New approach on the alkylthiol determination in water by in situ derivatization SPME followed by GC-ECD/NPD analysis

Alkylthiols are very reactive and highly volatile compounds, and thus it is difficult to determine these in the water phase. In the present work, an in situ derivatization step prior to solid-phase microextraction (SPME) has been developed for their determination in water samples. The dinitrobenzylation reaction was selected because the high chemical stability of the corresponding thioethers formed provides a significant increase in the distribution coefficient between the SPME fibre and the aqueous phase, and a potential increase in the selectivity and sensitivity. Therefore, different derivatization reaction conditions (i.e. pH, temperature, reaction time and derivatizating reagent concentration) have been studied. Then, the main parameters affecting to the SPME process, that is coating selection, extraction time profile, extraction and desorption temperatures, have been optimized. Finally, a method based on a simple 2,4-dinitrophenylation reaction at pH 8–10, in 60?min at 75°C, coupled to direct SPME using PDMS-DVB fibres at 30°C for 45?min is proposed. The performance of the method provided a good linearity and precision data, and the detection limits were in the low ng?L^?1 level.     

Determination of sterols in biological samples by SPME with on-fiber derivatization and GC/FID

A new procedure for the determination of sterols in serum samples is proposed. The system consists of coating a Solid Phase Microextraction (SPME) microfiber in headspace mode with the derivatizing agent N,O-bis(trimethylsilyl)trifluoracetamide (BSTFA) and then applying this coated fiber to the simultaneous extraction and derivatization of three precursors in the cholesterol biosynthesis pathway (desmosterol, lathosterol and lanosterol) and two phytosterols (sitosterol and sitostanol) in serum samples. Optimization of the analytical procedure via the application of an experimental design, a study of matrix effects, and an analysis of serum pool samples are all described and discussed.     

代谢组学GC-MS分析方法中样品衍生化技术的新进展

代谢组学是通过考察生物体系受刺激或扰动前后(如某个特定的基因变异或环境变化后)代谢产物的动态变化,研究生物体系代谢网络的一种技术,其研究对象主要是内源性小分子物质.这些物质大部分极性强,难挥发,在气相色谱-质谱分析前,需要进行适当的化学衍生处理.近几年来化学衍生技术发展迅速,本文主要从衍生试剂种类、衍生条件和衍生效果(包括衍生效率、重复性和产物稳定性等)出发,综述了已报道的衍生方法的特点,并展望了衍生技术的发展前景.     

In situ derivatization hollow fibre liquid-phase microextraction for the determination of biogenic amines in food samples

Hollow fibre liquid-phase microextraction with in situ derivatization using dansyl chloride has been successfully developed for the high-performance liquid chromatography-ultraviolet (HPLC-UV) determination of the biogenic amines (tryptamine, putrescine, cadaverine, histamine, tyramine, spermidine) in food samples. Parameters affecting the performance of the in situ derivatization process such as type of extraction solvent, temperature, extraction time, stirring speed and salt addition were studied and optimized. Under the optimized conditions (extraction solvent, dihexyl ether; acceptor phase, 0.1 M HCl; extraction time, 30 min; extraction temperature, 26 °C; without addition of salt), enrichment factors varying from 47 to 456 were achieved. Good linearity of the analytes was obtained over a concentration range of 0.1–5 μg mL⁻¹ (with correlation coefficients of 0.9901–0.9974). The limits of detection and quantification based on a signal-to-noise ratio of 3–10, ranged from 0.0075 to 0.030 μg mL⁻¹ and 0.03 to 0.10 μg mL⁻¹, respectively. The relative standard deviations based on the peak areas for six replicate analysis of water spiked with 0.5 μg mL⁻¹ of each biogenic amine were lower than 7.5%. The method was successfully applied to shrimp sauce and tomato ketchup samples, offering an interesting alternative to liquid–liquid extraction and solid phase extraction for the analysis of biogenic amines in food samples.     

