Resolution of the enantiomers of tetrahydrozoline by chiral HPLC. The racemization of the enantiomers via an imine–enamine tautomerism

Resolution of the enantiomers of the sympathomimetic drug tetrahydrozoline was obtained by chiral HPLC. The isolated enantiomers racemize easily and chiral HPLC experiments allowed the determination of the racemization rate constant. This process occurs via an imine–enamine tautomerism which was studied by UV and ¹H NMR spectroscopies.     

Biological activities of α-pinene and β-pinene enantiomers

The antimicrobial activities of the isomers and enantiomers of pinene were evaluated against bacterial and fungal cells. The agar diffusion test showed that only the positive enantiomers of the α- and β-isomers of pinene were active. The minimal inhibitory concentration (MIC) and minimal microbicidal concentration (MMC) of these monoterpenes were also determined, confirming that the positive enantiomers exhibited microbicidal activity against all fungi and bacteria tested with MICs ranging from 117 to 4,150 μg/mL. However, no antimicrobial activity was detected with the negative enantiomers up to 20 mg/mL. Time-kill curves showed that (+)-α-pinene and (+)-β-pinene were highly toxic to Candida albicans, killing 100% of inoculum within 60 min. By contrast, the bactericidal effect occurred after 6 h in methicillin-resistant Staphylococcus aureus (MRSA). In combination with commercial antimicrobials, ciprofloxacin plus (+)-α-pinene or (+)-β-pinene presented synergistic activity against MRSA whereas an indifferent effect against all fungi was detected when amphotericin B was combined with the positive enantiomers of pinene. The potential of (+)-α-pinene and (+)-β-pinene to inhibit phospholipase and esterase activities was also evaluated, and the best inhibition results were obtained with Cryptococcus neoformans. C. albicans biofilm formation was prevented with the MIC concentration of (+)-α-pinene and twice the MIC value of (+)-β-pinene. Finally, the cytotoxicity of the positive enantiomers of pinene to murine macrophages was evaluated, and 250 μg/mL of (+)-α-pinene and (+)-β-pinene reduced the cell viability to 66.8% and 57.7%, respectively.     

Enantioselective extraction of mandelic acid enantiomers by <Emphasis Type="SmallCaps">L</Emphasis>-dipentyl tartrate and <Emphasis Type="Italic">β</Emphasis>-cyclodextrin as binary chiral selectors

A new binary chiral selector system effective for the enantioselective extraction of racemic mandelic acid is presented. While L-dipentyl tartrate and β-cyclodextrin had a very low enantioselectivity as single selectors, a preferential extraction of D-mandelic acid to the organic phase was found in the binary selector system. Using decanol as organic solvent and pH of a phoshate buffer equal to 2.3, the distribution coefficients of D-and L-mandelic acids as high as 14.9 and 7.0, respectively, and the enantioselectivity value of 2.1 were found at optimum concentration of β-cyclodextrin.     

Can enantiomers be separated in achiral chromatographic systems?

Consideration of chromatography of a nonracemic mixture on an achiral sorbent from a stereochemical point of view allows the claim that partial separation of the excess enantiomer zone from the racemate zone is possible only with analytes capable of self-associating under the conditions of the chromatographic column. It is from these positions that features of this process can be explained and conditions for its maximal proceeding formulated.     

High-performance liquid chromatography of α-amino acid enantiomers on eremomycin-modified silica

The chromatographic behavior of enantiomers of α-amino acids was studied on new chiral stationary phases based on silica gel with macrocyclic glycopeptide antibiotic eremomycin and its aglycone immobilized on the surface. The retention of adsorbates and enantioselectivity of their separation were studied as functions of the structure of the side group of α-amino acids, eluant pH, concentration of organic modifier in the eluant, and temperature. The mechanism of the chiral recognition of α-amino acid enantiomers is discussed.     

