Laboratory to Laboratory Reproducibility of High Performance Liquid Chromatographic Retention Indices

Abstract

Using seven typical drugs, the intra-and inter-laboratory reproducibility of the measured HPLC retention indices, relative retention times, and adjusted relative retention times using the same mobile phase and various reversed-phase C-18 columns were determined. Within a given laboratory, the respective relative standard deviations were ± 0.99%, ± 1.78%, and ± 2.63%. Between laboratories, the respective relative standard deviations were found to be ± 12.6%, ± 30.2%, and ± 34.8%. These results indicated that the HPLC retention index scale may be more useful in comparing data between laboratories.     

Influence of mobile phase composition on retention factors in different HPLC systems with chemically bonded stationary phases

The influence of mobile phase composition on the retention of selected test analytes in different normal- and reversed-phase chromatographic systems is studied. A novel adsorption model for an accurate prediction of the analyte retention in the column chromatography with binary mobile phase is proposed. Performance of the model is compared with the retention model reported in the literature. Both models are verified for different HPLC systems by use of three criteria: (a). the sum of squared differences between the experimental and theoretical data, (b). approximation of the standard deviation, and (c). the Fisher test.     

Simultaneous determination of caffeine and non-steroidal anti-inflammatory drugs in pharmaceutical formulations and blood plasma by reversed-phase HPLC from linear gradient elution

A reversed-phase HPLC procedure based on methanol-water gradient elution for determining caffeine and non-steroidal anti-inflammatory drugs with UV absorbance detection is proposed. Chromatographic operational conditions were selected by considering the peak resolution and the retention times of the first and last eluted compounds. The method was suitably validated and successfully applied to the determination of: caffeine, indoprofen, ketoprofen, naproxen, fenbufen and ibuprofen in blood plasma samples and several analgesic/antiphlogistic pharmaceutical formulations.     

Thermodynamic investigations on shape selective separation behaviors of poly(4-vinylpyridine)-grafted silica for polycyclic aromatic hydrocarbons in both normal-phase and reversed-phase high-performance liquid chromatography

With the successful implementation of poly(4-vinylpyridine)-grafted silica prepared by grafting-from approach (GF-VP(n)) as a stationary phase for the separation of polycyclic aromatic hydrocarbons (PAHs) in normal-phase HPLC, this paper describes the chromatographic retention behaviors of PAHs with GF-VP(n) in reversed-phase HPLC. Significantly higher retention factor along with enhanced shape selectivity were observed with GF-VP(n). Thermodynamic study on the retention behaviors of PAHs with GF-VP(n) in normal-phase and reversed-phase HPLC revealed that retention of PAHs was exothermic in both phases. Furthermore, higher entropic contribution was observed in reversed-phase HPLC compared to normal-phase HPLC.     

Investigation of different combinations of derivatization, separation methods and electrospray ionization mass spectrometry for standard oligosaccharides and glycans from ovalbumin

Derivatization procedures using 1-phenyl-3-methyl-5-pyrazolone (PMP) and 2-aminonaphthalene trisulfone (ANTS) were selected among a number of well known methods for labelling carbohydrates. PMP derivatives were selected owing to our laboratory's previous high-performance liquid chromatography/electrospray ionization mass spectrometry (HPLC/ESI-MS) experience with these, whereas the ANTS-labelled compounds were prepared for fluorophore-assisted carbohydrate electrophoresis (FACE) separation. ANTS-oligosaccharide standards were characterized to study their ionization patterns. Reversed-phase and normal-phase HPLC systems were coupled on-line with ESI-MS. Each necessitated its own mobile phase system which, in turn, imposed some important changes in the ionization conditions used and/or on the ionization patterns and spectra obtained. Following characterization of the intact glycoprotein ovalbumin with ESI-MS, its glycans were detached using the enzyme PNGase-F. The glycans were subjected to PMP and ANTS derivatization. It was very difficult to separate ANTS derivatives by reversed-phase HPLC owing to lack of retention, and normal-phase HPLC offered reasonable retention with limited separation. PMP compounds overall yielded better normal- and reversed-phase separations and improved sensitivity over the ANTS-labelled sugars, for which negative mode ESI had to be used. The combination of ESI of intact ovalbumin and ESI of PMP-glycans gave rise to the detection of over 20 different glycoforms, excluding the possible presence of structural isomers for each sugar composition detected.     