Supercritical fluid extraction with in situ chiral derivatization for the enantiospecific determination of ibuprofen in urine samples

In situ chiral derivatization was used to obtain diastereomeric amides of ibuprofen for their subsequent extraction with supercritical carbon dioxide. For this purpose, ibuprofen [racemic 2-(4-isobutylphenyl)propionic acids] was previously extracted on a C-18 SPE device and quantitatively transferred into the supercritical fluid extraction (SFE) vessel for derivatization and extraction with (R)-1-(naphthen-1-yl)ethylamine as chiral derivatizing base, and a mixture of 1-(3-dimethylaminopropyl)-3-ethylcarbodiimide and 1-hydroxybenzotriazole as reagents, in order to obtain and extract the corresponding diastereoisomeric amides, which were subsequently determined by liquid chromatography. The influence of different extraction and derivatization variables (pressure, temperature, extraction time in the static and dynamic extraction modes, and amount of chiral base) on the extraction efficiency was studied. Spiked and native urine samples containing ibuprofen were used to demonstrate the application of this method. The absolute recovery, selectivity, precision and accuracy of the combined solid-phase extraction (SPE)/SFE approach were compared to those provided by conventional liquid–liquid extraction. The results indicated that SFE seems to be an effective choice for in situ derivatization since analysis times and solvent consumption were dramatically reduced.     

Development of a method for the rapid determination of pentachlorophenol in leather using supercritical fluid extraction with in situ derivatization

Pentachlorophenol (PCP) was extracted from leather with supercritical carbon dioxide and in situ acetylated under static SFE conditions in the presence of triethylamine. During the dynamic extraction step, the derivatives were removed from the matrix and collected with either a pure liquid (light petroleum) or a liquid-solid (light petroleum-solid sorbent (C18, alumina, Florisil or Celite)) trap. To prevent restrictor plugging, a suitable restrictor was designed. The clean-up of the extracts was optimized in this study. Different internal standards were tested and it was shown that not all of them were usable. The SFE results were compared with those obtained by Soxhlet extraction with methanol. With SFE instead of conventional Soxhlet extraction, the overall time required for determination of PCP in leather can be reduced from about 2 days to approx. 3 hours.     

In situ aqueous derivatization and determination of non-steroidal anti-inflammatory drugs by salting-out-assisted liquid-liquid extraction and gas chromatography-mass spectrometry

A new analytical method for the determination of trace levels of five non-steroidal anti-inflammatory drugs (NSAIDs: clofibric acid, ibuprofen, naproxen, diclofenac and ketoprofen) in water samples is described. The analytical procedure involves in situ aqueous derivatization with N-(3-dimethylaminopropyl)-N'-ethylcarbodiimide hydrochloride (EDC) and 2,2,2-trifluoroethylamine hydrochloride (TFEA) and salting-out liquid-liquid extraction (SALLE), followed by gas chromatography-programmed temperature vaporizer-mass spectrometry (GC-PTV-MS). The influence of several parameters on the efficiency of the derivatization (stirring time, reaction time, reagent concentration and pH), and the extraction (solvent, volume, salts and stirring time) and injection steps (liner, injection volume, liner temperature, injection time, venting time and venting flow) was investigated. The detection limits of the method in water varied from 0.042 μg/L for ibuprofen to 1.2 μg/L for ketoprofen. The relative standard deviations (RSD) values were found to be relatively low (<10% for all compounds). The methodology developed was applied to the determination of NSAIDs in several environmental matrices including tap, river, sea and influent and effluent waste water samples. The results obtained show the presence of ibuprofen and naproxen in the influent waste water sample.     

In situ derivatization and hollow fiber membrane microextraction for gas chromatographic determination of haloacetic acids in water

An alternative method for gas chromatographic determination of haloacetic acids (HAAs) in water using direct derivatization followed by hollow fiber membrane liquid-phase microextraction (HF-LPME) has been developed. The method has improved the sample preparation step according to the conventional US EPA Method 552.2 by combining the derivatization and the extraction into one step prior to determination by gas chromatography electron captured detector (GC-ECD). The HAAs were derivatized with acidic methanol into their methyl esters and simultaneously extracted with supported liquid hollow fiber membrane in headspace mode. The derivatization was attempted directly in water sample without sample evaporation. The HF-LPME was performed using 1-octanol as the extracting solvent at 55 °C for 60 min with 20% Na₂SO₄. The linear calibration curves were observed for the concentrations ranging from 1 to 300 μg L⁻¹ with the correlation coefficients (R²) being greater than 0.99. The method detection limits of most analytes were below 1 μg L⁻¹ except DCAA and MCAA that were 2 and 18 μg L⁻¹, respectively. The recoveries from spiked concentration ranged from 97 to 109% with %R.S.D. less than 12%. The method was applied for determination of HAAs in drinking water and tap water samples. The method offers an easy one step high sample throughput sample preparation for gas chromatographic determination of haloacetic acids as well as other contaminants in water.     

