Sulfoxides oxidation with

The widely used Moifatt-Pfltzner oxidation works with in situ formed adducts of dimethyl sulfoxide with dehydrating agents, e.g. DCC, AcjO, SO], P4O10, CCXTl] (K.E, Pfitzner, 1965 A.H. Fenselau, 1966 K.T. Joseph, 1967 J.G. Moffatt, 1971 D. Martin, 1971) or oxalyl dichloride (Swem oxidation M. Nakatsuka, 1990). A classical procedure is the Oppenauer oxidation with ketones and aluminum alkoxide catalysts (C. Djerassi, 1951 H. Lehmann, 1975). All of these reagents also oxidize secondary alcohols to ketones but do not attack C = C double bonds or activated C —H bonds. 

Trilialophenols can be converted to poly(dihaloph.enylene oxide)s by a reaction that resembles radical-initiated displacement polymerization. In one procedure, either a copper or silver complex of the phenol is heated to produce a branched product (50). In another procedure, a catalytic quantity of an oxidizing agent and the dry sodium salt in dimethyl sulfoxide produces linear poly(2,6-dichloro-l,4-polyphenylene oxide) (51). The polymer can also be prepared by direct oxidation with a copper—amine catalyst, although branching in the ortho positions is indicated by chlorine analyses (52). 

Esters derived from the primary alcohols are the most stable and those derived from the tertiary alcohols are the least stable. The decomposition temperature is lower in polar solvents, eg, dimethyl sulfoxide (DMSO), with decomposition occurring at 20°C for esters derived from the tertiary alcohols (38). Esters of benzyl xanthic acid yield stilbenes on heating, and those from neopentyl alcohols thermally rearrange to the corresponding dithiol esters (39,40). The dialkyl xanthate esters catalytically rearrange to the dithiol esters with conventional Lewis acids or trifluoroacetic acid (41,42). The esters are also catalytically rearranged to the dithiolesters by pyridine Ai-oxide catalysts (43) ... 

Cellulose dissolved in suitable solvents, however, can be acetylated in a totally homogeneous manner, and several such methods have been suggested. Treatment in dimethyl sulfoxide (DMSO) with paraformaldehyde gives a soluble methylol derivative that reacts with glacial acetic acid, acetic anhydride, or acetyl chloride to form the acetate (63). The maximum degree of substitution obtained by this method is 2.0 some oxidation also occurs. Similarly, cellulose can be acetylated in solution with dimethylacetamide—paraformaldehyde and dimethylformamide-paraformaldehyde with a potassium acetate catalyst (64) to provide an almost quantitative yield of hydroxymethylceUulose acetate. 

Isomerization of 3-cephems (27) to 2-cephems (28) takes place in the presence of organic bases (e.g. pyridine) and is most facile when the carboxyl is esterified. Normally an equilibrium mixture of 3 7 (3-cephem/2-cephem) is reached. Since the 2-cephem isomers are not active as antibacterial agents, the rearrangement proved to be an undesirable side reaction that complicated acylation of the C-7 amine under certain conditions. A method for converting such mixtures to the desired 3-cephem isomer involves oxidation with concomitant rearrangement to the 3-cephem sulfoxide followed by reduction. Additions... 

Dimethyl sulfoxide reacts with trifluoroacetic anhydride at low tempera ture to give a complex that is an efficient reagent for the oxidation of alcohols to carbonyl compounds [40 41] This reagent can be used to oxidize primary and secondary aliphatic alcohols, cycloalkyl alcohols, and allylic, homoallylic, ben-zylic, acetylenic, and steroidal alcohols (equation 19)... 

The preparation of isothiazolidin-3-one 5-oxide and 5,5-dioxide derivatives of azetidin-3-ones was described (99EUP100069), starting from penicillanic acid sulfoxide amides in the presence of halogenating agents in anhydrous inert solvents or even without them. Through rearrangement and oxidation with conventional methods, compounds 73 could be obtained. For some derivatives the usefulness, as intermediates for the preparation of novel p-lactam analogs or active substances in formulations for antimicrobial therapy, is claimed. 

