Molecular Imprinting of Cyclodextrins Leading to Synthetic Antibodies

Molecularly imprinted cyclodextrins were applied to HPLC stationary phases forefficient recognition of nano-scaled guests in water. When cholesterol was usedas a template molecule, the imprinted polymer selectively retained this guest morestrongly and selectively than did non-imprinted polymer. The imprinting effect inthe retention behavior was consistent with previously reportedphysicochemical analyses.Immobilization of the imprinted cyclodextrin polymer on the surfaceof silica gel in water was also successful. The polymer-silica gel compositesobtained had sufficient physical strength, and were useful for HPLC stationary phases. Thesemolecularly imprinted polymers could recognize steroids, amino acid derivatives,dipeptides, and antibiotics. Moreover, we found that the enantio-selectivity towardthe template molecules was significantly promoted. This methodology has greatpotential for the recognition of large guest molecules in water, and can be analternative to affinity chromatography for the separation of bio-molecules.     

Use of Chemically Bonded β‐Cyclodextrin Silica Stationary Phase for Liquid Chromatographic Separation of Structural Isomers

The retention behavior of five disubstituted benzene derivatives and two naphthalene derivatives is examined by using a chemically bonded β‐cyclodextrin silica stationary phase with the moiety containing the s‐triazine. The chromatographic results of five disubstituted benzene derivatives and two naphthalene derivatives show that effective separation is achieved on this stationary phase by high‐performance liquid chromatography. The results of the present investigation indicate that the formation of inclusion complexes plays a dominant role in the separation mechanism. However, the selectivity can be significantly enhanced by the n‐n interactions between the s‐triazine ring of the chemically bonded β‐cyclodextrin silica stationary phase and the aromatic ring of solutes. For example, the effective separation of the o‐, m‐, and p‐toluidine isomers on this stationary phase with the moiety containing the s‐triazine ring was better than on that of some β‐cyclodextrin bonded stationary phases without the moiety containing s‐triazine ring.     

Urea bonded cyclodextrin derivatives onto silica for chiral HPLC

Several structurally well-defined perfunctionalised cyclodextrin chiral stationary phases (CD CSPs) for high performance liquid chromatography have been successfully prepared by immobilisation of perfunctionalised cyclodextrins on silica through urea linkage(s) using the Staudinger reaction. These CSPs show high chiral recognition efficiency and are utilised in the resolution of various types of racemic compounds. This paper reviews the development of sixteen perfunctionalised cyclodextrin-based CSPs, their preparation, and their application to enantioseparation of seventy-seven racemic compounds under a range of separation conditions.     

氮杂冠醚、环糊精混合功能基键合硅胶液相色谱固定相的合成与评价

冠醚键合固定相主要用于一些无机离子的分离,我们用连续固液相法合成了一系列冠醚键合硅胶固定相,并成功地用于有机化合物的分离［１～４］;β－ＣＤ的内腔疏水而外缘亲水,可以选择性地包结含苯环及萘环的化合物,且具有手性拆分能力,已被用于手性色谱固定相［５,...     

Development of dinitrophenylated cyclodextrin derivatives for enhanced enantiomeric separations by high-performance liquid chromatography

The synthesis and evaluation of new dinitrophenyl (DNP) substituted beta-cyclodextrin (beta-CD) chiral stationary phases (CSPs) for the enantioseparation of various classes of chiral analytes by HPLC are presented. The dinitrophenyl substituted beta-CD derivatives are synthesized and covalently bonded to functionalized 5 microm spherical porous silica gel. These are the first reported derivatized cyclodextrin which contains pi-electron deficient substituents (i.e., pi-acidic moieties). The column performance in terms of their ability to separate enantiomers is evaluated. A variety of different dinitro-substituted aryl groups are investigated and compared. The pH of the mobile phase buffers, the buffer composition, the number and position of the dinitro groups on the phenyl ring substituent, the degree of substitution, and the bonding strategy all greatly affect the performance of the CSPs. A large variety of racemic compounds have been separated successfully on these CSPs. The bonded dinitrophenyl-derivatized cyclodextrins are stable in all three mobile phase modes, namely, the reversed-phase, polar organic, and normal phase modes. No degradation in column performance was observed in any mode of operation even after more than 1000 injections. The analytical applicability of these types of CSPs for enantiomeric separations is discussed in detail.     

