Asymmetric reactions synthesis

TiIV-based Lewis acids are effective in ring-forming reactions such as Diels-Alder reactions (Scheme 25).94 Besides the usual TiX4 compounds (X = halide or alkoxide), Cp2Ti(OTf)2 is also a reactive catalyst for the Diels-Alder reaction,95 and it has been reported that [( PrO)2Ti(bpy)(OTf) ( PrOLQXOTf) is even more effective than Cp2Ti(OTf)2.96 In asymmetric synthesis, reactions with chiral dienophiles have been widely investigated. 

This final chapter summarizes the enzyme-catalyzed asymmetric reactions and introduces some new developments in the area of asymmetric synthesis. Among the new developments, cooperative asymmetric catalysis is an important theme because it is commonly observed in enzymatic reactions. Understanding cooperative asymmetric catalysis not only makes it possible to design more enan-tioselective asymmetric synthesis reactions but also helps us to understand how mother nature contributes to the world. 

The enzymatic reduction of a thiocarbonyl compound has been investigated [159] for the first time, in order to provide a new route for enan-tiopure thiols, molecules which are currently needed for asymmetric synthesis. Reaction of easily available /1-thioxoesters with baker s yeast under classical conditions did furnish the expected thiols, but with lower enantiomeric purity and moderate conversion rate, due to the competitive hydrolysis of the thioxo group into a carbonyl leading to an alcohol. However, conditions (ethyl acrylate, dry yeast) were found to improve the production of (S)-ethyl 3-mercaptobutanoate. Cyclic thioxo esters led to high stereoselectivity of cis (1S,2S) products, but with moderate chemical yields. 

Most of the known asymmetric synthesis reactions equilibrating from pro-chiral racemic mixtures are photocyclizations where ring systems that include one or two asymmetric C atoms are created as a first or the final product. 

SINGLE ASYMMETRIC SYNTHESIS REACTIONS OF ACHIRAL ALDEHYDES AND CHIRAL ALLYL ORGANOMETALLICS... 

DOUBLE ASYMMETRIC SYNTHESIS REACTIONS OF CHIRAL C—X ELECTROPHILES AND 40... 

If the thermodynamics of the process favors the formation of products in asymmetric synthesis reaction, it is possible to convert prochiral ketone to corresponding chiral amine and obtain high overall yield on prochiral ketone. 

Simple esters cannot be allylated with allyl acetates, but the Schiff base 109 derived from o -amino acid esters such as glycine or alanine is allylated with allyl acetate. In this way. the o-allyl-a-amino acid 110 can be prepared after hydrolysis[34]. The Q-allyl-o-aminophosphonate 112 is prepared by allylation of the Schiff base 111 of diethyl aminomethylphosphonates. [35,36]. Asymmetric synthesis in this reaction using the (+ )-A, jV-dicyclohex-ylsulfamoylisobornyl alcohol ester of glycine and DIOP as a chiral ligand achieved 99% ec[72]. 

There have been several reviews of asymmetric synthesis via chiral organoboranes (6,8,378,382,467—472). Asymmetric induction in the hydroboration reaction may result from the chiraHty present in the olefin (asymmetric substrate), in the reagent (asymmetric hydroboration), or in the catalyst (catalytic asymmetric hydroboration). 

Asymmetric synthesis is a method for direct synthesis of optically active amino acids and finding efficient catalysts is a great target for researchers. Many exceUent reviews have been pubHshed (72). Asymmetric syntheses are classified as either enantioselective or diastereoselective reactions. Asymmetric hydrogenation has been appHed for practical manufacturing of l-DOPA and t-phenylalanine, but conventional methods have not been exceeded because of the short life of catalysts. An example of an enantio selective reaction, asymmetric hydrogenation of a-acetamidoacryHc acid derivatives, eg, Z-2-acetamidocinnamic acid [55065-02-6] (6), is shown below and in Table 4 (73). 