Determination of pharmaceutical and personal care products in wastewater by capillary electrophoresis with UV detection

Capillary electrophoresis (CE) offers a fast and cost-effective alternative analytical technique to LC-MS/MS for separation and quantitation of many PPCP compounds in wastewater. In this study, we have developed a method that can simultaneously analyze eight different PPCP compounds in untreated wastewater (ibuprofen, triclosan, carbamazepine, caffeine, acetaminophen, sulfamethoxazole, trimethoprim, and lincomycin), using capillary electrophoresis with UV detection (CE-UV). The method detection limit (MDL) ranged from 1.6 to 68.7 ppb through solid phase extraction. The standard limit of quantification (LOQ) ranged from 0.63 to 7.72 ppm. Factors affecting separation and quantification of PPCPs, such as pH, electrophoretic potential, buffer strength, buffer type, and additives, were investigated and optimized. Water samples from two different wastewater treatment plants were collected and analyzed. The results obtained were comparable with those of LC-MS/MS. The technique developed in this study provides a low cost, simple, fast, and relatively sensitive method for determination of various PPCPs in wastewater samples for PPCP screening.     

Response surface methodology for optimization of cyanamide analysis by in situ derivatization and dispersive liquid–liquid microextraction

Cyanamide is widely used for agricultural purposes; therefore, its residues can be found in water. A new method was developed for its quantification using in situ derivatization with 2,6‐dimethyl‐4‐quinolinecarboxylic acid N‐hydroxysuccinimide ester followed by dispersive liquid–liquid microextraction (DLLME) and high‐performance liquid chromatography/fluorescence analysis. Multivariate chemometric techniques were successfully used to obtain the optimum conditions for direct derivatization and DLLME extraction. Derivatization parameters and DLLME extraction conditions were optimized by a two‐step design, 2^k factorial design for screening, and central composite design for optimization. Best derivatization conditions were addition of 600 μL of derivatizing reagent, a temperature of 4 ºC, and pH 8.5, whereas for optimum extraction 800 μL of solvent, 30% NaCl conc. w/v, and pH 3.8 were chosen. The analytical performance of the method for routine analysis was evaluated. Excellent linearity was achieved from 10 to 200 µg L⁻¹ with a correlation factor of 0.9996. Precision ranged from 3.5% to 5.5% for intraday assays and 8.5% to 8.6% for interday assays. The mean recoveries performed on water from different origins (ground, river, sea, tap, and mineral) at three levels of concentration (20, 75, and 200 µg L⁻¹) ranged from 90.2% to 110.2%. Copyright © 2014 John Wiley & Sons, Ltd.     

Evaluation of pharmaceutical activities of G-protein coupled receptor targeted pharmaceuticals in Chinese wastewater effluent

The occurrence of biologically active pharmaceuticals in aquatic environments raised the potential risks to aquatic species. Among these marketed biological active pharmaceuticals, it has been estimated that 40% of them target G-protein-coupled receptors (GPCRs). We have illustrated pharmaceutical activities of GPCR targeted pharmaceuticals in English and Japanese wastewater by the in vitro transforming growth factor-α (TGFα) shedding assay. However, as the most important producer and consumer of pharmaceuticals, the occurrence of GPCR targeted pharmaceuticals in China had remained unclear. In this study, we investigated the pharmaceutical activities of GPCR targeted pharmaceuticals in secondary effluents of Chinese wastewater treatment plants. We discovered antagonistic activities against angiotensin (AT1) receptor at up to 7.2 × 102 ng-valsartan-equivalent quantity/L in Chinese wastewater for the first time as well as agonistic activities against dopamine (D2) receptor. Furthermore, in parallel with the assay, we determined concentrations of GPCR targeted pharmaceuticals in target wastewater by liquid chromatography coupled with tandem mass spectrometry (LC–MS/MS). Through the comparison of predicted antagonistic activities calculated by concentrations and potency values from the assay, we found that the measured antagonistic activities against AT1 receptor from the assay were higher than the predicted AT1 activities from valsartan, irbesartan, and losartan, indicating the potential existence of other unknown AT1 antagonists in wastewater.     

