Highly selective separations by capillary electrochromatography: molecular imprint polymer sorbents

Molecular imprint polymers (MIPs) are synthesized in the presence of a template, or 'imprint' molecule which results in the formation of specific recognition cavities complementary to the template in shape and chemical functionality. The resultant MIP then acts as a selective binding medium for the template molecule. The utility of MIPs lies in the selectivity of the rebinding process, which is based on molecular recognition. In many cases, the selectivity achieved with MIPs toward a particular molecule is comparable to that observed with antibodies. This has led to the application of MIPs to several areas of analytical chemistry including immunoassays, sensors and separations media. One of the most successful application areas of MIPs has been as chromatographic sorbents, where they have been utilized predominately in chiral separations. The use of MIP sorbents in CEC is attractive in that it combines the selectivity of a molecular recognition process with the enhanced flow dynamics of CEC, which can result in higher efficiency and shorter analysis times. This paper will review the use of molecular imprinted stationary phases in CEC. Following a brief introduction to molecular imprinting, various methodologies for preparation of MIP-CEC capillaries in addition to applications of the technique will be discussed.     

分子烙印聚合物对抗胆碱能类药物的选择性固相吸附行为研究

以3种结构类似的抗胆碱能药物盐酸新托品(1116)、盐酸苯环壬酯(8021)和盐酸戊乙奎醚(8018)为模板分子合成分子烙印聚合物,采用固相萃取-高效液相色谱法(SPE-HPLC)考察各MIP对乙腈溶液中结构类似的药物1116、8021、8018及盐酸卡马特灵(1113)、氯苯那敏(CPA)和樟柳碱(AT3)的固相吸附行为,探讨MIP特异性识别的影响因素及机理。结果表明,在MIP合成中,功能单体、交联剂及引发剂的种类和用量、引发方式、模板分子与功能单体的比例等因素对MIP的特异性识别能力均有重要影响。以1116、8021和8018为模板分子、甲基丙烯酸(MAA)为功能单体、三羟甲基丙烷三甲基丙烯酸酯(TRIM)为交联剂,在乙腈中合成的各MIP均表现出较强的特异性识别能力。其中,MIP对待测物的非特异性吸附主要由其网状结构表面游离的极性基团引起;MIP的特异性识别过程中,识别位点与待测物的空间结构匹配起着更为重要的作用。     

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.     

Molecularly Imprinted Electrochemical Sensors

In this review, the applications of molecularly imprinted polymer (MIP) materials in the area of electrochemical sensors have been explored. The designs of the MIPs containing different polymers, their preparation and their immobilization on the transducer surface have been discussed. Further, the employment of various transducers containing the MIPs based on different electrochemical techniques for determining analytes has been assessed. In addition, the general protocols for getting the electrochemical signal based on the binding ability of analyte with the MIPs have been given. The review ends with describing scope and limitations of the above electrochemical based MIP sensors.     

Preparation and computational investigation of molecular imprinted polymers for Clidinium Bromide

Molecular imprinted polymers (MIPs) are polymers that possess recognition sites specific for a predetermined target molecule (Template). Inspired by the idea of biological natural receptors, they behave like synthetic molecular recognition elements. They have been developed into a promising tool in several crucial applications, including analytical methods, drug delivery, and catalysis. The non-covalent imprinting is more commonly used approach in the preparation of MIPs because of its simplicity. In this approach, intermolecular interactions between the template molecule (T) and the functional monomer (FM) are the forces that govern the performance of the resulting MIP. Hence, studying these interactions is very important to elucidate and understand the imprinting mechanism. This paper focuses on preparation of two MIPs for a Clidinium Bromide (CB), using two different types of FMs. These MIPs are characterized by using IR and SEM techniques. Adsorption isotherm properties to CB are assayed for them. Then the structures of the pre-polymerization complexes of prepared MIPs were investigated using Density Functional Theory (DFT) calculations at B3LYP/6-31G level in a vacuum and other media. Finally, Bader's Quantum Theory of Atoms in Molecules (QTAIM) was used to prove the existence and nature of intermolecular interactions between CB and FM. The theoretical results were in complete agreement with experiments and indicated that the use of AM as FM is preferred over MA in the MIP preparation for CB.     

