共查询到19条相似文献,搜索用时 203 毫秒
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微波聚合快速制备分子印迹毛细管电色谱整体柱 总被引:10,自引:0,他引:10
以甲基丙烯酸为功能单体、己二醇二甲基丙烯酸酯为交联剂、 对羟基苯甲酸为模板分子, 采用微波辐射聚合的方式快速制备了分子印迹毛细管电色谱整体柱, 并取得了较好的印迹效果. 分子印迹材料的原位制备5 min即可完成, 大大快于国内外传统的方法. 相似文献
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2,4-二氯苯氧乙酸分子印迹整体柱的制备、表征及色谱性能研究 总被引:5,自引:3,他引:5
以2,4-二氯苯氧乙酸分子为模板,甲基丙烯酸为单体,乙二醇二甲基丙烯酸酯为交联剂,甲苯和十二醇为混合致孔剂,采用热引发原位聚合法制备了作为高效液相色谱固定相的分子印迹整体柱.用红外光谱、扫描电镜、比表面积分析法对聚合物进行了表征.考察了模板分子在不同条件下合成的印迹整体柱及空白整体柱上容量因子的变化规律,同时探讨了流动相中甲醇的体积分数、pH值、流速对印迹整体柱分离性能的影响.结果表明,在优化的合成条件下制备的分子印迹整体柱可在15 min内分离2,4-二氯苯氧乙酸及其类似物苯氧乙酸,分离度为1.52.对柑桔提取液进行了分离测试,结果满意. 相似文献
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采用分子印迹整体柱富集-高效液相色谱法选择性分离分析了植物样品中痕量细胞分裂素的含量。结果表明,以激动素为模板分子,甲基丙烯酸(MAA)为功能单体,乙二醇二甲基丙烯酸酯(EGDMA)为交联剂,甲苯与十二醇为致孔剂,可在不锈钢柱管中原位聚合制备激动素分子印迹整体柱;与非分子印迹整体柱对比,该分子印迹整体柱能选择性富集4种细胞分裂素,具有较好的重复性和高的萃取效率;在优化的实验条件下,激动素(K)、激动素核苷(KR)、反式-玉米素(tZ)和meta-topolin(mT)的平均加标回收率分别为91.9%、80.0%、87.5%和50.2%,相对标准偏差均小于11.8%。本方法已成功地用于不同植物样品中4种细胞分裂素的分离和分析。 相似文献
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分子印迹整体柱在高效液相色谱和电色谱手性分离中的应用 总被引:15,自引:0,他引:15
在常规不锈钢色谱管中以甲基丙烯酸为功能单体,采用原位聚合法制备了(5S,11S)-特罗格尔碱(S-TB)的印迹整体柱。考察了流动相中添加不同量的醋酸和水对分离的影响,结合台阶梯度洗脱模式在S-TB整体柱上实现了对TB消旋体的快速分离。另外,以碱性单体2-二甲基乙基胺甲基丙烯酸酯(DAMA)为功能单体,在毛细管中采用原位聚合法制备了毛细管分子印迹整体柱,用于在毛细管电色谱(CEC)中对消旋体1,1′-联-2-萘酚(BNL)进行手性分离。结果表明,以AMA为功能单体可以制备其他酸性模板的分子印迹聚合物,从而扩大了分子印迹聚合物MIP)在CEC分离中的应用范围。 相似文献
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分子印迹整体柱在高校液相色谱和电色谱手性分离中的应用 总被引:4,自引:0,他引:4
在常规不锈钢色谱管中以甲基丙烯酸为功能单体,采用原位聚合法制备了(5S,11S)-特罗格尔碱(S-TB)的印迹整体柱.考察了流动相中添加不同量的醋酸和水对分离的影响,结合台阶梯度洗脱模式在S-TB整体柱上实现了对TB消旋体的快速分离.另外,以碱性单体2-二甲基乙基胺甲基丙烯酸酯(DAMA)为功能单体,在毛细管中采用原位聚合法制备了毛细管分子印迹整体柱,用于在毛细管电色谱(CEC)中对消旋体1,1'-联-2-萘酚(BNL)进行手性分离.结果表明,以DAMA为功能单体可以制备其他酸性模板的分子印迹聚合物,从而扩大了分子印迹聚合物(MIP)在CEC分离中的应用范围. 相似文献
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三聚氰胺分子印迹整体柱识别性能的研究 总被引:1,自引:0,他引:1
以三聚氰胺(MAM)为模板分子,甲基丙烯酸(MAA)为功能单体,二甲基丙烯酸乙二醇酯(EGDMA)为交联剂,原位聚合法制备了对MAM有很强选择性识别能力的分子印迹整体柱。采用脉冲洗脱法快速筛选MAM的洗脱剂,通过前沿色谱法测定了整体柱对MAM的结合容量。实验表明,所制备的印迹整体柱对MAM有极强亲和作用力,即使在强极性流动相中(甲醇或甲醇-水(V/V=80/20)),MAM在印迹柱上也有强保留,不被洗脱。实验测得结合位点数(Lt)和解离常数(Kd)分别为:印迹柱Lt=2.28×103μmol/g,Kd=2.45×10-5mol/L;空白柱Lt=366μmol/g,Kd=23.7mo/L。该印迹整体柱有望作为固相萃取柱,在线或离线选择性富集样品中的MAM。 相似文献
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Monolithic molecularly imprinted polymer for sulfamethoxazole and molecular recognition properties in aqueous mobile phase 总被引:1,自引:0,他引:1
A monolithic molecularly imprinted polymer (monolithic MIP) for sulfamethoxazole (SMO) was prepared by in situ polymerization method as the HPLC stationary phase. By optimizing the polymerization conditions, the monolithic MIP showed highly specific recognition for the template SMO over its three structurally related analogs. As shown by SEM and the pore size distribution profile, the resultant MIP monolith showed a main pore diameter of 594 nm and a large specific surface area of 124 m2 g−1, this allowed the mobile phase to flow through the column with low backpressure. Furthermore, the recognition abilities of the monolithic MIP in aqueous and organic media were studied. The results exhibited that the monolithic MIP possessed excellent recognition ability in aqueous media. Hydrophobic interactions, in addition to shape recognition, were the dominant effect for recognition in the mobile phase with high water content. Moreover, the binding sites and the dissociation constant were also determined by frontal chromatography as 122 μmol g−1 and 1.88 × 10−5 mol L−1, respectively, which demonstrated that the obtained SMO-MIP monolith had a high binding capacity and strong affinity ability to the template molecule. Furthermore, the resultant SMO-MIP monolith was used as HPLC column directly to determine the SMO contents in three kinds of pharmaceutical tablets with the optimized aqueous mobile phase. 相似文献
