Sulfoxides stereochemistry

In analogy to the transformations observed for other compounds, a similar process was proposed for the interconversion of thiaspirane sulfoxides and to explain the dependence of the thermolytic process on sulfoxide stereochemistry. Scheme 1 shows the probable mechanism of the transformation. Stereochemical transformations of the C30 Nuphar thiaspiranes have been observed on quarter-nization of thiobinupharidine (16) (equatorial sulfur atom). The quaternized quinolizidine system is transformed from the trans to the cis form with inversion of the relative configuration of the corresponding C-7 or C-7. ... 

Kielbasinski, P., Rachwalski, M., Mikolajczyk, M., et al. 2008. Nitrilase-catalysed hydrolysis of cyanomethyl p-tolyl sulfoxide Stereochemistry and mechanism. Tetrahedron Asymmetry, 19 562-7. 

C NMR has been used to assign the sulfoxide stereochemistry of a series of 6-substituted penicillins (Harrison and Hodge, 1976a). The chi-rooptical properties of penicillins and their sulfoxides containing various 6 substituents have been the subject of two publications (Richardson et al., 1977 Busson et al., 1977). 

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). 

To control the stereochemistry of 1,3-dipolar cycloaddidon reacdons, chiral auxiliaries are introduced into either the dipole-part or dipolarophile A recent monograph covers this topic extensively ° therefore, only typical examples are presented here. Alkenes employed in asymmetric 1,3-cycloaddidon can be divided into three main groups (1) chiral allyhc alcohols, f2 chiral amines, and Hi chiral vinyl sulfoxides or vinylphosphine oxides. 

Tin, nitratodiphenyltris(dimethy) sulfoxide)-structure, 1,77 Tin, nitratotris(triphenyltin)-structure, 1, 47 Tin,tetrakis(acetato)-stereochemistry, 1,94 Tin, tetrakis(diethyldithiocarbamato)-angular parameters, 1, 57 Tin, tetrakis(ethyldithiocarbamato)-angular parameters, 1, 57 Tin, tetranitrato-stereochemistry, 1, 94 Tin, tri-n-butylmethoxy-, 3, 208 Tin alkoxides physical properties, 2, 346 Tin bromide, 3, 194 Tin bromide hydrate, 3,195 Tin carboxylates, 3, 222 mixed valence, 3, 222 Tin chloride, 3, 194 hydroformylation platinum complexes, 6, 263 Tin chloride dihydrate, 3,195 Tin complexes, 3, 183-223 acetyl ace tone... 

Uranium, pentakis(dimethyl sulfoxide)dioxy-stereochemistry, I, 74 Uranium, pentakis(urea)dioxy-stereochemistry, 1,74 Uranium, tetrakis(bipyridyl)-stereochemistry, I, 94 structure, 1, 24... 

Ytterbium, trinitratotris(dimethyl sulfoxide)-structure, 1, 97 Ytterbium, tris(acetylacetone)(4-ammo-3-penten-stereochemistry, 1,81 Ytterbium complexes acetylacetone, 2,373 dipositive oxidation state hydrated ions, 3,1109 polypyrazolylborates, 2,255 Ytterbium(III) complexes ethyl glycinate, diacetate... 

Accordingly, there have been numerous studies on the stereochemistry of these a-sulfinyl carbanions56-77. Representative data on the reactions of a-lithiosulfoxides derived from benzyl sulfoxides with some electrophiles are listed in Table 13. Although the stereochemistry depends on the substituent on the sulfinyl function, the diastereomeric ratio remains the same regardless of the electrophile used for each sulfoxide. 

Rearrangements have been included in which sulfoxides participate not only as reactants but also as products. Reactions have been classified according to mechanism, but although the main emphasis has been on mechanism and stereochemistry, special attention to synthetic applications has also been given wherever appropriate. 

In addition to the synthetic applications related to the stereoselective or stereospecific syntheses of various systems, especially natural products, described in the previous subsection, a number of general synthetic uses of the reversible [2,3]-sigmatropic rearrangement of allylic sulfoxides are presented below. Several investigators110-113 have employed the allylic sulfenate-to-sulfoxide equilibrium in combination with the syn elimination of the latter as a method for the synthesis of conjugated dienes. For example, Reich and coworkers110,111 have reported a detailed study on the conversion of allylic alcohols to 1,3-dienes by sequential sulfenate sulfoxide rearrangement and syn elimination of the sulfoxide. This method of mild and efficient 1,4-dehydration of allylic alcohols has also been shown to proceed with overall cis stereochemistry in cyclic systems, as illustrated by equation 25. The reaction of trans-46 proceeds almost instantaneously at room temperature, while that of the cis-alcohol is much slower. This method has been subsequently applied for the synthesis of several natural products, such as the stereoselective transformation of the allylic alcohol 48 into the sex pheromone of the Red Bollworm Moth (49)112 and the conversion of isocodeine (50) into 6-demethoxythebaine (51)113. 

When enantiomerically pure allyl p-tolyl sulfoxide is deprotonated and then treated with electrophilic 2-cyclopentenone, a conjugate addition occurs forming a new carbon-carbon bond with very high control of absolute stereochemistry (equation 25)65. See also Reference 48. Similarly, using more substituted enantiomerically pure allylic sulfoxides leads to virtually complete diastereocontrol, as exemplified by equations 26 and 27 the double bond geometry in the initial allylic sulfoxide governs the stereochemistry at the newly allylic carbon atom (compare equations 26 vs. 27)66. Haynes and associates67 rationalize this stereochemical result in terms of frontier molecular orbital considerations... 

Enantiomerically pure 3-tolyl-2-sulfinyl-2-cyclopentenone 37 undergoes smooth, mild and diastereoselective conjugate hydride addition with lithium tri(sec-butyl)borohydride to afford ultimately 3-tolylcyclopentanone 38 in 93% enantiomeric purity (equation 35)78. The absolute stereochemistry of product 38 is consistent with a chelated intermediate directing hydride addition from that diastereoface containing the sulfoxide lone pair. 

The absolute stereochemistry at the sulfoxide sulfur atom in some /J-phenylsulfinyl radicals (prepared in situ by treating 2-bromo-3-phenylsulfinylbutanes with tributylstan-nane) controls the stereochemistry (i.e., cis vs. trans) of the olefinic products which are formed104. Implicit in this result is that loss of the sulfinyl group occurs more rapidly than rotation about C-2-C-3 of the intermediate radical105. 

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