Time-resolved flash spectroscopic investigations of the reactions of singlet arylhalocarbenes

The results of time-resolved laser flash spectrometric studies of singlet arylhalocarbenes are reviewed. In particular, the absolute rate constants for reactions of phenylchlorocarbene and related carbenes with alkenes are summarized and systematized. The experiments described provide the basis for a detailed examination of carbenic reactivity-selectivity principles. The results of studies on the influence of temperature on the absolute rate constants for carbene reactions are consistent with the existence of transient carbene/alkene intermediates.     

The Preparation, Characterization and Biological Activity of Palladium(II) and Platinum(II) Complexes of Tridentate NNS Ligands Derived from S-methyl- and S-benzyldithiocarbazates and the X-ray Crystal Structure of the [Pd(mpasme)Cl] Complex

New complexes of general formula, [M(NNS)Cl] (M = Pd^II, Pt^II; NNS = anionic forms of the 6-methyl-2-formylpyridine Schiff bases of S-methyl- and S-benzyldithiocarbazates) have been prepared and characterized by a variety of physico-chemical techniques. Based on conductance and spectral evidence, a square-planar structure is assigned to these complexes. The crystal and molecular structure of the [Pd(mpasme)Cl] complex (mpasme=anionic form of the 6-methyl-2-formylpyridine Schiff base of S-methyldithiocarbazate) has been determined by X-ray diffraction. The complex has a distorted square-planar geometry with the ligand coordinated to the palladium(II) ion via the pyridine nitrogen atom, the azomethine nitrogen atom and the thiolate sulfur atom; the fourth coordination position around the palladium(II) ion is occupied by the chloride ligand. The distortion from a regular square-planar geometry is ascribed to the restricted bite angle of the ligand. Both the Schiff bases exhibit strong cytotoxicity against the human ovarian cancer (Caov-3) cell lines, the S-methyl derivative being two times more active than the S-benzyl derivative. The [Pt(mpasme)Cl] complex is moderately active but the palladium(II) complex is weakly active against this cancer. None of the complexes of Hmpsbz are active against Caov-3. The Schiff base, Hmpasme exhibits moderate activity against the bacteria, MRSA, P. aeruginosa and S. typhimurium but is inactive against B. subtilis. Coordination of the ligand with palladium(II) substantially reduces its activity. The Schiff base, Hmpasbz and its palladium(II) and platinum(II) complexes are inactive against these bacteria. The Schiff bases and their palladium(II) and platinum (II) complexes are inactive against the pathogenic fungi, C. albican, Aspergillus ochraceous and Saccharomyces cerevisiae.     

Synthesis,spectroscopic and structural characterization of the mer isomer of ammonium bis(phenylpyruvic acid thiosemicarbazone)-cobalt(III) hemihydrate

Summary Phenyl pyruvate thiosemicarbazone (H₂PPVATSC) coordinates in its binegative thiolate form to cobalt(III) in the complex isolated from basic medium. An X-ray structure determination of the resulting meridional isomer was found to contain mutually cis sulphur, trans nitrogen, and trans oxygen donor atoms, respectively. The two five-membered rings formed by each ligand are puckered towards each other, resulting in a distortion from regular octahedral geometry about the cobalt atom. The complex was found to exhibit only a metal-based one electron reversible reduction at -0.97 V, while the parent ligand yields a c.v. profile consisting of two irreversible reduction peaks at -0.75 and -1.05V respectively, the latter corresponding to the reduction of the azomethine group.     

Cobalt and manganese nets via their wires: facile transformation in metal-diorganophosphates

The manganese and cobalt complexes [M(dtbp)2]n (M=Mn, Co; dtbp=di-tert-butyl phosphate), which exist as one-dimensional molecular wires, transform to [M(dtbp)2(bpy)2.2H2O]n by the addition of 4,4-bipyridine (bpy) at room temperature; the latter compounds form noninterpenetrating rectangular grid structures.     

