空气敏感固体化合物红外光谱测试方法

在红外光谱测试中对某些能升华而又对空气敏感的金属有机化合物可以经过真空处理得到合适的测试样品。但这种方法不适用于不能升华的样品。一般固体样品适用的红外常规压片和糊状制样方法,因其操作过程较长,故在空气敏感的样品制样中必需有保护环境。在上述二种方法中,以糊状法制样更适合于空气敏感样品。这时,油层包复在样品粒子表面,起着隔离空气的作用,使样品在光谱测量过程的短时间中免于(或不致很快)破坏。但油糊(石蜡油或氟油)制     

钾盐矿床中含石膏盐分析方法的研究

由于现行标准《岩石矿物分析规程》(DZG93-08)对含石膏钾盐样品分析方法的叙述较为粗略,同时没有国家一级有证标准物质进行质量监控,因此在测定含石膏钾盐样品时较为困难。本文讨论了溶矿温度、称样量、以及放置时间对含石膏钾盐样品溶解的影响。得出在称样量为0.5000g,水温80℃,放置时间为24小时,用电感耦合等离子体发射光谱法测定,以样品中各组分百分数加和、溶液中元素阴阳离子平衡以及加标回收实验进行数据质量监控。测试数据符合《地质矿产实验室测试质量管理规范》对钾盐样品分析质量的要求。     

X射线光电子能谱测定固体粉末样品的制备方法比较

样品制备方法对X射线光电子能谱测试结果具有较大影响,以导电样品锂电材料和不导电样品奶粉为测试对象,探讨了不同制样方法对两者测试效果的影响.试验结果表明,导电样品锂电材料使用导电胶铜片制样效果较好,而不导电样品奶粉使用导电胶压片或3M胶带压片效果较好.     

锥形色谱分离系统及其分离纯化的方法

本发明公开了一种锥形色谱分离系统及其分离纯化方法,其中分离纯化的方法包括:将加压装置与加样装置相连,利用加压装置进行压力调节,以便压实填料;将待分离样品通过加样装置加入到分离装置中,同时利用加压装置,使待分离样品迅速、均匀的通过出样孔喷出,形成雾化样液,并快速进入填料床面;待分离样品吸附完成后,将洗脱液供给至储液装置中进行样品洗脱处理。由此,可以根据实验需要适时选择加样装置和加压装置,实现均匀、快速的加样,并对储液装置进行压力调节,操作简便,保障分离纯化的实验效果以及实验操作的安全性。     

微波消解-电感耦合等离子体质谱(ICP-MS)法测定土壤七种金属元素

实验室比对盲样测定是检验实验室能力验证、实验室资质认定、机构考核的主要手段。为研究并解决测试实验室比对土壤盲样中铍、钒、镍、铜、锌、镉、铅的含量,采用微波消解电感耦合等离子体质谱(ICP-MS)法对土壤盲样进行研究,探讨了不同消解酸体系,检出限和定量限、测试模式和干扰消除、精密度和加标回收率、质控样品进行研究。结果表明：用6 mL HNO3,2 mL HCl和1 mL HF为混合酸体系,各待测元素标准曲线相关系数大于0.9995,检出限在0.001~2.985 mg.L-1^,定量限在0.003~9.94 mg.L-1^,采用氦气碰撞模式测试钒、镍、铜、锌、镉和铅,可以有效的降低多原子离子的干扰;采用no gas模式测试铍,可以有效的提高铍的测试灵敏度。方法精密度为0.2%~6.2%(n=6),加标回收率为92.3%~110.6%,采用土壤标准样品(GSS-4)进行全过程质控研究分析,各元素结果均在标准值参考范围内。用ICP-OES法测试土壤盲样中七种待测金属元素含量与用铑为内标的ICP-MS进行比对,测量分析结果基本一致。     

