Enantiomeric mixtures

In another example of enantioselective distillation, it was the enantiomeric mixture to resolve itself which contributed to create a chiral environment. Thus, non-racemic mixtures of a-phenylethylamine were enantiomerically enriched by submitting to distillation different salts of this amine with achiral acids [199]. 

All enantioselective separation techniques are based on submitting the enantiomeric mixture to be resolved to a chiral environment. This environment is usually created by the presence of a chiral selector able to interact with both enantiomers of the mixture, albeit with different affinities. These differences in the enantiomer-selector association will finally result in the separation that is sought. 

The implications for films cast from mixtures of enantiomers is that diagrams similar to those obtained for phase changes (i.e., melting point, etc.) versus composition for the bulk surfactant may be obtained if a film property is plotted as a function of composition. In the case of enantiomeric mixtures, these monolayer properties should be symmetric about the racemic mixture, and may help to determine whether the associations in the racemic film are homochiral, heterochiral, or ideal. Monolayers cast from non-enantiomeric chiral surfactant mixtures normally will not exhibit this feature. In addition, a systematic study of binary films cast from a mixture of chiral and achiral surfactants may help to determine the limits for chiral discrimination in monolayers doped with an achiral diluent. However, to our knowledge, there has never been any other systematic investigation of the thermodynamic, rheological and mixing properties of chiral monolayers than those reported below from this laboratory. 

Syntheses of naphthyridone derivatives follow the same procedures as those of quinolones, except that substituted 2-aminopyridines (Gould-Jacobs modification) or substituted nicotinic ester/nicotinoyl chloride are used instead of anilines or o-halobenzoic acid derivatives. Most of the recently introduced quinolone antibacterials possess bicyclic or chiral amino moieties at the C-7 position, which result in the formation of enantiomeric mixtures. In general, one of the enantiomers is the active isomer, therefore the stereospecific synthesis and enantiomeric purity of these amino moieties before proceeding to the final step of nucleophilic substitution at the C-7 position of quinolone is of prime importance. The enantiomeric purity of other quinolones such as ofloxacin (a racemic mixture) plays a major role in the improvement of the antibacterial efficacy and pharmacokinetics of these enan-... 

One of the most powerful methods for determining enantiomer composition is gas or liquid chromatography, as it allows direct separation of the enantiomers of a chiral substance. Early chromatographic methods required the conversion of an enantiomeric mixture to a diastereomeric mixture, followed by analysis of the mixture by either GC or HPLC. A more convenient chromatographic approach for determining enantiomer compositions involves the application of a chiral environment without derivatization of the enantiomer mixture. Such a separation may be achieved using a chiral solvent as the mobile phase, but applications are limited because the method consumes large quantities of costly chiral solvents. The direct separation of enantiomers on a chiral stationary phase has been used extensively for the determination of enantiomer composition. Materials for the chiral stationary phase are commercially available for both GC and HPLC. 

In a study of the flash vacuum pyrolysis of chiral isopropylidene N-isopropyl-N-(a-methylbenzyl)aminomethylenemalonates, (/ )- and (S)-(1239), McNab and Monahan demonstrated the existence of another intermediate (1242) in the reaction pathway from the methyleneketene (1240) to the pyrrolinone (1243) [87CC138 88JCS(P 1)869]. Pyrolysis of the enantiomers (R) and (S) of compound 1239 resulted in the formation of an enantiomeric mixture of l-isopropyl-5-methyl-5-phenyl-2-pyrrolin-5-one (1243), where incomplete chirality loss was observed (see Scheme 50). 

The enantiomeric purity of protected amino acids used in peptide synthesis can be determined by pre-column partial deprotection followed by derivatization with Marfey s reagent (116). The Marfey diastereoisomers can be easily resolved and determined by RP-HPLC using an ODS-Hypersil column288. Fifteen amino acids collected from mammalian tissues were derivatized with Marfey s reagent and subjected to two-dimensional TLC. Each individual spot (enantiomeric mixture of a diasteroisomer) was then resolved by RP-HPLC. Except for tyrosine (46) and histidine (117), subnanomole quantities of enantiomers could be analyzed289,290. 

The chiral reagent 122 was proposed for derivatization of enantiomeric mixtures of amino acids. Good HPLC separations were obtained for the diasteroisomer derivatives of a series of amino acids, including some unusual a-amino acids with long or bulky side chains, aryl and hetaryl groups, and -substituted /J-amino acids297. 

Rifamycin B (136), a macrocyclic antibiotic of the ansamycin class, associates enan-tioselectively with amino alcohols. As 136 bears a carboxyl group, it can be used as a host molecule to resolve enantiomeric mixtures by CE. This was applied to analyze a variety of drugs, including terbutalin (137), bamethan (138), norphenylephrine (139),... 

