Simultaneous assay of four stereoisomers of diltiazem hydrochloride. Application to in vitro chiral inversion studies

Summary The simultaneous stereospecific assay of four stereoisomers of diltiazem hydrochloride in bulk drug and aqueous solution was developed using HPLC on a Chiralcel OF column. The four isomers were quantitated with good precision by the internal standard method. The chiral inversion of (+)-cis-diltiazem hydrochloride in vitro, stability of its (2S, 3S) configuration in the solid and aqueous states was examined by HPLC. Chiral inversion of (+)-cis-diltiazem hydrochloride was not observed in the solid state, and its (2S, 3S) configuration was stable to heat, humidity and light. Chiral inversion of (+)-cis-diltiazem hydrochloride (2S, 3S) was observed in aqueous solution under UV, but not in aqueous solution stored at 80°C for 5 h nor under visible light for 10 h. The (+)-cis-diltiazem hydrochloride (2S, 3S) epimerized to (+)-trans-diltiazem hydrochloride (2R, 3S) with a half-life of 5 h in aqueous solution under UV but the reverse chiral inversion of (+)-trans-diltiazem hydrochloride (2R, 3S) to (+)-cis-diltiazem hydrochloride (2S, 3S) was not observed.     

Synthesis of 2,4-dimethyl-6-oxo-2,4-heptadienoic acid derivatives from 2,4,6-trimethylpyrylium salts

Reaction 2,4,6-trimethylpyrylium salts with sodium cyanide in boiling water yielded the bicyclic lactone 1,3,5-trimethyl-6,8-dioxabicyclo[3.2.1]oct-2-en-7-one (6) along with a series of stereoisomers of 2,4-dimethyl-6-oxo-2,4-heptadienonitrile (5), which were the sole products when the reaction was carried out at room temperature. Compound 6, along with 3,5-dimethylphenol (7), was also obtained by refluxing 5 briefly in aqueous sodium hydroxide. However, when 5 was refluxed for a prolonged period in aqueous sodium acetate, 3,5-dimethyl-5-(2-oxopropyl)-furan-2-one (8), along with some 7, was generated instead. Compound 8 could also be produced from 6 on prolonged refluxing with aqueous sodium acetate, indicating that 6 was the kinetically-controlled and 8 the thermodynamically-controlled product.     

拟除虫菊酯分子设计中的生物同一性

讨论了在拟除虫菊酯分子设计中利用生物同一性，对先导化合物进行一系列化 学改造和修饰，以获得新的拟除虫菊酯。     

Synthesis of spiro[(6-phenyl-3,4-dihydro-2H-1,3-dioxine)-2<Emphasis Type="Italic">R</Emphasis>(<Emphasis Type="Italic">S</Emphasis>), 3′-(19′,28′-oxidooleanan)]-4-ones and X-ray diffraction analysis of their configuration

The structure of two stereoisomeric spiroadducts of allobetulone with 5-phenyl-2,3-dihydrofuran-2,3-dione was established by X-ray diffraction (XRD) analysis. The crystals of the 2R isomer are orthorhombic, P2₁2₁2₁, a = 10.825(5) Å, b = 12.849(6) Å, c = 23.358(9) Å; V = 3249(2) ų, Z = 4, d _calc = 1.200 g/cm³; the crystals of the 2S isomer hemihydrate are triclinic, P1, a = 11.505(7) Å, b = 12.192(8) Å, c = 13.123(8) Å; α = 103.35(5)°, β = 100.80(5)°, γ = 90.98(5)°; V = 1756(2) ų, Z = 2, d _calc = 1.127 g/cm³. The molecular structure of the spiroadducts is discussed.     

Novel modified chiral NiII complexes with the Schiff bases of (E)-and (Z)-2-aminobut-2-enoic acids: Synthesis and study

Ni^II complexes with the Schiff bases of (E)-and (Z)-2-aminobut-2-enoic acids were obtained with (S)-N-(2-benzoylphenyl)-1-(2-chlorobenzyl)pyrrolidine-2-carboxamide and (S)-N-(2-benzoylphenyl)-1-(3,4-dimethylbenzyl)pyrrolidine-2-carboxamide as new chiral auxiliaries. Asymmetric addition of nucleophiles to the C=C bond of these complexes was studied. Published in Russian in Izvestiya Akademii Nauk. Seriya Khimicheskaya, No. 3, pp. 428–435, March, 2006.     

A validated LC–MS/MS method for the simultaneous determination of 20‐(S)‐protopanaxatriol and its two active metabolites in rat plasma: Application to a pharmacokinetics study

We present a validated liquid chromatography with tandem mass spectrometry method for simultaneous determination of 20‐(S )‐protopanaxatriol and its two oxidative stereoisomeric metabolites (20S ,24S )‐epoxy‐dammarane‐3,6,12,25‐tetraol (M1) and (20S ,24R )‐epoxy‐dammarane‐3,6,12,25‐tetraol (M2) in rat plasma. 20‐(S )‐Protopanaxatriol, M1, and M2 were extracted with methanol and separated on an ACQUITY HSS T₃ column. The mass spectrometry detection was accomplished in selected reaction monitoring mode with precursor‐to‐product ion transitions of m/z 493.4→143.1 for M1 and M2, m/z 475.4→391.3 for 20‐(S )‐protopanaxatriol, and m/z 459.4→375.3 for 20‐(S )‐protopanaxadiol (internal standard). The method showed good linearity over the concentration ranges of 1–1000 ng/mL for 20‐(S )‐protopanaxatriol and 0.5–200 ng/mL for M1 and M2, with correlation coefficients of more than 0.995. The lower limits of quantification for 20‐(S )‐protopanaxatriol, M1, and M2 were 1, 0.5, 0.5 ng/mL, respectively. The intra‐ and interday precisions (RSD, %) were less than 10.41% while the accuracy (relative error, %) ranged from –3.14 to 8.73%. Under the current conditions, M1 and M2 were completely separated within 3 min. The validated assay was successfully applied to evaluating pharmacokinetic profiles of 20‐(S )‐protopanaxatriol, M1, and M2 in rat.     

