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Sulfide chiral auxiliary

The oxidation of heteroatoms and, in particular, the conversion of sulfides to asymmetric sulfoxides has continued to be a highly active field in biocatalysis. In particular, the diverse biotransformations at sulfur have received the majority of attention in the area of enzyme-mediated heteroatom oxidation. This is particularly due to the versatile applicability of sulfoxides as chiral auxiliaries in a variety of transformations coupled with facile protocols for the ultimate removal [187]. [Pg.253]

In 1986, Puchot et al.104 studied the nonlinear correlation between the enantiomeric excess of a chiral auxiliary and the optical yield in an asymmetric synthesis, either stoichiometric or catalytic. Negative NLEs [(—)-NLEs] were observed in the asymmetric oxidation of sulfide and in [.S ]-proline-mediated asymmetric Robinson annulation reactions, while a positive NLE [(+)-NLEs]... [Pg.492]

The first attempts to develop reactions offering control over the absolute stereochemistry of a chiral center, created by y-selective substitution of an achiral allylic alcohol-derived substrate, involved the use of chiral auxiliaries incorporated in the nucleofuge. The types of stereodirecting groups utilized vary, and have included sulfoximines [15], carbamates [16], and chiral heterocyclic sulfides [17-19]. [Pg.263]

The enantiomeric synthesis of rranj-3,4-disubstituted tetrahydrothiophenes using a sulfur ylide cycloaddition has been reported <990L1667>. The sulfur ylide derived from the action of cesium fluoride on sulfide 111 underwent an asymmetric cycloaddition with chiral a,p-unsaturated camphorsultam amide 112 giving tetrahydrothiophene 113 (80% de). The configuration was confirmed by cleavage of the chiral auxiliary followed by reductive desulfurization with Raney-Ni which gave known carboxylic acid 114. [Pg.103]

Chiral sulfoxides have emerged as versatile building blocks and chiral auxiliaries in the asymmetric synthesis of pharmaceutical products. The asymmetric oxidation of prochiral sulfides with chiral metal complexes has become one of the most effective routes to obtain these chiral sulfoxides.We have recently developed a new heterogeneous catalytic system (WO3-30% H2O2) which efficiently catalyzes both the asymmetric oxidation of a variety of thioethers (1) and the kinetic resolution of racemic sulfoxides (3), when used in the presence of cinchona alkaloids such as hydroquinidine 2,5-diphenyl-4,6-pyrimidinediyl diether [(DHQD)2-PYR], Optically active sulfoxides (2) are produced in high yields and with good enantioselectivities (Figure 9.3). ... [Pg.288]

Asymmetric oxidation of prochiral sulfides is one of the most effective routes for the preparation of chiral sulfoxides. These latter molecules attract great interest, as they are useful synthons for some drugs. They can also be used as chiral auxiliaries due to their configurational stability. The oxidation can be performed by using complexes... [Pg.293]

Organometallic compounds asymmetric catalysis, 11, 255 chiral auxiliaries, 266 enantioselectivity, 255 see also specific compounds Organozinc chemistry, 260 amino alcohols, 261, 355 chirality amplification, 273 efficiency origins, 273 ligand acceleration, 260 molecular structures, 276 reaction mechanism, 269 transition state models, 264 turnover-limiting step, 271 Orthohydroxylation, naphthol, 230 Osmium, olefin dihydroxylation, 150 Oxametallacycle intermediates, 150, 152 Oxazaborolidines, 134 Oxazoline, 356 Oxidation amines, 155 olefins, 137, 150 reduction, 5 sulfides, 155 Oxidative addition, 5 amine isomerization, 111 hydrogen molecule, 16 Oxidative dimerization, chiral phenols, 287 Oximes, borane reduction, 135 Oxindole alkylation, 338 Oxiranes, enantioselective synthesis, 137, 289, 326, 333, 349, 361 Oxonium polymerization, 332 Oxo process, 162 Oxovanadium complexes, 220 Oxygenation, C—H bonds, 149... [Pg.196]

Biooxidation of chiral sulfides was initially investigated in the 1960s, especially through the pioneering work of Henbest et al. [101]. Since then, many developments have been reported and are summarized in reviews [102,103], It would be helpful to reveal some structural or mechanistic details of enzymes involved in theoxidation processes. Biotransformations are also of great current interest for the preparation of chiral sulfoxides, which are useful as synthetic intermediates and chiral auxiliaries. Because extensive review of these transformations is beyond the scope of this chapter, only highlights are discussed in comparison with the abiotic enantioselective oxidations described earlier. Biooxidations by microorganisms and by isolated enzymes are discussed in Sections 6C.12.1. and 6C.12.2. [Pg.348]

