Cetyl‐alcohol‐reinforced hollow fiber solid/liquid‐phase microextraction and HPLC–DAD analysis of ezetimibe and simvastatin in human plasma and urine

A new cetyl‐alcohol‐reinforced hollow fiber solid/liquid‐phase microextraction (CA–HF–SLPME) followed by high‐performance liquid chromatography–diode array detection (HPLC–DAD) method was developed for simultaneous determination of ezetimibe and simvastatin in human plasma and urine samples. To prepare the CA–HF–SLPME device, the cetyl‐alcohol was immobilized into the pores of a 2.5 cm hollow fiber micro‐tube and the lumen of the micro‐tube was filled with 1‐octanol with the two ends sealed. Afterwards, the prepared device was introduced into 10 mL of the sample solution containing the analytes with agitation. Under optimized conditions, calibration curves plotted in spiked plasma and urine samples were linear in the ranges of 0.363–25/0.49–25 μg L^?1 for ezetimibe/simvastatin and 0.193–25/0.312–25 μg L^?1 for ezetimibe/simvastatin in plasma and urine samples, respectively. The limit of detection was 0.109/0.174 μg L^?1 for ezetimibe/simvastatin in plasma and 0.058/0.093 μg L^?1 for ezetimibe/simvastatin in urine. As a potential application, the proposed method was applied to determine the concentration of selected analytes in patient plasma and urine samples after medication and satisfactory results were achieved. In comparison with reference methods, the CA–HF–SLPME–HPLC–DAD method demonstrates considerable potential in the biopharmaceutical analysis of selected drugs.     

Diisothiocyanates as heterodienophiles or dipolarophiles in the presence of α‐thioxothioamides or mesoionic thiazoles

Reactions of α‐thioxothioamides ( 1 ) with diisothiocyanates were carried out in the hope of generating the N,N′‐bis(1,3‐thiazoline‐2‐thiones) ( A ). Although that purpose could not be achieved, we succeeded in preparing the monocycloadducts 7 from the phenylene‐1,2‐diisothiocyanate ( 4 ). The benzimidazole derivatives 8 and 9 were also characterized and a mechanism was assumed to account for this intramolecular process. On the other hand, the regioselective synthesis of the N,N′‐biimidazole ( 13 ) containing the phenylene bridge was performed by the treatment of the 5‐aminothiazolium chloride ( 2 ) with the diisothiocyanate ( 4 ) in a basic medium. The mesoionic derivative 13 probably arises from the monoimidazolium‐4‐thiolate ( 12 ) which was shown to react with the salt 2 under similar conditions to give the primary cycloadduct 14 as an intermediate towards the bis(imidazolium) ( 13 ). © 2001 John Wiley & Sons, Inc. Heteroatom Chem 12:617–624, 2001     

Addition of isocyanides to α‐(methylthio)‐benzylidenamidinium iodides: A surprising access to 2‐(dialkylamino)imidazoles and 3,5‐diamino‐2H‐pyrrolium salts

A number of 2‐(dialkylamino)‐5‐(methylthio)imidazoles 2 are obtained by treating the formamidinium iodides 1a,b with isocyanides R³ NC under mild conditions. Reduction of these species can occur in the reaction medium to furnish the corresponding imidazoles 3 . In some cases, double cycloaddition across the imine bond of starting salts 1 also provides the (azetidin‐1‐yl‐methylene)ammonium iodides 4 . Reactions with tert‐butyl and isopropyl isocyanides in refluxing acetonitrile convert the acetamidinium iodide 1c into the 3,5‐diamino‐2H‐pyrrolium salts 7 . Mechanisms are suggested to account for these ring‐closure processes. © 2000 John Wiley & Sons, Inc. Heteroatom Chem 11:370–376, 2000     

Chitosan loaded with silver nanoparticles,CS‐AgNPs,using thymus syriacus,wild mint,and rosemary essential oil extracts as reducing and capping agents

The present study describes the green method for the preparation of chitosan loaded with silver nanoparticles (CS‐AgNPs) in the presence of 3 different extracted essential oils. The essential oils play dual roles as reductant and capping agents. The reducing power and DPPH (2,2‐diphenyl‐1‐picrylhydrazyl) assay for the 3 essential oils—Thymus syriacus (T), wild mint (M), and rosemary (R)—have been reported. The preparation of CS‐AgNPs was performed by 2 steps. The 3 previously extracted essential oils have been used as reducing and capping agent in the first step, while in the second step, silver nanoparticles were integrated in chitosan. The integration of AgNPs in the structure of chitosan was confirmed by ultraviolet‐visible, Fourier transform infrared spectroscopy, scanning electron microscopy techniques, and energy dispersive X‐ray. Surface plasmon resonance confirmed the formation of CS‐AgNPs with maximum absorbance at λ_max between 405 ‐ 410 and 410 ‐ 430 nm for colloidal and films of CS‐AgNPs, respectively. The intensity of bands at 3408 cm^?1 in the fourier transform infrared spectroscopy measurements was decreased substantially and shifted slightly to lower frequency (?υ = 43 cm^?1). Scanning electron microscopy shows a spherical morphology of AgNPs with size of 62 nm for both colloidal and film samples, and energy dispersive X‐ray analysis shows peaks confirming AgNPs formation.     

Enantioselective determination of modafinil in pharmaceutical formulations by capillary electrophoresis, and computational calculation of their inclusion complexes

A fast capillary electrophoretic method is described for the separation and determination of the enantiomers of the novel wake-promoting agent, modafinil. Several parameters affecting the separation were studied, including the type and concentration of chiral selector, buffer pH, buffer concentration, voltage and temperature. Good chiral separation of the racemic mixture was achieved in less than 5 min with resolution factor Rs?=?2.51, using a bare fused-silica capillary and a background electrolyte (BGE) of 25 mM H₃PO₄?1 M tris solution; pH 8.0; containing 30 mg mL^?1 of sulfated-β-cyclodextrin (S-β-CD). The separation was carried out in normal polarity mode at 25 ^?C, 18 kV and using hydrostatic injection. Acceptable validation criteria for selectivity, linearity, precision, and accuracy were included. The developed method was successfully applied to the assay of enantiomers of modafinil in pharmaceutical formulations. The computational calculations for the enantiomeric inclusion complexes rationalized the reasons for the different migration times between the modafinil enantiomers.     

Uranium and fluorine cycles in the nuclear industry

In the nuclear fuel cycle, fluorine is currently not recycled. In this paper, we have examined the possible routes to implement such a cycle. Because UF₆ deconversion requires an excess of water, aqueous HF is produced. Two alternatives are then possible: either separate HF from H₂O or recycle the HF-H₂O in the deconversion process. Alternative UF₆ deconversion could also be implemented to resorb the high UF₆ inventory.