维拉帕米和布比卡因的毛细管电泳手性拆分

运用毛细管电泳法，以羧甲基聚合β-环糊精为手性剂，对维拉帕米及布比卡因进行了拆分。考察了手性剂的种类、浓度及缓冲液的pH值对分离的影响。结果表明：羧甲基聚合β-环糊精对这两种药物对映体有极好的拆分效果。从协同效应方面解释了羧甲基聚合β-环糊精具有良好拆分能力的原因。     

羧甲基聚合-β-环糊精作为选择剂应用于毛细管电泳法拆分手性化合物

提出了一种用毛细管电泳拆分3种未衍生化的氨基酸对映体(苯丙氨酸,酪氨酸,色氨酸)和一种手性药物(芬氟拉明)的方法.以水溶性羧甲基聚合-β-环糊精为手性选择荆,采用毛细管区带电泳模式,考察了手性选择剂浓度、缓冲溶液pH值、柱温及电压对分离的影响.4种手性化合物在各自优化的试验条件下,均达到基线分离.此法操作简单,可用于这4种手性化合物的质量控制.     

手性离子液体在毛细管电泳手性分离中的应用

简要介绍了手性离子液体用于毛细管电泳手性分离的一般原理,系统地介绍了基于手性离子液体的毛细管电泳对映体拆分的一元手性选择体系和二元手性选择体系,并在国内外研究现状的基础上展望了手性离子液体在毛细管电泳手性分离中的应用前景。     

毛细管电泳手性选择剂去硫酸基硫酸软骨素C的研究开发及新药西尼地平对映体的拆分

研究开发了一种新型的毛细管电泳多糖手性选择剂去硫酸基硫酸软骨素C,并用于二氢吡啶类药物对映体的分离。建立了新药西尼地平对映体的拆分方法,同时考察了背景电解质pH值、手性添加剂浓度、工作电压等因素对手性分离的影响。优化的背景电解质pH值 为2.50、手性添加剂的质量浓度为30 g/L,工作电压为10 kV。以去硫酸基硫酸软骨素C为毛细管电泳手性选择剂拆分新药西尼地平对映体,操作简单方便,西尼地平两对映体得到了基线分离,分离度达2.01。     

基于环糊精手性选择剂的几种手性药物对映体的毛细管电泳拆分

以环糊精(-αCD、-βCD和-γCD)为手性选择剂,采用毛细管电泳对扑尔敏、异丙嗪和二氧异丙嗪对映体进行了分离,考察了手性选择剂的浓度、缓冲液pH值及有机添加剂对手性分离的影响,并就拆分机理进行了初步探讨.     

聚合-β-环糊精作手性选择剂的毛细管电泳法分离4种光学活性农药中间体

以聚合-β-环糊精作为毛细管区带电泳手性选择剂,成功分离了2-苯氧丙酸(PPA)、顺式-功夫菊酸(cis-PA)、1-苯基-2-(对甲苯基)乙胺(PTE)和1-苯基-2-(对甲氧基苯基)乙胺(PME)4种光学活性农药中间体的对映体。考察了不同手性选择剂及其浓度、背景电解质的pH等操作条件对分离的影响。结果表明,在12kV操作电压下、30mmol／Ltris-HCl背景电解质中,用14g／L聚合-β-CD作为手性选择剂,PPA和cis-PA对映体在pH6．0时,PIE和PME对映体分别在pH2．5和pH3．0时可以被较好分离。在优化的分离条件下,用聚合-β-CD作毛细管区带电泳手性选择剂分离PIE对映体的分离度为1．513,成功测定了两种旋光性PIE的对映体过量值。     

基于非手性离子液体的毛细管电泳法拆分3种手性药物

建立了以非手性离子液体1-正丁基-3-甲基咪唑氯(［BMIM］Cl)为手性分离的添加剂、β-环糊精作为手性选择剂的毛细管区带电泳(CZE)分离扑尔敏、氯霉素前体和氧氟沙星3种对映体的方法,并与未添加［BMIM］Cl的CZE分离情况进行了对比研究。发现［BMIM］Cl对手性药物的拆分有协同作用,不仅能够增加对映体的分离度,还能有效地抑制毛细管内壁对样品分子的吸附作用,改善峰形。采用离子液体辅助手性选择剂(尤其是环糊精)的CZE改进方法,为其他毛细管电泳难以分离的手性药物的分离分析提供了新的方法。     

