离子迁移谱法快速筛查保健食品中非法添加降糖类药品

采用电喷雾离子迁移谱法(IMS),建立了保健食品中12种降糖类化学药物盐酸二甲双胍、盐酸苯乙双胍、甲苯磺丁脲、格列本脲、格列美脲、格列喹酮、格列吡嗪、格列齐特、盐酸罗格列酮、盐酸吡格列酮、瑞格列奈、那格列萘的快速筛查方法。考察了离子源电压、迁移管电压和迁移管温度对降糖类化学药品迁移时间和信号强度的影响,最终条件设定为:离子源电压2.5kV,迁移管电压7.0kV,进样口温度180℃,迁移管温度180℃,谱图叠加次数10,分析时间30s,采集谱图时长25ms。为保证迁移时间稳定,采用色氨酸作为校准物质进行迁移时间校正,同时进行长期稳定性考察。结果表明12种降糖药物的迁移时间在7.977~17.153ms之间,检出限在0.02~8μg·mL-1之间,在4个月内迁移时间的相对标准偏差(RSD)小于5%。16个保健食品样品用该方法进行检测,其中有6个样品检出二甲双胍,检出苯乙双胍的样品有7个,同时检出苯乙双胍和二甲双胍的样品有1个。该方法可用于建立保健食品中非法添加药品的IMS迁移时间数据库,并用于其快速筛查。     

超高效液相色谱-串联质谱法快速检测降糖类保健食品中的10种非法添加物

建立了超高效液相色谱-串联质谱快速检测降糖类保健食品中10种非法化学降糖药物(盐酸苯乙双胍、那格列奈、格列齐特、盐酸吡格列酮、盐酸罗格列酮、格列吡嗪、瑞格列奈、格列美脲、格列苯脲、格列喹酮)的方法。样品经甲醇超声提取,用Thermo Hypersil Gold色谱柱分离,采用三重四极杆质谱进行定性及定量分析。10种药物在1~1000μg/L范围内线性关系良好,检出限为0.1~1.5μg/L,在低、中、高3个添加水平范围内的平均回收率为82.5%~111.9%,相对标准偏差为2.1%~7.8%。     

利用高场非对称波形离子迁移谱技术快速鉴别降糖中药中的西药成分

为了快速检测降糖中成药中非法添加的西药成分,本研究采用热解吸-高场非对称波形离子迁移谱(FAIMS)技术扫描对比中成药降糖胶囊与对照标准品盐酸二甲双胍、盐酸苯乙双胍和格列本脲的图谱。设定热解吸管的加热温度为160℃,测试压强为107 kPa,电场强度范围设定为仪器最大电场强度的0~100%,补偿电压范围为"6~+6 V。实验中对3种标准品及其组合的谱图建立了含有补偿电压(CV)值、电场强度(E/N)值和电流强度(A I)3个变量的8组指纹识别点。结果表明,供试品与3种对照品混合物的图谱一致。经液相色谱比对实验验证,供试品中含有盐酸二甲双胍、盐酸苯乙双胍和格列本脲。本研究提出了一种基于FAIMS技术快速检测降糖中成药中非法添加西药成分的新方法。     

分子印迹固相萃取-液相色谱质谱联用对4种磺酰脲类除草剂残留的测定

采用苄嘧磺隆分子印迹固相萃取柱(MISPE)对加标大米中的苄嘧磺隆、甲磺隆、苯磺隆和烟嘧磺隆4种磺酰脲类除草剂进行净化和富集预处理,并采用LC-MS方法进行定量分析.质谱条件为:正离子检测模式(M+H),检测质量范围为m/z 200 ～800 ,毛细管电压3.93 kV,锥孔电压20 V,脱溶剂温度250 ℃,辅助气流速4 L/min.4种磺酰脲类除草剂在0.01 ～0.70 mg·L~(-1)范围内线性良好.回收率为68% ～100%,表明样品液中的烟嘧磺隆、甲磺隆、苯磺隆和苄嘧磺隆能直接被分子印迹固相萃取柱中的印迹位点保留,而杂质几乎不被保留.分子印迹固相萃取柱对磺酰脲类除草剂表现出良好的识别性能.     

