Carboxylic acids, resolution with

On the other hand, resolution of racemic a-halo carboxylic acids (93) with butanol can be effected with lipase (Table 7 and equation 35). Applications of enzyme-catalyzed acyl transfer reactions, among many others, are the synthesis of the pheromone (5)-sulcatol (95 equation 36) and of (/ )-glycidylbu-... 

Fig. 17. Kinetic resolution of alcohols (A and A ) and carboxylic acids (B) with an i -selective enzyme the site of chirality is shown by an asterisk.

Palkowitz and coworkers [15] reported classical resolution of the imidazo-lyl carboxylic acid (1) with (-)-cinchonidine, as part of an integrated approach to triacid angiotensin II antagonists. The (/ )-enantiomer of (1) thus obtained was then subjected to peptidic coupling with amino ester (2), prepared from rran -4-hydroxy-L-proline, a widely available chirality-pool material. 

This method is widely used for the resolution of chiral amines and carboxylic acids Analogous methods based on the formation and separation of diastereomers have been developed for other functional groups the precise approach depends on the kind of chem ical reactivity associated with the functional groups present m the molecule... 

This was transformed into the quaternary d-bromocamphorsulphonate, m.p. 265°, but no resolution has yet been effected. The lactam of 3-carboxyhexahydrocarbazole-1 ll-)3 8 -dipropionic acid (XXIV, with a carboxyl group at C ), CigH jO N, rn.p. 257-8°, has also been prepared. The same authors, with Holmes, have synthesised the lactam of 11-ethylhexahydrocarbazole-l-)3-propionic acid, Ci,H3iON, m.p. 106-8-107-5°, of which (XXrV) is a carboxy-derivative. 

The latter approach is used in the enantioselective determination of a Phase I metabolite of the antihistaminic drug, terfenadine. Terfenadine is metabolized to several Phase I compounds (Fig. 7-13), among which the carboxylic acid MDL 16.455 is an active metabolite for which plasma concentrations must often be determined. Although terfenadine can be separated directly on Chiralpak AD - an amy-lose-based CSP - the adsorption of the metabolite MDL 16.455 is too high to permit adequate resolution. By derivatizing the plasma sample with diazomethane, the carboxylic acid is converted selectively to the methyl ester, which can be separated in the presence of all other plasma compounds on the above-mentioned CSP Chiralpak AD [24] (Fig. 7-14). Recently, MDL 16.455 has been introduced as a new antihistaminic drug, fexofenadine. 

The synthesis of key intermediate 12, in optically active form, commences with the resolution of racemic trans-2,3-epoxybutyric acid (27), a substance readily obtained by epoxidation of crotonic acid (26) (see Scheme 5). Treatment of racemic 27 with enantio-merically pure (S)-(-)-1 -a-napthylethylamine affords a 1 1 mixture of diastereomeric ammonium salts which can be resolved by recrystallization from absolute ethanol. Acidification of the resolved diastereomeric ammonium salts with methanesulfonic acid and extraction furnishes both epoxy acid enantiomers in eantiomerically pure form. Because the optical rotation and absolute configuration of one of the antipodes was known, the identity of enantiomerically pure epoxy acid, (+)-27, with the absolute configuration required for a synthesis of erythronolide B, could be confirmed. Sequential treatment of (+)-27 with ethyl chloroformate, excess sodium boro-hydride, and 2-methoxypropene with a trace of phosphorous oxychloride affords protected intermediate 28 in an overall yield of 76%. The action of ethyl chloroformate on carboxylic acid (+)-27 affords a mixed carbonic anhydride which is subsequently reduced by sodium borohydride to a primary alcohol. Protection of the primary hydroxyl group in the form of a mixed ketal is achieved easily with 2-methoxypropene and a catalytic amount of phosphorous oxychloride. 

Several early reports dealt with the resolution of racemic aziridine-2-carboxylic acids [72, 73], Treatment of ( )-78 (Scheme 3.25) with (-)-trans-2,3-bis(hydroxydi-phenylmethyl)-l,4-dioxaspiro[5.4]decane (79), for example, afforded the 1 1 ratio inclusion compound 80. Upon distillation, the inclusion compound 80 gave en-antiomerically pure (-)-78 in 33% yield. 

Most resolution is done on carboxylic acids and often, when a molecule does not contain a carboxyl group, it is converted to a carboxylic acid before resolution is attempted. However, the principle of conversion to diastereomers is not confined to carboxylic acids, and other groupsmay serve as handles to be coupled to an optically active reagent. Racemic bases can be converted to diastereomeric salts with active acids. Alcohols can be converted to diastereomeric esters, aldehydes to diastereomeric hydrazones, and so on. Even hydrocarbons can be converted to diastereomeric inclusion... 

