Cyclohexanones stereoselective reactions

The stereoselective reactions in Scheme 2.10 include one example that is completely stereoselective (entry 3), one that is highly stereoselective (entry 6), and others in which the stereoselectivity is modest to low (entries 1,2,4, 5, and 7). The addition of formic acid to norbomene (entry 3) produces only the exo ester. Reduction of 4-r-butylcyclohexanone (entry 6) is typical of the reduction of unhindered cyclohexanones in that the major diastereomer produced has an equatorial hydroxyl group. Certain other reducing agents, particularly sterically bulky ones, exhibit the opposite stereoselectivity and favor the formation of the diastereomer having an axial hydroxyl groi. The alkylation of 4-t-butylpiperidine with benzyl chloride (entry 7) provides only a slight excess of one diastereomer over the other. 

Addition of ynamines to electron-deficient olefins has been used to prepare cyclobutenes. Ficini, Eman, and Touzin have investigated the [2+2] cycloaddition to AW-diethylaminopropyne to 4-methylcyclohexenone. The reaction was stereoselective, and gave the isomeric adducts (93) and (94) in a 9 1 ratio. Acid hydrolysis of the adducts gave the substituted cyclohexanone (95). Reaction of the ynamine with 1-cyanocyclopentene, catalysed by magnesium bromide, gave the cyclobutene (96). Hydrolysis of (96) with acetic acid gave almost exclusively the cyclobutanone (97). Hydrolysis with hydrochloric acid gave a 20 80 mixture of (97) and its epimer (98). 

Allylmagnesium, allylindium, and allylbismuth generally showed a preference for axial addition to cyclohexanones. Allylmagnesium was the most stereoselective. Reactions with an a-methylated enone (carvone) were the most selective, except that allylbismuth was unreactive with this substrate [25c]. 

Cyanoallene, when treated with the morpholine enamine of cyclohexanone, undergoes a 1,3-cycloaddition reaction to form 72 (89). The reaction between cyanoallene and diendiamine 73a produces di-1,2-cycloaddition adduct 73 (i 9). The 4a-azonioanthracene ion (73b) readily undergoes a 1,4-cycloaddition reaction with nucleophilic dienophiles such as enamines (89a). The cycloaddition is stereoselective so that the a- and... 

When an enolate is forced to take the E configuration, e.g, the enolate derived from cyclohexanone, predominant formation of the anti-aldol might be expected. Surprisingly, early experiments gave more or less stereorandom results in that the reaction with benzaldehyde gave a ratio of. vvtt/ant/ -aldols of 48 521B 23, Contrarily, recent investigations24 reveal a substantial anti selectivity (16 84), which is lowered in a dramatic manner (50 50) by the presence of lithium salts. Thus, the low stereoselectivity in the early experiments may be attributed to impurities of lithium salts or lithium hydroxide. 

A DFT study found a corresponding TS to be the lowest energy.167 This study also points to the importance of the solvent, DMSO, in stabilizing the charge buildup that occurs. A further computational study analyzed the stereoselectivity of the proline-catalyzed aldol addition reactions of cyclohexanone with acetaldehyde, isobu-tyraldehyde, and benzaldehyde on the basis of a similar TS.168 Another study, which explored the role of proline in intramolecular aldol reactions, is discussed in the next section.169... 

With less hindered hydride donors, particularly NaBH4 and LiAlH4, confor-mationally biased cyclohexanones give predominantly the equatorial alcohol, which is normally the more stable of the two isomers. However, hydride reductions are exothermic reactions with low activation energies. The TS should resemble starting ketone, so product stability should not control the stereoselectivity. A major factor in the preference for the equatorial isomer is the torsional strain that develops in the formation of the axial alcohol.117... 

Wittig-type olefination has been reported. The reaction is thought to involve the salt (47) and shows little stereoselectivity. 2.2.2 Ketones.- The stereochemistry of olefination of 2,3-epoxy- and protected 2-hydroxy cyclohexanones with ethylidenetriphenyl-... 

The stereoselective intramolecular Henry reactions have been reported by Seebach. The Michael addition of doubly deprotonated acetyl acetaldehyde to l-methylenedioxyphenyl-2-nitroethene followed by subsequent intramolecular nitro-aldol cyclization leads to the diastereomerically pure cyclohexanone derivative, where the nitro and OH groups are cis as shown in Eq. 3.73.114 This reaction is applied to the synthesis of l-desoxy-2-lycorinone as shown in Eq. 3.74.115... 

The development of conditions for stoichiometric formation of both kinetically and thermodynamically controlled enolates has permitted the extensive use of enolate alkylation reactions in multistep synthesis of complex molecules. One aspect of the reaction which is crucial in many cases is the stereoselectivity. The alkylation step has a stereoelectronic preference for approach of the electrophile perpendicular to the plane of the enolate, since the electrons which are involved in bond formation are the n electrons. A major factor in determining the stereoselectivity of ketone enolate alkylations is the difference in steric hindrance on the two faces of the enolate. The electrophile will approach from the less hindered of the two faces, and the degree of stereoselectivity depends upon the steric differentiation. For simple, conformationally based cyclohexanone enolates such as that from 4 - /- b u ty I eye I o h cx an o ne, there is little steric differentiation. The alkylation product is a nearly 1 1 mixture of the cis and trans isomers. 

The role of the metal catalyst in the hydrogenation reaction and its stereoselectivity has been widely studied (9). Group Vtll metals are generally used, but different behaviours are observed. In the hydrogenation of disubstituted phenols palladium mainly gives cyclohexanone derivatives, rhodium and platinum are very selective for the c/5 isomer, whereas nickel is more selecive for the tra/ 5 isomer (9). 

In analogy to 23, the chiralities of [2.2]meta- and [10]paracyclophanecarboxylic acids were also deduced from the results of kinetic resolutions 40-77>. For the application of Horeau s method, (—)-[10]paracyclophanecarboxylic acid (14) was transformed by stereoselective hydrogenation and subsequent sodium borohydride reduction of an intermediate cyclohexanone into the (—)-cis-cyclohexanol 94 which on reaction with racemic 2-phenylbutanoic anhydride afforded a 15% excess of the Ievorotatory acid thereby proving (in agreement with the kinetic resolution of the anhydride of 14, vide supra) the chirality (5) for (—)-14 and all its derivatives 40). Optical comparison with dioxa[10]paracyclophanecarboxylic acid (16) confirmed this result63,108). 

Highly stereoselective aldol reactions of lithium ester enolates (LiCR1 R2CC>2R3) with (/0-2-(/ -tolylsulfiny I (cyclohexanone have been attributed to intermediacy of tricoordinate lithium species which involve the enolate and the sulfinyl and carbonyl oxygens of the substrates.43 The O-metallated /<-hydroxyalkanoatcs formed by aldol-type reaction of carbonyl compounds with enolates derived from esters of alkanoic acids undergo spontaneous intramolecular cyclization to /1-lactones if phenyl rather than alkyl esters are used the reaction has also been found to occur with other activated derivatives of carboxylic acids.44... 

Dimethyldioxirane has also been used as the epoxidizing agent in a key step in the synthesis of A-norsteroids69,70. The reaction occurs in dichloromethane-acetone and is highly regio- and stereoselective as shown in equation 9. Dioxiranes may also be generated in situ, by reaction of potassium monoperoxysulfate (sold commercially as OXONE) and cyclohexanones. In this case, cyclohexene derivatives may be smoothly epoxidized in 40-100% yields (equation 10)71. 

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