超高效液相色谱-四极杆/静电场轨道阱高分辨质谱快速筛查及定量分析保健品中11种非法添加降糖药物

基于超高效液相色谱-四极杆/静电场轨道阱质谱建立了保健品中11种非法添加化学降糖药(那格列奈、盐酸吡格列酮、格列喹酮、格列齐特、格列吡嗪、格列本脲、盐酸二甲双胍、瑞格列奈、盐酸苯乙双胍、盐酸罗格列酮、格列美脲)的快速筛查和定量分析方法。样品采用甲醇提取,C18色谱柱(100 mm×4.6 mm, 2.7 μm)分离,用10 mmol/L乙酸铵水溶液和乙腈进行梯度洗脱,正离子模式扫描。化合物一级质谱的分辨率为70000,二级质谱分辨率为17500。实验结果表明,11种化合物在0.005~0.5 mg/L范围内具有良好的线性(线性相关系数均大于0.99),各降糖类药物检出限为2.7~5.1 μg/kg,回收率为87.3%~98.3%,相对标准偏差为2.18%~5.21%。本方法具有准确、简便、快速的特点,可用于降糖类保健品中11种降糖药物的定性筛查和定量分析。     

固相萃取/高效液相色谱法对中成药和保健品中7种降糖化学药物的测定

建立了一种固相萃取/高效液相色谱测定保健品中格列吡嗪、格列齐特、格列本脲、格列喹酮、盐酸二甲双胍、盐酸苯乙双胍和瑞格列奈7种降糖化学药物的方法.采用阳离子周相萃取柱,对提取液进行净化处理.得到的不同洗脱液分别进样,用液相色谱进行分析,采用ZORBAX SB-C18柱,以乙腈-0.02mol/L磷酸缓冲盐(pH 2.8)作为流动相进行梯度洗脱,7个色谱峰分离良好,两次进样在40min内可以完成,外标法定量.在3种不同剂型中药制剂中的添加回收率在83%～101%之间.     

分子印迹固相萃取-高效液相色谱法同时检测烟叶中磺酰脲类农药残留

以氯磺隆（CS）为模板分子,甲基丙烯酸为功能单体,三羟甲基丙烷三甲基丙烯酸酯为交联剂,在二氯甲烷氛围中,经沉淀聚合制备氯磺隆分子印迹聚合物（CS-MIP）微球。将该聚合物微球作为填料制得分子印迹固相萃取柱用于样品前处理,建立了分子印迹固相萃取-高效液相色谱（MIP-SPE-HPLC）同时检测烟叶中6种磺酰脲类除草剂残留的分析方法。针对氯磺隆、甲磺隆、苄嘧磺隆、苯磺隆、胺苯磺隆和烟嘧磺隆6种磺酰脲类除草剂,在烟叶中加标0.50~50 μg/g,经氯磺隆分子印迹固相萃取柱（CS-MIP-SPE）净化和富集,高效液相色谱（HPLC）检测,其平均回收率为77.60%~102.05%,相对标准偏差为0.16%~7.07%,检出限为0.08~0.46 μg/g。将MIP-SPE-HPLC方法用于实际农药残留检测,结果表明可同时满足烟叶中多种磺酰脲类除草剂残留量的检测要求。     

基于N,O-双异丁烯酰乙醇胺为交联功能单体的苯磺隆分子印迹聚合物膜的制备及其性能研究

以苯磺隆为模板分子, N,O-双异丁烯酰乙醇胺为交联功能单体, 在尼龙-6膜上通过紫外光照引发合成了分子印迹聚合物膜, 并用扫描电镜对其表面形态进行了表征. 用紫外分光光谱法研究了模板分子与交联功能单体之间的相互作用. 印迹因子的测定和底物竞争渗透实验结果表明, 分子印迹聚合物膜对模板分子苯磺隆具有较高的选择性, 而非分子印迹聚合物膜没有选择性.     

三氟甲基嘧啶磺酰脲的合成与除草活性

以三氟乙酰乙酸乙酯和盐酸胍为原料,经环合、氯化、甲氧基化、胺化反应合成了4种2-氨基-4-取代-6-三氟甲基嘧啶中间体(Ⅰa~Ⅰd),Ⅰ与邻甲氧羰基苯磺酰异氰酸酯亲核加成,合成了3种含不同取代嘧啶环的磺酰脲化合物(Ⅱb~Ⅱd)。其中2-氨基-4-二甲胺基-6-三氟甲基嘧啶(Ⅰd)和N[-2-(′4-二甲胺基-6-三氟甲基)嘧啶基]-2-甲氧羰基苯磺酰脲(Ⅱd)为新化合物,结构经1H NMR和MS表征。初步除草活性测定结果表明,N-[2-′(4-甲氧基-6-三氟甲基)嘧啶基]-2-甲氧羰基苯磺酰脲(Ⅱc)在浓度为200 ga.i./ha时对稗草和马唐的防效分别为70%和50%。     

糖尿病患者尿液中常见药物含量的高效液相色谱法测定

建立了高效液相色谱/二极管阵列检测法同时测定糖尿病患者尿液中二甲双胍、格列吡嗪和替米沙坦3种常用药物含量的方法.室温条件下以2.5 mmol/L十二烷基硫酸钠-20 mmol/L磷酸二氢钠(pH 4.6)-乙腈为流动相,梯度洗脱,实现了3种药物的有效分离.采用3种不同检测波长,测得二甲双胍、格列吡嗪和替米沙坦的检出限分...     