Microextraction by packed sorbent for the analysis of pharmaceutical residues in environmental water samples by in situ derivatization-programmed temperature vaporizer-gas chromatography-mass spectrometry

The present work describes the development and validation of a method for the determination of five non-steroidal anti-inflammatory drugs (NSAIDs: clofibric acid, ibuprofen, naproxen, diclofenac and ketoprofen) in water samples. The fully automated method includes in situ aqueous derivatization followed by analyte enrichment by microextraction by packed sorbent (MEPS) coupled directly to programmed temperature vaporizer-gas chromatography-mass spectrometry (PTV-GC-MS). The MEPS variables, such as sample volume, elution solvent, elution volume, fill and injection speed and washing steps were optimized. It was possible to use the MEPS polymer (silica-C18) 250 times. Ibuprofen-d3 was used as internal standard. The reproducibility of the method, calculated as the relative standard deviation (RSD), was below 10% for all compounds. Detection limits in ultrapure water were between 3.0 and 110 ngL(-1) for ibuprofen and ketoprofen, respectively. External calibration was used in the determination of NSAIDs in several types of water samples, including tap, river, sea and influent and effluent wastewater. The results obtained revealed the presence of ibuprofen and naproxen in the influent wastewater sample and of naproxen in the effluent wastewater sample.     

Development of a simultaneous liquid-liquid extraction and chiral derivatization method for stereospecific GC-MS analysis of amphetamine-type stimulants in human urine using fractional factorial design

A stereospecific gas chromatography-mass spectrometry analysis method for amphetamine-type stimulants in human urine was recently developed. For maximum efficiency, liquid-liquid extraction and chiral derivatization of the analytes using (R)-(-)-alpha-methoxy-alpha-(trifluoromethyl)phenylacetyl chloride were performed simultaneously. The effects of (1) use of saturated sodium chloride in 2.0 m sodium hydroxide, (2) extraction solvent volume, (3) percentage of triethylamine, (4) derivatization reagent volume, (5) sample mixing time, (6) incubation temperature and (7) incubation time on method sensitivity and variability were assessed using a two-level, eight-run Plackett-Burman design followed by a fold-over design. The use of saturated sodium chloride solution and the derivatization reagent volume were significant factors (ANOVA, p < 0.01). The saturated sodium chloride solution decreased sensitivity whereas an increased volume of derivatization reagent increased sensitivity. Calibration curves for all analytes were linear between 5 and 500 microg/L, with correlation coefficients of >0.99. Detection limits were 相似文献   

Using HPLC for the determination of platinum drugs in biological matrixes after derivatization with diethyldithiocarbamate

Challenges and pitfalls in the application of diethyldithiocarbamate derivatization for LC analysis of cisplatin and oxaliplatin, as well as the suitability of this method for different biological matrices with implications for use in routine practice have been identified. The LC of platinum drugs presents a significant challenge. They are polar compounds with poor retention on reverse phase packings. Cisplatin also exhibits poor absorption in UV and ionization in mass spectrometry. Therefore, we developed and optimized a derivatization approach for the LC analysis of total platinum in plasma, plasma ultrafiltrate, peritoneal fluid, and urine. Derivatization in urine proved to be difficult due to the complexity of the matrix, and extended testing was required. Our results highlight the important issues affecting the efficiency, reliability, and suitability of platinum drug derivatization. Although precolumn derivatization is less selective than its postcolumn counterpart, the application of precolumn derivatization is a simple, rapid, and universal approach for the determination of platinum drugs by HPLC. One of its major advantages is that it allows a more affordable analysis using UV detection without the need for additional high-end instrumentation such as a MS detector.     

Headspace sampling with in situ carbodiimide-mediated derivatization for the determination of ibuprofen in water samples

A method using headspace generation and in situ derivatization with water soluble EDC (1-[3-(dimethylamino)propyl]-3-ethylcarbodiimide) and TFEA (2,2,2-trifluoroethylamine) has been optimized for the determination of ibuprofen (2-(p-isobutylphenyl)propionic acid), one of the most common non-steroid anti-inflammatory drug (NSAIDs) residues in surface and wastewater samples. Derivatization was carried out in the vial of the headspace sampler (HS) in only 15 min, after which instrumental measurements were made with gas chromatography-mass spectrometry (GC-MS). As the injection system, a programmed temperature vaporizer (PTV) in the solvent-vent injection mode is proposed in order to increase the sensitivity of the measurements. The effects of the variables affecting HS generation, the derivatization reaction, and the instrumental PTV conditions were studied. A limit of quantification as low as 32 ng/L was achieved, and repeatability values were below 10%. Accuracy of the method was evaluated using spiked ultrapure water at three concentration levels, obtaining apparent recoveries between 96% and 104%. The proposed method was applied to the quantification of ibuprofen in sea water and urban wastewater samples.     