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Theophylline imprinted monolithic columns were designed and prepared for rapid separation of a homologous series of xanthine derivatives, caffeine, and theophylline by an in situ thermal-initiated copolymerization technique. Caffeine and theophylline were fully separated both under isocratic and gradient elutions on this kind of monolithic molecularly imprinted polymers (MIP) column. The broad peak showed in isocratic elution could be improved in gradient elution. Some chromatographic conditions such as mobile phase composition, flow rate, and the temperature on the retention times were investigated. Hydrogen bonding interaction and hydrophobic interaction played an important role in the retention and separation. The binding capacity was evaluated by static adsorption and Scatchard analysis, which showed that the dissociation constant (KD) and the maximum binding capacity (Qmax) were 1.50 mol/L, and 236 micromol/g for high affinity binding site, and 7.97 mol/L and 785 micromol/g for lower affinity binding site, respectively. Thermodynamic data (DeltaDeltaH and DeltaDeltaS) obtained by Van't Hoff plots revealed an enthalpy-controlled separation. The morphological characteristics of monolithic MIP were investigated by scanning electron microscope, which showed that both mesopores and macropores were formed in the monolith. The present monolithic MIP column was successfully applied for the quantitative determination of caffeine and theophylline in different kinds of green tea. 相似文献
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Rapid and efficient chiral separation of nateglinide and its L-enantiomer on monolithic molecularly imprinted polymers 总被引:6,自引:0,他引:6
A monolithic molecularly imprinted polymer (monolithic MIP) was designed and prepared for chiral separation of nateglinide and its L-enantiomer. The enantiomers were rapidly separated on this novel monolithic MIP based chiral stationary phase (MIP-CSP), whereas the enantioseparation was not obtained on the non-imprinted polymer (NIP). Chiral recognition was found to be dependent on the stereo structures and the arrangement of functional groups of the imprinted molecule and the cavities on MIP. Thermodynamic data (deltadeltaH and deltadeltaS) obtained by Van't Hoff plots revealed an enthalpy-controlled enantioseparation. The binding capacity was evaluated by frontal analysis. Monolithic nateglinide-MIP had an effective number of binding sites Bt = 41.15 micromol g(-1) with a dissociation constant of Kd = 7.40 mM. The morphological characteristics of the monolithic MIP were investigated by pore analysis and scanning electron microscope (SEM). Results showed that both mesopores and macropores were formed in the monolith. Over all, this study presents a new and practical possibility for providing high rates of mass transfer, fast separations and high efficiencies without the pressure constraints of the traditional bulk molecularly imprinted polymers, through the monolithic MIPs. 相似文献
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分子印迹整体柱快速分离烟酰胺及烟酸 总被引:6,自引:0,他引:6
以药物烟酰胺为模板分子,甲基丙烯酸为功能单体,乙二醇二甲基丙烯酸酯为交联剂,甲苯和正十二醇的混合溶液为致孔剂,采用原位聚合法制备了具有特定识别性能和分离能力的分子印迹聚合物,并将其作为高效液相色谱固定相,实现了模板分子与烟酸在2 min内的快速分离。在规格为50 mm×4.6 mm i.d.色谱柱上,以纯水为流动相(流速为7.0 mL/min)、操作温度为室温的色谱条件下,模板分子与烟酸的分离度达1.8。讨论了流动相中有机溶剂含量、醋酸及碱含量和流速对分离的影响。结果表明,原位聚合法制备的整体分子印迹聚合物在以纯水作流动相时对模板分子与其类似物有快速分离能力,这对于体内药物的分离富集研究具有很好的应用前景。 相似文献