Selective separation and enrichment of glibenclamide in health foods using surface molecularly imprinted polymers prepared via dendritic grafting of magnetic nanoparticles

In this paper, the novel surface molecularly imprinted polymers based on dendritic‐grafting magnetic nanoparticles were developed to enrich and separate glibenclamide in health foods. The density functional theory method was used to give theoretical directions to the synthesis of molecularly imprinted polymers. The polymers were prepared by using magnetic nanoparticles as supporting materials, methacrylic acid as the functional monomer, and ethylene glycol dimethacrylate as the cross‐linker. The characteristics of magnetic nanoparticles and polymers were measured by transmission electron microscope and SEM, respectively. The enriching ability of molecularly imprinted polymers was measured by Freundlich Isotherm. The molecularly imprinted polymers were used as dispersive SPE materials to enrich, separate, and detect glibenclamide in health foods by HPLC. The average recoveries of glibenclamide in spiked health foods were 81.46–93.53% with the RSD < 4.07%.     

Molecularly imprinted solid-phase extraction for the screening of antihyperglycemic biguanides

A new molecularly imprinted polymer (MIP) was specifically synthesized as a smart material for the recognition of metformin hydrochloride in solid-phase extraction. Particles of this MIP were packed into a stainless-steel tubing (50 mm x 0.8 mm i.d.) equipped with an exit frit. This micro-column was employed in the development of a molecularly imprinted solid-phase extraction (MISPE) method for metformin determination. The MISPE instrumentation consisted of a micrometer pump, an injector valve equipped with a 20-microl sample loop, a UV detector, and an integrator. With CH3CN as the mobile phase flowing at 0.5 ml/min, 95 +/- 2% binding could be achieved for 1200 ng of metformin from one injection of a phosphate-buffered sample solution (pH 2.5). Methanol + 3% trifluoroacetic acid was good for quantitative pulsed elution (PE) of the bound metformin. The MISPE-PE method, with UV detection at 240 nm, afforded a detection limit of 16 ng (or 0.8 microg/ml) for metformin. However, the micro-column interacted indiscriminately with phenformin with a 49 +/- 2% binding. A systematic investigation of binding selectivity was conducted with respect to sample composition (including the solvent, matrix, pH, buffer and surfactant effects). An intermediate step of differential pulsed elution used acetonitrile with 5% picric acid to remove phenformin and other structural analogues. A final pulsed elution of metformin for direct UV detection was achieved using 3% trifluoroacetic acid in methanol.     

Preparing molecularly imprinted membranes by phase inversion to separate kaempferol

Molecularly imprinted membranes (MIMs) were studied to separate special target molecule – kaempferol, an important active pharmaceutical ingredient. The kaempferol MIM were prepared by the liquid–solid phase inversion method. The effects of polyphenylene sulfone, LiCl, and ZnCl₂ on membrane performance were studied, a high Flux MIM was prepared, then the kaempferol molecularly imprinted polymer membrane, non‐molecularly imprinted membrane, and non‐molecularly imprinted polymer membrane were prepared to investigate adsorption capacity. From adsorption isotherm curve, the maximum equilibrium adsorption quantity was 890 µg/g, and it was MIM. The MIM and molecularly imprinted polymer membrane give high selectivity towards kaempferol; the non‐molecularly imprinted membrane and non‐molecularly imprinted polymer membrane showed low adsorption quantity and selectivity. The reuse experiment of the MIM indicated that it has good reuse property. All the results showed binding sites were important in the separation process of MIMs. Copyright © 2016 John Wiley & Sons, Ltd.     

Determination of 2,6-Dichlorophenol by Surface-Enhanced Raman Scattering with Molecular Imprinting

A novel method has been reported for 2,6-dichlorophenol using surface-enhanced Raman scattering (SERS). SiO₂/gold composites were selected as the SERS substrates to provide the response of gold nanoparticles. Molecular imprinting was subsequently used for the development of a specific detector to 2,6-dichlorophenol with precipitation polymerization. The molecularly imprinted polymer provided sensitive and selective SERS detection for the determination of 2,6-dichlorophenol. The intensity and concentration obeyed a linear relationship from 1?×?10^?5 to 1?×?10^?9?mol?L^?1 2,6-dichlorophenol. The sensitivity of SERS with the molecularly imprinted polymers provides a promising approach for practical analysis.     

