Instrumentation for SFC systems: Different sampling and restriction designs

Different designs of injection and restriction devices for capillary supercritical fluid chromatography (SFC) have been investigated with respect to their practical applicability and usefulness for reproducible and accurate qualitative and quantitative analyses. In combination with a self-made instrument a fast switching valve is preferable as an injection device compared to a split-injector, and an integral restrictor made from the end of the fused silica (FS) separation column was superior to a linear restrictor made by coupling a small diameter FS-column to the separation column.     

The application of capillary SFC,packed column SFC,and capillary SFC-MS in the analysis of controlled drugs

Multi–component mixtures of controlled drugs, drug impurities, and adulterants have been analyzed by capillary SFC-FID, packed column SFC-UV, and capillary SFC-MS. Isocratic packed column SFC has been performed with binary and ternary mobile phases using a single syringe pump. The combination of capillary SFC and double focusing MS is described with reference to MS source pressures and the spectra obtained. The use of negative temperature programming in SFC is described.     

A model for quantitatively describing linear velocity programming in capillary SFC

Summary Linear velocity in capillary SFC is commonly controlled by restricting capillaries. In this paper, a model is described that quantitatively predicts the linear velocity of a supercritical fluid in SFC using tapered or ceramic frittype restrictors. In this model, the flow from the restricting capillary is assumed to be an isentropic expansion. The variation of the linear velocity as a function of pressure, temperature and cross-sectional area of the restricting aperture was predicted by this model. This predictive capability is important to the use of gradient programming in capillary SFC. Finally, the ideal variable restrictor for gradient programming was found to be one that could reversibly increase or decrease the linear velocity independent of the pressure, temperature, and/or density conditions used to create the gradient.     

SFC in analysis of aromatic plants

Capillary SFC was applied to the analysis of Some plant volatile oils. The results were compared with those obtained by capillary GC. For thyme oil, SFC without derivatization gave about the same percentage composition of the main compounds as CGC with silylation, thus eliminating one working step. For a complex mixture of peppermint oil or basil oil, SFC seems to give more reliable quantification than CGC, especially for oxygenated compounds. However, the separation efficiency of CGC for monoterpene hydrocarbons was, as expected, much better than that of SFC.     

Quantitation in miniaturized GC and SFC systems

Separations of high efficiency and/or speed can be achieved in capillary GC by capillary columns of lower internal diameter (< 50 μm). Sampling techniques for the analytical application of narrow bore fused silica columns have been evaluated with regard to quantitation. On-column injection cannot be applied. Therefore liquid samples have to be vaporized in external devices before they enter the chromatographic system. Sample introduction by syringe with subsequent splitting must and can be applied but requires special syringes with perfect piston sealing because of the high inlet pressures needed even with hydrogen as carrier gas. For general analytical applications, valve systems should be developed to eliminate both the syringe and the septum from instrumental GC set-up's. In SFC using either narrow bore capillary or packed microbore columns, time-controlled valve sampling with partial displacement of the sample from the loop seems to be an adequate technique because of the very high inlet pressures involved. Splitting in combination with valve operation can also be applied in capillary SFC at least to samples of good solubility in the mobile phase. A disadvantage of splitting in SFC is that another restriction for the adjustment of the split flow is necessary.     

Open tubular column supercritical fluid chromatography/mass spectrometry on a benchtop mass spectrometer

A benchtop SFC/MS system is described which utilizes supercritical carbon dioxide in a 50 micron diameter open tubular column interfaced directly to an unchanged commercially available benchtop capillary GC/MS system equipped with a chemical ionization (CI) source. A small amount of methane reagent gas was admitted co-axially to a capillary restrictor at the exit of the capillary chromatographic column. This make-up gas served as the CI reagent gas and appeared to optimize the sensitivity of the system while providing abundant (M+1) ions for the analytes investigated in this study. Good chromatographic intergrity was obtained for the GC/MS test compound, decafluorotriphenylphosphine (DFTPP), but the capillary restrictor appeared to cause some tailing of the ion current profiles resulting from low nanogram levels of caffeine and some fatty acid esters. Improvements in the SFC/MS capillary restrictor interface and the pumping system of the benchtop GC/MS system should increase the capability of this system for future applications.     