Aerosol ionic redistribution: the ionization repression effect revisited

An investigation using matched dual nebulizers to allow introduction of K as the analyte and Cs as the concomitant in the same and in separate aerosol droplets has been used to study the ionization repression effect. The results demonstrate that ionization repression achieves an equilibrium status at the same molar ratio when these entities are introduced in the same or in separate droplets. However, the magnitude of the enhancement observed as the ratio was varied was considerably greater when Cs and K were introduced in the same droplets. Measurement of the K aerosol size distributions demonstrated that nebulization of the analyte and concomitant in the same solution caused a significant reduction in the median aerosol diameter. This aerosol ionic redistribution resulted in an increase in the amount of analyte transported to the flame and a lateral shift of analyte toward the flame's edge. Thus, the enhancement not attributed to ionization repression originated from increased analyte transport moderated in part by a shift in the analyte atom population away from the central portion of the flame and the absorption light path.     

Non-interpenetrating transition metal diorganophosphate 2-dimensional rectangular grids from their 1-dimensional wires: structural transformations under mild conditions

The manganese, cobalt, and cadmium complexes [M(dtbp)2]n (M = Mn (1) and Co 2) and [Cd(dtbp)2(H2O)]n (3) (dtbp = di-tert-butyl phosphate), which exist as one-dimensional molecular wires, transform to non-interpenetrating rectangular grids [M(dtbp)2(bpy)2.2H2O]n (M = Mn (4), Co (5), and Cd (6)) by the addition of 4,4-bipyridine (bpy) at room temperature. Products 4-6 have also been prepared by a room-temperature reaction or by solvothermal synthesis in methanol through a direct reaction between the metal acetate, di-tert-butyl phosphate, and 4,4'-bipyridine (bpy) in a 1:2:2 molar ratio. Single-crystal X-ray structure determination of 4-6 shows that these compounds are composed of octahedral transition metal ions woven into a two-dimensional grid structure with the help of bpy spacer ligands. The axial coordination sites at the metal are occupied by bulky unidentate dtbp ligands, which prevent any interpenetration of the individual grids. The change of reaction conditions from solvothermal to hydrothermal, for the attempted synthesis of a magnesium grid structure, however leads to the isolation of an organic phosphate [(H2bpy)(H2PO4)2] (7) and an inorganic phosphate [Mg(HPO4)(OH2)3] (8). Compound 7 can also be prepared quantitatively from a direct reaction between bpy and H3PO4. The new organic phosphate 7 is a unique example of a phosphate material with alternating layers of [H2bpy]2+ cations and [H2PO4]- anions that are held together by hydrogen bonds. Solid-state thermal decomposition of 4-6 produced the respective metaphosphate materials [M(PO3)2] (M = Mn (9), Co (10), and Cd (11)). All new metal-organic phosphates have been characterized by elemental analysis, thermal analysis (TGA, DTA, DSC), and IR and NMR spectroscopy. The metaphosphate ceramic materials were characterized by IR spectral and powder X-ray diffraction studies.     

Novel Sulfonamide Derivatives as Inhibitors of Histone Deacetylase

Inhibition of the enzyme histone deacetylase (HDAC) is emerging as a novel approach to the treatment of cancer. A series of novel sulfonamide derivatives were synthesized and evaluated for their ability to inhibit human HDAC. Compounds were identified which are potent enzyme inhibitors, with IC₅₀ values in the low nanomolar range against enzyme obtained from HeLa cell extracts, and with antiproliferative effects in cell culture. Extensive characterization of the structure–activity relationships of this series identified key requirements for activity. These include the direction of the sulfonamide bond and substitution patterns on the central phenyl ring. The alkyl spacer between the aromatic head group and the sulfonamide functionality also influenced the HDAC inhibitory activity. One of these compounds, m 11.1 , also designated PXD101, has entered clinical trials for solid tumors and haematological malignancies.     

Experimental Techniques for Finite Shear Strain Measurement within Two Advanced High Strength Steels

Experimental Mechanics - There is a growing need to experimentally characterize local shear deformation in advanced high strength steels (AHSS) for the calibration of stress-state dependent...