Synthesis of a molecularly imprinted polymer for the selective solid-phase extraction of chloramphenicol from honey

Solid-phase extraction (SPE) with a molecularly imprinted polymer (MIP) as sorbent has been investigated for the clean-up of the broad-spectrum bacteriostatic antibiotic chloramphenicol (CAP) in honey samples. The MIP was prepared by using methacrylic acid (MAA) as functional monomer, ethylene glycol dimethacrylate (EDMA) as cross-linker, chloroform as porogen and CAP as template molecule. The binding behaviour of the template CAP on the MIP was evaluated by high-performance liquid chromatography, and then the MIP was applied as a sorbent in SPE to selectively extract CAP from honey. It was shown that recoveries of nearly 100% of a CAP standard solution and up to 94% from spiked honey samples could be obtained after SPE.     

咖啡因分子印迹固相萃取柱的制备及应用

以咖啡因作为模板分子,α-甲基丙烯酸为功能单体,乙二醇二甲基丙烯酸酯为交联剂,制备了咖啡因分子印迹聚合物(MIP)。与非印迹聚合物(NIP)相比,MIP对咖啡因具有更高的吸附容量和选择性,MIP和NIP对咖啡因的最大静态吸附量分别为28.1和16.5mg/g,相对选择因子为1.25。以咖啡因分子印迹聚合物为固相萃取填料,结合高效液相色谱(HPLC),建立了茶水中咖啡因浓度及人饮茶后血清中咖啡因浓度的检测方法。考察了洗脱剂种类和用量对咖啡因回收率的影响。当萃取柱依次以2mL水活化,水溶液上样,2mL水淋洗,6mL甲醇-乙酸(9∶1,V/V)洗脱,咖啡因在MIP固相萃取柱上的回收率达到97.5%,而在NIP柱上的回收率仅为54.9%。     

Development of a molecularly imprinted polymer for the analysis of avermectin

Five molecularly imprinted polymers (MIPs) were synthesized for a large molecule, avermectin, using different preparation techniques, monomers, and polymerization solvents. Selectivities (α) of each were compared using HPLC and different mobile phases containing various levels of acetic acid. Selectivity (α) for avermectin was greatest (α estimated ≥18) when the polymer was prepared non-covalently (utilizing only non-covalent interactions between avermectin and monomer) in chloroform using methacrylic acid (MAA) monomer and evaluated in chloroform. When evaluated in acetonitrile, an MIP prepared in acetonitrile provided better selectivity (α=8.4) than the polymer prepared in chloroform. Optimizing mobile phase conditions by adding acetic acid was much more important when MIPs were evaluated in chloroform than in acetonitrile. MIPs prepared with MAA provided better selectivity than a polymer prepared with acrylamide monomer. Covalent preparation of two MIPs utilizing a covalent bond between avermectin and monomer before polymerization did not improve selectivity but did improve peak shape in chromatograms. Specificity was demonstrated by comparing the selectivity of avermectin with eprinomectin (α=3.0), a compound with a very similar structure. Results indicate that an MIP can be prepared for the large avermectin molecule, and has the potential to simplify sample preparation and to reduce the time needed for analysis.     