配体交换毛细管区带电泳拆分未衍生化氨基酸

以铜(Ⅱ)-L-谷氨酸络合物为手性分离选择剂,对苯丙氨酸、酪氨酸和色氨酸3种非衍生芳香族氨基酸的手性对映体拆分进行了研究,建立了一种快速、简便拆分未衍生化的氨基酸对映体的配体交换毛细管电泳方法.在使用10 mmol/L NH4AC(pH 5.0),5 mmol/L CuSO4和10 mmol/L L-谷氨酸的条件下,成功地拆分了苯丙氨酸、酪氨酸手性对映体;色氨酸手性对映体也得到部分分离;考察了电泳缓冲液组成、pH值等影响分离效果的因素.     

离子液体作为添加剂的毛细管电泳法拆分盐酸金刚乙胺

将新离子液体[EIMCH2CONHBu]BF4用于毛细管电泳法拆分手性药物,建立了以β-环糊精为手性选择剂拆分盐酸金刚乙胺对映体的毛细管电泳方法。分别考察了离子液体浓度,手性选择剂浓度,缓冲溶液种类、浓度及pH值,分离电压等参数对分离度的影响,从而确定了盐酸金刚乙胺对映体的最佳拆分条件:[EIMCH2CONHBu]BF4溶液体积分数3.2%,β-环糊精18 mmol/L,NaH2PO4 15 mmol/L,缓冲液pH 3.03,分离电压15 kV。在优化的实验条件下,盐酸金刚乙胺对映体得到基线分离,分离度可达1.51。实验结果表明[EIMCH2CONHBu]BF4能够增强β-环糊精的手性拆分能力,对手性拆分有协同作用。     

使用二元环糊精体系毛细管电泳法分离手性药物

采用高效毛细管区带电泳法，分别以羟丙基-β-环糊精（HP-β-CD）和高磺化-β-环糊精（HS-β-CD）及二者混合物为手性选择剂，研究了5种药物的对映体分离，并取得很好的对映体分离结果。比较了HP-β-CD和HS-β-CD手性识别能力，分析了二元环糊精体系的“协同效应”。     

Enantioseparation of α-Amino Acids by Capillary Electrophoresis Using L-Cysteine-Modified Cyclodextrins as Chiral Selectors

Capillary electrophoresis (CE) is a powerful separation technique that was used in a wide range of analytical chemical applications. Cyclodextrins(CDs) are the most commonly used chiral selectors in chiral capillary electrophoresis at the present time. Under neutral conditions, however, native CDs are neutral and usually applicable only for the enantioseparation of charged analyses. To overcome this defect we modified α- and β-CD with a L-cysteine moiety and used the CD derivatives as chiral selectors for the separation of a-amino acid enantiomers by the ligand exchange mode.     

Evaluation of the enantioselectivity of glycogen-based dual chiral selector systems towards basic drugs in capillary electrophoresis

Several chiral reagents including cyclodextrins (CDs) and derivatives, crown ethers, proteins, chiral surfactants and polymers have been involved in dual selector systems for enantioseparation of a series of chiral compounds by capillary electrophoresis (CE). In comparison to the chiral reagents above-mentioned, there is no report concerning the use of polysaccharides in dual chiral CE system. In this paper we first investigate the enantioselectivity of polysaccharide-based dual selector systems towards some chiral drugs. During our recent work, glycogen belonging to the class of branched polysaccharides has been used as a novel chiral selector in CE. In this study, three glycogen-based dual chiral CE systems have been established for enantiomeric separations of several racemic basic drugs consisting of duloxetine, cetirizine, citalopram, sulconazole, laudanosine, amlodipine, propranolol, atenolol and nefopam. These three dual systems combined glycogen (neutral polysaccharide) with chondroitin sulfate A (CSA, ionic polysaccharide), β-CD and HP-β-CD, respectively. It was found that the dual system of glycogen/CSA exhibited good enantioselective properties toward the tested drugs. More importantly, compared to the single selector systems, synergistic effect was observed when glycogen was used with CSA for most of the analytes. This indicated the enhancement of enantioseparation observed for these analytes in glycogen/CSA system might be due to some favorable interaction effects between glycogen and CSA. Moreover, in order to evaluate the stereoselectivity of glycogen/CSA, the influences of buffer pH and selector concentration on enantioseparation of the studied drugs were also investigated.     