Stereoisomeric effects in thermo‐remendable polymer networks based on Diels–Alder crosslink reactions

This study describes the synthesis, the spectroscopic, and the thermal characterization of linear and crosslinked polymers as well as a number of corresponding model compounds, containing Diels–Alder adducts derived from furan and maleimide groups. The thermal reversibility (rDA, DA) of structurally varied model compounds, polymeric and network structures were studied by differential scanning calorimetry, where possible in combination with ¹H NMR spectroscopy. It was established that the endo and exo DA stereoisomers show significantly different thermal responses: the rDA of the endo DA‐adducts typically takes place at 20–40 K lower temperatures than that of the corresponding exo DA‐adducts in all cases, with the exception of some aromatic maleimides. Although in situ isomerization was observed to a limited extent and only in some cases, this effect is not expected to influence the thermoremendability of DA‐crosslinked networks being dependent on two separate stereoisomeric rDA steps. © 2010 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 48: 3456–3467, 2010     

Crystallographic report: Triorganotin 2‐(p‐chlorophenyl)‐3‐methylbutyrates

The crystal structures of two triorganotin butyrates were determined. Tricyclohexyltin 2‐(p‐chlorophenyl)‐3‐methylbutyrate was determined to have a distorted tetrahedral geometry. Trimethyltin 2‐(p‐chlorophenyl)‐3‐methylbutyrate, on the other hand, was found to be polymeric in nature with a trigonal bipyramidal configuration. The three methyl groups are located in the equatorial positions with the axial positions occupied by oxygen atoms from two different carboxylate groups. Copyright © 2003 John Wiley & Sons, Ltd.     

Chemoenzymatic synthesis and HPLC analysis of the stereoisomers of miyakosyne A [(4E,24E)-14-methyloctacosa-4,24-diene-1,27-diyne-3,26-diol], a cytotoxic metabolite of a marine sponge Petrosia sp., to determine the absolute configuration of its major component as 3R,14R,26R

Six samples [(3R,14R,26R)-, (3R,14S,26R)-, (3S,14R,26S)-, and (3S,14S,26S)-1, a mixture of (3R,14R,26S)- and (3S,14R,26R)-1, and a mixture of (3R,14S,26S)- and (3S,14S,26R)-1] of miyakosyne A [1, (4E,24E)-14-methyloctacosa-4,24-diene-1,27-diyne-3,26-diol] were synthesized starting from the enantiomers of citronellal (2), employing olefin cross metathesis and R-selective asymmetric acetylation of a stereoisomeric mixture of acetylenic alcohols with vinyl acetate and lipase PS as key reactions. Separation of the eight stereoisomer of 1 by reversed phase HPLC at −56 °C was achieved after their esterification with (1R,2R)-2-(anthracene-2,3-dicarboximido)cyclohexanecarboxylic acid (16), and the natural miyakosyne A was found to be a mixture of 95.7% of (3R,14R,26R)-1 and 4.3% of (3R,14S,26R)-1. This is different from the (3R,14S,26R)-configuration of 1 as tentatively assigned by X-ray analysis.     

Synthesis of derivatives and production of antiserum for class specific detection of pyrethroids by indirect ELISA

Two series of haptens including 3-phenoxybenzoic acid (PBA) and 3-(2-chloro-3, 3,3-trifluoroprop-1-enyl)-2,2-dimethylcyclo-propanecarboxylic acid (CF₃MPA) were used to prepare immunogens through attachment of 4-C or 6-C handles. Class selective antibodies were produced by immunising rabbits. Ab502 showed the highest reactivity towards tau-fluvalinate (IC₅₀ 1.3 ng mL^?1), λ-cyhalothrin (IC₅₀ 2.3 ng mL^?1), cyfluthrin (IC₅₀ 2.2 ng mL^?1) and fenpropathrin (IC₅₀ 18.5 ng mL^?1) among the antibodies in a competitive ELISA. The effects of methanol, pH and salt concentration were optimised for maximum efficiency of the ELISA (Enzyme-Linked ImmunoSorbent Assay). Ab502 (1:80000)/2-OVA-1(0.2 µg mL^?1) was chosen for ELISA optimisation. Finally, 0.05 M phosphate buffered saline (PBS) at pH 6.5 containing 30% methanol (v/v) was used to dilute the standards. Target analytes in honey samples were extracted with ethyl acetate by sonication. The samples were spiked with three different concentrations of each compound (tau-fluvalinate, 0.5 ng g^?1, 3 ng g^?1, 12 ng g^?1; λ-cyhalothrin and cyfluthrin 1 ng g^?1, 5 ng g^?1, 65 ng g^?1). The recoveries were 36–59% at the lowest spiking concentration and 61–81% at the higher concentration. This assay might be useful to screen pyrethroid residues in honey or other matrix.