邻苯二甲酸二（2-丙基庚）酯分子印迹固相萃取剂的制备及其应用

以邻苯二甲酸二辛酯（DOP）为虚拟模板分子,α-甲基丙烯酸（MAA）为功能单体,乙二醇二甲基丙烯酸酯（EDMA）为交联剂,采用沉淀聚合法制备了对邻苯二甲酸二（2-丙基庚）酯（DPHP）具有高选择性的分子印迹聚合物（MIP）。用紫外分光光度法探索了不同功能单体与模板分子的结合能力,与功能单体丙烯酸（AA）相比,MAA与DOP的结合能力更强,其最佳结合的物质的量比为6：1。考察MIP对DOP、DPHP、邻苯二甲酸二甲酯（DMP）、邻苯二甲酸二丁酯（DBP）的选择吸附性能,发现该聚合物对DPHP具有更高的选择吸附性。以制备的聚合物为固相萃取填料,结合HPLC分析,考察了淋洗剂与洗脱剂的种类和用量对DPHP回收率的影响。将DPHP甲醇溶液加载至萃取柱后用1 mL甲醇-水（1：9,v/v）淋洗,5 mL甲醇-乙酸（9：1,v/v）洗脱,DPHP在分子印迹固相萃取（MISPE）柱上的回收率达到96.8%,而在非印迹固相萃取（NISPE）柱上的回收率仅为52.9%。将建立的MISPE-HPLC方法应用于测定兔口服DPHP后不同时间点兔血清中DPHP的浓度,发现其血药浓度的最大值为5.88 μg/mL,达峰值时间为4 h,DPHP加标回收率为90.0%~92.0%,相对标准偏差小于5%。     

Computational design and synthesis of molecular imprinted polymers with high selectivity for removal of aniline from contaminated water

A computational approach was developed to screening functional monomers and polymerization solvents for rational design of molecularly imprinted polymer (MIP). It was based on the comparison of the binding energy of the complexes between the template and different functional monomers. The effect of the polymerization solvent was included using the polarizable continuum model. According to the theoretical calculation results, the MIP with aniline as template was prepared by emulsion polymerization method using acrylamide (AAM) as functional monomer and divinylbenzene as cross-linker in carbon tetrachloride. The synthesized MIP was then tested by equilibrium-adsorption method, and the MIP demonstrated high removal efficiency to the aniline. The results of this study have indicated the possibility of using computer aided design for rational selection of functional monomers and solvents capable of removal of aniline from contaminated water.     

1-氨基乙内酰脲分子印迹聚合物的制备和吸附性能研究

以1-氨基乙内酰脲(AHD)为模板分子,α-甲基丙烯酸(MAA)为功能单体,乙二醇二甲基丙烯酸酯(EDMA)为交联剂,采用本体聚合方法合成了分子印迹聚合物(M IP),考察了模板分子与功能单体不同比例下制备的M IP对模板分子的吸附性能。通过Scatchard分析,表明该印迹聚合物上存在一类等价的吸附位点,其结合位点的离解常数KD=4.33mmol/L。     

Synthesis and evaluation of new lipomonosaccharide-imprinted polymers as MISPE supports

Molecular imprinted polymers (MIP) were prepared by the copolymerization of styrene (S) or methyl methacrylate (MMA) and methacrylic acid (MAA) using ethylene glycol dimethacrylate (EGDMA) as the crosslinker with molar ratios of [monomer]/[crosslinker] and [MAA]/[template] of 3:7 (to obtain a rigid structure) and 1:6 (to optimise hydrogen interactions), respectively. The polymerizations occurred in presence of the template molecule (MIP) - GlcNcouma - an amphiphilic monosaccharide. The same materials, non-imprinted polymers (NIP), were also prepared in absence of the template. These MIPs were characterized and used as SPE supports for selective enrichment. The results showed the correlation between retention efficiency and the porogen character of the polymerization solvent.     

Preparation and Adsorption Ability of Molecularly Imprinted Polymer Microspheres for Malachite Green

Molecularly imprinted polymer (MIP) microspheres were synthesized through precipitation polymerization using malachite green (MG) as template, methacrylic acid (MAA) as monomer, and trimethylolpropane trimethacrylate (TRIM) as cross-linker. The microsphere structure of MIP was characterized by IR spectroscopy and SEM. The influence of preparation conditions such as monomer and cross-linker dosages on the polymer absorption of MG in acetonitrile solution was also explored. Under the optimum synthesis conditions (0.25 mmol MG, 1.5 mmol MAA, 2.5 mmol TRIM, 40 mL acetonitrile), the prepared MIP microspheres have a binding capacity as high as 2000 µg g^?1 of MG with an imprinting factor of above 4.0. The result suggests that the prepared MIP microspheres are promising material for the selective extraction of MG in complicated matrix solutions.     