Simultaneous enantioseparation of four beta2-agonists by capillary electrophoresis with cyclodextrin additives. Study of the enantioselective mechanism

The simultaneous capillary electrophoretic enantioseparation of adrenergic beta(2)-agonists enantiomers (trantinterol, mabuterol, clenbuterol, bambuterol) was studied with beta-cyclodextrin, ethyl-beta-CD, methyl-beta-CD, hydroxypropyl-beta-CD, and hydroxyethyl-beta-CD as chiral selector. The type and concentration of the chiral selector and buffer pH played a very important role in the enantioseparation of the analyzed compounds. Hydroxypropyl-beta-CD was found to be the most effective complexing agent and allowed excellent chiral/achiral resolutions compared to the other CDs. The simultaneous enantioseparation of four beta(2)-agonists was achieved using 100 mM citric acid-10 mM Na(2)HPO(4) buffer at pH 2.5 containing 120 mM hydroxypropyl-beta-CD with an applied voltage of 20 kV. Method validation in terms of repeatability, linearity, and limits of detection and quantification was performed. The effect of structural features of analytes on R(s) and t(m) was studied. Complexation binding constants for the interactions between the four compounds and three different CDs were evaluated for elucidating the enantioseparation mechanism. It was found that very small differences in the chemical structure of the analytes resulted in significant changes in stereoselective recognition.     

The Use of Dual Cyclodextrin Chiral Selector Systems in the Enantioseparation of Pharmaceuticals by Capillary Electrophoresis: An Overview

Cyclodextrin (CD) derivatives are the most efficient and frequently used chiral selectors (CSs) in capillary electrophoresis (CE). There are situations when the use of a single CD as CS is not enough to obtain efficient chiral discrimination of the enantiomers; in these cases, sometimes this problem can be resolved using a dual CD system. The use of dual CD systems can often dramatically enhance enantioseparation selectivity and can be applied for the separation of many analytes of pharmaceutical interest for which enantioseparation by CE with another CS systems can be problematic. Usually in a dual CD system an anionic CD is used together with a neutral one, but there are situations when the use of a cationic CD with a neutral one or the use of two neutral CDs or even two ionized CDs can be an efficient solution. In the current review we present general aspects of the use of dual CD systems in the analysis of pharmaceutical substances. Several examples of applications of the use of dual CD systems in the analysis of pharmaceuticals are selected and discussed. Theoretical aspects regarding the separation of enantiomers through simultaneous interaction with the two CSs are also explained. Finally, advantages, disadvantages, potential and new direction in this chiral analysis field are highlighted.     

Azithromycin as a new chiral selector in capillary electrophoresis

In capillary electrophoresis (CE), separation of enantiomers of a chiral compound can be achieved through the chiral interactions and/or complex formation between the chiral selector and the enantiomeric analytes on leaving their diastereomeric forms with different stability constants and hence different mobilities. A great number of chiral selectors have been employed in CE and among them macrocyclic antibiotics exhibited excellent enantioselective properties towards a wide number of racemic compounds. The use of azithromycin (AZM) as a chiral selector has not been reported previously. This work reports the use of AZM as a chiral selector for the enantiomeric separations of five chiral drugs and one amino acid (tryptophan) in CE. The enantioseparation is carried out using polar organic mixtures of acetonitrile (ACN), methanol (MeOH), acetic acid and triethylamine as run buffer. The influences of the chiral selector concentration, ACN/MeOH ratio, applied voltage and capillary temperature on enantioseparation are investigated. The results show that AZM is a viable chiral selector in CE for the enantioseparation of the type of chiral drugs investigated.     

