Oxidation stereoselectivity

Stereoselective functionalization of enolates derived from 2-acyl-2-alkyl-1,3-dithiane 1-oxides Stereoselective enolate alkylation. There has been much interest over recent years in the enantio- and diastereocontrol of enolate alkylation.19 Most methods which do not rely on asymmetric alkylating agents hinge on a derivatization of the ketonic substrate with an enantiomerically pure auxiliary. Examples of such chiral auxiliaries include oxazolines20 and oxazolidi-nones.21 We reasoned that the sulfoxide unit present in our 2-acyl-2-alkyl-1,3-dithiane 1-oxide substrates might be expected to influence the transition-state geometry of a ketone enolate, perhaps by chelation to a metal counterion, and hence control the stereochemistry of alkylation. 

Reduction of ot-keto epoxides. Epoxidation of cyclic allylic alcohols results mainly in the epoxide syn to the hydroxyl group (4, 76). Schlessinger et al. have reported a method for isomerization of the alcohol group by oxidation to the ketone and reduction to the anh-alcohol. In a model case, 2->4, pyridinium chloro-chromate buffered with sodium acetate was found to be the most satisfactory oxidant. Stereoselective reduction to 4 was found to be a more difficult problem, but eventually triisobutylaluminum was found to effect this reduction in high yield. 

Banerjee, A. Stereoseiective microbiai Baeyer-Viiiiger oxidations. Stereoselective Biocatalysis). 2000, 867-876... 

Oxidative decomposition of cyclopropyl-substituted Fischer-carbene complexes with pyridin-ium iV-oxide stereoselectively leads to cyclopropylcarboxylates. ... 

Lactam antibiotics (penicillins and cephalosporins) microbial oxidation (microbes ) n-Butyric acid is oxidized stereoselectively to (R)-(5-hydroxybutyric acid [82]... 

Unsaturated chiral a-hydroxy esters are of interest due to possible reactions with the carbon double bond. They can easily be obtained from optically active cyanohydrins according to the Pinner method [35a]. Epoxidation of the chiral alcohols 9 with achiral oxidants, e.g., m-chloroperoxybenzoic acid (m-CPBA), yields a mixture of both possible epoxides 10a and 10b. With chiral (Sharpless titanium tartrate system) oxidants stereoselective epoxidation results. Using (+) dimethyl tartrate [(+) DMT] only the erythro isomer 10a is obtained (Scheme 6) [35b]. 

Open-chain 1,5-polyenes (e.g. squalene) and some oxygenated derivatives are the biochemical precursors of cyclic terpenoids (e.g. steroids, carotenoids). The enzymic cyclization of squalene 2,3-oxide, which has one chiral carbon atom, to produce lanosterol introduces seven chiral centres in one totally stereoselective reaction. As a result, organic chemists have tried to ascertain, whether squalene or related olefinic systems could be induced to undergo similar stereoselective cyclizations in the absence of enzymes (W.S. Johnson, 1968, 1976). 

Oxidation of olefins and dienes provides the classic means for syntheses of 1,2- and 1,4-difunctional carbon compounds. The related cleavage of cyclohexene rings to produce 1,6-dioxo compounds has already been discussed in section 1.14. Many regio- and stereoselective oxidations have been developed within the enormously productive field of steroid syntheses. Our examples for regio- and stereoselective C C double bond oxidations as well as the examples for C C double bond cleavages (see p. 87f.) are largely selected from this area. 

Recent syntheses of steroids apply efficient strategies in which open-chain or monocyclic educts with appropiate side-chains are stereoselectively cyclized in one step to a tri- or tetracyclic steroid precursor. These procedures mimic the biochemical synthesis scheme where acyclic, achiral squalene is first oxidized to a 2,3-epoxide containing one chiral carbon atom and then enzymatically cyclized to lanostetol with no less than seven asymmetric centres (W.S. Johnson, 1%8, 1976 E.E. van Tamden, 1968). 