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Molecularly imprinted monolithic columns for selective separation of enrofloxacin were prepared by Reversible Addition-Fragmentation Chain Transfer (RAFT)-mediated radical polymerization. Different ratios of initiation system were used in the synthesis. The structures of the monoliths were characterized to study the relationship between the synthetic conditions and morphology of the monolithic material. The separation performance of the monoliths was evaluated by liquid chromatography. Under optimized synthetic conditions, a monolithic molecularly imprinted polymer (MIP) with high selectivity and improved column efficiency was obtained. The research has shown that RAFT polymerization provides more adjustable conditions for making monolithic materials with different morphologies. The results also demonstrated that homogeneous macro-pore size distribution and large specific surface area are the key factors providing good separation ability and column efficiency for MIP monolithic structures. 相似文献
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A method for direct determination of DL-tetrahydropalmatine (DL-THP) in Corydalis yanhusuo, a traditional Chinese herb, by L-THP imprinted monolithic precolumn on-line/off-line coupling with reversed-phase high performance liquid chromatography (RP-HPLC) was developed. The L-THP imprinted monolithic column has been prepared by in situ polymerization using methacrylic acid (MAA) and ethylene dimethacrylate (EDMA) as functional monomer and cross-linker, respectively. With the optimization of chromatographic conditions, such as mobile phase composition, flow rate, column temperature and sample loading, for the separation of enantiomer, DL-THP was base-line separated on the MIP. The imprinted monolithic column was used as a precolumn for fractionation of the C. yanhusuo extract. Both the non-retained and retained fractions were separated by RP-HPLC. Meanwhile, the D-THP and L-THP can be detected in the non-retained and retained fractions, respectively. Additionally, direct determination of L-THP using molecularly imprinted monolith on-line coupling with a reversed-phase column was acquired. 相似文献
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This report provided the first example of using pivot concept to prepare monolithic molecularly imprinted polymers (MIPs) with ketoprofen (KET) imprints, in which metal ions were employed as mediator between the functional monomer and the template to achieve higher fidelity of imprint. To solve metal ions in pre-polymerization system, a new ternary porogen of dimethyl sulfoxide-toluene-isooctane was developed for preparation of MIP monoliths with high porosity and good permeability. The effect of polymerization parameters such as the nature of metal ions, the ratio of template to metal ion and the degree of crosslinking, on the permeability, morphology and affinity of the metal ion mediated MIP monolith were studied. The experiments demonstrated that Ni(2+), Co(2+) and Zn(2+) can be applied as pivot to prepare KET-imprinted monolith. Relative to monolithic MIP without metal ions, all the ion-mediated macropore MIP monoliths showed enhanced permeability, capacity factor and selectivity factor. High permeability (1.06×10(-7)mm(2)) was obtained on the Co(2+)-mediated MIP monolith and great selectivity factor (3.84) was achieved on the Ni(2+)-mediated one. The stoichiometric displacement model was constructed to investigate the recognition mechanism of metal-ion mediated MIP. The results indicate that metal ion as pivot not only improves the affinity but also allows the fine-tuning on the macroporous structure of MIP monolith. 相似文献
