Ketone prochiral

Chiral aluminium hydride for the asymmetric reduction of prochiral ketones... 

Efficient enantioselective asymmetric hydrogenation of prochiral ketones and olefins has been accompHshed under mild reaction conditions at low (0.01— 0.001 mol %) catalyst concentrations using rhodium catalysts containing chiral ligands (140,141). Practical synthesis of several optically active natural... 

The hydride-donor class of reductants has not yet been successfully paired with enantioselective catalysts. However, a number of chiral reagents that are used in stoichiometric quantity can effect enantioselective reduction of acetophenone and other prochiral ketones. One class of reagents consists of derivatives of LiAlH4 in which some of die hydrides have been replaced by chiral ligands. Section C of Scheme 2.13 shows some examples where chiral diols or amino alcohols have been introduced. Another type of reagent represented in Scheme 2.13 is chiral trialkylborohydrides. Chiral boranes are quite readily available (see Section 4.9 in Part B) and easily converted to borohydrides. 

Enantioselective reductions of prochiral ketones by means of oxazaborolidines 97CLY9. 

In order to broaden the field of biocatalysis in ionic liquids, other enzyme classes have also been screened. Of special interest are oxidoreductases for the enan-tioselective reduction of prochiral ketones [40]. Formate dehydrogenase from Candida boidinii was found to be stable and active in mixtures of [MMIM][MeS04] with buffer (Entry 12) [41]. So far, however, we have not been able to find an alcohol dehydrogenase that is active in the presence of ionic liquids in order to make use of another advantage of ionic liquids that they increase the solubility of hydrophobic compounds in aqueous systems. On addition of 40 % v/v of [MMIM][MeS04] to water, for example, the solubility of acetophenone is increased from 20 mmol to 200 mmol L ... 

Table 2.1 Desymmetrization of prochiral ketones by the BV reaction using O2 as the oxidant and the CHMO mutant 1-K2-F5 as the catalyst [90].

Probably the first non-covalent immobilization of a chiral complex with diazaligands was the adsorption of a rhodium-diphenylethylenediamine complex on different supports [71]. These solids were used for the hydride-transfer reduction of prochiral ketones (Scheme 2) in a continuous flow reactor. The inorganic support plays a crucial role. The chiral complex was easily... 

Chiral diamino carbene complexes of rhodium have been merely used in asymmetric hydrosilylations of prochiral ketones but also in asymmetric addition of aryl boron reagents to enones. 

Stereochemical Studies of the Enantio-differentiating Hydrogenation of Various Prochiral Ketones over Tartaric Acid-Modified Nickel Catalyst... 

The improvements in MNi so far achieved were mostly due to our efforts to eliminate the N site from MNi by changing preparation variables of the catalyst, while the other important factor i has not been satisfactorily considered. In the present study, hydrogenation of various prochiral ketones with TA-MNi almost freed from the N site were carried out in order to gain insight into the mode of stereo control on MNi, which was expected to determine the stereochemistry of the reaction and to take part in the origin of the factor i. 

Taking the above mentioned characteristics of the two modes into consideration, we introduced the concept of stereo-control in the enantio-differentiating hydrogenation of various functionalized prochiral ketones on TA-MNi based on the coexistence of 2P and IP on the site of the catalyst. That is the IP function coimteracts the 2P function when IP and 2P coexist, and the relative contribution of the two modes determine the stereochemistry of the product produced in excess and also relates qualitatively to the i factor. 

The Rh-catalysed asymmetric hydrosilylation of prochiral ketones has been studied with complexes bearing monodentate or heteroatom functionalised NHC ligands. For example, complexes of the type [RhCl(l,5-cod)(NHC)] and [RhL(l,5-cod)(NHC)][SbFg ], 70, where L = isoquinoline, 3,5-lutidine and NHC are the chiral monodentate ligands 71 (Fig. 2.11). 