Optically active a-alkoxycarbonylthioaldehydes were prepared from the corresponding a-dichloroacetates by treatment with bis(tributyltin)sulfide and tetrabutylammonium fluoride309 8-arylmenthols were used as chiral auxiliaries and the thioaldehydes underwent asymmetric hetero-Diels-Alder cycloaddition (equation 48). [Pg.1417]

The oxidative imination of sulfides and sulfoxides via nitrene transfer processes leads to N-substituted sulfilimines and sulfoximines. This reaction is interesting as chiral sulfoximines are efficient chiral auxiliaries in asymmetric synthesis, a promising class of chiral ligands for asymmetric catalysis and key intermediates in the synthesis of pseudopeptides [169]. However, very few examples of such iron-catalyzed transformations have been described. [Pg.119]

S)-Phenyl-2-oxazolidinone.6 A one-pot route to this chiral auxiliary involves reduction of L-phenylglycine and BF3 etherate in DME with borane-dimethyl sulfide complex at a temperature maintained at 82°. The resulting phenylglycinol is then treated with trichloromethyl chloroformate (or the more expensive triphosgene). [Pg.257]

The typical S-oxidation with BVMOs allows the formation of chiral sulfoxides from organic sulfides. This oxidation has received much interest in organic chemistry due to its use in the synthesis of enantiomerically enriched materials as chiral auxiliaries or directly as biologically active ingredients. This reaction has been studied extensively with CHMO from Adnetohacter showing high enantioselectivi-ties in the sulfoxidation of alkyl aryl sulfides, disulfides, dialkyl sulfides, and cychc and acyclic 1,3-dithioacetals [90]. CHMO also catalyzes the enantioselective oxida-hon of organic cyclic sulfites to sulfates [91]. [Pg.357]

Oxaziridines. Davis has developed the use of chiral 2-sulfonyloxaziridines derived from camphorsulfonic acid as chiral auxiliaries in the asymmetric oxidation reactions. Although other oxaziridines may be preferable, the camphor-derived oxaziridines can be used for the oxidation of sulfides and disulfides to sulfoxides and thiosulfinates as well as for the epoxidation of alkenes. On the other hand, the camphoryloxaziridines are the preferred reagents for hydroxylation of lithium enolates of esters, amides, and ketones, as utilized in the synthesis of kjellmanianone (eq 17). ... [Pg.174]

Thus far, discussion has centered around the reaction of alkenes with a source of electrophilic oxygen as a route to epoxides [the C=C + O protocol]. However, a second general approach is represented by the reaction of carbonyl compounds with amphophilic carbon centers [the C=0 + C protocol]. For example, sulfonium yhdes are known to convert aldehydes and ketones to epoxides much recent work has focused on asymmetric induction using this methodology, a topic which has been the subject of a concise review in the past year <04ACR611>. As an illustration, the D-mannitol derived chiral sulfide 42 serves as a useful chiral auxiliary in the sulfonium methylide epoxidation of aldehydes to provide terminal monosubstituted oxiranes (e.g., 44) in fair to excellent yield and good enantiomeric excess <04CC1076>. [Pg.61]

In most cases, the sulfoxides produced after the asymmetric transformation are reduced with sodium or aluminium amalgam, or Raney nickel. The sulfoxide may also be reduced by LiAffl into a sulfide, winch after quaternarization becomes a leaving group [474], If the carbon skeleton of the substrate bears appropriate substituents, the sulfoxide can suffer [2,3] sigmatropic rearrangements [497, 498] or Pummerer rearrangements. In all these types of applications, the chiral auxiliary is never recovered. [Pg.79]

Annulation /raw-3,4-Disubstituted tetrahydrothiophenes are obtained from conjugated carbonyl compounds and chloromethyl trimethylsilylmethyl sulfide in a reaction mediated by CsF. When the conjugated carbonyl component bears a chiral auxiliary, the process is amenable to synthesis of enantiopure derivatives. [Pg.96]

The asymmetric oxidation of sulfides represents a straightforward access to chiral sulfoxides that are useful compounds for asymmetric synthesis as chiral auxiliaries and also for the synthesis of biologically active molecules. Among the different methods to perform these reactions, titanium-mediated thioether oxidation is one of the most attractive. Indeed, Kagan ° and Modena independently showed that the use of chiral titanium complexes derived from Sharpless reagent allows the asymmetric oxidation of prochiral sulfides (Scheme 7.6). [Pg.143]


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See also in sourсe #XX -- [ Pg.424 ]




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Sulfides chiral

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