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Zian Lin Fan Yang Xiwen He Xiaomiao Zhao Yukui Zhang 《Journal of chromatography. A》2009,1216(49):8612-8622
A novel type of macroporous molecularly imprinted hybrid silica monolithic column was first developed for recognition of proteins. The macroporous silica-based monolithic skeleton was synthesized in a 4.6 mm i.d. stainless steel column by a mild sol–gel process with methyltrimethoxysilane (MTMS) as a sole precursor, and then vinyl groups were introduced onto the surface of the silica skeleton by chemical modification of γ-methacryloxypropyltrimethoxysilane (γ-MAPS). Subsequently, the molecularly imprinted polymer (MIP) coating was copolymerized and anchored onto the surface of the silica monolith. Bovine serum albumin (BSA) and lysozyme (Lyz), which differ greatly in molecular size, isoelectric point, and charge, were representatively selected for imprinted templates to evaluate recognition property of the hybrid silica-based MIP monolith. Some important factors, such as template–monomer molar ratio, total monomer concentration and crosslinking density, were systematically investigated. Under the optimum conditions, the obtained hybrid silica-based MIP monolith showed higher binding affinity for template than its corresponding non-imprinted (NIP) monolith. The imprinted factor (IF) for BSA and Lyz reached 9.07 and 6.52, respectively. Moreover, the hybrid silica-based MIP monolith displayed favorable binding characteristics for template over competitive protein. Compared with the imprinted silica beads for stationary phase and in situ organic polymer-based hydrogel MIP monolith, the hybrid silica MIP monolith exhibited higher recognition, stability and lifetime. 相似文献
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In this study, the molecular imprinting method was used to separate enantiomeric forms of chiral antidepressant drug, R,S-citalopram (R,S-CIT) in aqueous solution by CEC system combining the advantages of capillary electrophoresis (CE) and high-performance liquid chromatography (HPLC). For that, an amino acid-based molecularly imprinted monolithic capillary column was designed and used as a stationary phase for selective separation of S-citalopram (S-CIT) for the first time. S-CIT was selectively separated from the aqueous solution containing the other enantiomeric form of R-CIT, which is the same in size and shape as the template molecule. Morphology of the molecularly imprinted (MIP S-CIT) and non-imprinted (NIP S-CIT) monolithic capillary columns was observed by scanning electron microscopy. Imprinting efficiency of MIP S-CIT monolithic capillary column used for selective S-CIT separation was verified by comparing with NIP S-CIT and calculated imprinting factor (I.F:1.81) proved the high selectivity of the MIP S-CIT for S-CIT. Cavities formed for S-CIT form enabled selective (α = 2.08) separation of the target molecule from the other enantiomeric R-CIT form. Separation was achieved in a short period of 10 min, with the electrophoretic mobility of 7.68 × 10−6 m2/Vs for R,S-CIT at pH 7.0 10 mM PB and 50% ACN ratio. The performance of both MIP S-CIT and NIP S-CIT columns was estimated by repeating the R,S-CIT separations with intra-batch and inter-batch studies for reproducibility of retention times of R,S-CITs. Estimated RSD values that are lower than 2% suggest that the monolithic columns separate R,S-CIT enantiomers without losing separation efficiency. 相似文献