Molecularly imprinted beads by surface imprinting

Molecular imprinting is a state-of-the-art technique for imparting molecular recognition properties to a synthetic polymeric matrix. Conventionally, the technique is easily carried out using bulk imprinting, where molecularly imprinted polymers (MIPs) are prepared in large chunks and post-treatment processes like grinding and sieving are then required. However, this strategy tends to produce sharp-edged, irregular MIP bits with a limited scope of direct application. In addition, due to the creation of binding sites within the polymeric bulk, the issue of the hindrance of adsorbate diffusion (especially in the case of macromolecules) during template rebinding makes the MIPs prepared through this approach unsuitable for practical applications. Thus over the years, many efforts to address the limitations of conventional molecular imprinting techniques have resulted in new imprinting methodologies. Systems like suspension and precipitation polymerization, where MIPs with tunable morphologies can be prepared, have been developed. Additionally, strategies like surface imprinting have also been employed. Ultimately, both of these approaches have been combined to prepare regularly shaped surface-imprinted MIP beads. Such an approach incorporates the advantages of both methodologies at the same time. Given their desirable physical morphologies and favorable adsorption kinetics, MIPs prepared in this manner show significant promise for industrial applications. Therefore, they will be the main focus of this review.     

对羟基苯甲酸、水杨酸分子印迹聚合物分子识别性质的 研究

以对羟基苯甲酸(4-HBA)为模板分子,4-乙烯吡啶(4-Vpy)为功能单体,制备得到了4-HBA分子印迹聚合物P(4-HBA),研究了该聚合物的分子识别机理,并与在同样条件下制备的水杨酸(SA)分子印迹聚合物P(SA)进行了分子识别能力的比较。结果表明：P(SA)比P(4-HBA)具有更好的分子识别能力。这是由于SA的酸性较4-HBA强,因此与碱性功能单体4-Vpy之间的静电作用更强,从而得到的复合物更稳定。本实验结果证明：功能单体与模板分子形成稳定的复合物是得到分子识别能力高的模板聚合物的前提条件。本文将有助于对分子印迹的过程以及分子印迹聚合物分子识别机理的进一步理解,并且对于根据模板分子的性质预测MIP的分子识别能力也将具有一定的指导意义。     

Molecularly imprinted polymers—potential and challenges in analytical chemistry

Among the variety of biomimetic recognition schemes utilizing supramolecular approaches molecularly imprinted polymers (MIPs) have proven their potential as synthetic receptors in numerous applications ranging from liquid chromatography to assays and sensor technology. Their inherent advantages compared to biochemical/biological recognition systems include robustness, storage endurance and lower costs. However, until recently only few contributions throughout the relevant literature describe quantitative analytical applications of MIPs for practically relevant analyte molecules and real-world samples. Increased motivation to thoroughly evaluate the true potential of MIP technology is clearly attributed to the demands of modern analytical chemistry, which include enhanced sensitivity, selectivity and applicability of molecular recognition building blocks at decreasing costs. In particular, the areas of environmental monitoring, food and beverage analysis and industrial process surveillance require analytical tools capable of discriminating chemicals with high molecular specificity considering increasing numbers of complex environmental contaminants, pollution of raw products and rigorous quality control requested by legislation and consumer protection. Furthermore, efficient product improvement and development of new products requires precise qualitative and quantitative analytical methods. Finally, environmental, food and process safety control issues favor the application of on-line in situ analytical methods with high molecular selectivity. While biorecognition schemes frequently suffer from degrading bioactivity and long-term stability when applied in real-world sample environments, MIPs serving as synthetic antibodies have successfully been applied as stationary phase separation matrix (e.g. HPLC and SPE), recognition component in bioassays (e.g. ELISA) or biomimetic recognition layer in chemical sensor systems. Examples such as MIP-based selective analysis of flavones/flavonoids in wine, the determination of mycotoxins in beverages and analysis of organic contaminants in environment samples will elucidate the perspectives of this technology and will be contrasted with the challenges of rational MIP design providing control on binding site density, receptor capacity and selectivity.     

