毛细管电泳测定4个不对称合成化合物的光学纯度

采用毛细管电泳技术,以α-环糊精、β-环糊精和β-环糊精聚合物为手性选择剂,对4种不对称合成物3-(二乙基氨基)-1-苯基-1-丙醇(a)、1-苯基-3-(1-哌啶）-1-丙醇(b)、3-吗啉-1-对甲苯基-1-丙醇(c)和1-（4-氯苯基）-3-吗啉-1-丙醇(d)的消旋体和光学活性异构体进行了手性分离。 结果发现,使用20 kV的分离电压,以浓度为30 g/L的β-环糊精聚合物的80 mmol/L三羟甲基氨基甲烷缓冲溶液（pH=3.2）为背景电解质溶液,4种化合物在40 min内均可得到基线分离。 根据对映异构体峰面积和保留时间的比值确定了4种不对称化合物的光学纯度。 测定的RSD均不大于1.5%。     

高效毛细管电泳法分离1-甲基-3-苯基丙胺对映体

提出了高效毛细管电泳拆分手性药物中间体1-甲基-3-苯基丙胺的方法。研究了缓冲溶液pH值、手性选择剂质量浓度、柱温、电压等因素对分离度的影响。在缓冲溶液浓度15mmol.L-1(NaH2PO4-Na2HPO4,pH7.6)、运行电压15kV、手性选择剂浓度为20g.L-1、毛细管温度18℃条件下,在4min内成功地分离了1-甲基-3-苯基丙胺对映体,其分离度为1.65。     

二甲基-β-环糊精作为手性选择剂对尼索地平对映体的毛细管电泳拆分研究

以二甲基-β-环糊精(DM-β-CD)为手性添加剂,用毛细管电泳法对消旋体药物尼索地平进行拆分研究。考察了二甲基-β-环糊精浓度、背景电解质种类、缓冲溶液pH值、十二烷基硫酸钠(SDS)浓度、分离电压、温度对对映体分离的影响。结果表明,以pH 8.0的30 mmol/L磷酸二氢钠-磷酸氢二钠溶液(含38mmol/L二甲基-β-环糊精,30 mmol/L SDS)为缓冲液,分离电压15 kV,毛细管温度18℃,检测波长254 nm时,尼索地平对映体达到最佳分离,分离度为1.95,对映体迁移时间分别为13.0、13.54 min。该方法简单、快速、经济,可用于尼索地平对映体的手性分离。     

N-(2-甲基-6-乙基苯基)丙氨酸对映体的毛细管电泳分离

采用高效毛细管区带电泳法,以β-环糊精及其衍生物作为手性选择剂,对外消旋N-(2-甲基-6-乙基苯基)丙氨酸(EMPA)的两个对映体进行了手性分离,比较了环糊精种类、环糊精浓度、电解质溶液pH值、温度和电场强度对分离的影响.实验结果表明,采用2,6-O-二甲基-β-环糊精为手性选择试剂,环糊精浓度为40mmol/L、电解质溶液pH=5.5及温度为20℃时分离效果最佳,对映体基本达基线分离,线性范围为20～200mg/L,最低检测限为10mg/L.     

毛细管电泳法手性拆分4种氨酸和2种手性药物对映体

以双(6-氧-β-羧甲基-1,4-丁烯二酸单酯)-β-环糊精(DOCB-β-CD）作为手性添加剂,利用毛细管电泳对氨基酸和手性药物对映体进行拆分研究。 以20 mmol/L磷酸盐为缓冲溶液,考察了手性添加剂的浓度及缓冲溶液的pH值与分离电压等对拆分效果的影响,并在其优化条件下,实现了4种DL-氨基酸（苯丙氨酸、色氨酸、酪氨酸和组氨酸）以及手性药物（罗格列酮和酮洛芬）对映体的基线分离。     

加压毛细管电色谱法分离1-甲基-3-苯基丙胺对映体

运用毛细管电色谱(pCEC)模式,以羟丙基-β-环糊精(HP-β-CD)作为手性选择剂,对1-甲基-3-苯基丙胺对映体进行手性分离。1-甲基-3-苯基丙胺对映体在最佳的条件下如:手性选择剂浓度10g/L、流动相配比:V(乙腈)∶V(磷酸盐体系)=60∶40溶液(5mmol/L)、背景电解质pH=7.6、柱温16℃和分离电压10kV达到了基线分离,该方法重现性好、简便、快捷。     

