure analysis revealed that three platinum atoms in 1 are connected with three squarates which adopt bis(unidentate) binding modes. The squarato ligands span relatively long intramolecular Ptcdots, three dots, centeredPt distances (4.8842(3)-5.2699(3)A). A pair of cis positioned isopropylamine ligands completes a square planar coordination sphere of each Pt(II) ion. The square-planar coordination of complex 2 consists of two cis positioned isopropylamine ligands and two nitrato ligands. The results of cytotoxicity assay of trimer 1, monomer 2 and cis-diamminedichloroplatinum(II) (cisplatin) performed on human bladder tumor cell line T24 provide evidence that complex 2 is less cytotoxic compared to cisplatin and that the survival of tumor cells after exposure to 1 was minimally reduced.     

Fluconazole analogues containing 2H-1,4-benzothiazin-3(4H)-one or 2H-1,4-benzoxazin-3(4H)-one moieties,a novel class of anti-Candida agents

As a part of our program to develop new antifungal agents, a series of fluconazole analogues was designed and synthesized wherein one of the triazole moieties in fluconazole was replaced with 2H-1,4-benzothiazin-3(4H)-one or 2H-1,4-benzoxazin-3(4H)-one moiety. The new chemical entities thus synthesized were screened against various fungi and it was observed that the compounds 4a and 4i are potent inhibitors of Candida strains. The structure–activity relationship for these compounds is discussed.     

Isonicotinamide as entering ligand on trans-[Ru(NH3)4P(OR)3(H2O)]22+, (R = Me,Pr, iPr and Bu)

trans-[Ru(NH₃)₄P(OR)₃(H₂O)]²⁺ (R = Me, Pr, ⁱPr, and Bu) reacts with isonicotinamide at second-order- specific rates k₁ of 1.2, 2.3, 7.4 and 8.1 M⁻¹ s⁻(25 °C, μ = 0.10 NaCF₃COO/CH₃COOH), respectively, for R = Me, Pr, ⁱPr and Bu. The products trans- [Ru(NH₃)₄P(OR)₃isn](PF₆)₂ have been isolated and characterized by micro analysis, cyclic voltammetry, and electronic spectral data. The aquation rates k₋₁ for the isonicotinamide (isn) derivatives are 5.2 × 10⁻², 5.9 × 10⁻², 2.0 × 10⁻¹ and 3.4 × 10⁻¹ s⁻¹ for R= Me, Pf, Bu and ⁱPr, respectively. The activation parameters for the forward and backward reactions indicate the same mechanism for all of them. The substitution proceeds by a dissociative mechanism with a significant outer-sphere association of trans-[Ru(NH₃)₄P(OR)₃(H₂O)]²⁺ complexes with isn. Assuming k₁ as indicative of the lability of the coordinated water molecule on the monophosphite complexes, the following sequence of increasing trans-effect mav be proposed: P(OMe)₃ <P(OEt)₃ <P(OPr)₃ <P(OⁱPr)₃ <P(OBu)₃. The affinity of the monophosphite complexes for isn increases according to P(OMe)₃ ⋍ P(OⁱPr)₃ < P(OEt)₃ < P(OPr)₃ ⋍ P(OBu)₃.     

Synthesis, characterization and cytotoxic activity of substituted benzyl iminoether Pt(II) complexes of the type cis- and trans-[PtCl2{E-N(H)=C(OMe)CH2-C6H4-p-R}2] (R=Me, OMe, F). X-ray structure of trans-[PtCl2{E-N(H)=C(OMe)CH2-C6H4-p-F}2

New substituted benzyl iminoether derivatives of the type cis- and trans-[PtCl(2){E-N(H)C(OMe)CH(2)-C(6)H(4)-p-R}(2)] (R=Me (1a, 2a), OMe (3a, 4a), F (5a, 6a)) have been synthesized and characterized by elemental analyses, FT-IR spectroscopy and NMR techniques. The iminoether ligands are in the E configuration, which is stable in solution and in the solid state, as confirmed by the (1)H NMR data. Complex trans-[PtCl(2){E-N(H)C(OMe)CH(2)-C(6)H(4)-p-F}(2)] (6a) was also characterized by an X-ray diffraction study. Complexes 1a-6a have been tested against a panel of human tumor cell lines in order to evaluate their cytotoxic activity. cis-Isomers were significant more potent than the corresponding trans-isomers against all tumor cell lines tested; moreover, complexes 1a and 5a showed IC(50) values from about 2-fold to 6-fold lower than those exhibited by cisplatin, used as reference platinum anticancer drug.     

Isolation and physico-chemical properties of native histone complexes: dimer (H2-H2B), tetramer (H3-H4)2 and octamer (H3-H4-H2A-H2B)2

The paper is concerned with the isolation of the native histone complexes: dimer (H2A-H2B), tetramer (H3-H4)2 and octamer (H3-H4-H2A-H2B)2 from the calf thymus chromatin under soft conditions (hydroxyl apatite) fractionation with the subsequent gel filtration). Parameters of hydroxyl apatite saturation with chromatin are determined. The complexes obtained are free of DNA and nonhistone proteins. Absorption spectra parameters, quantum efficiencies and fluorescence spectra typical of the corresponding histone oligomers are established. Comparison of free tyrosine fluorescence spectra with histone tyrosyl ones revealed a long-wave shift in the latter.