Synthesis and chromatographic evaluation of molecularly imprinted polymers prepared by the substructure approach for the class-selective recognition of glucuronides

Two series of molecularly imprinted polymers (MIPs) for the class-selective recognition of glucuronides have been prepared by using lipophilic substructures of the target analyte as template molecule and potent host monomers against oxyanions, that are expected to establish a strong stoichiometric interaction with the single carboxylic group of the template. The polymers were tested as stationary phases in liquid chromatography for specific recognition. A preliminary investigation of the imprinting properties of eleven MIPs was carried out, by comparing the retention time of the template and of structurally related compounds on the MIP column with that on the corresponding non-imprinted polymer (NIP). The two polymers showing the best performance were selected to further test cotinine, mycophenolic acid, testosterone and their respective glucuronides as model compounds. The high specificity obtained against glucuronides and the different chemical structure of the parent drug make the two MIPs class-selective imprinted receptors, also suitable for SPE application.     

Retentivity and enantioselectivity of uniformly-sized molecularly imprinted polymers for (S)-nilvadipine in aqueous and non-aqueous mobile phases.

Uniformly-sized molecularly imprinted polymers (MIPs) for (S)-nilvadipine have been prepared by a multi-step swelling and polymerization method using methacrylic acid or 4-vinylpyridine (4-VPY) as a functional monomer, ethylene glycol dimethacrylate (EDMA) as a cross-linker, and toluene, chloroform, cyclohexanol or phenylacetonitrile as a porogen. The chiral recognition abilities of the MIPs for nilvadipine were evaluated using aqueous and non-aqueous mobile phases. Among the MIPs, the (S)-nilvadipine-imprinted 4-VPY-co-EDMA polymers prepared using toluene as a porogen showed the highest recognition ability for nilvadipine in both aqueous and non-aqueous mobile phases. In addition to molecular shape recognition, hydrogen-bonding interactions of the NH proton of nilvadipine with a pyridyl group of the (S)-nilvadipine-imprinted 4-VPY-co-EDMA polymers could play an important role in the retention and chiral recognition of nilvadipine in aqueous and non-aqueous mobile phases. Furthermore, the MIP for (S)-nilvadipine gave the highest molecular recognition ability when a porogenic solvent during polymerization was used as the mobile phase modifier.     

The complete replacement of antibodies by protein-imprinted poly(ethylene-co-vinyl alcohol) in sandwich fluoroimmunoassays

The replacement of antibodies by molecularly imprinted polymers (MIPs) has been investigated for many decades. However, indirect protocols (including natural primary and secondary antibodies) are still utilized to evaluate the ability of MIP thin films to recognize target molecules. MIPs can be prepared as either a thin film or as particles, and cavities that are complementary to the template can be generated on their surfaces. We have prepared thin film MIPs and particle MIPs prepared by solvent evaporation and phase inversion, respectively, from solutions of poly(ethylene-co-vinyl alcohol) (pEVAL) in the presence of the target analytes amylase, lysozyme, and lipase. These were first adsorbed on MIP thin films and by MIP particles that contain fluorescent quantum dots. Sandwich fluoroimmunoassays were then conducted to quantify them in MIP-coated 96-well microplates. The method was applied to determine amylase in saliva, and results were compared with a commercial analytical system.

Recent advances on noncovalent molecular imprints for affinity separations

Molecularly imprinted polymers (MIPs) are tailor-made synthetic materials capable of selectively rebinding a target analyte, or a group of structurally related compounds based on a combination of recognition mechanisms including size, shape, and functionality. Among the advantageous properties of MIPs are the achievable specific affinity, the relative ease of preparation, and their mechanical and chemical robustness, which renders them ideal materials for applications as stationary phase (e. g., affinity chromatography or SPE), or as antibody mimics (e. g., biomimetic assays). Here, we review recent advancements on the application of MIPs in affinity separations and biomimetic assays, which have focused on the synthesis of size- and shape-uniform particles facilitating reproducibility, improved binding site accessibility, and enhanced affinity. While MIPs certainly offer promising potential as selective separation phase in a variety of applications, deeper understanding of the fundamental interactions governing imprinting, and rational understanding of the imprinting mechanism has yet to be achieved for providing rational guidelines in deliberately designing next-generation MIP materials.     