Biphasic recognition chiral extraction — novel way of separating pantoprazole enantiomers

This paper presents a biphasic recognition chiral extraction system developed as a new chiral separation technology for the separation of pantoprazole enantiomers, combining a hydrophilic β-CD derivative in the aqueous phase and a hydrophobic tartaric acid in the organic phase which preferentially recognise the (R)-enantiomer and (S)-enantiomer, respectively. In this study, a number of factors which influence the efficiency of the extraction were investigated including types of organic solvents, β-CD and tartaric acid esters and their concentrations, pH and temperature. As a result, enantioselectivity for pantoprazole enantiomers can be improved up to 1.42 under optimised conditions; in addition, it is clear that the combined action of β-CD and tartaric acid esters leads to formation of the biphasic chiral extraction system with a stronger separation capacity than a monophasic chiral extraction system.     

Chiral separation of triazole pesticide enantiomers by high performance liquid chromatography

Four triazole enantiomers of diclobutrazol (erythro form) (1), paclobutrazol (erythro form) (2), diniconazole (3) and uniconazole (4) have been separated by high performance liquid chro-matography (HPLC) on chiral stationary phase (CSP) OA-4700. Chromatographic data and a chiral recongnition model are presented for the separation of these pesticide enantiomers. The influence of column temperature and composition of mobile phase have been described.     

Synthesis of 4-aryl-substituted β-lactam enantiomers by enzyme-catalyzed kinetic resolution

Enantiopure 4-phenyl- and 4-(p-tolyl)-2-azetidinones 3a, 3b, 4a and 4b (with e.e.s of ≥96%) were prepared through lipase-catalyzed asymmetric butyrylation of the primary OH group of N-hydroxymethylated β-lactams (±)-5 and (±)-6 at the (R)-stereogenic centre or by lipase-catalyzed asymmetric debutyrylation of O-butyryloxymethyl-2-azetidinones (±)-7 and (±)-8 at the (R)-stereogenic centre. The ring-opening of lactams 5a, 5b, 6b and 8a with HCl/EtOH afforded the corresponding β-amino ester enantiomers 9a, 9b, 10a and 10b with e.e.s of ≥92%.     

Separation of racemiccloso-3,3-(η3,2-norbornadienyl)rhodacarboranes into enantiomers by HPLC on chiral stationary phasesinto enantiomers by HPLC on chiral stationary phases

Racemiccloso-rhodacarboranes,vis. closo-(η^3,2-C₇H₃-2-CR ₂ ¹ )-1-R²-2-R³-3,1,2-RhC₂B₉H₉ (R¹=R²=R³=H; R¹=H, R²=R³=Me; R¹=R²=R³=Me) and (closo-2,2-(η^3,2-C₇H₇-2-CH₂)-2,1,7-RhC₂B₉H₁₁), were successfully separated into enantiomers by high-performance liquid chromatography (HPLC). Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 4, pp. 759–761, April, 2000.     

A straightforward synthesis of both enantiomers of α-vinylalanine and α-ethynylalanine

This report describes the synthesis of enantiomerically pure (S)- and (R)-α-vinylalanines and (S)- and (R)-α-ethynylalanines, four quaternary α-amino acids, using a straightforward synthetic route and starting from (S)- and (R)-N-Boc-N,O-isopropylidene-α-methylserinals.     

Investigation on chiral capillary columns and their application in separation of enantiomers

Six chiral diamide stationary phases (CSPs), namely N-(3-carbobenzoxypropionyl)-L-Val-tert-butylamide (CSP-1), N-undecenoyl-L-Val-S-α-phenylethylamide (CSP-2), N-undecenoyl-L-Val-R-α-phenylethylamide (CSP-3), OV-225-L-Val-tert-butylamide (CSP-4), XE-60-L-Val-tert-butylamide (CSP-5) and polycyanoethyl vinyl siloxane-L-Val-tert-butylamide (CSP-6), were inves-tigated and CSP-6 was crosslinked within narrow bore (70 μm) fused silica capillary columns. Theseparation of amino acid enantiomers on this narrow bore column by gas chromatography (GC) isillustrated.     

