Host–Guest Interactions of Risperidone with Natural and Modified Cyclodextrins: Phase Solubility, Thermodynamics and Molecular Modeling Studies

The solubility of risperidone (Risp) in aqueous buffered cyclodextrin (CD) solution was investigated for α-, β-, γ- and HP-β-CD. The effects of pH, ionic strength and temperature on complex stability were also explored. Neutral Risp tends to form higher order complexes (1:2) with both β- and HP-β-CD, but only 1:1 type complexes with α-, and γ-CD. The tendency of Risp to complex with cyclodextrins is in the order β-CD > HP-β-CD > γ-CD > α-CD. The 1:1 complex formation constant of Risp/HP-β-CD increases with increasing ionic strength in an opposite trend to the inherent solubility (S ₀) of Risp, thus indicating significant hydrophobic effect. The hydrophobic effect contributes to the extent of 72% towards neutral Risp/HP-β-CD complex stability, while specific interactions contribute only 4.7 kJ/mol. Thermodynamic studies showed that 1:1 Risp/HP-β-CD complex formation is driven by a favorable enthalpy change (ΔH ⁰=−31.2 kJ/mol, ΔS ⁰=−7 J/mol.K) while the 1:2 complex is largely driven by entropy changes (ΔH ⁰=−5.0 kJ/mol, ΔS ⁰=42 J/mol.K). Complex stability was found to vary with pH, with a higher formation constant for neutral Risp. Molecular mechanical computations using MM (atomic charges and bond dipole algorithms) and Amber force fields, which were carried out to explore possible sites of interactions between Risp and CDs and to rationalize complex stoichiometry, produced similar results concerning optimal inclusion complex geometries and stoichiometries.     

A tetra-coordinate nickel(II) complex as neutral carrier for nitrate-selective PVC membrane electrode

The potentiometric response properties and applications of a tetra-coordinate nickel(II) complex with relatively high selectivity toward nitrate ion are described. The nickel(II) complex of 5,7,12,14-tetramethyl-1,4,8,11-tetraazacyclotetradeca-4,6,11,13-tetraene was used as a neutral carrier into plasticized poly(vinyl chloride) (PVC) membrane. The influence of several variables was investigated in order to optimize the potentiometric response and selectivity of the electrode. The resulting membrane electrode incorporating 31.0% PVC, 61.0% dioctyl phthalate (DOP) as plasticizer, 3% methyltrioctylammonium chloride (MTOAC) as a cationic additive and 5% carrier (all w/w) demonstrates a Nernstian response slope of −59.6 mV per decade over the concentration range of 5×10⁻⁶-1×10⁻¹ M NO₃⁻. The electrode exhibits a fast response time (≤10 s), a detection limit of 2.5×10⁻⁶ M, and can be used over a wide pH range of 4-12. The electrode shows improved selectivity in comparison to most of the previously reported nitrate-selective electrodes. It was successfully applied to the determination of nitrate ion in natural water samples.     

Synthesis,Characterization and Crystal Structures of new Coordination Polymers of Cerium(III) and Samarium(III) Containing 2,6‐Pyridinedicarboxylic Acid

The reaction of 2,6‐pyridinedicarboxylic acid ( 1 , LH₂) with CeCl₃·7H₂O and Sm(NO₃)₃·6H₂O in the presence of triethylamine led to the coordination polymer complexes [M(L)(LH)(H₂O)₂]·4H₂O [M = Ce ( 2 ) and Sm ( 3 )]. Both complexes were characterized by elemental analyses, IR spectroscopy and the crystal structures of 2 and 3 . Crystal data for 2 at ?80 °C: monoclinic, space group P2₁/c, a = 1404.6(1), b = 1122.1(1), c = 1296.1(1) pm, β = 102.09(1)°, Z = 4, R₁ = 0.0217 and for 3 at ?80 °C: monoclinic, space group P2₁/c, a = 1395.1(1), b = 1120.1(1), c = 1282.8(1) pm, β = 102.71(1)°, Z = 4, R₁ = 0.019.     

Preparation of Diazo Phenyl Sulfides. Kinetics and Mechanism of the Diazo Coupling Reaction of p-Nitrobenzenediazo Phenyl Sulfide with β-Naphthol under Various Conditions

Aryldiazophenyl sulfides prepared from diazotised arylamines and thiophenol at controlled pH, are coupled with β-naphthol yielding the corresponding azo dye. A kinetic study of the diazo coupling reaction of p-nitrobenzenediazo phenyl sulfide with β-naphthol under various conditions revealed that the reaction is of first order kinetics with respect to the diazo phenyl sulfide, and that the rate of coupling measured colorimetrically is influenced by the hydrogen ion concentration and by the ionising power of the medium.     

Thermodynamic studies of the binding of bidentate nitrogen donors with methyltrioxorhenium (MTO) in CHCl3 solution

Methyltrioxorhenium (MTO) adduct formation with bidentate nitrogen donors 2,2'-bipyridine (bpy), 4,4'-dimethyl-2,2'-bipyridine (Me(2)bpy), 4,4'-di-tert-butyl-2,2'-bipyridine (tBu2bpy), 1,10-phenanthroline (phen), 5-methyl-1,10-phenanthroline (5-Mephen), 5-chloro-1,10-phenanthroline (5-Clphen), 4,7-dimethyl-1,10-phenanthroline (Me2phen) has been studied at different temperatures in CHCl3 solution. Spectrophotometeric measurements have been carried out to obtain the thermodynamic parameters. All complexes are enthalpy stabilized whereas the entropy changes counteract the adduct formation. The results are discussed in terms of different basicities of the bidentate N-donors.     