The most recent, and probably most elegant, process for the asymmetric synthesis of (+)-estrone appHes a tandem Claisen rearrangement and intramolecular ene-reaction (Eig. 23). StereochemicaHy pure (185) is synthesized from (2R)-l,2-0-isopropyhdene-3-butanone in an overall yield of 86% in four chemical steps. Heating a toluene solution of (185), enol ether (187), and 2,6-dimethylphenol to 180°C in a sealed tube for 60 h produces (190) in 76% yield after purification. Ozonolysis of (190) followed by base-catalyzed epimerization of the C8a-hydrogen to a C8P-hydrogen (again similar to conversion of (175) to (176)) produces (184) in 46% yield from (190). Aldehyde (184) was converted to 9,11-dehydroestrone methyl ether (177) as discussed above. The overall yield of 9,11-dehydroestrone methyl ether (177) was 17% in five steps from 6-methoxy-l-tetralone (186) and (185) (201). 

Enzyme-Catalyzed Asymmetric Synthesis. The extent of kinetic resolution of racemates is determined by differences in the reaction rates for the two enantiomers. At the end of the reaction the faster reacting enantiomer is transformed, leaving the slower reacting enantiomer unchanged. It is apparent that the maximum product yield of any kinetic resolution caimot exceed 50%. 

Kinetic Resolutions. From a practical standpoint the principal difference between formation of a chiral molecule by kinetic resolution of a racemate and formation by asymmetric synthesis is that in the former case the maximum theoretical yield of the chiral product is 50% based on a racemic starting material. In the latter case a maximum yield of 100% is possible. If the reactivity of two enantiomers is substantially different the reaction virtually stops at 50% conversion, and enantiomericaHy pure substrate and product may be obtained ia close to 50% yield. Convenientiy, the enantiomeric purity of the substrate and the product depends strongly on the degree of conversion so that even ia those instances where reactivity of enantiomers is not substantially different, a high purity material may be obtained by sacrificing the overall yield. 

In recent years there has been a proliferation of new reactions and reagents that have been so useful in organic synthesis that often people refer to them by name. Many of these are stereoselective or regioselecth/e methods. While the expert may know exactly what the Makosza vicarious nucleophilic substitution, or the Meyers asymmetric synthesis refers to, many students as well as researchers would appreciate guidance regarding such "Name Reactions". 

The Darzens condensation reaction has been used with a wide variety of enolate equivalents that have been covered elsewhere. A recent application of this important reaction was appljed toward the asymmetric synthesis of aziridine phosphonates by Davis and coworkers.In this application, a THF solution of sulfinimine 34 (0.37 mmol, >98% ee) and iodophosphonate 35 (0.74 mmol) was treated with LiHMDS (0.74 mmol) at -78 °C to give aziridine 36 in 75% yield. Treatment of 36 with MeMgBr removed the sulfinyl group to provide aziridine 37 in 72% yield. 

Darzens reaction can be used to efficiently complete the stereoselective synthesis of a"-substituted epoxy ketones. As an example, Enders and Hett reported a technique for the asymmetric synthesis of a"-silylated a,P-epoxy ketones. Thus, optically active a -silyl a-bromoketone 38 was treated with LDA followed by the addition of benzaldehyde to give a"-silyl epoxyketone 40 in 66% yield with good... 

Catalytic asymmetric synthesis with participation and formation of heterocycles (including asymmetric phase transfer reactions and asymmetric reactions with chiral Lewis catalysts) 93MI1. 

Asymmetric Heck reaction in synthesis of heterocycles 97T7371. 

Asymmetric synthesis of 3-amino (3-lactams via Staudinger ketene-imine cycloaddition reaction 98KGS1448. 

See e.g. (a) W. Cahhuthehs, Cycloaddition Reactions in Organic Synthesis, Tetrahedron Organic Chemistry Series Vol. 8 Pergamon Press Elmsford, NY 1990 (b) I. OjiMA, Catalytic Asymmetric Synthesis, VCH Publishers. Inc. New York. 1993 ... 

Asymmetric synthesis is a stimulating academic challenge, but since it has become clear that most chiral drugs can be administered safely only in the enantiomerically pure form, the industrial need for asymmetric methods has made research in asymmetric synthesis absolutely necessary [5]. This has driven a renaissance in the discipline of organic chemistry, because all of the old-established reactions need to be reinvestigated for their application in asymmetric synthesis [6]. This has also applied... 

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