Evaluation of hydrophobic interaction between acidic drugs and bovine serum albumin by reversed-phase high-performance liquid chromatography

The contribution of hydrophobic interaction to the protein binding of acidic drugs has been evaluated in terms of a new hydrophobic index (r-value), defined as the slope of the log-log plots of capacity factor vs. reciprocal of methanol concentration in an aqueous binary mobile phase, measured by the reversed-phase high-performance liquid chromatography. The logarithms of the binding constants (log K1) of the selected acidic drugs and the related aromatic carboxylic acids indicated linear relationship with their r-values, suggesting that the effect of hydrophobicity on protein binding can be explained similarly to that on the retention onto the reversed-phase stationary ligand.     

Relationship between gas chromatographic behaviour and topological, physicochemical, and quantum chemically calculated charge parameters for neuroleptica

Gas chromatographic retention indices for a number of neuroleptic drugs on an apolar phase, OV-101, and a polar phase, OV-17, are correlated with parameters describing various properties of the separated molecules. The gas chromatographic behaviour is related to the same parameters as those used in quantitative structure activity relationships. The molecular connectivity indices and log k' in a reversed-phase HPLC system were chosen as parameters describing the apolar interactions of the molecules with the stationary phase. As properties involved in more specific interactions, and related to the presence of overall or local polarity, the molecular dipole moment and the charge on the N-atom were selected and quantum chemically calculated. It is found that the retention indices on the apolar phase, OV-101, can be successfully correlated with molecular connectivity indices, which are also used in QSAR studies. The retention indices on OV-17 show a high correlation with the charge on the N-atom. Evidence of the importance of this N-atom in pharmacological activity is known.     

Estimation of High-Performance Liquid Chromatographic Retention Indices of Glucuronide Metabolites

Abstract

The retention indices of several glucuronide metabolites and their parent compounds were measured using a reversed-phase HPLC system. It was found that the typical glucuronide metabolite had a retention index 244 ± 31 units lower than the parent compound.     

Weak cation-exchange restricted-access material for on-line purification of basic drugs in plasma

A methylcellulose-immobilized weak cation-exchange (MC-WCX) silica-based restricted-access material (RAM) was developed. The MC-WCX consists of an MC outer surface and 2-carboxyethyl phase internal surface, allowing for direct analysis of basic drugs in plasma. The retention properties of the MC-WCX were evaluated for sulpiride, quinidine, ranitidine, and desipramine. The MC-WCX retained model drugs by cation-exchange, and retained drugs were eluted with the mobile phase containing small amount of acids or salts compared with the MC strong cation-exchanger (MC-SCX). These results indicated the ease of use of the MC-WCX solid-phase extraction (SPE) column when coupled to a reversed-phase analytical column in column-switching high-performance liquid chromatography (HPLC), and various detection principals. Further direct analysis of model drugs in plasma using the MC-WCX SPE column in a column-switching HPLC system successfully performed with sufficient recovery. It is concluded that the MC-WCX is useful for the analysis of basic drugs in plasma.     

Retention of some monoamine oxidase inhibitory drugs on a β-cyclodextrin polymer-coated silica column

The retention of seventeen monoamine oxidase inhibitory drugs (mono- and disubstituted derivatives of propargylamine) was determined on a β- cyclodextrin polymer (β-CDP)-coated silica column using methanol-0.05 M K₂HPO₄ (6:4, v/v) as the eluent. The inclusion complex formation between the drugs and a water-soluble β-cyclodextrin polymer was studied by charge-transfer chromatography carried out on reversed- phase TLC layers. The capacity factors were correlated with the various physico-chemical parameters and with the inclusion complex-forming capacity of the monoamine oxidase inhibitory drugs. Calculations indicated that the inclusion complex-forming capacity of the drugs does not influence their retention on a β-CDP column, that is, the water-soluble and water-insoluble β-CDPs show different retention characteristics. The specific hydrophilic adsorption surface of the solutes significantly influences the retention in HPLC. The results suggest that the selectivity of the β-CDP-coated silica support may be different from that of the traditional alkyl-bonded reversed-phase columns.     