Examination of Template Structural Effects on CEC Chiral Separation Performance of Molecule Imprinted Polymers Made by a Generalized Preparation Protocol

Some acidic chiral templates were used to prepare open tubular (OT) molecule imprinted polymer (MIP) capillary columns to explore the effects of molecular structures of templates on chiral recognition capabilities and to verify the feasibility of the general MIP preparation protocol introduced in the previous study. The templates are phenyl carboxylic acids and their derivatives. Optimization was carried out for chiral separation of template enantiomers for each MIP column through varying pH and composition of eluent. It was found that the preparation protocol can be successfully applied for the appropriate templates with functional groups fulfilling the three-points interaction rule. The chiral separation performances were quite satisfactory for MIPs of such templates although they are yet inferior to the separation performances of the MIP columns fabricated with the templates of profen drugs (2-arylpropionic acids with a large substituent on the phenyl ring). Subtle variations of the template molecular structures have been found to be critical to enhance chiral recognition ability of the resultant MIP column.     

An insight into molecularly imprinted polymers for capillary electrochromatography

Molecularly imprinted polymers (MIPs) are actively being developed as a practical tool for affinity chromatographic supports. From the viewpoint of separation science, capillary electrochromatography (CEC) might be one of the more promising chromatographic techniques to be used in combination with the MIPs. However, up to the present, very little MIP work has involved CEC. This review gives a full overview of MIP including current trends in MIP, methods for the characterization of MIP, and methods for the preparation of MIP with particular emphasis on application of the resulting materials in CEC. To prepare MIPs with selectivity predetermined for a particular substance or group of structural analogues is an important factor for the development of a new format of CEC. From the fundamental research with the batch method, a better knowledge of imprint formation and imprint recognition will be helpful for expanding the application area of the combination of MIPs with CEC.     

Selective sample treatment using molecularly imprinted polymers

The molecularly imprinted polymers (MIPs) are synthetic polymers possessing specific cavities designed for a target molecule. By a mechanism of molecular recognition, the MIPs are used as selective sorbents for the solid-phase extraction of target analytes from complex matrices. MIPs are often called synthetic antibodies in comparison with immuno-based sorbents; they offer some advantages including easy, cheap and rapid preparation and high thermal and chemical stability. This review describes the use of MIPs in solid-phase extraction with emphasis on their synthesis, the various parameters affecting the selectivity of the extraction, their potential to selectively extract analytes from complex aqueous samples or organic extracts, their on-line coupling with LC and their potential in miniaturized devices.     

Preparation,evaluation and characterization of quercetin-molecularly imprinted polymer for preconcentration and clean-up of catechins

Molecularly imprinted polymer (MIP) for solid extraction and preconcentration of catechins have been successfully prepared by a thermal polymerization method using quercetin as template, 4-vinylpyridine as functional monomer and ethylene glycol dimethacrylate as crosslinker. A solution mixture of acetone and acetonitrile was used as porogen. Systematic investigations of the influence of monomer, cross-linker, porogen, as well as polymerization conditions on the properties of the MIPs were carried out. The quercetin MIPs were evaluated according to their selective recognition properties for quercetin, structurally related compounds (catechin, epigallocatechin gallate and epicatechin) and a unrelated compound of similar molecular size (α-tocopherol). Good binding was observed for quercetin, catechin and epigallocatechin gallate with an optimized MIP in a solid phase extraction system. Adsorption and kinetic characteristics were evaluated for catechins which indicated that the synthesized polymer had high adsorption capacity and contained homogeneous binding sites. Chemical and morphological characterization of the MIP was investigated by FTIR, SEM and BET, which confirmed a high degree of polymerization. Finally, the MIP was successfully applied to the clean-up and preconcentration of catechins from several natural samples.     