In 2000, Woodward et al. reported that LiGaH4, in combination with the S/ 0-chelate, 2-hydroxy-2 -mercapto-1,1 -binaphthyl (MTBH2), formed an active catalyst for the asymmetric reduction of prochiral ketones with catecholborane as the hydride source (Scheme 10.65). The enantioface differentiation was on the basis of the steric requirements of the ketone substituents. Aryl w-alkyl ketones were reduced in enantioselectivities of 90-93% ee, whereas alkyl methyl ketones e.g. i-Pr, Cy, t-Bu) gave lower enantioselectivities of 60-72% ee. 

On the other hand a direct hydrogen transfer through a Meerwein-Ponndorf mechanism, involving coordination of both the donor alcohol and the ketone to the copper site may also be considered. In this case, by using alcohols other than 2-propanol, we could expect some difference in stereochemistry. This would also imply the possibility of carrying out the enantioselective reduction of a prochiral ketone with a chiral alcohol as donor. 

Whereas general activities and selectivities for hydrogenations of ketones are similar to those of aldehydes, one big difference exists between the two. The hydrogenation of prochiral ketone carbonyls produces chiral carbons. Over symmetrical catalysts, racemic alcohols are formed however, over unsymmet-rical surfaces, enantioselectivity may occur. Enantioselective hydrogenations of ketones is an increasingly active research held and is covered in Chapter 3. Here we discuss that aspect of stereoselectivity associated with ring systems. 

Enantiometrically pure alcohols are important and valuable intermediates in the synthesis of pharmaceuticals and other fine chemicals. A variety of synthetic methods have been developed to obtain optically pure alcohols. Among these methods, a straightforward approach is the reduction of prochiral ketones to chiral alcohols. In this context, varieties of chiral metal complexes have been developed as catalysts in asymmetric ketone reductions [ 1-3]. However, in many cases, difficulties remain in the process operation, and in obtaining sufficient enantiomeric purity and productivity [2,3]. In addition, residual metal in the products originating from the metal catalyst presents another challenge because of the ever more stringent regulatory restrictions on the level of metals allowed in pharmaceutical products [4]. An alternative to the chemical asymmetric reduction processes is biocatalytic transformation, which offers... 

Among the most active catalysts for the asymmetric transfer hydrogenation of prochiral ketones and imines to chiral alcohols and amines are arene-ruthenium(II) amino-alcohol (or primary/ secondary 1,2-diamine)-based systems, with an inorganic base as co-catalyst, developed by Noyori139-141 and further explored by others (Scheme 27).142-145... 

Complexation of (124) and (125) with [ Rh(COD)Cl 2] in the presence of Si(OEt)4, followed by sol-gel hydrolysis condensation, afforded new catalytic chiral hybrid material. The catalytic activities and selectivities of these solid materials have been studied in the asymmetric hydro-gen-transfer reduction of prochiral ketones and compared to that of the homogeneous rhodium complexes containing the same ligands (124) and (125) 307... 

The asymmetric organosilane reduction of prochiral ketones has been studied as an alternative to the asymmetric hydrogenation approach. A wide variety of chiral ligand systems in combination with transition metals can be employed for this purpose. The majority of these result in good to excellent chemical yields of the corresponding alcohols along with a trend for better ee results with aryl alkyl ketones than with prochiral dialkyl ketones. 

A number of asymmetric hydrogenations of prochiral ketones to highly enan-tiomerically enriched alcohols are available. A select few are highlighted here. 

Asymmetric transfer hydrogenation can be employed in the asymmetric hydrogenation of prochiral ketones with a ruthenium complex of bis(oxazolinylmethyl) amine ligand 110. Enantioselectivities are greater than 95%.643... 

As an extension of the asymmetric hydrogenation of prochiral ketones to enantiomerically enriched alcohols, the reduction of imines has been a topic of interest in obtaining chiral amines of high enantiomeric purity. Several entries to enantiomerically enriched amines based on the approaches outlined above are available. These asymmetric hydrogenations have proved to be more difficult than those for prochiral ketones, but nevertheless show good promise. 

Kumada (44) showed that chiral ferrocenyl phosphine ligands on rhodium gave good optical yields of carbinols from prochiral ketones. 

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