溴化1-乙烯基-3-十二烷基咪唑硅胶键合固定相制备及其色谱性能

膜脂作为细胞质膜的主要组成部分,在生命活动中扮演着重要的作用,其涉及多种重要疾病的发生和发展过程。发展适用于膜脂分离分析的新型色谱材料对于其后续结构和生物学功能研究具有重要的意义。该文选用具有潜在生物相容性的离子液体溴化1-乙烯基-3-十二烷基咪唑（1-vinyl-3-dodecylimidazole bromide,VDI）为功能单体,通过一步法点击反应将其接枝到巯基功能化硅球表面,制备得到了新型溴化1-乙烯基-3-十二烷基咪唑硅胶键合固定相（Sil-VDI）。利用傅里叶变换红外光谱仪和热重分析仪对Sil-VDI固定相材料的结构进行表征,结果证明Sil-VDI色谱固定相已被成功制备。保留机制研究显示填充Sil-VDI色谱柱具有典型的反相/离子交换混合模式保留特性。基于此,采用不同疏水性物质烷基苯、多环芳烃、苯胺、苯衍生物和无机阴离子BrO₃ ^- 、NO₃ ^- 和IO₃ ^- 为测试物,对所制备固定相的色谱性能进行了研究。结果表明,该固定相对4类疏水性物质和无机阴离子均有较好的分离选择性和良好的峰对称性。进一步研究了所制备的Sil-VDI色谱柱对鸡蛋黄磷脂和肺腺癌细胞提取膜脂的分离效果,结果显示Sil-VDI色谱柱对2种磷脂样品均显示出了良好的分离能力。该文所制备的Sil-VDI色谱固定相合成方法简便,具有良好的分离分析应用潜能,后续工作会进一步研究该固定相在生物样品中的分离分析性能。     

High-performance liquid chromatography of biotin and analogues

Biotin, analogues, and chemical intermediates were separated by high-performance liquid chromatography (HPLC) using reversed-phase and anion-exchange chromatographic conditions. Reversed-phase separations provided a wide range of retention times and resolution of nearly all the biotin compounds from mixtures of the analogues. Anion-exchange separations gave generally shorter retention times as compared to reversed-phase separations and greater resolution between biotin l- and d-sulfoxide. However, fewer analogues were resolved from mixtures of the compounds with anion-exchange HPLC.     

Determination of antibacterial agents in microbiological cultures by high-performance liquid chromatography

A general high-performance liquid chromatographic (HPLC) procedure is described which allows the assay of several antibacterial drugs in combination in a matrix of bacterial cell cultures. The drugs assayed were dibromopropamidine, trimethoprim, sulphadiazine and sulphamerazine. It is also shown that p-aminobenzoic acid, which is an essential metabolite of many micro-organisms, does not interfere and can itself be quantified. The method uses solid-phase extraction on a cyclohexyl-bonded silica with subsequent separation of the analytes by reversed-phase HPLC. Tetrabutylammonium is used in order to reduce the retention of trimethoprim and dibromopropamidine and quantification is by ultraviolet detection at 254 nm. The analytical characteristics of the proposed method are shown for certain drug combinations.     

High-performance liquid chromatography systems for the separation of benzodiazepines and their metabolites

The high-performance liquid chromatographic (HPLC) retention characteristics of 21 benzodiazepine drugs and some of their metabolites have been examined on both silica and ODS-silica packing materials. Four HPLC systems have been considered and retention data are presented for the drugs on these systems. The correlation of retention data on the systems is considered with reference to the problem of identifying unknown benzodiazepines.     