毛细管区带电泳对手性药物盐酸美西律和盐酸异博定的对映体分离

应用环糊精-毛细管区带电泳体系对手性药物盐酸美西律和盐酸异博定的对映体分离进行了研究。结果表明, 在所研究的手性选择剂α-环糊精, β-环糊精, 二甲基-β-环糊精, 羟丙基β-环糊精和γ-环糊精中, 羟丙基β-环糊精对所研究的手性药物分离效果较好。对盐酸美西律和盐酸异博定的最佳羟丙基-β-环糊精浓度分别为30mmol/L和9mmol/L, 最佳缓冲溶液浓度为100mmol/L Tris-H3PO4(pH2.3)。向缓冲溶液中加入0.05%羟丙基纤维素(HPLC)可改善分离。盐酸美西律获得了接近基线的手性分离, 而盐酸异博定亦获得了较好的分离。     

毛细管电泳法手性拆分达卢生坦中间体2-羟基-3-甲氧基-3,3-二苯基丙酸

建立了毛细管电泳法拆分2-羟基-3-甲氧基-3,3-二苯基丙酸的方法.考察了背景电解质的pH值和浓度、手性选择剂的种类及浓度、有机改性剂种类及浓度对分离的影响,并对分离条件进行了优化.实验结果表明,在60 mmol/L磷酸氢二钠(pH=9.10)为运行缓冲溶液,舍35.7 mmol/L羟丙基-β-环糊精和5%甲醇的体系...     

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。     

西他沙星差向异构体的毛细管电泳分离

以γ-环糊精和D-苯丙氨酸为手性选择剂,采用毛细管区带电泳成功地分离了新型抗菌素西他沙星差向异构体。考察了添加剂的种类、浓度和缓冲溶液的pH对毛细管电泳分离西他沙星的影响。分离电压为15 kV,选用60 cm(有效长度52.5 cm)×50 μm i.d.的石英毛细管,缓冲溶液组成为10 mmol/L KH2PO4-K2HPO4(pH 4.5),10 mmol/L CuSO4,20 mmol/L γ-环糊精和 10 mmol/L D-苯丙氨酸。实验结果表明,添加剂的种类和浓度是影响西他沙星手性分离的重要因素,只有当 D-苯丙氨酸、铜离子和γ-环糊精同时存在并达到一定浓度时,西他沙星差向异构体在毛细管电泳中才具有良好的分离效果。该方法可用于西他沙星差向异构体的定量分析。     

肝糖选择剂-毛细管电泳手性拆分盐酸度洛西汀对映体及分离机制

以肝糖为毛细管电泳手性选择剂,对盐酸度洛西汀对映体的分离进行研究,建立了拆分方法.考察了手性选择剂浓度、运行缓冲液的离子强度、pH值及分离电压对手性分离的影响.在3.0% (m/V)肝糖、50 mmol/L Tris-H3PO4(pH 3.0)的运行缓冲液中,分离电压25 kV时,盐酸度洛西汀两对映体分离度达1.84.对分离机制进行了初步探讨.     

双丙酮-D-甘露糖醇—硼酸络合酸手性毛细管电泳法分离盐酸莱克多巴胺立体异构体

采用手性多羟基化合物—硼酸络合酸为手性选择剂,建立了分离盐酸莱克多巴胺4个立体异构体的手性毛细管电泳(NACE)方法。实验考察了手性选择剂的种类、浓度和三乙胺浓度对手性分离效果的影响。结果表明,双丙酮-D-甘露糖醇—硼酸络合酸手性选择剂的分离效果最好,优化的缓冲溶液组成为含100 mmol/L双丙酮-D-甘露糖醇、100 mmol/L硼酸和72 mmol/L三乙胺的甲醇溶液。在优化的实验条件下,盐酸莱克多巴胺的4个立体异构体均可以达到基线分离,质量浓度在6.2~200.0μg/mL范围内与峰面积分别呈现良好的线性关系,检测限和定量限分别为0.6μg/mL和2.0μg/mL,加标回收率为97.5%~102.5%,饲料中的提取回收率为66.4%~72.5%。方法可用于盐酸莱克多巴胺4个立体异构体的手性分离和含量测定。     

Synthesis and application of clindamycin succinate as a novel chiral selector for capillary electrophoresis

A novel chiral selector, clindamycin succinate, was synthesized and first used as a chiral selector in capillary electrophoresis (CE). The chiral resolution ability of this kind of clindamycin derivation was studied by CE using some racemic drugs as model analytes. From the experimental results, it was found that both resolution and selectivity of the selector were dependent on the following parameters: concentration of chiral selectors, pH of the running buffer, temperature of the capillary column, applied voltage and organic modifier used. The results show that the chiral selector possesses high resolution toward some racemic drugs, including ofloxacin, chlorphenamine, tryptophan, propranolol, sotalol and metoprolol. Excellent chiral resolution of these tested drugs was achieved under the optimal conditions of 50 mM clindamycin succinate, 10% MeOH v/v, 50 mM Tris buffer, pH 4.0, at 22 kV and 20 °C within 25 min.     