Application of molecularly imprinted polymer for solid phase extraction and preconcentration of Hydrochlorothiazide in pharmaceutical and serum sample analysis

A new polymeric sorbent prepared by utilizing molecular imprinting technology was used for the selective extraction of hydrochlorothiazide (HCT) from pharmaceutical and human serum sample. The molecularly imprinted polymer (MIP) was prepared using HCT as the template, methacrylic acid (MAA) as the functional monomer, ethylene glycol dimethacrylate (EDMA) as the cross-linker monomer, and dimethylformamide (DMF) as a solvent. The optimized conditions of MIPs as a selective sorbent for the preconcentration of the HCT were studied. The results showed that the drug could be quantitatively and selectively maintained in the column to be then eluted from the sorbent by using methanol-acetic acid mixture (9:1). HCT could be determined spectrophotometrically at λ_max = 270 nm. This method made it possible to quantitize HCT in the range of 0.1–21.0 μg ml^-1, by less than 0.55% of RSD%, with a detection limit (S/N = 3) of 0.073 ng ml^-1. The preconcentration factor of 1000, recoveries of up to 96% and retention capacity of 75.0 mg g_-1 were achieved using this technique.     

Use of an on-line imprinted polymer pre-column, for the liquid chromatographic-UV absorbance determination of carbaryl and its metabolite in complex matrices

A carbaryl and 1-naphtol molecular imprinted polymers (MIP1 and MIP 2, respectively) were prepared using suspension polymerization and tested for selective and reversible binding to carbaryl and 1-naphtol, respectively. In the suspension polymerization technique used, polymers of methacrylic acid (MAA), highly cross-linked with ethylene dimethacrylate, provide a specific binding sites for the carbaryl molecule and its metabolite when using it as a template to be removed after polymerization. The molecular imprinted polymer with a particle size of approximately 5 microm were isolated and packed into a pre-column (50 mm x 4.6 mm id) that was used to isolate carbaryl and its metabolite from complex matrices injected on a high performance liquid chromatography system using ultra-violet detection without extensive sample preparation and clean up. The HPLC method had a detection limit of 1.00 ng/mL and a linear response (r2 > 0.98) over the concentration range of 1.00-10.0 ng/mL.     

Development of a selective molecularly imprinted polymer-based solid-phase extraction for indomethacin from water samples

A selective molecularly imprinted solid-phase extraction (MISPE) for indomethacin (IDM) from water samples was developed. Using IDM as template molecule, acrylamide (AM) or methacrylic acid (MAA) as functional monomer, ethylene dimethacrylate (EDMA) as crosslinker, and bulk or suspension polymerization as the synthetic method, three molecularly imprinted polymers (MIPs) were synthesized and characterized with a rebinding experiment. It was found that the MIP of AM-EDMA produced by bulk polymerization showed the highest binding capacity for IDM, and so it was chosen for subsequent experiments, such as those testing the selectivity and recognition binding sites. Scatchard analysis revealed that at least two kinds of binding sites formed in the MIP, with the dissociation constants of 7.8 μmol L⁻¹ and 127.2 μmol L⁻¹, respectively. Besides IDM, three structurally related compounds — acemetacin, oxaprozin and ibuprofen — were employed for selectivity tests. It was observed that the MIP exhibited the highest selective rebinding to IDM. Accordingly, the MIP was used as a solid-phase extraction sorbent for the extraction and enrichment of IDM in water samples. The extraction conditions of the MISPE column for IDM were optimized to be: chloroform or water as loading solvent, chloroform with 20% acetonitrile as washing solution, and methanol as eluting solvent. Water samples with or without spiking were extracted by the MISPE column and analyzed by HPLC. No detectable IDM was observed in tap water and the content of IDM in a river water sample was found to be 1.8 ng mL⁻¹. The extraction efficiencies of the MISPE column for IDM in spiked tap and river water were acceptable (87.2% and 83.5%, respectively), demonstrating the feasibility of the prepared MIP for IDM extraction. Figure Molecularly imprinted polymer-based solid-phase extraction for indomethacin     

