基于虚拟仪器技术和网络的综合实验控制系统设计

为实现大型物理实验现场复杂多样的仪器控制,分析了物理实验的特点、过程、环境及仪器控制功能需求,利用虚拟仪器技术、计算机网络技术和数据库技术,建立了一套集成硬件和软件的综合控制管理信息系统,实现记录系统中示波器状态远程批量设置及波形数据自动采集、控制探测系统的高压电源并发加压或退压、保障各测试项目间测试仪器之间时间关联、监控UPS电量和远端现场图片或视频状态。给出了系统的关键的设计思路,列举了某型示波器控制的通用控制代码。结果表明,系统达到了一人总控或多人分权控制实验过程中多种多台仪器的目标,方便快捷地实现不同品牌不同类型示波器的相同功能。     

Determination of topotecan in human and mouse plasma and in mouse tissue homogenates by reversed-phase high-performance liquid chromatography

A sensitive and selective reversed-phase high-performance liquid chromatographic (HPLC) assay has been developed and validated for quantification of total topotecan in human and mouse plasma and in mouse tissue samples. Isocratic separation was achieved on a Zorbax SB-C(18) column and topotecan was monitored fluorimetrically. Two ranges of calibrations curves were used to determine lower levels of topotecan more accurately. Acceptable accuracy and precision was achieved for all matrices. Topotecan was stable upon repeated freeze-thawing for three cycles or storage for 24 h at ambient temperatures in spiked plasma samples and tissue homogenates, except in heart homogenates. In an additional validation experiment in which (14)C-labeled topotecan was administered to mice, the levels of unchanged topotecan were about 80-90% of the total radioactivity in tissue homogenates collected 10 min after drug administration and virtually similar as in plasma samples. However, results in tissue homogenates obtained 4 h post-drug administration indicated substantial metabolism of topotecan. This assay is suitable for studying the pharmacokinetics and tissue distribution of topotecan in mice. Our results demonstrate the importance of including all tissues of interest for pharmacokinetic studies in the validation procedure.     

A diagnostic tool for determining the quality of accuracy validation. Assessing the method for determination of nitrate in drinking water

Realistic internal validation of a method implies the performance validation experiments under intermediate precision conditions. The validation results can be organized in an X _Nr×Ns (replicates×runs) data matrix, analysis of which enables assessment of the accuracy of the method. By means of Monte Carlo simulation, uncertainty in the estimates of bias and precision can be assessed. A bivariate plot is presented for assessing whether the uncertainty intervals for the bias (E ± U(E)) and intermediate precision (RSDi ± U(RSDi) are included in prefixed limits (requirements for the method). As a case study, a method for determining the concentration of nitrate in drinking water at the official level set by 98/83/EC Directive is assessed by use of the proposed plot.     

Modelling the dynamics of stochastic local search on <Emphasis Type="Italic">k</Emphasis>-<Emphasis Type="SmallCaps">sat</Emphasis>

A new analytical tool is presented to provide a better understanding of the search space of k-sat. This tool, termed the local value distribution , describes the probability of finding assignments of any value q′ in the neighbourhood of assignments of value q. The local value distribution is then used to define a Markov model to model the dynamics of a corresponding stochastic local search algorithm for k-sat. The model is evaluated by comparing the predicted algorithm dynamics to experimental results. In most cases the fit of the model to the experimental results is very good, but limitations are also recognised.     

药物分析中薄层色谱的方法认证

在药物分析中,针对所要求的性能参数,对一个薄层色谱程序的各个环节必须进行的认证方法和认可标准进行了讨论。建议当提出结果报告时,应附上关于对方法的认证参数和认证方法的说明。     

Development and Validation of QuEChERS Followed by UHPLC-ToF-MS Method for Determination of Multi-Mycotoxins in Pistachio Nuts

Pistachios are one of the types of tree nut fruits with the highest mycotoxin contamination, especially of aflatoxins, worldwide. This study developed a Quick, Easy, Cheap, Effective, Rugged, and Safe (QuEChERS) method that was followed by Ultra-High Performance Liquid Chromatography combined with Time-of-Flight Mass Spectrometry (UHPLC–ToF-MS) for the determination of mycotoxins in pistachios. Different approaches to dispersive solid phase extraction as a clean-up method for high lipid matrices were evaluated. For this, classic sorbents such as C18 (octadecyl-modified silica) and PSA (primary secondary amine), and new classes of sorbents, namely EMR-Lipid (enhanced matrix removal-lipid) and Z-Sep (modified silica gel with zirconium oxide), were used. The QuEChERS method, followed by Z-Sep d-SPE clean-up, provided the best analytical performance for aflatoxins (AFB1, AFB2, AFG1 and AFG2), ochratoxin A (OTA), zearalenone (ZEA), toxin T2 (T2) and toxin HT-2 (HT2) in pistachios. The method was validated in terms of linearity, sensitivity, repeatability, interday precision and recovery; it achieved good results according to criteria imposed by Commission Regulation (EC) no. 401/2006. The method was applied to real samples and the results show that pistachios that are available in Portuguese markets are safe from mycotoxins that are of concern to human health.     

