Reactions of 2-arsa- and 2-stiba-1,3-dionato lithium complexes with group 4-7 metal halides

The reactions of a range of 2-arsa- and 2-stiba-1,3-dionato lithium complexes with group 4-7 metals have been investigated. These have given rise to several complexes in which an arsadionate acts as a chelating ligand; [V{η²-O,O-OC(Bu^t)AsC(Bu^t)O}₃], [M{η²-O,O-OC(Bu^t)AsC(Bu^t)O}₂(DME)], M=Cr or Mn; or as an η¹-As-diacylarsenide, [MnBr(CO)₄{As[C(O)Bu^t]₂Li(DME)}]₂. In addition, reactions of lithium arsadionates with TaCl₅ have led to metal mediated arsadionate decomposition reactions and arsadionate oxidative coupling reactions to give the known arsaalkyne tetramer, As₄C₄Bu^t₄, and the new tetraacyldiarsane, [{As[C(O)Mes]₂}₂] Mes=mesityl, respectively. The treatment of several lithium arsadionates with [MoBr₂(CO)₂(PPh₃)₂] has also initiated arsadionate decomposition reactions and the formation of the metal carboxylate complexes, [MoBr(CO)₂{η²-O₂C(R)}(PPh₃)₂] R=Bu^t, Ph, Mes. The X-ray crystal structures of six of the prepared complexes are discussed.     

Heavy metal phosphate nanophases in silica: influence of radiolysis probed via f-electron state properties

We have assessed the feasibility of carrying out time- and wavelength-resolved laser-induced fluorescence measurements of radiation damage in glassy silica. The consequences of alpha decay of Es-253 in LaPO₄ nanophases embedded in silica were probed based on excitation of 5f states of Cm³⁺, Bk³⁺, and Es³⁺ ions. The recorded emission spectra and luminescence decays showed that alpha decay of Es-253 ejected Bk-249 decay daughter ions into the surrounding silica and created radiation damage within the LaPO₄ nanophases. This conclusion is consistent with predictions of an ion transport code commonly used to model ion implantation. Luminescence from the ⁶D_7/2 state of Cm³⁺was used as an internal standard. Ion-ion energy transfer dominated the dynamics of the observed emitting 5f states and strongly influenced the intensity of observed spectra. In appropriate sample materials, laser-induced fluorescence provides a powerful method for fundamental investigation of alpha-induced radiation damage in silica.     

Characterization of plutonium contamination at the former nuclear weapons testing range,at Maralinga in South Australia

Re-suspension studies on soils contaminated with plutonium during nuclear weapons tests were performed by use of a mechanical dust-raising apparatus. Airborne dust was analyzed in terms of mass and²⁴¹Am activities for particle sizes less than 7 m. The AMAD was determined as 4.8 to 6 m, for re-suspended soil. Also, surface soil was characterized in the laboratory by means of sieving and microparticle classification, yielding mass and²⁴¹Am activity distributions with respect to size. Data indicate the granularity of plutonium contamination at both major and minor trial sites. Depth profile analyses for undisturbed, areas demonstrate that most (74% on average) of the americium and plutonium activity is found in the top 10 mm of soil. Plutonium and americium activities were found to be enhanced in the inhalable fraction over their values, in the total soil, and the enhancement factors were similar in re-suspended dust and surface soil. Observed enhancement factors ranged from 3.7 to 32.5.     

Singlet exciton trapping and heterofission in tetracene doped anthracene crystals

In tetracene doped anthracene, the magnetic field modulation of prompt tetracene fluorescence following excitation into the anthracene singlet manifold has been measured as a function of the magnetic field orientation and optical excitation energy. The results show that this modulation with low energy excitation is caused by singlet heterofission into one anthracene triplet exciton and one tetracene triplet. With higher excitation energies this modulation is due to both the singlet heterofission and also singlet homofission into a pair of anthracene triplet excitons. Heterofission occurs mainly from anthracene molecules next to a tetracene and competes with the singlet trapping. From the singlet trapping rate and from the magnetic modulation of tetracene prompt fluorescence the heterofission rate is estimated as ≈10^?11s^?1.     

New prodrugs derived from 6-aminodopamine and 4-aminophenol as candidates for melanocyte-directed enzyme prodrug therapy (MDEPT)

Two novel tyrosinase mediated drug delivery pathways have been investigated for the selective delivery of cytotoxic units to melanocytes from urea and thiourea prodrugs. The synthesis of these prodrugs is reported, as well as oximetry data that illustrate that the targets are substrates for tyrosinase. The stability of each of the prodrugs in (i) phosphate buffer and (ii) bovine serum is discussed, and the urea prodrugs are identified as lead candidates for further studies. Finally, HPLC studies and preliminary cytotoxicity studies in a melanotic and an amelanotic cell line, that illustrate the feasibility of the approach, are presented.     