Retention in capillary supercritical fluid chromatography

Supercritical fluid chromatography (SFC) sometimes exhibits GC-like behavior and sometimes LC-like behavior, depending on conditions. However, it is not always clear whether one of these types of behavior, or a combination, operates for a particular set of conditions for every solute in a mixture. For example, some components may be partitioned mostly by their vapor pressures, while others, in the same mixture, are partitioned predominantly by solvent-like properties of the mobile phase. Plots of retetion (as log of the capacity factor) vs. reciprocal temperature at constant pressure reveal a clear change in the character of the separation of well-behaved solutes. A thermodynamic explanation of the observed behavior is given, based on the assumption that partitioning is controlled by the heats of solution of solute in the mobile and stationary phases. A model of SFC retention as it deviates from pure-GC behavior on the same column is presented.     

Direct coupling of capillary supercritical fluid chromatography to high resolution mass spectrometry with minimum modification

Summary The coupling of a capillary supercritical fluid chromatograph with a high resolution double focusing mass spectrometer has been accomplished without any modifications to the pumping or ion source systems. The interface utilizes a direct insertion probe (DIP), which was originally designed for the direct analysis of solid samples, together with a trit restrictor as a decompression device. The DIP is placed opposite to the SFC restrictor, and it provides sufficient heat to prevent cluster formation and cooling resulting from the expansion of the supercritical fluid into the vacuum environment. Excellent mass spectra of standard polycyclic aromatic hydrocarbons under chemical-ionization (CI) conditions using methane as the reagent gas, and under charge-exchange (CE) conditions using CO₂ as the charge exchange medium were obtained.     

Fraction collection in capillary electrophoresis for various stand-alone mass spectrometers

A procedure for collecting fractions during capillary electrophoresis for their analysis using various stand-alone instruments is described. The results of a systematic study of the optimization and application of capillary electrophoresis (CE) in conjunction with a reverse-phase high-performance liquid chromatography electrospray ionization quadrupole time of flight-tandem mass spectrometry (RP-HPLC-ESI-Q-TOF-MS/MS) and inductively-coupled mass spectrometry (ICP-MS) to the analysis of the seed extract of the Japanese Pagoda Tree (Sophora japonica) are presented. The off-line coupling of CE to the matrix-assisted laser desorption/ionization-time of flight mass spectrometry (MALDI-TOF-MS) for the proteins mixture was applied. The cathode end of the capillary was placed inside a stainless steel needle using a coaxial liquid-sheath-flow configuration. The optimization of experimental parameters resulted in an efficient methodology for MS analysis of fractions. Several components contained in the extract of S. japonica were identified, some not previously known. It was demonstrated that low sensitivity, which is a real problem in off-line CE–MS analysis, could be tolerated because of a more flexible optimization of the CE separation conditions and the choice of independent stand-alone instruments for analysis of separated fractions. The estimated limit of detection for CE-RP-HPLC-ESI-Q-TOF-MS was 50 μM of polyphenols and for CE-ICP-MS, 1–100 μg/l.     

The solvent venting injection technique in capillary supercritical fluid chromatography

A solvent venting technique for injection of volumes up to 1 μl on 50 μm i.d. SFC columns has been compared to direct injection methods. The peak broadening and peak splitting observed with direct injection have been examined and found to be related to the starting pressure, the column temperature, and the sample solvent, in addition to the sample volume. The solvent venting technique removed peak splitting and improved the column efficiency. With a proper selection of experimental conditions, the sample recovery was 100%. The major part of the solvent was eluted in 15–20 s. Several applications have been demonstrated.     

Modeling of combined electroosmotic and capillary flow in microchannels

In the present study, theoretical model for the transient response of a capillary flow under the combined effects of electroosmotic and capillary forces at low Reynolds number is presented. The governing equation is derived based on the balance among the electrokinetic, surface, viscous and gravity forces. A non-dimensional transient governing equation for the penetration depth as a function of time is obtained by normalizing the viscous, gravity and electroosmotic forces with surface tension force. A new non-dimensional group for the electroosmotic force, E_o, is obtained through the non-dimensional analysis. This new non-dimensional group is a representation of combined electroosmosis and surface tension, i.e., capillarity. The numerical solution of governing equation is obtained to study the effect of different operating parameters on the flow front transport. In a combined flow, it is observed that the flow with positive and low negative magnitude E_o numbers, the attainment of equilibrium penetration depth is similar to a capillary flow. In case of high negative magnitude E_o numbers, complete filling of the channel is observed. The electrolyte with lower permittivity delays the progress of the flow front whereas a large EDL transports the electrolyte quickly. Higher viscous and gravity forces also delay the transport process in the combined flow. This model suggests that in combined flow the electrokinetic parameters also play an important role on the capillary flow and experiments are required to confirm this electrokinetic effect on capillary transport.     