邻香草醛分子印迹聚合物膜的制备及其透过选择性质的研究

采用紫外光引发原位聚合的方法制备了具有支撑膜的邻香草醛分子印迹聚合物膜. 紫外光度法测定了模板分子和功能单体之间的结合常数和化学计量比(n＝2). 用傅立叶红外光谱和扫描电镜分别测定了膜的结构和表面形貌; 膜渗透实验结果表明在干扰物存在时印迹膜对模板分子表现出良好的选择透过性能. 研究了分子印迹聚合物膜透过的机理、并为分子印迹技术应用于传感器领域增加了理论和实验方法.     

Simultaneous spectrophotometric determination of metformin hydrochloride and glibenclamide in binary mixtures using combined discrete and continuous wavelet transforms

In this work, a combined discrete and continuous wavelet transform analysis was developed for simultaneous spectrophotometric determinations of metformin hydrochloride and glibenclamide, two antidiabetic drugs, in binary mixtures without any chemical pretreatment. Absorption spectra were subjected to the 4-level db4 discrete wavelet transform (DWT) for signal de-noising. Selected continuous wavelet transform (CWT) families (rbio3.1 with scaling factor, a = 80, and gaus2, a = 60) were applied on these de-noised signals. Finally, a zero-crossing technique was used for the construction of calibration curves for both drugs. The proposed method was validated by analyzing synthetic mixtures of the investigated drugs with various concentrations. The amount of metformin hydrochloride and glibenclamide were determined by using CWT amplitudes in zero-crossing points. The mean recovery values of metformin hydrochloride and glibenclamide were found between 98.6-102.0 and 97.9-102.4% for rbio3 and 98.3-101.2 and 97.1-101.4% for gaus2 families, respectively. The obtained results showed that the developed method is a simple, rapid and precise procedure for the simultaneous determination of metformin hydrochloride and glibenclamide in binary mixtures.     

Chiral separation membranes from modified polysulfone having myrtenal-derived terpenoid side groups

Novel polymeric materials, having a chiral environment, were obtained by the reaction of lithiated polysulfone with chiral terpenoid myrtenal. The resulting polymers gave self-standing durable membranes. Molecularly imprinted membranes were prepared from the novel myrtenal-containing polysulfones by the presence of print molecules during the membrane preparation process. The d-isomer imprinted membrane showed d-isomer adsorption and diffusivity selectivity, and vice versa. As a result, the d-isomer imprinted membrane transported the d-isomer in preference to the l-isomer, and vice versa. The control non-imprinted membrane also showed permselectivity toward racemic glutamic acid mixtures. The expression of permselectivity for the molecularly imprinted membranes was synergistically due to adsorption and diffusivity selectivity.     

钴离子配位分子印迹聚合物膜渗透特性的研究

采用分子印迹技术紫外光引发原位聚合的方法制备了带支撑膜的钴离子配位分子印迹聚合物膜. 用扫描电镜测定了膜的表面形貌. 通过膜渗透实验表明, 在一定浓度钴离子存在下, 印迹膜对模板分子表现出良好的渗透选择性. 分别考察了阳离子和阴离子对印迹膜渗透模板分子的影响. 本工作有助于分子印迹技术应用于传感器技术和连续分离技术的研究.     

Molecularly imprinted solid phase extraction for rapid screening of metformin

A molecularly imprinted solid phase extraction (MISPE) method has been developed for the rapid screening of metformin. Newly synthesized molecularly imprinted polymer (MIP) particles were slurry-packed into a micro-column for selective solid phase extraction (SPE) of metformin. With CH₃CN flowing at 0.5 ml/min, a total binding capacity of 1600 ng metformin was determined for the 20 mg of MIP particles. A broad range of MISPE conditions was evaluated with respect to sample solvent, pH, and buffer compositions. A 95±2% binding could be achieved from one 20-μl injection of sample solution in acetonitrile plus phosphate buffer, up to 1200 ng of metformin. However, the micro-column interacted indiscriminately with phenformin, a structural analogue, to attain 49±2% binding. Separation of phenformin from metformin was ultimately achieved, using differential pulsed elution (DPE) with 1 M trifluoromethacrylic acid in acetonitrile. Final pulsed elution (FPE) using 3% trifluoroacetic acid in methanol was good for the quantitative elution of metformin. The MISPE–DPE–FPE method, with UV detection at 240 nm, afforded a detection limit of 0.8 μg/ml (or 16 ng) for metformin. Each MISPE–DPE–FPE analysis required less than 5 min to complete.