Separation and quantitation of the four stereoisomers of itraconazole in pharmaceutical formulations by electrokinetic chromatography

The four stereoisomers of itraconazole were resolved for the first time by EKC using a CD as chiral selector. A study on the enantiomeric separation ability of different neutral CDs was carried out. Heptakis-2,3,6-tri-O-methyl-beta-CD was shown to provide the highest values for the enantiomeric resolution. The influence of some experimental conditions, such as pH, chiral selector concentration, and temperature, on the enantiomeric separation was also studied. The use of a 100 mM phosphate buffer (pH 2.5), 30 mM in heptakis-2,3,6-tri-O-methyl-beta-CD together with an applied voltage of 30 kV and a temperature of 20 degrees C enabled the separation of the enantiomers of itraconazole with high resolutions (Rs > 3.0). Finally, the method was validated and successfully applied to the quantitation of itraconazole in three pharmaceutical formulations.     

Chiral separation of dansyl amino acids in capillary electrophoresis using mono-(3-methyl-imidazolium)-beta-cyclodextrin chloride as selector

Enantioseparations of fourteen dansyl amino acids were achieved by using a positively-charged single-isomer beta-cyclodextrin, mono-(3-methyl-imidazolium)-beta-cyclodextrin chloride, as a chiral selector. Separation parameters such as buffer pH, selector concentration, separation temperature, and organic modifier were investigated for the enantioseparation in order to achieve the maximum possible resolution. Chiral separation of dansyl amino acids was found to be highly dependent on pH since the degree of protonation of these amino acids can alter the strength of electrostatic interaction and/or inclusion complexation between each enantiomer and chiral selector. In general, the chiral resolution of dansyl amino acids was enhanced at higher pH, which indicates that the carboxylate group on the analytes may interact with the imidazolium group of cationic cyclodextrin. For most analytes, a distinct maximum in enantioresolution was obtained at pH 8.0. Moreover, the chiral separation can be further improved by careful tuning of the separation parameters such as higher selector concentration (e.g. 10 mM), lower temperature, and addition of methanol. Enantioseparation of a standard mixture of these dansyl amino acids was further achieved in a single run within 30 min.     

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。     

应用四甲基氢氧化铵控制电渗流的毛细管电泳方法分离多沙唑嗪及其中间体的对映体

建立了毛细管电泳手性分离多沙唑嗪中间体对映体的方法,并同时分离了多沙唑嗪对映体。考察了不同种类季铵盐对电渗流及分离的影响,其中四甲基氢氧化铵(TMB)能有效控制电渗流并提高组分的分离度。实验还考察了其他因素,如pH值、分离电压和磷酸二氢钠浓度对分离的影响。所用的毛细管为40 cm(有效长度30 cm)×50 μm,缓冲液为12 mmol/L β-环糊精、30 mmol/L TMB、60 mmol/L 磷酸二氢钠(pH 2.2),分离电压为20 kV。在此条件下多沙唑嗪及其中间体的对映体均达到了基线分离。实验结果表明,一些用β-环糊精不能完全分离的对映体通过加入TMB控制电渗流能达到满意的分离效果。     

高效毛细管电泳电导法拆分苯丙氨酸对映体

以未涂层融硅石英毛细管(50 cm×75μm)为分离柱,2 mmol/L NaAc 2 mmol/L HAc 0.5 mmol/LCu2 (pH 4.0)作为电泳运行液,分离电压15 kV,建立了苯丙氨酸对映体的高效毛细管电泳-电导分离检测的方法。对缓冲溶液的种类、浓度、分离电压、有机改性剂等因素对分离的影响进行了讨论,并对拆分机理进行了初步探讨。     

Enantioselective Separation of Basic Drugs by CE with Polygalacturonic Acid as a Novel Chiral Selector

Polygalacturonic acid, a linear high molecular weight homopolysaccharide was investigated as a chiral selector in capillary zone electrophoresis for the separation of enantiomers of basic drugs. The choices of running buffer pH and concentration of chiral selector were found to be important for the improvement of enantioselectivity. The effects of background electrolyte concentration and the capillary temperature on the separation were also examined. Enantioseparations were carried out in the acidic conditions using 1.5% polygalacturonic acid (w/v) in a 40 mM phosphate buffer under an applied voltage of 15 kV. The optimization of these separations was dependent on the nature of the analytes and could be achieved by the proper choice of experimental conditions. A brief mechanism of enantiorecognition by polygalacturonic acid was also given.