液液萃取-GC-MS法测定水中硝基苯质量控制指标研究

采用液液萃取–气相色谱–质谱法测定水中硝基苯,通过统计全国多家实验室的测定数据,对平行样测定结果相对偏差、空白加标回收率、样品加标回收率、空白加标回收率相对偏差及样品加标回收率相对偏差5个质控指标进行分析,得出质控指标评价标准。在概率P,γ均为0.90时,平行样测定结果允许最大相对偏差应控制在11.0%;当空白加标浓度为0.2～30μg/L时,回收率控制范围为59%～113%;当样品未检出、加标浓度在0.25～50μg/L时,样品加标回收率控制范围为56%～110%;空白加标、样品加标回收率最大相对偏差应分别控制在10.0%和11.1%。在概率P和γ均为0.95时,平行样测定结果允许最大相对偏差应控制在13.5%;当空白加标浓度为0.2～30μg/L时,回收率的控制范围为50%～122%;当样品未检出、加标浓度在0.25～50μg/L时,样品加标回收率控制范围为49%～117%;空白加标、样品加标回收率最大相对偏差应分别控制在12.6%和14.6%。     

红外吸收法测定碳化铪粉末中的氧含量

应用氧氮分析仪建立碳化铪粉末中氧的测定方法。针对碳化铪熔点极高的特性,对加热功率、称样量和空白值等测定条件进行探讨,选择适合的助熔剂和高温石墨坩埚,确定了最佳测试条件。将该方法用于实际样品测定,测定结果的相对标准偏差小于2.0%(n=9),样品的加标回收率为98.1%～102.6%。     

红外显微技术在天然药物分析中的应用

在天然药物的成分研究中,某些化合物的含量极少,常规红外测试的需样量一般为2mg,若运用红外显微技术,仅需10——100μg样品即可测定,同样能取得较为满意的结果。一、基本原理微量样品特别是固体样品的红外光谱测定,多借助于红外光谱仪的聚焦器完成,若运用     

烟叶样品在进行近红外分析测试前的样品处理方法

本发明涉及烟叶样品在进行近红外分析测试前的样品处理方法，属烟草样品的近红外光谱分析测试技术领域。本发明的烟叶样品在进行近红外分析测试前的样品处理方法包括干燥粉碎及压样三步骤，其中：a．粉碎步骤为：将干燥的样品取出并静止10S后放入家用食物搅拌器中进行粉碎处理，粉碎时间为20-30S，粉碎粒度达375μm以下；b．压样步骤为：将质量为300g的重锤自然平稳置入装有粉碎后样品的样品杯中，取出重锤，随后将样品杯放入仪器样品池内进行测量10min就能完成一个烟叶样品的测试工作。本发明具有操作简单、节省时间、成本低、效率高等优点。     

提高气体同位素质谱计线性的研究

连续流装置与气体同位素比值质谱计联用,已应用于众多领域,在自动进样器配合下,能批量完成样品前处理和数据采集工作.因实验条件一致,连续流的数据重现性不亚于双路进样(计制样误差);但因样品信号随含量变化,不像双路进样系统那样,能始终保持样品气与参考气在相同条件下测试,所以,连续流的同位素比值或δ[1]值时,更易受分馏效应[2]影响.即同一气体在不同进样量时,测出的同位素比值有较明显差别.为尽可能缩小这种差别,必须在相互制约的质谱参数中寻找最佳配合.     

On-line multidimensional supercritical fluid chromatography/capillary gas chromatography

A new analytical technique combining on-line supercritical fluid chromatography with capillary gas chromatography has been developed. The supercritical fluid sample effluent is decompressed through a restrictor directly into a conventional capillary gas chromatographic injection port. This technique allows for not only direct (100%) sample transfer from the supercritical fluid chromatograph to the gas chromatograph but also for selective or multi-step heartcutting of various sample peaks as they elute from the supercritical fluid chromatograph. Heartcut times are determined by monitoring the responses from the flame ionization or ultraviolet absorbance detectors on the supercritical fluid chromatograph. This report describes the operational setup and provides the results of heartcut reproducibility experiments using normal hydrocarbon and aromatic test mixtures. Results from studies where operational parameters were varied, such as GC injector temperature, will also be provided. The potential usefulness of this new technique for selective heartcutting will also be demonstrated using complex hydrocarbon streams.     