Selective extraction based on poly(MAA‐VB‐EGMDA) monolith followed by HPLC for determination of hordenine in plasma and urine samples

Hordenine is an active compound found in several foods, herbs and beer. In this work, a novel sorbent was fabricated for selective solid‐phase extraction (SPE) of hordenine in biological samples. The organic polymer sorbent was synthesized in one step in the plastic barrel of a syringe by a pre‐polymerization solution consisting of methacrylic acid (MAA), 4‐vinylphenylboronic acid (VB) and ethylene glycol dimethacrylate (EGDMA). The conditions for preparation were optimized to generate a poly(MAA‐VB‐EGMDA) monolith with good permeability. The monolith exhibited good enrichment efficiency towards hordenine. By using tyramine as the internal standard, a poly(MAA‐VB‐EGMDA)‐based SPE‐HPLC method was established for analysis of hordenine. Conditions for SPE, including volume of eluting solvent, pH of sample solution, sampling rate and sample volume, were optimized. The proposed SPE‐HPLC method presented good linearity (R² = 0.9992) within 10–2000 ng/mL and the detection limits was 3 ng/mL, which is significantly more sensitive than reported methods. The method was also applied in plasma and urine samples; good capability of removing matrices was observed, while hordenine in low content was well extracted and enriched. The recoveries were from 90.6 to 94.7% and from 89.3 to 91.5% for the spiked plasma and urine samples, respectively, with the relative standard deviations <4.7%. Copyright © 2014 John Wiley & Sons, Ltd.     

Isolation and determination of estrogens in water samples by solid‐phase extraction using molecularly imprinted polymers and HPLC

Advanced SPE with molecularly imprinted polymers (MIP) was used in this study. A noncovalent imprinting approach was applied to separate 17β‐estradiol, estriol, and estrone from water samples. Polymer material was prepared by bulk polymerization with methacrylic acid as a functional monomer, divinylbenzene and ethyleneglycol dimethacrylate as crosslinkers, and acetonitrile, acetonitrile/toluene (3:1, v/v) or isooctane/toluene (1:99, v/v) as a porogen. We also prepared an MIP film on a silica gel surface with methacrylic acid and ethyleneglycol dimethacrylate as monomers and acetonitrile as a solvent. Qualitative and quantitative hormone analyses were carried out by HPLC with various detection techniques, including UV/visible spectroscopic detection (diode array detection) and electrochemical detection (CoulArray). The results of the study indicate that MIP technology is an excellent method for the quality control of estrogens in environmental analyses with a low quantification limit for 17β‐estradiol of around 26 (diode array detection) and 0.25 ng/mL (electrochemical detection). The proposed method was found to be suitable for routine determinations of the analyzed compound in environmental laboratories.     

Micro flow sensor on a chip for the determination of terbutaline in human serum based on chemiluminescence and a molecularly imprinted polymer

Based on a molecularly imprinted polymer (MIP) as the recognition element, a novel chemiluminescence (CL) micro flow sensor on a chip for the determination of terbutaline in human serum is described. The MIP was prepared by using terbutaline as the template, methacrylic acid (MAA) as the functional monomer, ethylene glycol dimethacrylate (EGDMA) as the cross-linking monomer, and acetonitrile as the solvent. The chip was fabricated from two 50 mm × 40 mm × 5 mm transparent poly (methylmethacrylate) (PMMA) slices. The microchannels on the chip etched by CO₂ laser were 200 μm wide and 150 μm deep. The microsensor cell filled with 2 mg MIP for selectively on line adsorbing terbutaline was 10 mm long, 1 mm wide, and 0.5 mm deep. All reagents were controlled by the syringe pump with an accurate timer. The on line adsorbed terbutaline by the MIP can enhance the CL intensity of the reaction of luminol with ferricyanide. The enhanced CL intensity is linear with terbutaline concentration from 8.0 to 100 ng/mL with a detection limit of 4.0 ng/mL (3σ). The micro flow sensor provides for good reproducibility with the relative standard deviation of 3.6% (n = 7) for 20 ng/mL terbutaline.     