Cyclodextrin carbamates as novel chiral stationary phases for capillary gas chromatography

The following carbamate derivatives of cyclodextrins (CDs) were prepared as novel chiral stationary phases for capillary gas chromatography: hexakis(2,6-di-O-pentyl)-α-cyclodextrin hexa(3-n-propyl, 3-isopropyl, and 3-phenylcarbamate), heptakis-(2,6-di-O-pentyl)-β-cyclodextrin hepta(3-n-propyl, 3-isopropyl, and 3-phenylcarbamate), and octakis(2,6-di-O-pentyl)-γ-cyclodextrin octa(3-n-propyl, 3-isopropyl, and 3-isopropyl, and 3-phenylcarbamate). Metal capillary columns coated with these stationary phases resolved many kinds of racemic mixture. In general, they were especially effective towards polar compounds such as free alcohols, amines, and epoxides. The types of sample which were effectively resolved depended on the cavity size of the CD: α-CD derivatives were specifically effective toward compounds having linear alkyl chains, and β-CD derivatives toward compounds with phenyl groups. The results indicate that chiral separation with the cyclodextrin carbamates depends on the formation of inclusion complexes and also on the hydrogen-bonding interactions between the samples and the CD carbamates.     

Separation of isomeric naphthalenesulphonic acids by micro high-performance liquid chromatography with mobile phases containing cyclodextrin

Aromatic sulphonic acids are important dye intermediates and the determination of the individual isomers after their preparation by sulphonation of the parent aromatic hydrocarbon is important for the monitoring of the dye production process. For this purpose, either reversed-phase chromatography with mobile phases containing strong electrolytes as additives or capillary zone electrophoresis with working electrolytes containing cyclodextrins can be used to separate and determine not only individual sulphonation products with various numbers of sulphonic groups, but also various isomeric di- and trisulphonic acids. However, the separation of some isomers using either of the two techniques is not fully satisfactory. In the present work, HPLC with mobile phases containing cyclodextrins was employed to improve previously achieved separations of aromatic sulphonic acids. Because of the high cost of cyclodextrin, microcolumn HPLC with diode-array detection on the columns prepared in laboratory by supercritical fluid packing technique was employed for this purpose. Capillary columns packed with various octadecyl silica gel materials were compared and their stability and efficiency were found suitable for the separation of the compounds tested. The selectivity of separation of some isomers improved significantly with respect to the previous methods. Procedures were designed for separation and analytical control of technological processes producing dye intermediates.     

全衍生化羟丙基-β-环糊精固定相的制备及应用

研究了3, 5-二甲基苯基异氰酸酯对羟丙基-β-环糊精固定相的手性识别影响.通过异氰酸丙基三乙氧基硅烷作偶联剂,将羟丙基-β-环糊精键合到3-氨丙基硅烷化硅胶上,再用3, 5-二甲基苯基异氰酸酯对β-环糊精和硅胶其余羟基进行衍生化,制得一种新型的3, 5-二甲基苯基氨基甲酸酯全衍生化羟丙基-β-环糊精键合硅胶手性固定相.在反相色谱条件下,对9种手性药物进行了拆分,结果表明,3, 5-二甲基苯基氨基全衍生化固定相较之羟丙基-β-环糊精固定相有更好的分离效果.     