β-Cyclodextrin-based chiral nanocomposite for thin-layer chromatographic detection of enantiomers of fluoxetine

Enantioselective analysis or separation is very essential for improved therapeutic effects of drugs as the pure enantiomeric drug formulations display potential benefits over racemates. In this work, we carried out (i) the synthesis of a nanocomposite of β-cyclodextrin and 3D graphene (G/β-CD NC), and (ii) its application for the detection of fluoxetine enantiomers [(RS)-FLX)] using a thin-layer chromatographic method. The synthesized nanocomposite was introduced into silica gel slurry while preparation of thin-layer plates. The separation conditions were optimized by altering pH, temperature, and mobile phase composition. The method is simple and easy to be optimized, and it can therefore be exploited to assess and monitor routine work of enantiomeric purity of drug enantiomers. The average precision (as measured by RSD) was in the region of 1.35‒1.65% for the enantiomers of (RS)-FLX. The measured limit of detection and limit of quantification for (RS)-FLX enantiomers were 1.8 and 5.4 mg mL^‒1, respectively.

     

Aphamines A–C,dimeric acyclic diterpene enantiomers from Aphanamixis polystachya

Aphamines A–C (1–3), three pairs of acyclic diterpene dimer enantiomers with an unprecedent ploymerization pattern, were discovered from Aphanamixis polystachya by NMR-guided isolation and chiral resolution. The elucidation of their novel carbon skeletons was achieved based on spectroscopic analysis, exciton chirality, and calculated electronic circular dichroism (ECD). Plausible Claisen rearrangement, 5-exo-trig cyclization, and reduction reactions may play important roles in the polymeric biosynthesis pathway. Compounds 1 and 3 showed inhibitory effects on nitric oxide (NO) production (IC₅₀: 6.71–15.36 μmol/L) and reduced the expression of iNOS in LPS-induced RAW 264.7 macrophages.     

Separation of α-cyclohexylmandelic acid enantiomers using biphasic chiral recognition high-speed counter-current chromatography

This work concentrates on a chiral separation technology named biphasic recognition applied to resolution of α-cyclohexylmandelic acid enantiomers by high-speed counter-current chromatography (HSCCC). The biphasic chiral recognition HSCCC was performed by adding lipophilic (−)-2-ethylhexyl tartrate in the organic stationary phase and hydrophilic hydroxypropyl-β-cyclodextrin in the aqueous mobile phase, which preferentially recognized the (−)-enantiomer and (+)-enantiomer, respectively. The two-phase solvent system composed of n-hexane-methyl tert-butyl ether–water (9:1:10, v/v/v) with the above chiral selectors was selected according to the partition coefficient and separation factor of the target enantiomers. Important parameters involved in the chiral separation were investigated, namely the types of the chiral selectors (CS); the concentration of each chiral selector; pH of the mobile phase and the separation temperature. The mechanism involved in this biphasic recognition chiral separation by HSCCC was discussed. Langmuirian isotherm was employed to estimate the loading limits for a given value of chiral selectors. Under optimum separation conditions, 3.5–22.0 mg of α-cyclohexylmandelic acid racemate were separated using the analytical apparatus and 440 mg of racemate was separated using the preparative one. The purities of both of the fractions including (+)-enantiomer and (−)-enantiomer from the preparative CCC separation were over 99.5% determined by HPLC and enantiomeric excess reached 100% for the (±)-enantiomers. Recovery for the target compounds from the CCC fractions reached 85–88% yielding 186 mg of (+)-enantiomer and 190 mg of (−)-enantiomer. The overall experimental results show that the HSCCC separation of enantiomer based on biphasic recognition, in which only if the CSs involved will show affinity for opposite enantiomers of the analyte, is much more efficient than the traditional monophasic recognition chiral separation, since it utilizes the cooperation of both of lipophilic and hydrophilic chiral selectors.     

