Axioms of an Experimental System

In this paper a system of axioms is presented todefine the notion of an experimental system. The primaryfeature of these axioms is that they are based solely onthe mathematical notion of a direct product decomposition of a set. Properties ofexperimental systems are then developed. This includesdefining negation, implication, conjunction, anddisjunction on the set of all binaryexperiments of the system and showing that the resulting structure is aregular orthomodular poset. The theory of observables ofexperimental systems is also developed. Finally, theusual models of experiments from classical as well as quantum physics are shown to satisfythe axioms of an experimental system, and a mechanism tocreate new models of the axioms is given.     

Synthèse de l'oxo-7 7H cyclohepta[b] pyridine et de quelques dérivés

This communication describes the synthesis of 7-one (7H) cyclohepta[b]pyridine and some derivatives (6,8-dimethyl; 8-methyl; 8-ethyl….). These compounds have been obtained by condensation of ketones with 2,3-diformylpyridine.     

Grating Recording for Moiré Testing

Experimental Techniques -     

Dramatic size effects and evidence of structural isomers in the reactions of rhodium clusters, Rhn+/-, with nitrous oxide

The reactions of gas phase rhodium clusters, Rhn+/- (n<30), with nitrous oxide, N2O, have been investigated under single collision conditions by Fourier transform ion cyclotron resonance mass spectrometry. The only significant reaction observed is the sequential generation of oxides. Absolute rate constants for the reactions of all clusters have been determined and, in the case of the cationic clusters especially, they exhibit large fluctuations as a function of cluster size with local minima observed for n=5, 19, 28. Striking similarities are observed with the variation in rate constants for these clusters in reactions with small hydrocarbons (C. Adlhart and E. Uggerud, J. Chem. Phys., 2005, 123, 214709). Corresponding size effects are also observed but are less marked in the reactions of the anionic clusters. The reactions of several clusters exhibit marked deviations from simple pseudo-first-order kinetics suggesting the presence of multiple isomeric forms: Rh11+, Rh12+ and Rh8- exhibit characteristic biexponential decays which are interpreted in terms of the existence of different structural forms of the cluster which have markedly different reactivity. By contrast, Rh6+, Rh7+ and Rh8+ show rates which apparently increase with time, probably due to collisional activation. Thermalisation of the clusters prior to reaction by exposure to pulses of argon results in changes to the kinetics of these anomalous systems which can be explained in terms of collision induced isomerisation.     

Ligand Reprogramming in Dinuclear Helicate Complexes: A Consequence of Allosteric or Electrostatic Effects?

The ditopic ligand 6,6'-bis(4-methylthiazol-2-yl)-3,3'-([18]crown-6)-2,2'-bipyridine (L(1)) contains both a potentially tetradentate pyridyl-thiazole (py-tz) N-donor chain and an additional "external" crown ether binding site which spans the central 2,2'-bipyridine unit. In polar solvents (MeCN, MeNO(2)) this ligand forms complexes with Zn(II), Cd(II), Hg(II) and Cu(I) ions via coordination of the N donors to the metal ion. Reaction with both Hg(II) and Cu(I) ions results in the self-assembly of dinuclear double-stranded helicate complexes. The ligands are partitioned by rotation about the central py--py bond, such that each can coordinate to both metals as a bis-bidentate donor ligand. With Zn(II) ions a single-stranded mononuclear species is formed in which one ligand coordinates the metal ion in a planar tetradentate fashion. Reaction with Cd(II) ions gives rise to an equilibrium between both the dinuclear double-stranded helicate and the mononuclear species. These complexes can further coordinate s-block metal cations via the remote crown ether O-donor domains; a consequence of which are some remarkable changes in the binding modes of the N-donor domains. Reaction of the Hg(II)- or Cd(II)-containing helicate with either Ba(2+) or Sr(2+) ions effectively reprogrammes the ligand to form only the single-stranded heterobinuclear complexes [MM'(L(1))](4+) (M=Hg(II), Cd(II); M'=Ba(2+), Sr(2+)), where the transition and s-block cations reside in the N- and O-donor sites, respectively. In contrast, the same ions have only a minor structural impact on the Zn(II) species, which already exists as a single-stranded mononuclear complex. Similar reactions with the Cd(II) system result in a shift in equilibrium towards the single-stranded species, the extent of which depends on the size and charge of the s-block cation in question. Reaction of the dicopper(I) double-stranded helicate with Ba(2+) shows that the dinuclear structure still remains intact but the pitch length is significantly increased.     

Antitumour bis(cyclopentadienyl) metal complexes: titanocene and molybdocene dichloride and derivatives

This Perspective will focus on recent developments in the field of antitumour metallocenes structurally related to titanocene dichloride. Despite extensive testing of titanocene dichloride which culminated in phase I and II clinical trials, further trials have been abandoned. While DNA has been implicated as the major target related to anticancer activity, identification of the active species and mechanism of action has been poorly understood and hence the design of second generation titanocene derivatives has not been possible. Recent mechanistic studies have provided a plausible mechanism for delivery of Ti to cancer cells via transferrin mediated endocytosis. This mechanism requires the presence of labile Cp-Ti bonds that hydrolyse on a time scale to deliver Ti to transferrin. A large range of titanocene derivatives in which the cyclopentadienyl rings have been substituted by both electron withdrawing and donating groups, including aromatic, alkyl and cyclic amines, have been prepared and tested for activity in the last 5 years. These results have shown that subtle structural effects can have a significant effect on biological activity and that biological activity is highly cell line dependent. However, the biological chemistry and cellular studies required to determine the mechanism of action of these new titanocenes have not been reported. In contrast, the bioorganometallic chemistry and cellular studies of molybdocene dichloride have implicated interaction with cellular thiols as the key reaction related to biological activity. Tailoring of the pseudohalide ligands by tuning the strength of the Mo-S bonds provides the opportunity to enhance cell uptake. Further research is required to establish the origin of antitumour activity.