Monodispersed, molecularly imprinted polymers for cinchonidine by precipitation polymerization

Three monodispersed, molecularly imprinted polymers (MIPs) for cinchonidine (CD) have been synthesized by precipitation polymerization. MIP1 was prepared using methacrylic acid (MAA) as a functional monomer and divinylbenzene (DVB) as a cross-linker and MIP2 was prepared with further addition of 2-hydroxyethyl methacrylate (HEMA) as a co-monomer. For the preparation of MIP3, core-shell type MIP, monodispersed DVB homopolymers, which are prepared by precipitation polymerization, were used as a core and CD-imprinted MAA-DVB copolymer phases were coated onto the core. Three MIPs synthesized gave monodispersed, spherical beads in micrometer sizes. The binding characteristics and molecular recognition properties of MIP1-3 were examined by Scatchard analysis and chromatographic studies. The association constant of CD with MIP1 was the highest among MIPs prepared, while that with MIP3 was the lowest. The template molecule, CD, was more retained than its stereoisomer, cinchonine, on the three MIPs, and the stereoseparation factor of 38 was obtained with MIP3.     

齐墩果酸分子印迹聚合物预组装体系的分子模拟及聚合物制备

以齐墩果酸(OA)为模板分子,三氟甲基丙烯酸(TFMAA)、α-甲基丙烯酸(MAA)、丙烯酰胺(AM)、4-乙烯基吡啶(4-VP)为功能单体,三氯甲烷、四氢呋喃、乙醇、甲醇和丙酮为溶剂,基于量子化学密度泛函理论(DFT)和ONIOM方法,采用Gaussian09软件模拟计算了模板分子与不同功能单体的印迹聚合物预组装体系的构型,探讨了模板分子与功能单体在不同印迹比例时所形成复合物的成键情况以及反应过程中的结合能,并采用自洽反应场极化连续模型(CPCM)计算了功能单体与模板分子在不同溶剂中的溶剂化能。结果表明,TFMAA与模板分子OA以1:1摩尔比形成复合物的结合能ΔE最高(-70.99kJ·mol~(-1)),结构最稳定,模板分子和功能单体在三氯甲烷中的溶剂化能最小。同时,采用实验方法验证模拟结果,并利用扫描电镜、傅里叶红外光谱仪和静态吸附实验对印迹聚合物的形貌、化学基团和吸附性能等进行表征。结果表明,模拟结果与实验结果完全一致,计算机模拟对分子印迹体系的筛选和机理研究提供了理论依据。     

分子模拟-活性自由基聚合法制备山奈酚分子印迹整体柱及其性能评价

通过分子模拟研究模板分子与功能单体的相互作用,可以缩短优化时间,为选取合适的功能单体以及模板分子/功能单体比例提供依据.本研究以山奈酚为模板分子,通过分子模拟优化实验条件,确定以甲基丙烯酸(MAA)为最优的功能单体,山奈酚/MAA最佳比例为1∶4 (w/w).此外,以二苄基三硫代碳酸酯(DBTTC)为可逆加成-链断裂转移剂,乙二醇二甲基丙烯酸酯(EDMA)为交联剂,实现了仅需优化引发剂和可逆加成-断裂链转移聚合(RAFT)试剂即可制得性能优异的山奈酚分子印迹整体柱.此整体柱对山奈酚和相似物槲皮素的分离度为1.52,相对标准偏差为1.8%.实验结果表明,分子模拟计算简化了实验步骤,以DBTTC为RAFT试剂得到了具有更好形态和结构的分子印迹整体柱.     