In order to make these oxidative reactions of 1,3-dienes catalytic, several reoxidants are used. In general, a stoichiometric amount of benzoquinone is used. Furthermore, Fe-phthalocyanine complex or Co-salen complex is used to reoxidize hydroquinone to benzoquinone. Also, it was found that the reaction is faster and stereoselectivity is higher when (phenylsulflnyl)benzoquinone (383) is used owing to coordination of the sulfinyl group to Pd, Thus the reaction can be carried out using catalytic amounts of PdfOAcji and (arylsulfinyl)benzoquinone in the presence of the Fe or Co complex under an oxygen atmosphere[320]. Oxidative dicyanation of butadiene takes place to give l,4-dicyano-2-butene(384) (40%) and l,2-dicyano-3-butene (385)[32l]. 

Convincing evidence for oxidative addition by inversion has been presented by the reaction of chiral (5)-( )-3-acetoxy-l-phenyl-1-butene (4) with Pd(0)(dppe), followed by the treatment with NaBF4 to give optically active the TT-allylpalladium complex (l/ ,25,35) 5 with 81% stereoselectivity[19]. 

Hydroboration-oxidation of a pinene (page 235) like catalytic IS stereoselective Addition takes place at the less hindered face and a single alcohol is produced in high yield (89%) Sug... 

Aldehydes react with alkenylborates to give 1,3-diols upon oxidation of the intermediate (300). Alkynylborates ate transformed by epoxides into homoallyhc alcohols and alkenylborates into 1,4-diols (300,301). Carbon dioxide reacts with alkenylborates to yield catboxyhc acids (302). The scope of these transformations is further extended by the use of functionalized electrophiles and borates, often reacting with high stereoselectivity. For example, in the... 

This chemical bond between the metal and the hydroxyl group of ahyl alcohol has an important effect on stereoselectivity. Asymmetric epoxidation is weU-known. The most stereoselective catalyst is Ti(OR) which is one of the early transition metal compounds and has no 0x0 group (28). Epoxidation of isopropylvinylcarbinol [4798-45-2] (1-isopropylaHyl alcohol) using a combined chiral catalyst of Ti(OR)4 and L-(+)-diethyl tartrate and (CH2)3COOH as the oxidant, stops at 50% conversion, and the erythro threo ratio of the product is 97 3. The reason for the reaction stopping at 50% conversion is that only one enantiomer can react and the unreacted enantiomer is recovered in optically pure form (28). 

An asymmetric synthesis of estrone begins with an asymmetric Michael addition of lithium enolate (178) to the scalemic sulfoxide (179). Direct treatment of the cmde Michael adduct with y /i7-chloroperbenzoic acid to oxidize the sulfoxide to a sulfone, followed by reductive removal of the bromine affords (180, X = a and PH R = H) in over 90% yield. Similarly to the conversion of (175) to (176), base-catalyzed epimerization of (180) produces an 85% isolated yield of (181, X = /5H R = H). C8 and C14 of (181) have the same relative and absolute stereochemistry as that of the naturally occurring steroids. Methylation of (181) provides (182). A (CH2)2CuLi-induced reductive cleavage of sulfone (182) followed by stereoselective alkylation of the resultant enolate with an allyl bromide yields (183). Ozonolysis of (183) produces (184) (wherein the aldehydric oxygen is by isopropyUdene) in 68% yield. Compound (184) is the optically active form of Ziegler s intermediate (176), and is converted to (+)-estrone in 6.3% overall yield and >95% enantiomeric excess (200). 

Chiral Alcohols and Lactones. HLAT) has been widely used for stereoselective oxidations of a variety of prochiral diols to lactones on a preparative scale. In most cases pro-(3) hydroxyl is oxidized irrespective of the substituents. The method is apphcable among others to tit-1,2-bis(hydroxymethyl) derivatives of cyclopropane, cyclobutane, cyclohexane, and cyclohexene. Resulting y-lactones are isolated in 68—90% yields and of 100% (164,165). 

Although details vary for particular cases, a common synthetic route to diol epoxides such as (30) frequently begins with the ketone (33) (78MI50700). The final epoxidation is often highly stereoselective. A general route to non-K-region arene oxides has been described (75JA3185). 

---