Dendrimer-Like Chiral Stationary Phases Derived from (1R, 2R)-(+)-1,2-Diphenylethylenediamine and 1,3,5-Benzenetricarbonyl Trichloride

Three dendrimers were synthesized directly on aminated silica gel using (1R, 2R)-(+)-1,2-diphenylethylenediamine and 1,3,5-benzenetricarbonyl trichloride as building blocks. The chiral stationary phases were obtained by modification of these dendrimers with phenyl isocyanate. All derivatives prepared on silica gel were characterized by FTIR spectrum, solid-state ¹H NMR and elemental analysis. The enantioseparation ability of the chiral stationary phases was preliminarily evaluated by high-performance liquid chromatography. The chiral stationary phase of one-generation dendrimer exhibited best enantioseparation ability.     

A new single‐urea‐bound 3,5‐dimethylphenylcarbamoylated β‐cyclodextrin chiral stationary phase and its enhanced separation performance in normal‐phase liquid chromatography

A new single‐urea‐bound chiral stationary phase based on 3,5‐dimethylphenylcarbamoylated β‐cyclodextrin was prepared through the Staudinger reaction of mono (6^A‐azido‐6^A‐deoxy)‐per(3,5‐dimethylphenylcarbamoylated) β‐cyclodextrin and 3‐aminopropyl silica gel under CO₂ atmosphere. The new phase exhibited good enantioseparation performance for 33 analytes using normal‐phase HPLC conditions; 19 of them were baseline separated. Effects of structure of analytes, alcoholic modifiers, and acidic/basic additives on separation performances of this new cyclodextrin chiral stationary phase have been studied in detail. The results showed that the retention and resolution of acidic and basic analytes on the CSP were greatly affected by the additives. Peak symmetry for some analytes could be improved by simultaneously adding acidic and basic additives to the mobile phase. This work expands the potential applications of the cyclodextrin‐based chiral stationary phases in the normal‐phase HPLC.     

Preparation of chiral oxazolinyl‐functionalized β‐cyclodextrin‐bonded stationary phases and their enantioseparation performance in high‐performance liquid chromatography

A simple procedure for the synthesis of three new oxazolinyl‐substituted β‐cyclodextrins (6‐deoxy‐6‐R‐(–)‐4‐phenyl‐4,5‐dihydrooxazolinyl‐β‐cyclodextrin, 6‐deoxy‐6‐S‐(–)‐4‐phenyl‐4,5‐dihydrooxazolinyl‐β‐cyclodextrin, and 6‐deoxy‐6‐S‐(–)‐(4‐pyridin‐1‐ium‐4‐methyl‐benzenesulphonate)‐4,5‐dihy‐drooxazolinyl‐β‐cyclodextrin) and their covalent bonding to silica are reported. The ability of these chiral stationary phase columns for separating compounds is also presented and discussed. Twenty‐eight compounds were examined in the polar‐organic mobile phase mode, and 11 β‐nitroethanols were tested in the reversed‐phase mode. Excellent enantioseparations were achieved for most of the analytes, even for several challenging compounds. The rigid and flexible structures of mono‐substituted chiral groups and the fragments around the rim of the β‐cyclodextrin cavity played an important role in the separation process. Factors such as π–π stacking, dipole–dipole interactions, ion‐pairing, and steric hindrance effects were found to affect the chromatographic performance. Moreover, the buffer composition, and percentages of organic modifiers in the mobile phase, were investigated and compared. The mechanisms involved in the separation were postulated based on the chromatographic data.     

COVALENTLY BONDING CHIRAL POLYURETHANE ON AMINATED SILICA GEL： A NEW STRATEGY TO PREPARE CHIRAL STATIONARY PHASE FOR HIGH PERFORMANCE LIQUID CHROMATOGRAPHY

Two polyurethanes of different molecular weights were prepared by the copolymerization of phenyl diisocyanate and diisopropyl tartrate. The polyurethanes having terminal isocyanate groups were reacted with 3-aminopropyl silica gel to afford two chiral stationary phases. The Mn of the two polyurethanes were 4057 g/mol and 6442 g/mol. The polyurethanes and the corresponding chiral stationary phases were characterized by FT-IR, 1H NMR and elemental analysis. The loading capacities of the polyurethanes on silica gel were 0.68 mmol units/g and 0.61 mmol units/g, respectively. The separation performance and the influence of additives, triethylamine and trichloroacetic acid, on the separation of chiral compounds were investigated by HPLC. The chiral stationary phase prepared from polyurethane with Mn of 4057 g/mol demonstrated better enantioseparation capability than that with Mn of 6442 g/mol. Additionally, it was found that the addition of triethylamine and trichloroacetic acid in the mobile phases significantly improved the enantioseparation for these two chiral stationary phases.     