Discrimination of penicillamine enantiomers using β-cyclodextrin modified CdSe/ZnS quantum dots

The authors describe a method for the differentiation of penicillamine (PA) enantiomers by using CdSe/ZnS quantum dots (QDs) modified with β-cylodextrin (β-CD-CdSe/ZnS QDs). Selective enantiorecognition of L-PA and D-PA was accomplished by virtue of selective host-guest interaction between the PAs and the β-CD pockets on the QDs. The fluorescence intensity of the modified QDs decreases in the presence of L-PA. On the contrary, it increases in the presence of D-PA. These findings form the basis for a new method for recognition of PA enantiomers. Under optimized conditions, a linear relationship exists between fluorescence intensity and D-PA concentration in the 0.1 to 5.0 mg L^?1 range, and between 0.8 and 5.0 mg L^?1 for L-PA. Detection limits are 0.06 mg L^?1 for D-PA, and 0.2 mg L^?1 for L-PA. The potential of this method has been demonstrated by the determination of D-PA in pharmaceutical formulations and L-PA in (spiked) environmental samples.

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Graphical abstract Selective and specific enantiorecognition of penicillamine (PA) enantiomers using β-cylodextrin modified CdSe/ZnS quantum dots is described. Fluorescence intensity increases in the presence of D-PA, but it decreases in the presence of L-PA. Results were the basis for analytical applications.

     

New approach to exclusive formation of both enantiomers of β-amino acid derivatives

A highly selective two-step approach to chiral β-amino esters via the hydride reductive amination of chiral allenes is reported. β-Enamino esters were obtained from the nucleophilic addition of amines to 2,3-allenoates bearing a chiral auxiliary. The reduction of the (1R)-(−)-10-phenylsulfonylisobornyl β-enamino esters gave the corresponding β-amino esters with S configuration whereas the reduction of the (1S)-(+)-10-phenylsulfonylisobornyl β-enamino esters led to β-amino esters with R configuration. The rationalization of the observed selectivity was supported by semi-empirical molecular orbital calculations (PM3).     

Addition products of chlorosulfonylisocyanate to (+)-3-carene and α-pinene enantiomers

Optically active lactams were synthesized from (+)-3-carene and α-pinene enantiomers. Their properties and structures were characterized. A pathway for preparing their trifluoroacetate salts was demonstrated.     

Equilibrium studies on reactive extraction of naproxen enantiomers using hydrophilic ��-cyclodetrin derivatives extractants

A simple and low-cost method using liquid?Cliquid extraction coupled with complexation reactive technique has been developed for enantioselective separation of naproxen enantiomers. Three kinds of modified ??-cyclodextrins including methyl-??-cyclodextrin (Me-??-CD), hydroxyethyl-??-cyclodextrin (HE-??-CD) and hydroxypropyl-??-cyclodextrin (HP-??-CD), were selected as hydrophilic chiral selectors for extraction naproxen from organic phase to aqueous phase. A systematic study of the factors affecting chiral separation performance were investigated. The experiment results obtained show that, HP-??-CD, HE-??-CD and Me-??-CD has stronger recognition abilities for S-naproxen than those for R-naproxen. Among the ??-CD derivatives studied, HP-??-CD has the strongest ability for chiral recognition and separation. Excellent enantioselectivity (a) of 1.59 is obtained under the optimal conditions of pH of 2.5 and temperature of 5 °C.     

A microbially based approach for the asymmetric synthesis of both enantiomers of R-and S-fluoxetine

Both enantiomers of fluoxetine were synthesized in five steps from ethyl benzoylacetate(1)using microbial-chemical approach with overall yields of 59% and 62% respectively.(S)-Enan-tiomer can be obtained in >99% e.e.by resting cell of baker's yeast and the R form was produced in 81 %e.e.by immobilized Geotrichum sp.G 38.     

Separation of drug enantiomers by capillary electrophoresis: α-cyclodextrin as chiral solvating agent

Summary Enantiomer separation by capillary zone electrophoresis was studied for a set of 59 chiral drugs. With -cyclodextrin as chiral solvating agent, six enantiomeric pairs could be resolved. Baseline separation was achieved for clidinium bromide, oxomemazine and tetryzoline, whereas ketamine, orphenadrine, tropicamide and others require further optimization. Aliphatic and monocyclic compounds prevail among compounds recognized by -cyclodextrin. Statistical analysis reveals that a medium degree of migration retardation offers the best chance for successful separation.Part II. For Part I see reference [18].