Molecular Recognition Ability of Molecularly Imprinted Polymer Nano- and Micro-Particles by Reversible Addition-Fragmentation Chain Transfer Polymerization

The role of molecularly imprinted polymers (MIPs) is changing from academic to applied researches. Challenging problems about MIP will be more highlighted in applicable uses and solving these problems is vital. The controlled/“living” radical polymerization (CLRP) techniques are applicable to solve the challenging problems in MIPs. The “living” nature of CLRP helps to improve the heterogeneity of binding sites in MIPs as a main challenge where precise control over sizes, compositions, and surface functionalities is achieved. Among different techniques of CLRP, reversible addition-fragmentation chain transfer (RAFT) technique presents distinguished benefits such as compatibility and tolerance to a wide range of functional monomers and mild reaction conditions rather than other CLRP techniques. In this review, in order to obtain more insights into the potential benefits of RAFT polymerization in fabrication of nano and micro MIP networks, recent research in advanced MIP materials for different templates with improved morphology, efficiency, and binding capacities with respect to traditional free radical polymerization (FRP) will be discussed. MIPs prepared via RAFT method have advantages of MIPs as high performance molecular recognition devices and CLRP as controllable polymerization mechanism, simultaneously.     

Uniformly-sized, molecularly imprinted polymers for (-)-epigallocatechin gallate, -epicatechin gallate and -gallocatechin gallate by multi-step swelling and polymerization method

Uniformly-sized, molecularly imprinted polymers (MIPs) for (-)-epigallocatechin gallate (EGCg), -epicatechin gallate (ECg) and -gallocatechin gallate (GCg) were prepared by a multi-step swelling and polymerization method using 2-vinylpyridine as a functional monomer, ethylene glycol dimethacrylate as a cross-linker and cyclohexanol as a porogen. Molecular recognition abilities of the obtained MIPs were evaluated in liquid chromatography using a mixture of ethanol and water, or ethanol as the eluent. Each MIP gave the highest molecular recognition ability for the respective template molecule. In addition, (-)-EGCg and -ECg had the same configuration (2R,3R) at positions 2 and 3, and therefore resulting in high cross reactivity each other. However, (-)-GCg, which has different configuration at position 2 with (-)-EGCg and -ECg, showed low cross reactivity with them. On the other hand, those MIPs showed no molecular recognition against (-)-epigallocatechin and -epicatechin, which have no gallate group at position 3. These results indicate that the MIPs prepared can recognize configuration at position 2 and a gallate group at position 3. Furthermore, the MIP for (-)-GCg could be successfully used for isolating (-)-EGCg and -ECg from green tea extract.     

Application of multivariate analysis to the screening of molecularly imprinted polymers for bisphenol A

A key issue in the synthesis of molecularly imprinted polymers (MIPs) is the identification and optimisation of the main factors that affect the material structure and its molecular recognition properties. This paper describes the application of an experimental design and multivariate analysis method for the synthesis of bisphenol A (BPA)-selective MIPs. Six factors with a large impact on the MIP synthesis and its analytical performance have been optimised: the amount of template, the type and the percentage of functional and cross-linking monomers, the polymerisation method (i.e. thermal or UV initiation) and the porogenic solvent. The polymers have been prepared in small-scale (mini-MIPs) and, after careful removal of the template, their BPA rebinding capacity has been evaluated and related to the MIP composition. Among the two functional monomers tested, namely 4-vinylpyridine (4-vpy) and methacrylic acid (MAA), the former rendered the best selectivity for BPA analysis. The partial least squares (PLS) models revealed that the photoinitiated polymers with a 1:1 ratio of 4-vinylpyridine to cross-linker (EDMA or TRIM) yield the highest specific binding. Such procedure is time and cost effective and can be used as a general tool in the preparation of MIPs for different analytes.