Stir bar sorptive extraction with in situ derivatization and thermal desorption-gas chromatography-mass spectrometry for determination of chlorophenols in water and body fluid samples

A new method, stir bar sorptive extraction (SBSE) with in situ derivatization and thermal desorption (TD)-gas chromatography-mass spectrometry (GC-MS), which is used for the determination of trace amounts of chlorophenols, such as 2,4-dichlorophenol (2,4-DCP), 2,4,6-trichlorophenol (2,4,6-TrCP), 2,3,4,6-tetrachlorophenol (2,3,4,6-TeCP) and pentachlorophenol (PCP), in tap water, river water and human urine samples, is described. The derivatization conditions with acetic acid anhydride and the SBSE conditions such as extraction time are investigated. Then, the stir bar is subjected to TD followed by GC-MS. The detection limits of the chlorophenols in tap water, river water and human urine samples are 1-2, 1-2, and 10-20 pg ml⁻¹ (ppt), respectively. The calibration curves for the chlorophenols are linear and have correlation coefficients higher than 0.99. The average recoveries of the chlorophenols in all the samples are higher than 95% (R.S.D. < 10%) with correction using added surrogate standards, 2,4-dichlorophenol-d₅, 2,4,6-trichlorophenol-¹³C₆, 2,3,4,6-tetrachlorophenol-¹³C₆ and pentachlorophenol-¹³C₆. This simple, accurate, sensitive and selective analytical method may be applicable to the determination of trace amounts of chlorophenols in liquid samples.     

用SPME/GC-MS方法检验涉火案件中痕量汽油残留物成分

在纵火、爆炸、凶杀等刑事案件中,经常会遇到痕量汽油残留组分的检验与认定。汽油主要由C12以前的烷烃、烯烃、环烷烃和芳香烃化合物组成。由于涉火案件现场中燃烧介质及其中所含汽油的燃烧时间和燃烧程度都不尽相同,那么残留在介质中的汽油组分多少及轻重组分相对含量会产生较     

Stir bar sorptive extraction with in situ derivatization and thermal desorption-gas chromatography-mass spectrometry for trace analysis of methylmercury and mercury(II) in water sample

A method for the trace analysis of methylmercury (MeHg) and Hg(II) in water sample was developed, which involved stir bar sorptive extraction (SBSE) with in situ alkylation with sodium tetraethylborate and thermal desorption (TD)-gas chromatography-mass spectrometry (GC-MS). The limits of quantification of MeHg and Hg(II) are 20 and 10 ng L⁻¹ (Hg), respectively. The method shows good linearity and the correlation coefficients are higher than 0.999. The average recoveries of MeHg and Hg(II) in tap or river water sample are 102.1-104.3% (R.S.D.: 7.0-8.9%) and 105.3-106.2% (R.S.D.: 7.4-8.5%), respectively. This simple, accurate, sensitive, and selective analytical method may be used in the determination of trace amounts of MeHg and Hg(II) in tap and river water samples.     

An affordable method for the simultaneous determination of the most studied pharmaceutical compounds as wastewater and surface water pollutants

There is still an increasing need of knowledge about the presence of pharmaceuticals in the environment in many countries. To contribute to the improvement of this knowledge it should be useful to get not only more reliable methods, but also analytical methods that do not require expensive equipment and, consequently, could be used even in the less developed areas. In the present work, a novel analytical method for the simultaneous determination of several priority pharmaceuticals, as aquatic media pollutants, in wastewater and surface water is reported. The method involves sample treatment by SPE, followed by LC with diode array and fluorescence detection. Parameters that affect the efficiency of the SPE step such as elution solvents, sample pH and cartridge sorbents were evaluated and optimized. The best results were obtained using acetone as elution solvent, acidifying samples to pH 2 and employing Oasis HLB as SPE sorbent. Recoveries of the pharmaceuticals from influent and effluent wastewater and surface water samples were in the range from 61.4 to 123%. LODs were in the range of 0.001–0.323 μg/L and LOQs were between 0.020 and 1.078 μg/L.     

原位衍生化技术在液相色谱和液相色谱-质谱联用分析中的应用

衍生化是将待分析物转化为更适合的物质形式以便于分析的有效手段。原位衍生化技术作为一种常用的柱前衍生化方法,可以在样品基质中同时完成分析物的萃取和衍生化,具有高效、灵敏和选择性好的优点。原位衍生化结合其他前处理技术广泛用于胺类、醛酮类、醇类、酚类、羧酸和巯基化合物的分析中,在生物、药物、食品、环境、化妆品分析等领域有广泛的应用。该文概述了原位衍生化的反应类型和代表性衍生试剂,综述了原位衍生化技术在液相色谱和液相色谱-质谱联用分析中的应用,并展望其发展趋势。