Treatment of pyridyl carbinol 51 with thionyl chloride leads to the corresponding chloride (52), Treatment of that intermediate with 5-methoxy-2-mercaptobenzimidazole (53), obtained from reaction of 4-methoxy-q-phenylenediamine with potassium ethylxanthate leads to displacement of halogen and formation of the sulfide (54). Finally, oxidation with 3-chloroperbenzoic acid produces the sulfoxide omeprazole (55) fl7]. 

The facile and selective oxidation of both primary and secondary hydroxy groups with certain nucleotides led Pfitzner and Moffatt (48) to explore the scope of the carbodiimide-methyl sulfoxide reagent with steroid and alkaloid alcohols. Relatively minor differences were apparent in the rate of oxidation of epimeric pairs of 3- and 17- hydroxy steroids whereas the equatorial lLx-hydroxyl group in several steroids was readily oxidized under conditions where the axial epimer was unreactive [cf. chromic oxide oxidation (51)]. 

Cholane-24-ol, oxidation with dimethyl sulfoxide, dicyclohexylcarbo-di-imide, and pyridinium trifluoro-acetate, 47, 25... 

Treatment of ethyl 2,7-di-/ert-butylthiepin-4-carboxylate (24) with 3-chloroperoxybenzoic acid at — 78 °C results in the benzene derivative 25 only, and no sulfur-oxidized products 80 however, the stable 2,7-di-ter/-butylthiepin (26) can be oxidized with 0-benzyl 00-hydrogen monoper-oxycarbonate at — 78 °C to give the corresponding S-oxide 27, which was monitored by HNMR spectroscopy at — 40°C. At —15 C, sulfoxide 27 was converted, via extrusion of sulfur monoxide, with a half-life of 5.5 hours to the benzene derivative 28.87 The oxidation reaction of 26 with excess of the monoperoxycarbonate did not proceed to the S,S-dioxide, even though the parent thiepin 1,1-dioxide is known to be stable at room temperature.15... 

In a recently published paper6, on the investigation of AN copolymerization with the quartemary salt of l,2-dimethyl-5-vinylpyridinium sulfate (DMVPS) in dimethyl sulfoxide (DMSO) with 2,2 -azoisobutyronitrile as initiator, and in aqueous medium in the presence of the potassium persulfate/sodium metabisulfite oxidation-reduction system at 60 °C, the authors found the reactivity of the monomers, especially that of MVPS (methylvinylpyridin sulfate) to depend significantly on the polarity of the medium. 

Ueno and coworkers49 have developed a procedure for the synthesis of chiral sulfinic acids. Treatment of (R)-( + )-23 with disulfide 24 and tributylphosphine in THF gave (S)-( — )-25. Compound 25 was oxidized with potassium permanganate to the sulfone, which was then reduced to the sulfinic acid, (S)-( — )-26, by treatment with sodium borohydride. Conversion of 26 or an analog to an ester would lead to diastereomers. If these epimers could be separated, then they would offer a path to homochiral sulfoxides with stereogenic carbon and sulfur atoms. 

The preference for the axial position in unhindered thiane-1-oxides has been known for some time. The spectra of the cis and trans isomers of the 2-, 3- and 4-methyl thiane-1-oxides, 169-171, were also measured. It was concluded from the 13C chemical shifts that the methyl groups preferred the equatorial positions. A comparison of the 170 chemical shifts obtained for sulfoxides 169-174 with those obtained for the cis and tram sulfoxide isomers of trans- 1-thiadecalin, 175 and 176, was consistent with this proposal. Sulfoxide 175 with the S=0 axial gave a shift about 17 ppm upfield from that of its equatorial isomer 176. For sulfoxides 169-174, the conformers proposed to have the S=0 axial gave shifts that were upfield from those of the supposed equatorial conformers. For tram-3, (rans-5-dimethylthiane-1 -oxide (177) with the oxygen axial, the 170 signal was 21 ppm upfield from the signal observed for the equatorial oxygen in cis-3, cis-5-dimethylthiane-l-oxide (178). 