Enantiopure (R)- and (S)-nipecotic acid (Nip) derivatives 64 were obtained following classical resolution of ethyl nipecotate with either enantiomer of tartaric acid and successive recrystallization of the corresponding salts [153, 154, 156] or by resolution of racemic nipecotic acid with enantiomerically pure camphorsul-fonic acid [154]. N-Boc protected pyrrolidine-3-carboxylic acid (PCA) 65 for the synthesis of homo-ohgomers [155] was prepared by GeUman from trans-4-hydroxy-L-prohne according to a known procedure [157]. 

One of the most important characteristics of IL is its wide temperature range for the liquid phase with no vapor pressure, so next we tested the lipase-catalyzed reaction under reduced pressure. It is known that usual methyl esters are not suitable for lipase-catalyzed transesterification as acyl donors because reverse reaction with produced methanol takes place. However, we can avoid such difficulty when the reaction is carried out under reduced pressure even if methyl esters are used as the acyl donor, because the produced methanol is removed immediately from the reaction mixture and thus the reaction equilibrium goes through to produce the desired product. To realize this idea, proper choice of the acyl donor ester was very important. The desired reaction was accomplished using methyl phenylth-ioacetate as acyl donor. Various methyl esters can also be used as acyl donor for these reactions methyl nonanoate was also recommended and efficient optical resolution was accomplished. Using our system, we demonstrated the completely recyclable use of lipase. The transesterification took place smoothly under reduced pressure at 10 Torr at 40°C when 0.5 equivalent of methyl phenylthioacetate was used as acyl donor, and we were able to obtain this compound in optically pure form. Five repetitions of this process showed no drop in the reaction rate (Fig. 4). Recently Kato reported nice additional examples of lipase-catalyzed reaction based on the same idea that CAL-B-catalyzed esterification or amidation of carboxylic acid was accomplished under reduced pressure conditions. ... 

If, according to a modified Horeau method (partial kinetic resolution of a racemate), an optically active carboxylic acid is treated with an excess of racemic amine or alcohol, the configuration of the carboxylic acid can be inferred from the optical rotation of the residual amine or alcohol [48]... 

Use of the relatively small cyclopropane ring drastically reduces the potential for deleterious steric bulk effects and adds only a relatively small lipophilic increment to the partition coefficient of the drug. One of the clever elements of the rolicyprine synthesis itself is the reaction of d,l tranylcypromine (67) with L-5-pyrrolidone-2-carboxylic acid (derived from glutamic acid) to form a highly crystalline diastereomeric salt, thereby effecting resolution. Addition of dicyclohexylcarbodiimide activates the carboxyl group to nucleophilic attack by the primary amine thus forming the amide rolicyprine (68). 

Adam, W., Lazarus, M., Boss, B. et al. (1997) Enzymic resolution of chiral 2-hydroxy carboxylic acids by enantioselective oxidation with molecular oxygen catalyzed by the glycolate oxidase from spinach (Spinacia oleracea). The Journal of Organic Chemistry, 62 (22), 7841-7843. 

Optical resolution methods with carane-3,4-diol are noteworthy for wide generality. Esters of various cyclopropane carboxylic acids with (1,S, 3A>,4A>,6A>)-carane-3,4-diol were prepared and all (lR)-isomers could easily be obtained by a simple silica gel column chromatography. 

Carboxylic acids, being weaker acids, react with la-a with inversion of configuration at the anomeric center to yield /2-0-acyl compounds (1,53). This mild and convenient method for 1 -0-acylation of carbohydrates is also useful for pharmacological drug modification (54) or for the resolution of carboxylic acids (53). 

Disubstituted (cyclobutadiene)Fe(CO)3 complexes in which the two substituents are different may exist as enantiomers. Racemic cyclobutadiene carboxylic acids or cyclobutadiene amine complexes of this type have been separated by classical resolution methodology234. These optically active (cyclobutadiene)Fe(CO)3 complexes are stable with respect to racemization at 120°C for 24 h. This stability contrasts with acyclic... 

Falk and Schlogl 42> as late as 1968 established the absolute configuration of compound 13a as (+) —(S)-4-carboxy[2.2]paracyclophane. They did this by kinetic resolution of the racemic carboxylic anhydride with ( —)-a-phenylethylamine this kinetically controlled amidation afforded the dextrorotatory compound (13) in 3.8% optical yield 42C The similar topology of the carboxyl-group environment in 13 and in a-substituted metallocene carboxylic acids (14), configurations con-... 

Applications. In the last decade a lot of research has been devoted to the development of catalytic routes to a series of asymmetric carboxylic acids that lack the acetamido ligand as additional functionality. In Figure 4.17 four are listed, which are important as anaesthetics for rheumatic diseases. Their sales in beat many bulk chemicals the turnover of Naproxen (retail) in 1990 was 700 million for 1000 tons. S-Naproxen is now being produced by Syntcx via resolution with a chiral auxiliary. The main patents from Syntex expired in the U.S. in 1993, the reason for a lot of activity to study alternative synthetic routes. Routes leading to an asymmetric centre are o asymmetric hydrogenation of an unsaturated acid, o asymmetric carbohydroxylation of a styrene precursor, o asymmetric hydroformylation of a styrene precursor and oxidation. 

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