Preparation of pyrenebutyric acid bonded silica stationary phases for the application to the separation of fullerenes

A novel immobilization method was proposed for the preparation of pyrenebutyric acid-bonded silica (PYB-silica) stationary phases. The pyrene moiety was grafted to silica gel through spacers of aminoalkyl silanes. The HPLC separation of C60, C70 and higher fullerenes on the new pyrenebutyric acid-bonded silica stationary phases was also studied. Based on the temperature effect, the intermolecular interaction between stationary phases and solutes and the retention mechanism were discussed. The results of column loading capacity test demonstrated the potential for the separation of fullerenes in large amounts on the PYB-silica stationary phases.     

环糊精衍生物气相色谱手性固定相研究进展

评述近年环糊精衍生物气相色谱手性固定相的研究进展,对环糊精衍生物进行分类并总结了近年来其在GC手性分离上的应用,介绍环糊精衍生物的手性分离机制及纯度问题进展,展望环糊精衍生物作GC手性固定相的应用前景。     

Click regulation of cyclodextrin primary face for the preparation of novel chiral stationary phases

In this study, a series of novel CD chiral stationary phases were fabricated by immobilization of mono‐6^A‐deoxy‐N₃‐cyclodextrin onto silica surfaces followed by click regulation of CD primary face with 4‐pentynoic acid (acidic moiety), 2‐propynylamine (alkaline moiety) and L‐propargylglycine (chiral amino acid moiety), respectively. Enantioseparations of various kinds of racemates including dansyl‐amino acids, chiral lactides and diketones were conducted in reversed phase modes on these chiral stationary phases, where nearly forty diketones and chiral lactides were firstly separated on cyclodextrin stationary phases. 4‐Pentynoic acid moiety can make the retention ability decline while amine moiety significantly enhanced the retention ability of the stationary phases. For most of the studied analytes, the chiral amino acid moiety had the most positive effects on both the retention time and the resolution. The inclusion complexation between chiral analytes and cyclodextrins were also investigated by fluorescence method.     

Synthesis of cationic beta-cyclodextrin derivatives and their applications as chiral stationary phases for high-performance liquid chromatography and supercritical fluid chromatography

Four cationic beta-cyclodextrin derivatives, namely mono-6-(3-methylimidazolium)-6-deoxy-perphenylcarbamoyl-beta-cyclodextrin chloride (MPCCD), mono-6-(3-methylimidazolium)-6-deoxyper(3,5-dimethylphenylcarbamoyl)-beta-cyclodextrin chloride (MDPCCD), mono-6-(3-octylimidazolium)-6-deoxyperphenylcarbamoyl-beta-cyclodextrin chloride (OPCCD) and mono-6-(3-octylimidazolium)-6-deoxyper(3,5-dimethylphenylcarbamoyl)-beta-cyclodextrin chloride (ODPCCD), have been synthesized and physically coated onto porous spherical silica gel to obtain novel chiral stationary phases (CSPs). The performances of these CSPs are studied on high-performance liquid chromatography (HPLC) and supercritical fluid chromatography (SFC) using 18 racemic aryl alcohols as test analytes. Among these four CSPs, OPCCD shows the best separation results for all analytes on both HPLC and SFC analyses. Chromatographic studies reveal that the CSPs consisting of an n-octyl group on the imidazolium moiety and phenylcarbamoyl groups on the cyclodextrin ring provide enhancement of analyte-chiral substrate interactions over CSPs bearing the methyl group on the imidazolium moiety and 3,5-dimethylphenylcarbamoyl groups on the cyclodextrin ring.     

