Understanding Retention Mechanisms And Adjusting Selectivity Of Basic Pharmaceutical Separations By Reversed Phase Liquid Chromatography PDF Download

Despite the wide range of HPLC stationary phases available for reversed-phase high-performance liquid chromatography (RP-HPLC) and the in-depth studies using probes to highlight differences between them, there is very little in the way of stationary phases which offer selectivity that is substantially different from that offered by the very commonly used alkyl-silicas. Therefore, the primary aim of the research programme was to explore and try to exploit LC stationary phases which offered genuinely different selectivity to alkyl-silicas for typical drug applications. Chiral stationary phases (CSP) potentially had different selectivity and in this context a secondary aim was to explore aspects of the enantioselectivity of CSP as well as their chemical selectivity. Claims of orthogonal selectivity had been made for pentafluorophenyl (PFP) phases and phases exhibiting the hydrophilic interaction liquid chromatography (HILlC) mode. However, the Ultra PFP phase was found to be very similar in selectivity to ACE 5 C18 for both amitriptyline and acemetacin related compounds. The ZIC-HILlC phase was shown to behave as a reversed-phase material at high aqueous content in the mobile phase. There was some indication of selectivity orthogonal to that of ACE 5 C18 with low aqueous content in the mobile phase but this occurred at low retention and with mobile phases unsuitable for use with C18 phases in coupled (column or phase) systems. Nonetheless the work carried out shed more light on the mechanisms taking place in the HILlC mode which is currently attracting so much interest. Also it was possible to put ZIC-HILlC to good use for polar plant metabolites and other applications. Chiral stationary phases (CSP) also offered the prospect of selectivity orthogonal to that of C18 phases. Given the proliferation of such phases though and the fact that it would be useful to use CSP that gave chiral separations for a broad spectrum of compound classes as well as giving orthogonal separations between different compounds, it was decided to carry out comparative studies of CSP classes in order to identify any redundancies and to seek out CSP that were complementary to one another. The Regis Whelk-01 CSP was shown to be much superior to other higher-generation Pirkle-concept CSP such as DACH-DNB and ULMO. Also it was shown to be complementary to the Chiralcel OD derivatised polysaccharide CSP and that both had something to offer alongside the widely used Chiralpak AD derivatised polysaccharide CSP. It was also found that a series of Chiralcel OD clones were virtually identical to Chiralcel OD and similarly for Chiralpak AD clones. Chiralpak lA, an immobilised version of Chiralpak AD, was not markedly less enantioselective than Chiralpak AD. Chiralcel OJ was less enantioselective than Chiralpak AD but the gap in performance was not as wide as between Whelk-01 and the other Pirkle-concept CSP. The information gathered during these studies should prove to be of enormous value for further work in chiral LC method development screening. Before embarking on applications work utilising the stationary phase selectivity that had been found, a study was carried out on the effectiveness of the high efficiencies obtainable with short run times through ultra-performance liquid chromatography (UPLC). It was found that, for a range of pharmaceutical applications, that it was still necessary in each case to adjust selectivity before increasing speed through working at higher temperatures with faster flow rates. In the course of this work some exceptionally high speed separations for example for paroxetine and related substances, benzodiazepines and flurbiprofen and related substances, were developed. With respect to the evaluation of CSP as orthogonal phases to alkyl silicas under reversed-phase conditions, the Whelk-01 CSP showed promise. However on closer inspection it was found that the Whelk-01 CSP had very similar selectivity to the alkyl silica phase, ACE 5 C18, and deviation from this only occurred in instances when there was interaction with the chiral recognition site to give a separation of enantiomers. This prompted the notion that, rather than using Whelk- 01 in a coupled column system with ACE 5 C18, it could be used on its own for the separation of both trace enantiomer and all other related substances. This was shown to be possible using (S)-naproxen, laevokalim and (S)-flurbiprofen as illustrative examples. The evaluation of the enantioselectivity of CSP led to an optimised resolution (suitable for scaling up for preparative work) of the enantiomers of the former 'legal-high' drug, mephedrone, on Whelk-01 under normal phase conditions. It was also shown that the infrequently used Chiralcel OJ derivatised polysaccharide CSP was ideal for developing an assay to determine trace amounts of (R)-nicotine in (S)-nicotine. Overall, the information obtained on stationary phase selectivity and retentivity through evaluation and application will be of great value in HPLC and UHPLC column selection and also selection of orthogonal phases for coupled column systems but, ultimately, moving forward, most value may be in aiding the design of two-dimensional LC systems for complex mixture analysis. This would particularly apply to the use of CSP with reversed-phase eluents in achiral-chiral systems.