A simple proof of the perturbative uniqueness of the Kerr solution

We present a mathematically simple and coordinate-free proof, based on the GHP spin-coefficient formalism, that a small stationary perturbation of a Kerr solution results in a new Kerr solution. Thus, under physically reasonable assumptions, we give a new and simple proof that a stationary black hole is given by a Kerr solution.     

A new approach to reduction of the Neumann problem in acoustic scattering to a non-hypersingular integral equation

The Neumann problem for the propagative Helmholtz equation inthe exterior of several bodies (obstacles) is studied in twoand three dimensions by a special modification of the boundaryintegral equation method. This modification can be called the'method of interior boundaries', because additional boundariesare introduced inside scattering bodies. The solution of theproblem is obtained in the form of a single layer potentialon the whole boundary. The density in the potential satisfiesthe uniquely solvable Fredholm equation of the second kind andcan be computed by standard codes. In fact our method holdsfor any positive wave numbers.     

Automated solid-phase extraction for determination of amodiaquine, chloroquine and metabolites in capillary blood on sampling paper by liquid chromatography

Summary A bioanalytical method using solid-phase extraction and high-performance liquid chromatography (LC) has been developed and validated for the determination of amodiaquine, chloroquine and their metabolites in 100 μL blood applied to sampling paper. The intra-assay precision for all analytes was <5% at 2000 nM, <7% at 750 nM and <10% at 100 nM. The interassay precision for all analytes was <4% at 2000 nM, <7% at 750 nM and <12% at 100 nM. The lower limit of quantitation was 100 nM for all analytes. The limit of detection was 30 nM in 100 μL venous blood applied to sampling paper.     

Detection and determination of antimalarial drugs and their metabolites in body fluids

This review of methods for determining antimalarial drugs in biological fluids has focused on the various analytical techniques for the assay of chloroquine, quinine, amodiaquine, mefloquine, proguanil, pyrimethamine, sulphadoxine, primaquine and some of their metabolites. The methods for determining antimalarials and their metabolites in biological samples have changed rapidly during the last eight to ten years with the increased use of chromatographic techniques. Chloroquine is still the most used antimalarial drug, and various methods of different complexity exist for the determination of chloroquine and its metabolites in biological fluids. The pharmacokinetics of chloroquine and other antimalarials have been updated using these new methods. The various analytical techniques have been discussed, from simple colorimetric methods of intermediate selectivity and sensitivity to highly sophisticated, selective and sensitive chromatographic methods applied in a modern analytical laboratory. Knowledge concerning the method for a particular study is determined by the type of application and the facilities, equipment and personnel available. Often is it useful to apply various methods when conducting a clinical study in malaria-endemic areas. Field-adapted methods for the analysis of urine samples can be applied at the study site for screening, and corresponding blood samples can be preserved for subsequent analysis in the laboratory. Selecting samples for laboratory analysis is based on clinical, parasitological and field-assay data. The wide array of methods available for chloroquine permit carefully tailored approaches to acquire the necessary analytical information in clinical field studies concerning the use of this drug. The development of additional field-adapted and field-interfaced methods for other commonly used antimalarials will provide similar flexibility in field studies of these drugs.     

Fast neutron radiative capture in silicon

Using the²⁸Si(n, γ)²⁹Si reaction, transitions to the ground state and first excited state in²⁹Si have been studied in the neutron energy range 3–14 MeV with improved neutron energy resolution (of about 100 keV). The 90° cross sections show considerable structure in the entire neutron energy range. Comparison with theoretical calculations shows that compound-nucleus and direct-semidirect processes account for the non-resonant part (smoothly varying part) of the cross section. A microscopic model is, however, required to describe the resonance structure. Continuum shell-model calculations have proven to be a very promising means towards a better understanding of the capture process in, and below, the giant resonance region in light nuclei. The angular distributions of gamma rays in the neutron energy range 8–14 MeV indicate that the capture reaction is mainly of direct character and that the effect of interference between the electric dipole and isoscalar quadrupole resonance is weak.     

Fast isolation of hydrophobic organic environmental contaminants from exposed semipermeable membrane devices (SPMDs) prior to GC analysis

Semipermeable membrane devices (SPMD) represent a passive sampling technology that is becoming widely used for monitoring of surface waters pollution. While "classic" procedures employ dialysis to recover target compounds from exposed SPMDs, in the present study analytes were isolated from cut membrane together with sequestering medium (triolein) using hexane as an extraction solvent. This approach allowed us to reduce the time needed for accomplishment of isolation step from 48 h to only 1 h. Automated gel permeation chromatography (GPC) clean-up is employed in the following step to separate triolein from analytes fraction. Musk compounds (MCs), polychlorinated biphenyls (PCBs), brominated flame retardants (BFRs) and several other persistent organochlorine compounds (OCs) were determined in the respective fraction by GC method employing selective detectors (MSD, ECD). As shown in a series of analyses of SPMDs deployed in various aquatic ecosystems, high recoveries and good repeatability of results together with a possibility to obtain the information on the pollution of sampling site at the day of sample arrival to laboratory make this newly implemented procedure an interesting alternative to time consuming dialysis.     

Magnetic percolation in diluted magnetic semiconductors

We demonstrate that the magnetic properties of diluted magnetic semiconductors are dominated by short ranged interatomic exchange interactions that have a strong directional dependence. By combining first principles calculations of interatomic exchange interactions with a classical Heisenberg model and Monte Carlo simulations, we reproduce the observed critical temperatures of a broad range of diluted magnetic semiconductors. We also show that agreement between theory and experiment is obtained only when the magnetic atoms are randomly positioned. This suggests that the ordering of diluted magnetic semiconductors is heavily influenced by magnetic percolation, and that the measured critical temperatures should be very sensitive to details in the sample preparation, in agreement with observations.