An altered mechanism of hydrolysis for a metal-complexed phosphate diester

Isotope effects in the nucleophile and in the leaving group were measured to gain information about the mechanism and transition state of the hydrolysis of methyl p-nitrophenyl phosphate complexed to a dinuclear cobalt complex. The complexed diester undergoes hydrolysis about 1011 times faster than the corresponding uncomplexed diester. The kinetic isotope effects indicate that this rate acceleration is accompanied by a change in mechanism. A large inverse 18O isotope effect in the bridging hydroxide nucleophile (0.937 +/- 0.002) suggests that nucleophilic attack occurs before the rate-determining step. Large isotope effects in the nitrophenyl leaving group (18Olg = 1.029 +/- 0.002, 15N = 1.0026 +/- 0.0002) indicate significant fission of the P-O ester bond in the transition state of the rate-determining step. The data indicate that in contrast to uncomplexed diesters, which undergo hydrolysis by a concerted mechanism, the reaction of the complexed diester likely proceeds via an addition-elimination mechanism. The rate-limiting step is expulsion of the p-nitrophenyl leaving group from the intermediate, which proceeds by a late transition state with extensive bond fission to the leaving group. This represents a substantial change in mechanism from the hydrolysis of uncomplexed aryl phosphate diesters.     

Capillary electrophoretic chiral separations using cyclodextrin additives: III. Peak resolution surfaces for ibuprofen and homatropine as a function of the pH and the concentration of β-cyclodextrin

Our recent extended peak resolution equation of capillary electrophoresis has been combined with the multiple equilibria-based electrophoretic mobility model of chiral separations to describe peak resolution as a function of the composition of the background electrolyte (pH and the β-cyclodextrin concentration) and a function of the operating variables (effective portion of the applied potential, dimensionless electroosmotic flow coefficient). Using the previously determined model parameters, the resolution surfaces were calculated for a Type I chiral separation (ibuprofen), and a Type III chiral separation (homatropine). In Type I separations resolution can be obtained only over a narrow pH range in the vicinity of the pK_a value, and above a minimum value, the concentration of β-cyclodextrin plays a lesser role. In Type III separations, the pH- and β-cyclodextrin concentration-dependent resolution surface has two lobes, on which the migration order of the enantiomers is opposite. This can be an advantage in trace component analysis. In both Type I and Type III separations, peak resolution varies strongly with the dimensionless electroosmotic flow coefficient when its value is changed in the − 1 to 1 range. The loci of the pH-dependent and the β-cyclodextrin concentration-dependent resolution maxima do not shift significantly when the dimensionless electroosmotic flow coefficient is changed. This fact provides the analyst with an additional resolution enhancement tool that does not alter the selectivity of the separation. The utility of the model and its theoretical predictions has been demonstrated by comparing measured and calculated R_s values for ibuprofen and homatropine.     

Binding energies of protonated betaine complexes: a probe of zwitterion structure in the gas phase

The dissociation kinetics of proton-bound dimers of betaine with molecules of comparable gas-phase basicity were investigated using blackbody infrared radiative dissociation (BIRD). Threshold dissociation energies were obtained from these data using master equation modeling. For bases that have comparable or higher gas-phase basicity, the binding energy of the protonated base.betaine complex is ~1.4 eV. For molecules that are ~2 kcal/mol or more less basic, the dissociation energy of the complexes is ~1.2 eV. The higher binding energy of the former is attributed to an ion-zwitterion structure which has a much larger ion-dipole interaction. The lower binding energy for molecules that are ~2 kcal/mol or more less basic indicates that an ion-molecule structure is more favored. Semiempirical calculations at both the AM1 and PM3 levels indicate the most stable ion-molecule structure is one in which the base interacts with the charged quaternary ammonium end of betaine. These results indicate that the measurement of binding energies of neutral molecules to biological ions could provide a useful probe for the presence of zwitterions and salt bridges in the gas phase. From the BIRD data, the gas-phase basicity of betaine obtained from the kinetic method is found to be 239.2 +/- 1.0 kcal/mol. This value is in excellent agreement with the value of 239.3 kcal/mol (298 K) from ab initio calculations at the MP2/6-31+g** level. The measured value is slightly higher than those reported previously. This difference is attributed to entropy effects. The lower ion internal energy and longer time frame of BIRD experiments should provide values closer to those at standard temperature.