Electrostatics of PEGylated micelles and liposomes containing charged and neutral lipopolymers

The electrostatics of large unilamellar vesicles (LUVs) of various lipid compositions were determined and correlated with steric stabilization. The compositional variables studied include (a) degree of saturation, comparing the unsaturated egg phosphatidylcholine (EPC) and the fully hydrogenated soy phosphatidylcholine (HSPC) as liposome-forming lipids; (b) the effect of 40 mol % cholesterol; (c) the effect of mole % of three methyl poly(ethylene glycol) (mPEG)-lipids (the negatively charged mPEG-distearoyl phosphoethanolamine (DSPE) and two uncharged lipopolymers, mPEG-distearoyl glycerol (DSG) and mPEG-oxycarbonyl-3-amino-1,2-propanediol distearoyl ester (DS)); and (d) the negatively charged phosphatidyl glycerol (PG). The lipid phases were as follows: liquid disordered (LD) for the EPC-containing LUV, solid ordered (SO) for the HSPC-containing LUV, and liquid ordered (LO) for either of those LUV with the addition of 40 mol % cholesterol. The LUV zeta potential and electrical surface potential (psi(0)) were determined. It was found that progressive addition of mPEG(2k)-DSPE to liposomes increases negative surface potential and reduces surface pH to a similar extent as the addition of PG. However, due to the "hidden charge effect", zeta potential was more negative for liposomes containing PG than for those containing mPEG(2k)-DSPE. Replacing mPEG-DSPE with mPEG(2k)-DS or mPEG-DSG had no effect on surface pH and surface potential, and zeta potential was approximately zero. Addition of low concentrations of cationic peptides (protamine sulfate and melittin) to PG- or mPEG-DSPE-containing liposomes neutralized the liposome negative surface potential to a similar extent. However, only in liposomes containing PG, did liposome aggregation occur. Replacing the negatively charged lipopolymer mPEG-DSPE with the neutral lipopolymers mPEG-DS or mPEG-DSG eliminates or reduces such interactions. The relevance of this effect to the liposome performance in vivo is discussed.     

Effect of sodium oxide doping on solid-solid interactions between V2O5 AND Al2O3

A V₂O₅/Al₂O₃ mixed solids sample was prepared with a molar ratio of 0.41 Na₂O (4 and 10 mol%) was added in the form of sodium nitrate prior to calcination in air in the temperature range 500–1000C. Solid-solid interactions between V₂O₅ and Al₂O₃ were studied using DTA and TG curves and their derivatives together with XRD techniques.The results obtained showed that Na₂O interacted with V₂O₅ at temperatures starting from 500C to yield a sodium/vanadium compound, Na_0.3V₂O₅ which remained stable and decomposed in part by heating at 1000C. V₂O₅ exists in orthorhombic and monoclinic forms in the case of pure mixed solids and those containing 4 mol% of Na₂O and preheated at 500C, and in monoclinic form in the case of the mixed solid doped with 10 mol% of Na₂O.Heating of pure and doped mixed oxide solids at 650C resulted in the conversion of most of the V₂O₅ into AlVO₄. Doping with sodium oxide enhanced the solid-solid interaction between V₂O₅ and Al₂O₃ at 650C to produce AlVO₄. The produced AlVO₄ decomposed completely on heating at 700C to form -Al₂O₃ and V₂O₅, (orthorhombic and monoclinic forms).The presence of Na₂O was found to decrease the relative intensity of the diffraction lines of -Al₂O₃ (corundum) produced at 750C which indicated some kind of hindrance of the crystallization process.Heating of pure and doped mixed solids at 1000C resulted in a further crystallization of acorundum together with V₂O₅ and sodium vanadate, Na_0.3V₂O₅. However, the intensities of diffraction lines relative to those of the sodium vanadium compound were found to decrease markedly by heating at 1000C, indicating partial thermal decomposition into vanadium and aluminium oxides.     

High-performance liquid chromatographic analysis of vancomycin in plasma, bone, atrial appendage tissue and pericardial fluid

Solid-phase extraction coupled with reversed-phase high-performance liquid chromatography and UV detection was employed for the analysis of the antibiotic vancomycin in patient plasma, bone, atrial appendage, and pericardial fluid. Vancomycin was quantitated in samples from patients undergoing cardiac surgery. Calibrations were linear in the range 3-100 micrograms/ml vancomycin; the lower limit of detection was approximately 3 micrograms/ml in fluids with an absolute limit of detection in bone samples of 0.75 microgram per injection.     

Divalent transition metal ion mixed ligand complexes with aliphatic dicarboxylic acids and imidazoles

Summary Mixed ligand metal complexes of Co^II, Ni^II and Cu^II with dicarboxylic aliphatic acids, H₂L (succinic, malic and tartaric) as primary ligands and with imidazoles, L (imidazole and 2-methylimidazole) as secondary ligands were prepared and characterized. MLL₂ and ML₄ molecular formulae were suggested for these complexes were Formation constants of the different complexes were determined pH-metrically at T = 25 ± 0.1°C and = 0.1 mol dm^–3 (NaClO₄). The stability of the mixed ligand complexes increased as the effective basicity of the dicarboxylic aliphatic acid anion increased, namely, tartarate < malate < succinate acid.