毛细管电泳在手性化合物分离中的应用进展

由于手性化合物尤其是手性药物的两个对映体具有不同的化学性质和生理活性,对手性化合物进行分离在医药、生物、食品和环境等领域都具有十分重要的意义。毛细管电泳由于其独特的优势已广泛应用于手性物质的分离。本文对2013~2015年毛细管电泳用于手性分离的最新进展进行了综述,并对其发展前景进行了展望。     

毛细管电泳新型手性分离体系研究进展

在现代分离科学中,手性化合物的分离分析一直是研究的重点和难点。相比于高效液相色谱（HPLC）、气相色谱（GC）等传统色谱分析方法,毛细管电泳（CE）技术凭借其高效率、低消耗、分离模式多样化等诸多优势,已经发展成为手性分离研究领域最有应用前景的分析方法之一。近年来,研究人员在CE手性分析方法的构建过程中,基于毛细管电动色谱（EKC）、配体交换毛细管电泳（LECE）、毛细管电色谱（CEC）等各种基础电泳模式,不断地对传统手性分离体系进行优化和改造,构建出了许多高性能的新型手性CE分离体系。如利用各类功能化离子液体以"手性离子液体协同拆分""手性离子液体配体交换""离子液体手性选择剂"等模式设计出多种基于离子液体的CE手性分离体系;利用纳米材料独特的尺寸效应、多样性、可设计性等特点,直接或与传统手性选择剂有机结合构建CE手性分离体系。此外,金属有机骨架材料修饰、低共熔溶剂修饰、非连续分段式部分填充等各式新颖的CE手性分离体系也都被研究人员成功开发,并表现出较大的发展潜力。该综述将对近年来（尤其是2015~2019年）此类新型CE手性分离体系的发展状况进行梳理,并结合相应的手性识别机理研究和手性CE方法实际应用情况,对该领域存在的问题及发展前景进行分析和展望。     

Enantioseparation of the anticoagulant drug phenprocoumon in capillary electrophoresis with UV and laser-induced fluorescence detection and application of the method to urine samples

The enantioseparation of phenprocoumon (PhC) in capillary electrophoresis (CE) has been studied using various cyclodextrins (CDs) such as native alpha, beta and gamma-CD and several neutral and randomly, as well as selectively substituted charged CD derivatives. Reversal of the enantiomer migration order was observed when using heptakis(2,3,6-tri-O-methyl (TM)-beta-CD as a chiral selector compared to all other CDs used. The detection of PhC was performed using either UV or laser-induced fluorescence (LIF) detection. The limit of detection (LOD) observed with LIF detection was ca. 20 times lower compared to UV. The method has been applied to the analysis of urine samples of the patient under treatment with PhC in combination with other drugs such as ramipril, hydrochlorothiazide, and nifedipine.     

Study of the enantioseparation capability of chiral dual system based on chondroitin sulfate C in CE

It has been reported that chiral dual system is able to improve the enantioseparation of enantiomers in many cases. Currently, the dual systems involved in CE chiral separation are mostly dual CDs systems, and the polysaccharides‐based chiral dual system was reported in only one paper. To the best of our knowledge, the use of chondroitin sulfate C (CSC)‐based dual system for enantiomeric separation has not been reported previously. Herein, four CSC‐based chiral dual systems, namely CSC/glycogen, CSC/chondroitin sulfate A (CSA), CSC/hydroxypropyl‐β‐CD (HP‐β‐CD), as well as CSC/β‐CD (β‐CD), were evaluated for the first time for their enantioseparation capability by CE in this paper. During the course of the work, the influences of chiral selector concentration and buffer pH values on enantioseparation in dual systems were systematically investigated. Under the optimized conditions, the dual system consisting of CSC and glycogen exhibited better separations toward nefopam, duloxetine, sulconazole, atenolol, laudanosine, and cetirizine enantiomers compared to the single CSC or glycogen system. The combination of CSC and HP‐β‐CD improved the separation of amlodipine and chlorphenamine enantiomers. However, no synergistic effect was observed in the CSC/CSA and CSC/β‐CD systems.