Aspects of surface modification, structure characterization, thermal stability and metal selectivity properties of silica gel phases-immobilized-amine derivatives

Four silica gel phases-bound-amine derivatives (I-IV) were prepared based on chemical immobilization technique. The surface modification was identified by determination of the coverage values in mmol g⁻¹ via thermal desorption method (1.463-1.807) and elemental analysis of nitrogen and carbon contents (1.089-2.456). Structure characterization related to immobilization of the amine derivatives was accomplished and evaluated by means of infrared (IR) and secondary ion mass spectrometric (SIMS) technique. The modified silica gel phases (I-IV) along with their interaction products with copper(II) were also examined by electron impact mass spectrometric analysis (EI-MS) as a method for evaluation of their thermal stability and structure elucidation. Potentiometric titration as a method of characterization was applied for the modified silica gel phases (II-IV) and their copper(II)-adduct. A series of bi- and trivalent metal ions were selected to focus more aspects of the selectivity properties incorporated into the modified silica gel phases for binding and interaction with these metals based on determination of the distribution coefficient and separation factor. The results of these evaluation processes were found to prove higher selectivity and preference of these four phases for binding with lead(II) and cadmium(II) compared to other metal ions.     

Enantiomer separation of chiral pharmaceuticals by capillary electrochromatography

Enantiomer separation of chiral pharmaceuticals by capillary electrochromatography (CEC) is achieved with open-tubular capillaries (o-CEC), with packed capillaries (p-CEC) or with monolithic capillaries. In o-CEC, capillaries are coated with a thin film containing cyclodextrin derivatives, cellulose, proteins, poly-terguride or molecularly imprinted polymers as chiral selectors. In p-CEC, typical chiral HPLC stationary phases such as silica-bonded cyclodextrin or cellulose derivatives, proteins, glycoproteins, macrocyclic antibiotics, quinine-derived and 'Pirkle' selectors, polyacrylamides and molecularly imprinted polymers are used as chiral selectors. Chiral monolithic stationary phases prepared by in situ polymerization into the capillary were also developed for electrochromatographic enantiomer separation.     

Comparison of enantioseparation of selected benzodiazepine and phenothiazine derivatives on chiral stationary phases based on β‐cyclodextrin and macrocyclic antibiotics

Enantioselective separation of some phenothiazine and benzodiazepine derivatives was studied on six different chiral stationary phases (CSPs) in HPLC. Selected CSPs, with respect to the structure of the separated compounds, were either based on β‐cyclodextrin chiral selectors – underivatized β‐cyclodextrin and hydroxypropyl ether β‐cyclodextrin, or on macrocyclic antibiotics – vancomycin, teicoplanin, teicoplanin aglycone, and ristocetin A. Measurements were carried out in a reversed‐phase separation mode. The influence of mobile phase composition on retention and enantioseparation was studied. Benzodiazepines could be enantioresolved with almost all the chiral stationary phases used, except for the vancomycin‐bonded CSP. Peak coalescence of oxazepam and lorazepam was observed if separation was carried out at laboratory temperature. Reduced temperature was required in some instances in order to avoid the on‐column racemization. Separation systems composed of teicoplanin‐bonded CSP and buffer‐methanolic or pure methanolic mobile phases were shown to be suitable even for preparative purposes due to high resolution values of the enantiomers. Enantioseparation of phenothiazine derivatives was more difficult to achieve but it was successful, at least partly, also with both types of the CSPs used (except for levomepromazine).     

Cyclodextrin dimer derivatives used as stationary phase for capillary gas chromatography

Summary Four cyclodetrin dimer derivatives were synthesized by linking two single cyclodextrin derivatives with difunctional spacer at the primary side of cyclodetrin. The separation properties of these cylodextrin dimer derivatives as CGC stationary phases were investigated and compared with those of the unbridged native cyclodextrin derivative. The results show that two recognition sites and one link spacer of these cyclodextrin dimer derivatives cooperate in separation and affect the separation of disubstituted benzene positional isomers.