Direct HPLC resolution of beta-aminoalcohol (tazifylline,ranolazine, sotalol) enantiomers

Summary A routine chiral analysis has been developed to control the optical purity of chiral drugs and to monitor their asymmetric synthesis. The recent advent of new chiral stationary phases for HPLC enabled us to achieve the direct resolution of chiral drugs without any derivatization. The factors affecting chiral resolution on a new alpha₁-acid glycoprotein column (EnantioPac, LKB) were assessed with three beta-aminoalcohols.     

Magnetic properties on holmium iron garnet in high magnetic field. Optical absorption spectra in the infra-red region

On single crystals of holmium iron garnet (HoIG), magnetic properties have been studied in magnetic field up to 150kOe applied parallel to the main crystallographic directions in the 4.2–300K temperature range. Above 130 K, the magnetization is isotropic and linear magnetic field dependent as previously found in polycrystals and predicted by Néel's ferrimagnetic theory. Nevertheless the paramagnetic Curie temperature is much higher than the polycrystal value. Below 130K, due to the onset of the umbrella structure, the ferrite magnetization presents a non linear field variation with [111] as easy direction. The field evolutions of the anisotropy constants (K ₁ andK ₂) were calculated. Optical absorption measurements of both 5₈5I ₆ and 5I ₈5I ₇ transitions are reported and compared to the results of the literature in terms of inequivalent magnetic sites.     

Influence de l'oxygene adsorbe sur la sulfatation de l'oxyde de nickel par le dioxyde de soufre

The interactions between gaseous sulfur dioxide and nickel oxide at 250° have been investigated by means of temperature-programmed desorption (TPD) and microcalorimetric techniques. Depending on the thermal treatment of the oxide, different NiO samples were prepared containing chemisorbed oxygen species, O¹, O², O³ and O⁴, with different energies. The calorimetric data indicated that the weakly-bound species O¹ is the most reactive of the oxygen forms towards sulfur dioxide. In this case, the TPD curves (m/e=48 andm/e=32) show a new peak at 710°; this may be correlated with the desorption of a sulfur-containing compound, probably NiSO₄, created by oxidation of sulfur according to the reaction S^IVS^VI. The regeneration of the species O¹ has been studied as a function of the temperature of oxygen adsorption; the most favourable temperature for the sulfation of nickel oxide appears to be about 400°.

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Zusammenfassung Die Wechselwirkung zwischen gasförmigen Schwefeldioxid und Nickeloxid bei 250° wurde mittels temperaturprogrammierter Desorption (TPD) und mikrokalorimetrischer Techniken untersucht. Abhängig von der thermischen Behandlung der Proben wurden verschiedene, die Sauerstoffspecies O¹, O², O³ und O⁴ mit unterschiedlichen Energien enthaltenden NiO-Proben hergestellt. Die kalorimetrischen Daten weisen darauf hin, dass die schwach gebundene Species O¹ gegenüber Schwefeldioxid die reaktivste von diesen Sauerstoffarmen ist. In diesem Falle zeigt die TPD-Kurve (m/e=48 undm/e=32) einen neuen Peak bei 710°; das kann mit der Desorption einer schwefelhaltigen Verbindung, wahrscheinlich NiSO₄, erklärt werden, die durch Oxydation von Schwefel entsprechend der Reaktion S^IVS^VI gebildet wird. Die Regeneration der Species O¹ wurde in Abhängigkeit von der Temperatur der Sauerstoffadsorption untersucht; die günstigste Temperatur für die Überführung von Nickeloxid in das Sulfat scheint etwa 400° zu sein.

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- 250° . , NiO, O¹, O², O³ O⁴ . , , O¹ - . , - (/=48 32) 710°, , NiSO₄ . O¹ . , 400°.

     

New Syntheses of Retinal and Its Acyclic Analog γ‐Retinal by an Extended Aldol Reaction with a C6 Building Block That Incorporates a C5 Unit after Decarboxylation. A Formal Route to Lycopene and β‐Carotene

Since the C₁₅ β‐end‐group aldehyde 10 ((β‐ionylidene)acetaldehyde), an excellent intermediate in the syntheses of retinoids, can be synthesized in many ways from β‐ionone, and since the corresponding acyclic C₁₅ ψ‐end‐group aldehyde 5 can easily be synthesized from citral ( 1 ) (Scheme 3), we applied the C₁₅+C₅ route to the syntheses of γ‐retinal ((all‐E)‐ 8 ) (Scheme 3) and retinal ((all‐E)‐ 13 ) (Scheme 4), and therefore, by coupling (2×C₂₀→C₄₀), to the preparation of lycopene ( 14 ) and β‐carotene ( 15 ) (Scheme 5). Our new syntheses of retinal ((all‐E)‐ 13 ) and γ‐retinal ((all‐E)‐ 8 use an extended aldol reaction with a C₆ building block that incorporates a C₅ unit after decarboxylation.     