Phase separation and structure in a concentrated colloidal dispersion of uniform plates

The structure and phase behaviour of a colloidal dispersion of plate-like particles are described. The plates are nickel (II) hydroxide and have short-range, repulsive interactions and a low polydispersity. As the concentration of the plates is increased, an equilibrium phase separation between a columnar phase and a less ordered phase is observed. Complementary measurements using small-angle neutron and small-angle X-ray scattering have been used to distinguish the columnar phase from other possible ordered structures. Previously isotropic-nematic phase transitions have been observed [#!ref1!#], however this dispersion forms the more highly ordered columnar phase, due to the aspect ratio and the low polydispersity of the plate-like particles. The concentration at which phase separation occurs, increases as the range of the particle interactions is reduced. This system provides an interesting model for comparison with theory and calculations of structures in liquid crystal and mesophase in which the particle interactions can be altered. Received 24 February 1999     

Assessment of limits of detection and quantitation using calculation of uncertainty in a new method for water determination

 An approach to the assessment of the limit of detection and the limit of quantitation using uncertainty calculation is discussed. The approach is based on the known evaluation of the limits of detection and quantitation as concentrations of the analyte equal to three and ten standard deviations of the blank response, respectively. It is shown that these values can be calculated as the analyte concentrations, for which relative expanded uncertainty achieves 66% and 20% of possible results of the analyte determination, correspondingly. For example, the calculation is performed for the validation of a new method for water determination in the presence of ene-diols or thiols, developed for analysis of chemical products, drugs or other materials which are unsuitable for direct Karl Fischer titration. A good conformity between calculated values and experimental validation data is observed. Received: 27 July 1998 · Accepted: 29 November 1998     

Hybrid numerical methods in static and dynamic fracture mechanics

In this article, the concept of the hybrid numerical methods is clarified. On the basis of this concept, various hybrid numerical methods used in static and dynamic fracture mechanics are classified into five categories: (i) hybrid experimental–numerical methods, (ii) hybrid numerical–experimental methods, (iii) hybrid analytical–numerical methods, (iv) hybrid numerical–analytical methods, and (v) hybrid numerical–numerical methods. Features of each category of hybrid numerical method are presented with pertinent numerical results.     

Quantitative AES and XPS: convergence between theory and experimental databases

Experimental spectral databases have been recorded for AES and XPS using fully calibrated instruments. These instruments have been calibrated so that the spectra have the true shape and peak area intensities may be integrated to give absolute yields for AES and relative yields for XPS. Removal of all the backgrounds requires care but may be completed by using information from both databases. The resultant yields may be compared with theory. The correlations for AES are the more complex and involve the total intensities for all transitions originating in each shell. The correlations are excellent using significant changes to the traditional approach. These involve the use of the Casnati et al. ionisation cross section and the restriction of the number of electrons for use in the inelastic mean free path calculations to electrons of 14 eV or less binding energy in the s, p or d sub-shells. The average ratio of experiment to theory is 1.04 with a standard uncertainty of the mean of 4%. Results for XPS are excellent using Scofield’s ionisation cross section together with the above rules for the inelastic mean free path calculations. Improvements for certain elements are still needed for removing the inelastically scattered Auger and photoelectrons in both databases. To assist analysts in using such databases a simpler measure of Auger electron intensity is developed involving differential spectra broadened with a Gaussian function of 15–20 eV width. The peak-to-peak intensities from these broadened spectra are reasonably closely related to the peak area of the direct spectra except in a few exceptional cases. The unbroadened differential spectra show strong contributions from the spectrometer resolution and changes in the chemical state which are avoided by the spectral broadening. To simplify calculations for the analyst when studying homogeneous materials by AES and XPS, the relative sensitivity factors are re-defined to be for an average matrix instead of the pure element. This leads to a matrix-less equation for calculating compositions from the spectra.