Experimental study of isopycnic focusing generated by coupled electric and gravitational field forces: Use in thin layer focusing and focusing field-flow fractionation

Various operational parameters affecting the formation of the density gradient generated by the electric field action on a binary pseudo-continuous carrier liquid composed of charged colloidal silica particles suspended in water and the isopycnic focusing of sample particles were investigated under conditions of static thin layer focusing and dynamic focusing field-flow fractionation. The properties and the behavior of the density gradient forming carrier liquid were studied. The experimental results are compared with theoretical predictions and discussed with respect to potential applications of the proposed concept not only for separation purposes but also for studies of interparticle interactions.     

The economics of residue analysis

Since the onset of residue analysis some 40 years ago, much attention has been paid to several analytical aspects [e.g., the fight to achieve lower limits of detection (LODs), the gain in specificity, and quality assurance]. In recent years, “omic approaches” have also been introduced to accomplish these purposes. However, when reviewing the literature, one “omic” of residue analysis is not represented: the economic.Residue analysis covers a broad working area, including banned (group A) substances and registered veterinary drugs (group B). Some 40 years ago, only thin-layer chromatography and gas chromatography with electron-capture detection were used for A substances, in combination with laborious sample clean-up and thus small sample throughput. The nominal or money price of such an analysis remained relatively stable from 1970 to 2010. However, the operational costs of analysis increased considerably over the years, in particular, personnel and equipment costs. But, higher operational costs were countered by much greater sample throughput, although this phenomenon remains limited.For B substances, the strategy of screening with microbiological inhibition tests at a very low price competes with sophisticated ultra-high-performance liquid chromatography with (high-resolution) mass spectrometry systems, where the number of analytes/run can theoretically reach 122,500.The question that we address in this contribution from an economics point of view is: “How do laboratories keep the balance between price of analysis, specificity, LOD, number of analytes, quantification and quality assurance?”     

Offline LC-GC x GC in combination with rapid-scanning quadrupole mass spectrometry

The present research is focused on the offline combination of normal-phase LC to double-oven GC x GC-quadrupole MS. Initially, a diesel sample was subjected to automated LC x GC in order to define the elution windows of four fractions, viz., saturated hydrocarbons, monocyclic aromatics, dicyclic aromatics, tri- + tetracyclic aromatics; each fraction was collected exploiting the LC system in a further analysis and subjected to large-volume-injection-GC x GC analysis using an apolar-polar column combination. The GC x GC operational conditions were tuned in relation to the specific separation requirements of each heart-cut. The main benefits of what can be defined as offline LC-GC x GC were: (i) the high first-dimension LC selectivity; (ii) the injection of high sample amounts in the GC x GC system, enabling the detection and quantification of a series of low-amount diesel constituents; (iii) improved GC x GC operational conditions for each heart-cut with respect to direct GC x GC.     

Advanced sedex ( nsitive etector of othermic processes)

The instrument described is suitable for the investigation of the thermal behaviour of substances and reaction mixtures under production conformable conditions; this is made possible by the sophisticated design of the sample chamber: easy stirring of the samples, measuring under any gas atmosphere and while bubbling gas through the sample, choice of the sample container and visual observation during the measurement. The control device allows the choice of one of three operational modes: constant temperature, linear increase in temperature, and adiabatic control; this permits the application of the SEDEX apparatus for a variety of methods including dynamic scanning, isoperibolic measurements, and (quasi) adiabatic studies.     

Advanced sedex (sensitive detector of exothermic processes)

The instrument described is suitable for the investigation of the thermal behaviour of substances and reaction mixtures under production conformable conditions; this is made possible by the sophisticated design of the sample chamber: easy stirring of the samples, measuring under any gas atmosphere and while bubbling gas through the sample, choice of the sample container and visual observation during the measurement. The control device allows the choice of one of three operational modes: constant temperature, linear increase in temperature, and adiabatic control; this permits the application of the SEDEX apparatus for a variety of methods including dynamic scanning, isoperibolic measurements, and (quasi) adiabatic studies.     