Detection of DNA adducts of benzo[a]pyrene using immunoelectrophoresis with laser-induced fluorescence. Analysis of A549 cells

Detection of benzo[a]pyrene diol epoxide (BPDE)-damaged DNA in a human lung carcinoma cell line (A549) has been performed using free zone affinity capillary electrophoresis with laser-induced fluorescence (LIF). Using BPDE as a model carcinogenic compound, the speed, sensitivity and specificity of this technique was demonstrated. Under free zone conditions, an antibody bound adduct was baseline-resolved from an unbound adduct in less than 2 min. The efficiencies of separation were in excess of 6 x 10(5) and 1 x 10(6) plates per meter for the antibody-bound and unbound adducts, respectively. Separation using a low ionic strength buffer permitted the use of a high electric field (830 V/cm) without the loss of resolving power. Using LIF detection, a concentration detection limit of roughly 3 x 10(-10) M was achieved for a 90-mer oligonuleotide containing a single BDPE. The use of formamide in the incubation buffer to enhance denaturing of DNA did not affect the stability of the complex between the antibody and the adducts. Using a fluorescently labeled BPDE-modified DNA adduct probe, a competitive assay was established to determine the levels of BPDE-DNA adducts in A549 cells.     

Evaluation of a high-performance thin-layer chromatographic technique for the determination of salbutamol serum levels in clinical trials.

Salbutamol concentrations were determined by high-performance thin-layer chromatography in the sera of two sets of ten volunteers at hourly intervals for 6 h after taking one 8-mg slow-release tablet. The influence of time lapse in processing of serum samples, i.e. centrifugation, extraction and chromatography, was studied. A statistical significant instability of salbutamol in the sera of patients was found which was not present in standard drug-free serum samples spiked with salbutamol and used for construction of standard curves.     

The role of β-cyclodextrin and hydroxypropyl β-cyclodextrin in the secondary chemical equilibria associated to the separation of β-carbolines by HPLC

The use of cyclodextrins (CDs) in HPLC as mobile phase additives provides a flexible alternative for the separation of chemically related compounds because these separations can be performed on conventional columns and are economically advantageous over the use of chiral stationary phases. The present paper describes the influence of the presence of β-cyclodextrin (β-CD) and 2-hydroxypropyl-β-cyclodextrin (HPβ-CD) on the separation of the β-carboline alkaloids norharmane, harmane and harmine. The nature of the stationary phase (reverse phases C₁ and C₁₈) affects the chromatographic separations and also the stability of the inclusion complexes that are developed. The changes in the proportion of the organic solvents at constant concentration of CDs (3 mM for β-CD and 15 mM for HPβ-CD) modify the retention factors (k′) for all alkaloids studied. The nature of the organic solvent in the mobile phase also changes the chromatographic parameters. The logarithm of the capacity factor (k′) is linearly increased with the proportion of water in the hydro-organic mobile phase (ethanolic or methanolic) but the slopes obtained vary depending on the CD added to the mobile phase. The role of competitive equilibria, i.e., chromatographic distribution and inclusion complexes formation is discussed. This paper was presented at XIIIth International Cyclodextrin Symposium. Torino, Italy, May, 14–17, 2006     

Screening an In-House Isoquinoline Alkaloids Library for New Blockers of Voltage-Gated Na+ Channels Using Voltage Sensor Fluorescent Probes: Hits and Biases

Voltage-gated Na⁺ (Na_V) channels are significant therapeutic targets for the treatment of cardiac and neurological disorders, thus promoting the search for novel Na_V channel ligands. With the objective of discovering new blockers of Na_V channel ligands, we screened an In-House vegetal alkaloid library using fluorescence cell-based assays. We screened 62 isoquinoline alkaloids (IA) for their ability to decrease the FRET signal of voltage sensor probes (VSP), which were induced by the activation of Na_V channels with batrachotoxin (BTX) in GH3b6 cells. This led to the selection of five IA: liriodenine, oxostephanine, thalmiculine, protopine, and bebeerine, inhibiting the BTX-induced VSP signal with micromolar IC₅₀. These five alkaloids were then assayed using the Na⁺ fluorescent probe ANG-2 and the patch-clamp technique. Only oxostephanine and liriodenine were able to inhibit the BTX-induced ANG-2 signal in HEK293-hNa_V1.3 cells. Indeed, liriodenine and oxostephanine decreased the effects of BTX on Na⁺ currents elicited by the hNa_V1.3 channel, suggesting that conformation change induced by BTX binding could induce a bias in fluorescent assays. However, among the five IA selected in the VSP assay, only bebeerine exhibited strong inhibitory effects against Na⁺ currents elicited by the hNav1.2 and hNav1.6 channels, with IC₅₀ values below 10 µM. So far, bebeerine is the first BBIQ to have been reported to block Na_V channels, with promising therapeutical applications.