An alternative approach is provided by NMR spectroscopy. Separate NMR signals can be in principle obtained for stable or short-lived diastereomeric derivatives of the enantiomeric mixtures, the intensities of which are correlated with the enantiomeric composition and their relative stereochemistry to the absolute configuration. For this reason, great effort has been continually devoted to the development of new chiral auxiliaries for NMR spectroscopy. The majority of these are dedicated to the chiral assay of molecules having polar functional groups. 

Recently, it was found that the commercially available heptakis(2,3,6-tri-0-methyl)-/i-cyclodextrin (permethylated /1-cyclodextrin, TRIMEB), induced nonequivalence in the NMR spectra, in CD3OD, of enantiomeric mixtures of trisubstituted allenes devoid of polar functional groups, thus affording a simple and general way to determinations of their enantiomeric purity63. 

This definition refers to an enantiomeric mixture produced in an asymmetric synthesis. In some cases where a diastereomeric mixture is produced, the definition has to be altered accordingly. Percent optical purity is an operational term that depends on optical rotation measurements. It is not necessarily equal to the percent enantiomeric purity (13), which is a more meaningful term and is the extent to which one enantiomer is formed in excess over the other ... 

These schemes have been frequently suggested [105-107] as possible mechanisms to achieve the chirally pure starting point for prebiotic molecular evolution toward our present homochiral biopolymers. Demonstrably successftd amplification mechanisms are the spontaneous resolution of enantiomeric mixtures under race-mizing conditions, [509 lattice-controlled solid-state asymmetric reactions, [108] and other autocatalytic processes. [103, 104] Other experimentally successful mechanisms that have been proposed for chirality amplification are those involving kinetic resolutions [109] enantioselective occlusions of enantiomers on opposite crystal faces, [110] and lyotropic liquid crystals. [Ill] These systems are interesting in themselves but are not of direct prebiotic relevance because of their limited scope and the specialized experimental conditions needed for their implementation. 

Using cyclohexylamine, as M ef, the data for various enantiomeric mixtures ofl-(l-naphthyl)ethylamine (M) display a linear relationship between RPIj /RPP and ee. Enantiomeric impurieties as small as about 2% can currently be detected with this method." " Variable-temperature FT-ICR-MS measurements of the ligand... 

Similar differentiation between enantiomers by means of NMR can also be achieved by the use of chiral lanthanide shift reagents (243). Tris-[3-(heptafluoropropylhydroxymethylene)-d-camphorato] -europium was used for the first time (244) for determining the enantiomeric content of benzyl methyl sulfoxide 34. The enantiomeric composition of the partially resolved methyl p-tolyl sulfoxide 41 was estimated using tris-[3-(r-butylhydroxymethylene)-c -camphorato]-europium (245). Another complex of europium, tris-[3-(trifluoro-methylhydroxymethylene)-c -camphorato] europium (TFMC), in contrast to those mentioned above, was effective in the differentiation of various enantiomeric mixtures of chiral sulfinates (107), thiosul-finates (35), and sulfinamides (246). 

Two other direct methods of GC analysis on chiral stationary phases of enantiomeric mixtures are ... 

Stereoselective polymerization may proceed by ionic or coordination mechanisms. In many cases one admits that in the counterion or in the catalytic complex enantiomeric active centers exist, which give rise to predominantly (R) or (S) chains, respectively. Such centers may exist prior to polymerization or may be formed by reaction of a nonchiral precursor with the enantiomeric mixture of the monomers. Alternatively, one can think that the stereoselectivity depends mainly on the interaction between the entering monomer molecule (which is chiral) and the last unit in the chain (also chiral) according to this hypothesis, the enantiomeric excess inside each chain is generally low, because the occurrence of an accidental error brings about an inversion of the sense of stereoselection. 

If an enantiomer is chemically pure it is possible to determine its degree of enantiomeric purity by measuring its optical rotation relative to a standard value, e.g if an enantiomeric mixture contains 1% of enantiomer A and 99% of enantiomer B [a] will be reduced by 2% compared to the value for optically pure B. Examples of the measurement of optical rotation as a quality control check are found in the BP monographs for Timolol maleate, Tobramycin and Phenylephrine Hydrochloride. 

This cycloaddition-reduction-hydrolysis sequence was also used in an approach to butyrolactones related to ribonolactone (71). These compounds are inducing agents of hunger and satiety in mammalians. Here, a subsequent aldol 1,3-diol reduction was used, and the required carboxy function was established by oxidation of the aromatic ring with ruthenium tetroxide. Cycloaddition of benzonitrile oxide to allyl alcohol afforded an enantiomeric mixture of isoxazolines 55 and 56, which were treated with sodium hydride and methyl iodide to achieve separation by chromatography on cellulose triacetate (71). 0-Demethylation, followed by... 

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