Contemporary sample stacking in CE: a sophisticated tool based on simple principles

Sample stacking is a general term for methods in CE which are used for on-line concentration of diluted analytes. During the stacking process, analytes present at low concentrations in a long injected sample zone are concentrated into a short zone (stack). The stacked analytes are then separated and individual zones are detected. Thus stacking provides better separation efficiency and detection sensitivity. Many papers have been published on stacking till now, various procedures have been described, and, many names have been proposed for stacking procedures utilizing the same principles. This contribution brings an easy and unified view on stacking, describes the basic principles utilized, makes a list of recognized operational principles and brings an overview of principal current procedures. Further, it surveys selected recent practical applications ordered according to their operational principles and includes the terms, nicknames, and acronyms used for these actual stacking procedures. This contribution may help both newcomers and experts in the field of CE to orient themselves in the already quite complex topic of sample stacking.     

A fully automatic apparatus for stripping voltammetry Application to the determination of triphenyltin compounds

An apparatus for automatic stripping voltammetry is described. The polarograph unit (sweep generator, potentiostat, and current read-out) is constructed from operational amplifier modules and the various operations of sample injection, pre-electrolysis, stripping, etc are controlled by a cam cycle-timer. Application to the determination of submicrogram concentrations of triphenyltin acetate and hydroxide is described.     

Selective flow injection analysis of ultra-trace amounts of Cr(VI), preconcentration of it by solvent extraction, and determination by electrothermal atomic absorption spectrometry (ETAAS)

A rapid, robust, sensitive and selective time-based flow injection (FI) on-line solvent extraction system interfaced with electrothermal atomic absorption spectrometry (ETAAS) is described for analyzing ultra-trace amounts of Cr(VI). The sample is initially mixed on-line with isobutyl methyl ketone (IBMK). The Cr(VI) is complexed by reaction with ammonium pyrrolidine dithiocarbamate (APDC), and the non-charged Cr(VI)–PDC chelate formed is extracted into IBMK in a knotted reactor made from PTFE tubing. The organic extractant is separated from the aqueous phase by a gravity phase separator with a small conical cavity and delivered into a collector tube, from which 55 μl organic concentrate is subsequently introduced via an air flow into the graphite tube of the ETAAS instrument. The operations of the FI-system and the ETAAS detector are synchronously coupled. A significant advantage of the approach is that matrix constituents, such as high salt contents, effectively are eliminated. The extraction procedure was optimized by a simplex approach. A central composite design was subsequently employed to verify the estimated operational optimum. An 18-fold enhancement in sensitivity of Cr(VI) was achieved after preconcentration for 99 s at a sample flow rate of 5.5 ml min⁻¹, as compared to direct introduction of 55 μl of sample, yielding a detection limit (3σ) of 3.3 ng l⁻¹. The sampling frequency was 24.2 samples h⁻¹. The proposed method was successfully evaluated by analyzing a NIST Cr(VI)-reference material, synthetic seawater and waste waters, and waste water samples from an incineration plant and a desulphurization plant, respectively.     

Application of a temperature-controllable microreactor to simple and rapid protein identification using MALDI-TOF MS

We have carried out a simultaneous thermal denaturation and trypsin digestion of proteins using a temperature-controllable microreactor. This is a simple and rapid sample preparation technique for use before matrix-assisted laser desorption ionization time-of-flight mass spectrometry. In contrast to a conventional sample preparation method, which involves several chemical treatments, our sample preparation was performed using only trypsin digestion with the thermal denaturation of the target protein. Optimization of the reactor operational parameters for trypsin digestion using a temperature-controllable microreactor was carried out. The entire trypsin digestion procedure took about 11 min, and consisted of 1 min for the thermal denaturation of the sample protein (3 microl, 0.2 microM) at 85 degrees C, and 10 min for digestion of the protein at 37 degrees C. The resulting sequence coverage ranged from 24% to 57%, which was sufficient for practical protein identification.