On the utility of predictive chromatography to complement mass spectrometry based intact protein identification

The amino acid sequence determines the individual protein three-dimensional structure and its functioning in an organism. Therefore, “reading” a protein sequence and determining its changes due to mutations or post-translational modifications is one of the objectives of proteomic experiments. The commonly utilized approach is gradient high-performance liquid chromatography (HPLC) in combination with tandem mass spectrometry. While serving as a way to simplify the protein mixture, the liquid chromatography may be an additional analytical tool providing complementary information about the protein structure. Previous attempts to develop “predictive” HPLC for large biomacromolecules were limited by empirically derived equations based purely on the adsorption mechanisms of the retention and applicable to relatively small polypeptide molecules. A mechanism of the large biomacromolecule retention in reversed-phase gradient HPLC was described recently in thermodynamics terms by the analytical model of liquid chromatography at critical conditions (BioLCCC). In this work, we applied the BioLCCC model to predict retention of the intact proteins as well as their large proteolytic peptides separated under different HPLC conditions. The specific aim of these proof-of-principle studies was to demonstrate the feasibility of using “predictive” HPLC as a complementary tool to support the analysis of identified intact proteins in top-down, middle-down, and/or targeted selected reaction monitoring (SRM)-based proteomic experiments.     

High-performance liquid chromatographic separation of molecular species of neutral phospholipids.

Molecular species of neutral phospholipids, phosphatidylcholine (PC) and phosphatidylethanolamine (PE), were resolved by reversed-phase high-performance liquid chromatography (HPLC) using mobile phases of acetonitrile-methanol-water containing tetraalkylammonium phosphates (TAAPs). Competitive interactions of TAAPs and analyte solutes with a reversed-phase HPLC column resulted in reduced retention of PC or PE with concomitant increase in detection sensitivity. The chromatographic data for PC and PE were distinctly different from those for negatively charged phospholipids where ion-pair retention mechanisms prevailed. While PC (or PE) components eluted at longer retention times with a larger size of TAAP, an increase in the TAAP concentration invariably caused a decrease in phospholipid retention times. Optimization of HPLC conditions by using high concentrations (25-100 mM) of tetramethylammonium phosphate in acetonitrile-methanol-water (70:22:8) facilitated elution of components with improved peak symmetry. HPLC separations of neutral phospholipids derived from animal sources were more complex than those from soybeans.     

一种评价固定相表面硅羟基残余的新方法

常规的反相色谱柱评价方法未涉及固定相表面残余硅羟基活性的评价.本文以阿米替林的不对称度作为指标,发展了一种评价固定相表面残余硅羟基的新方法,并对十种不同品牌的反相色谱柱进行评价.基于评价结果,选取其中两支色谱柱对碱性抗茵药物进行色谱分离.结果表明,发展的评价方法能够很好地反映反相固定相的硅羟基残余情况,可以为选择色谱柱分离有机碱提供有价值的信息.     

Liquid chromatographic profiles of individual compounds of technical toxaphene

The elution orders of 20 hexa- to nonachlorobornanes and five hexa- to octachlorocamphenes were studied with normal-phase silica and amino phase HPLC, reversed-phase HPLC, as well as gel-permeation chromatography (GPC). Twenty-one compounds of technical toxaphene (CTTs) are commercially available and four were isolated from environmental samples. Structure-activity relationships and chromatographic properties were deduced from the data sets derived on these LC systems. The retention on silica (low-resolution LC and HPLC) increased with the polarity of the CTTs. The elution order of CTTs on amino normal-phase HPLC was, for the most part, the same as on silica normal-phase HPLC. The degree of chlorination determined the elution order of CTTs on C18 RP-HPLC. CTTs eluted from medium-pressure GPC with decreasing molecular size. Chlorobornanes with dichloro substituents on the six-membered ring eluted after the chloroboranes without geminal chlorine atoms on secondary carbons, indicating that these congeners are larger. Altogether, the results increase the knowledge of complex substance class and may serve as a tool in order to gain further standard components.