Capillary supercritical fluid chromatography with simultaneous flame ionization and mass spectrometric detection

A simple interface between a capillary supercritical fluid chromatograph and an Extranuclear Simulscan mass spectrometer is described. The SFC column is directly inserted into the ion source through the existing GC-interface. The system is equipped with a splitting device which allows simultaneous EI/MS and flame ionization detection when CO₂ is used as the supercritical phase. The effect of source temperature and pressure on CO₂ clustering was studied for optimization of source conditions. The performance of the system was evaluated with a series of model compounds and standard mixtures.     

Arsenic speciation by coupling capillary zone electrophoresis with mass spectrometry

Summary Capillary zone electrophoresis (CZE) has been coupled with mass spectrometry to enable the identification of mineral and organometallic compounds of arsenic in speciation studies. The electrophoretic effluent was introduced through a concentric interface into the mass spectrometer. Make-up liquid was added to enable electric contact at the outlet of the separation capillary and to assist the electronebulization process. After ionization, the ions were analyzed and quantified with an ion-trap detector. Optimization of the coupling conditions (geometry of the concentric interface, composition and flow rate of the sheath liquid, electronebulization and detection conditions) is described. The results show that the geometry of the concentric interface and the positioning of the outlet of the separation capillary have a critical effect on stability and sensitivity. Programming the electronebulization and detection conditions throughout the analysis enabled identification and quantification of the seven arsenic compounds of interest (neutral, and positively or negatively charged species) in less than 20 min at the ppm level. Limits of detection ranged from 0.5 to 3.3 mg L⁻¹, corresponding to amounts injected ranging from 15 to 60 pg. The linear dependence of mass spectrometric response on arsenic concentration was verified for concentrations ranging from 5 to 200 mgL⁻¹. For the two positively charged species, arsenobetaine and arsenocholine, an on-line preconcentration technique (field-amplified sample injection) enabled reduction of the detection limits by approximately one order of magnitude to 110 and 160 μgL⁻¹, respectively.     

Recent advances in capillary electrophoresis‐mass spectrometry: Instrumentation,methodology and applications

Capillary electrophoresis (CE) offers fast and high‐resolution separation of charged analytes from small injection volumes. Coupled to mass spectrometry (MS), it represents a powerful analytical technique providing (exact) mass information and enables molecular characterization based on fragmentation. Although hyphenation of CE and MS is not straightforward, much emphasis has been placed on enabling efficient ionization and user‐friendly coupling. Though several interfaces are now commercially available, research on more efficient and robust interfacing with nano‐electrospray ionization (ESI), matrix‐assisted laser desorption/ionization (MALDI) and inductively coupled plasma mass spectrometry (ICP) continues with considerable results. At the same time, CE‐MS has been used in many fields, predominantly for the analysis of proteins, peptides and metabolites. This review belongs to a series of regularly published articles, summarizing 248 articles covering the time between June 2016 and May 2018. Latest developments on hyphenation of CE with MS as well as instrumental developments such as two‐dimensional separation systems with MS detection are mentioned. Furthermore, applications of various CE‐modes including capillary zone electrophoresis (CZE), nonaqueous capillary electrophoresis (NACE), capillary gel electrophoresis (CGE) and capillary isoelectric focusing (CIEF) coupled to MS in biological, pharmaceutical and environmental research are summarized.     

Supercritical ammonia as mobile phase in capillary chromatography

Instrumentation was assembled that allows the use of supercritical ammonia as mobile phase in capillary supercritical fluid chromatography. Several modifications of the typical chromatographic system were necessary, especially with respect to injection and detection. In addition, the stabilities of various polysiloxane stationary phases were studied. The chromatography of polarizable and polar basic materials was demonstrated using a nonpolar polysiloxane stationary phase.