All attempts to prepare other [2 + 4] cycloadducts of sulfoxides 115 with dienophiles such as maleic anhydride, ethyl azodicarboxylate, etc., have failed60. A method for preparing ordinary alkyl-substituted thiirene oxides (e.g. 18 R1 = R2 = alkyl) is still lacking. 

Whereas acyclic sulfoxides form complexes with various metal salts, thiirane oxides react with copper(II) chloride or bromide163 in benzene at room temperature to give the thiolsulfonate 146a. In alcoholic solution below 0 °C the major products are sulfinates (149). Similar results are obtained in the reaction of thiirane oxides with ethanesulfinyl chloride163 as summarized in equation 60. 

The syntheses of perhalogenated dithiethanes and their oxidation products (214-219) have been recently reported247. The method is based on the photochemical dimerization of thiophosgen or its fluoro- and bromo-analogues followed by partial oxidation with trifluoroperacetic acid to the desired sulfoxides (or sulfones)248 as shown in equation 84. 

The Pummerer reaction346 of conformationally rigid 4-aryl-substituted thiane oxides with acetic anhydride was either stereoselective or stereospecific, and the rearrangement is mainly intermolecular, while the rate-determining step appears to be the E2 1,2-elimination of acetic acid from the acetoxysulfonium intermediates formed in the initial acetylation of the sulfoxide. The thermodynamically controlled product is the axial acetoxy isomer, while the kinetically controlled product is the equatorial isomer that is preferentially formed due to the facile access of the acetate to the equatorial position347. The overall mechanism is illustrated in equation 129. 

Bordwell and Boutan (BB)81 carried out extensive work on the methylsulfmyl group in 1957. It must be emphasized that they found that the preparation of pure arylmethyl sulfoxides from arylmethyl sulfides by oxidation was not a trivial matter. The frequently recommended reagent, hydrogen peroxide in acetic acid, tended to give sulfoxides contaminated with appreciable quantities of sulfones, which could not be removed by fractional crystallization. Oxidation by nitric acid was found to be more satisfactory. 

Optically pure (S)-benzyl methyl sulfoxide 139 can be converted to the corresponding a-lithio-derivative, which upon reaction with acetone gave a diastereomeric mixture (15 1) of the /S-hydroxysulfoxide 140. This addition reaction gave preferentially the product in which the configuration of the original carbanion is maintained. By this reaction, an optically active epoxy compound 142 was prepared from the cyclohexanone adduct 141181. Johnson and Schroeck188,189 succeeded in obtaining optically active styrene oxide by recrystallization of the condensation product of (+ )-(S)-n-butyl methyl sulfoxide 143 with benzaldehyde. 

Benzenediamine (129) gave 2-phenylquinoxaline (132) [BzCH2SOMe or BzCH(SOMe)2, PhH, AcOH, reflux, 2 h 35% after separation from another product aerial or sulfoxide oxidation required with the first reagent). 

An a-fluorinated phosphinyl sulfoxide derivative, prepared as a mixture of diastereomers by the treatment of lithiated (a-fluoromethyl)diphenylphosphine oxide with menthyl p-toluenesulfinate, has been used for the preparation of enan-tiomerically pure 1-fluorovinyl and 1-fluoromethyl sulfoxides [76]. (E)-Diethyl ferf-butylsulfinylmethylphosphonate 117 has been prepared by the sulfinylation... 

The reaction of the aldehyde 174, prepared from D-glucose diethyl dithio-acetal by way of compounds 172 and 173, with lithium dimethyl methyl-phosphonate gave the adduct 175. Conversion of 175 into compound 176, followed by oxidation with dimethyl sulfoxide-oxalyl chloride, provided diketone 177. Cyclization of 177 with ethyldiisopropylamine gave the enone 178, which furnished compounds 179 and 180 on sodium borohydride reduction. 0-Desilylation, catalytic hydrogenation, 0-debenzyIation, and acetylation converted 179 into the pentaacetate 93 and 5a-carba-a-L-ido-pyranose pentaacetate (181). 

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