Chiral auxiliaries catalysis

Clearly, there is a need for techniques which provide access to enantiomerically pure compounds. There are a number of methods by which this goal can be achieved . One can start from naturally occurring enantiomerically pure compounds (the chiral pool). Alternatively, racemic mixtures can be separated via kinetic resolutions or via conversion into diastereomers which can be separated by crystallisation. Finally, enantiomerically pure compounds can be obtained through asymmetric synthesis. One possibility is the use of chiral auxiliaries derived from the chiral pool. The most elegant metliod, however, is enantioselective catalysis. In this method only a catalytic quantity of enantiomerically pure material suffices to convert achiral starting materials into, ideally, enantiomerically pure products. This approach has found application in a large number of organic... 

Chiral oxazolines developed by Albert I. Meyers and coworkers have been employed as activating groups and/or chiral auxiliaries in nucleophilic addition and substitution reactions that lead to the asymmetric construction of carbon-carbon bonds. For example, metalation of chiral oxazoline 1 followed by alkylation and hydrolysis affords enantioenriched carboxylic acid 2. Enantioenriched dihydronaphthalenes are produced via addition of alkyllithium reagents to 1-naphthyloxazoline 3 followed by alkylation of the resulting anion with an alkyl halide to give 4, which is subjected to reductive cleavage of the oxazoline moiety to yield aldehyde 5. Chiral oxazolines have also found numerous applications as ligands in asymmetric catalysis these applications have been recently reviewed, and are not discussed in this chapter. ... 

Abstract While the use of stoichiometric amounts of sparteine and related ligands in various asymmetric reactions often lead to highly enantioselective transformations, there have been far fewer applications of sparteine to asymmetric catalysis. The aim of this review is to highlight recent advances in the field of asymmetric transformations that use sparteine as chiral auxiliary, emphasizing the use of substoichiometric or catalytic amounts of this ligand. 

The chiral auxiliaries anchored to the substrate, which is subjected to diastereoselective catalysis, is another factor that can control these reactions. These chiral auxiliaries should be easily removed after reduction without damaging the hydrogenated substrate. A representative example in this sense is given by Gallezot and coworkers [268], They used (-)mentoxyacetic acid and various (S)-proline derivates as chiral auxiliaries for the reduction of o-cresol and o-toluic acid on Rh/C. A successful use of proline derivates in asymmetric catalysis has also been reported by Harada and coworkers [269,270], The nature of the solvent only has a slight influence on the d.e. [271],... 

A number of groups have reported the preparation and in situ application of several types of dendrimers with chiral auxiliaries at their periphery in asymmetric catalysis. These chiral dendrimer ligands can be subdivided into three different classes based on the specific position of the chiral auxiliary in the dendrimer structure. The chiral positions may be located at, (1) the periphery, (2) the dendritic core (in the case of a dendron), or (3) throughout the structure. An example of the first class was reported by Meijer et al. [22] who prepared different generations of polypropylene imine) dendrimers which were substituted at the periphery of the dendrimer with chiral aminoalcohols. These surface functionalities act as chiral ligand sites from which chiral alkylzinc aminoalcoholate catalysts can be generated in situ at the dendrimer periphery. These dendrimer systems were tested as catalyst precursors in the catalytic 1,2-addition of diethylzinc to benzaldehyde (see e.g. 13, Scheme 14). 

The plot eepjod = f(eeaux) in an enantioselective reaction is a simple operation that can sometimes be very informative from both synthetic and mechanistic perspectives. This plot is now widely used in mechanistic discussions concerning enantioselective catalysis. However, some cautions are needed, since this approach has to be combined with additional studies in order to get firm conclusions. If linearity is observed, one cannot reach conclusions on the mechanism, since even with species involving several chiral auxiliaries one may remain linear, as in the ML2 model with g = 1 in Eq. (7.3). If there are deviations from linearity, this could be a piece of information on the mechanism, for example, aggregations at some level of the chemical system, or some competitive mechanisms. References 27, 44, and 68 are only three among many published examples. 

The stereochemistry of the addition can be controlled through the attachment of a chiral auxiliary or using asymmetric catalysis. Addition of 0-benzylhydroxylamine to unsaturated imide 51 (equation 33) bearing a chiral auxiliary was found to proceed with high diastereoselectivity at the a-position". ... 