Application of multivariate analysis to the screening of molecularly imprinted polymers (MIPs) for ametryn

Among the solid-phase extraction (SPE) techniques, a novel system for a triazine herbicide named ametryn, has been developed based on a molecular imprinted polymer (MIP) phase. Through this method, the synthesis of the complementary to ametryn MIP was accomplished and the factors influencing its efficiency have been optimized. Through the optimization process, the type and the amounts of functional monomer and solvents, template amount, cross-linker, initiator as well as the polymerization temperature were considered to be evaluated. Based on the obtained results, the optimum conditions for the efficient polymerized sorbent, considering the recovery efficiency were solvent: acetonitrile, 6.41 mL; monomer: methacrylic acid, 5.41 mmol; template: 1.204 mmol; cross-linker: 27.070 mmol; initiator: 2.03 mmol; temperature: 40.86 degrees C. The optimum molar ratio among the template, monomer and cross-linker for ametryn was 1:4.49:22.48. The reversed-phase HPLC-UV was used for the ametryn determination, using an isocratic solvent delivery system (acetonitrile: H(2)O, 60:40), flow-rate of 0.8 mL min(-1) and a UV wavelength of 220 nm. In line with the obtained results, using central composite design (CCD) can increase the precision and accuracy of synthesis and optimization of MIP to ametryn and possibly other similar analogues.     

Synthesis and Evaluation of Molecularly Imprinted Polymers as Sorbents for Selective Extraction of Coumarins

Coumarin, 7-hydroxycoumarin and dicoumarol molecularly imprinted polymers (MIP) were synthesized by bulk polymerization. Methacrylic acid and 4-vinylpyridine were tested as functional monomers and methanol, ethanol, acetonitrile, toluene and chloroform were tested as porogens. The binding capabilities of the imprinted polymers were assessed by equilibrium binding analysis. Highest binding capacity was obtained for MIP prepared for the template 7-hydroxycoumarin synthesized in methacrylic acid as functional monomer, chloroform as porogen and methanol/water as analyte solvent. Scanning electron microscopy analysis documented its appropriate morphology. ATR-FTIR spectra confirmed successful polymerization of MIP. Coumarin structural analogues were employed to evaluate the polymer selectivity and it was found that polymer prepared for 7-hydroxycoumarin was selective for its template molecule. Kinetic studies showed relatively fast adsorption of analytes to MIPs (1 h). Rebinding properties of MIPs were evaluated by adsorption isotherms. The calculated data fitted well with experimental data showing that Freundlich isotherm is suitable for modelling the adsorption of tested coumarins on prepared MIPs. Applicability of polymer prepared for 7-hydroxycoumarin was tested for the selective extraction of coumarins from the sample of chicory.     

Molecularly imprinted polymers for triazine herbicides prepared by multi-step swelling and polymerization method. Their application to the determination of methylthiotriazine herbicides in river water

Uniformly-sized, molecularly imprinted polymers (MIPs) for atrazine, ametryn and irgarol were prepared by a multi-step swelling and polymerization method using ethylene glycol dimethacrylate as a cross-linker and methacrylic acid (MAA), 2-(trifluoromethyl) acrylic acid (TFMAA) or 4-vinylpyridine either as a functional monomer or not. The MIP for atrazine prepared using MAA showed good molecular recognition abilities for chlorotriazine herbicides, while the MIPs for ametryn and irgarol prepared using TFMAA showed excellent molecular recognition abilities for methylthiotriazine herbicides. A restricted access media-molecularly imprinted polymer (RAM-MIP) for irgarol was prepared followed by in situ hydrophilic surface modification using glycerol dimethacrylate and glycerol monomethacrylate as hydrophilic monomers. The RAM-MIP was applied to selective pretreatment and enrichment of methylthiotriazine herbicides, simetryn, ametryn and prometryn, in river water, followed by their separation and UV detection via column-switching HPLC. The calibration graphs of these compounds showed good linearity in the range of 50-500 pg/mL (r > 0.999) with a 100 mL loading of a river water sample. The quantitation limits of simetryn, ametryn and prometryn were 50 pg/mL, and the detection limits were 25 pg/mL. The recoveries of simetryn, ametryn and prometryn at 50 pg/mL were 101%, 95.6% and 95.1%, respectively. This method was successfully applied for the simultaneous determination of simetryn, ametryn and prometryn in river water.