Organometallic compounds asymmetric catalysis, 11, 255 chiral auxiliaries, 266 enantioselectivity, 255 see also specific compounds Organozinc chemistry, 260 amino alcohols, 261, 355 chirality amplification, 273 efficiency origins, 273 ligand acceleration, 260 molecular structures, 276 reaction mechanism, 269 transition state models, 264 turnover-limiting step, 271 Orthohydroxylation, naphthol, 230 Osmium, olefin dihydroxylation, 150 Oxametallacycle intermediates, 150, 152 Oxazaborolidines, 134 Oxazoline, 356 Oxidation amines, 155 olefins, 137, 150 reduction, 5 sulfides, 155 Oxidative addition, 5 amine isomerization, 111 hydrogen molecule, 16 Oxidative dimerization, chiral phenols, 287 Oximes, borane reduction, 135 Oxindole alkylation, 338 Oxiranes, enantioselective synthesis, 137, 289, 326, 333, 349, 361 Oxonium polymerization, 332 Oxo process, 162 Oxovanadium complexes, 220 Oxygenation, C—H bonds, 149... 

There are several possibilities for asymmetric synthesis in catalysed cyclopropanation and very substantial progress has already been made especially with catalyst development. The option of covalently attaching chiral auxiliaries to diazo compounds or to substrates, e.g. alkenes for cyclopropanation, has been discussed above in the subsection on diastere-oselectivity. The fact that many of the processes require metal catalysis makes the alternative option of using chiral catalysts particularly attractive and potentially more rewarding for commercial exploitation. The double option of combining the use of a chiral catalyst with a diazo compound carrying a chiral auxiliary is also available. For convenience, the double option is also included in this subsection. 

Some of the most impressive advances in the area of catalytic, enantioselective aldol addition reactions have taken place in the development of catalytic methods for enantioselective acetate aldol additions, a reaction type that has long been recalcitrant. Thus, although prior to 1992 a number of chiral-auxiliary based and catalytic methods were available for diastereo- and enantiocontrol in propionate aldol addition reactions, there was a paucity of analogous methods for effective stereocontrol in the addition of the simpler acetate-derived enol silanes. However, recent developments in this area have led to the availability of several useful catalytic processes. Thus, in contrast to the state of the art in 1992, it is possible to prepare acetate-derived aldol fragments utilizing asymmetric catalysis with a variety of transition-metal based complexes of Ti(IV), Cu(II), Sn(II), and Ag(I). 

The oxidative imination of sulfides and sulfoxides via nitrene transfer processes leads to N-substituted sulfilimines and sulfoximines. This reaction is interesting as chiral sulfoximines are efficient chiral auxiliaries in asymmetric synthesis, a promising class of chiral ligands for asymmetric catalysis and key intermediates in the synthesis of pseudopeptides [169]. However, very few examples of such iron-catalyzed transformations have been described. 

Asymmetric catalysis with chiral ligands [82] is commonly considered to be advantageous instead of using chiral auxiliaries. Catalytic asymmetric Michael reactions are known [83], but not with iron as the catalytically active metal. Only two reports on iron catalyzed catalytic asymmetric Michael reaction with dipeptides [84] or diamino thioethers [85] exist, but the enantioselectivities were disappointing (18% ee and 10% ee, respectively). 

Taddol has been widely used as a chiral auxiliary or chiral ligand in asymmetric catalysis [17], and in 1997 Belokon first showed that it could also function as an effective solid-liquid phase-transfer catalyst [18]. The initial reaction studied by Belokon was the asymmetric Michael addition of nickel complex 11a to methyl methacrylate to give y-methyl glutamate precursors 12 and 13 (Scheme 8.7). It was found that only the disodium salt of Taddol 14 acted as a catalyst, and both the enantio- and diastereos-electivity were modest [20% ee and 65% diastereomeric excess (de) in favor of 12 when 10 mol % of Taddol was used]. The enantioselectivity could be increased (to 28%) by using a stoichiometric amount of Taddol, but the diastereoselectivity decreased (to 40%) under these conditions due to deprotonation of the remaining acidic proton in products 12 and 13. Nevertheless, diastereomers 12 and 13 could be separated and the ee-value of complex 12 increased to >85% by recrystallization, thus providing enantiomerically enriched (2S, 4i )-y-methyl glutamic add 15. 

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