C2-symmetric

Hanessian and Devasthale, 1996] Hanessian, S., and Devasthale, P. Design and synthesis of novel, pseudo C2 symmetric inhibitors of HIV protease. Bioorg. Med. Chem. Lett. 6 (1996) 2201-2206... 

The antibiotic rifamycin provides an example of a different and more common situation in which a target structure which has no overall symmetry has imbedded within it a Ci-symmetrical or nearly symmetrical substructure that, in turn, can be converted retrosynthetically to either a C2-symmetrical precursor or a pair of precursors available from a common intermediate. 6... 

Several highly enantioselective Diels-Alder reactions are known for which the di-enophile does not fit any of the above classes. Corey and coworkers applied the chiral aluminum reagent 36 with a C2-symmetric stilbenediamine moiety (videsu-pra) to the Diels-Alder reaction of maleimides as dienophiles [54] (Scheme 1.68). In most asymmetric Diels-Alder reactions the reactants are usually relatively simple dienes such as cyclopentadiene or monosubstituted butadienes, and unsym-... 

Chiral C2-symmetric bisoxazoline-copper(II) complexes [30, 31] were introduced as catalysts for cycloaddition and ene reactions of glyoxylates with dienes [9] leading to intense activity in the use of these catalyst for different cycloaddition reactions. 

To account for the course of this reaction theoretical calculations of the coordination of ketomalonate 37 to copper(II) and zinc(II) have revealed that the six-membered ring system is slightly more stable than the five-membered ring system (Scheme 4.30). The coordination of 37 to catalyst (l )-39 shows that the six-membered intermediate is C2-symmetric with no obvious face-shielding of the carbonyl functionality (top), while for the five-membered intermediate (bottom) the carbonyl is shielded by the phenyl substituent. Calculations of the transition-state energy for the reaction of the two intermediates with 1,3-cyclohexadiene leads to the lowest energy for the five-membered intermediate this approach is in agreement with the experimental results [45]. 

Eor the application of C2-symmetric bis-oxazoline-Lewis acids in other catalytic reactions (a) Mukaiyama-aldol reactions see, e.g., D.A. Evans, M.C. Kozlowski,... 

Although carpanone s complex structure possesses no element of symmetry, it was suggested1 that carpanone could form in nature through an intramolecular cycloaddition of a C2-symmetric bis(qui-... 

The elegant biomimetic synthesis of carpanone by Chapman and coworkers commences with the base-induced isomerization of 2-allyl-4,5-methylenedioxyphenol (4)3 to 2-(/ran.y-l-propenyl)-4,5-methylenedioxyphenol (3) (see Scheme 2). Compound 3, as simple as it is, is actually the key intermediate in this synthesis oxidative dimerization of 3 could result in the formation of carpanone (1) through the intermediacy of the C2-symmetric and highly reactive bis(quinodimethide) 2. 

The C2-symmetric epoxide 23 (Scheme 7) reacts smoothly with carbon nucleophiles. For example, treatment of 23 with lithium dimethylcuprate proceeds with inversion of configuration, resulting in the formation of alcohol 28. An important consequence of the C2 symmetry of 23 is that the attack of the organometallic reagent upon either one of the two epoxide carbons produces the same product. After simultaneous hydrogenolysis of the two benzyl ethers in 28, protection of the 1,2-diol as an acetonide ring can be easily achieved by the use of 2,2-dimethoxypropane and camphor-sulfonic acid (CSA). It is necessary to briefly expose the crude product from the latter reaction to methanol and CSA so that the mixed acyclic ketal can be cleaved (see 29—>30). Oxidation of alcohol 30 with pyridinium chlorochromate (PCC) provides alde-... 

Metzner et al. also prepared the selenium analogue 17 of their C2 symmetric chiral sulfide and tested it in epoxidation reactions (Scheme 1.6) [8]. Although good enantioselectivities were observed, and a catalytic reaction was possible without the use of iodide salts, the low diastereoselectivities obtained prevent it from being synthetically useful. 

To control the first factor, one of the two lone pairs of the sulfide must be blocked such that a single diastereomer is produced upon alkylation. For C2 symmetric sulfides this is not an issue, as a single diastereomer is necessarily fonned upon alkylation. To control the second factor, steric interactions can be used to favor one of the two possible conformations of the ylide (these are generally accepted to be the two conformers in which the electron lone pairs on sulfur and carbon are orthogonal) [14], The third factor can be controlled by sterically hinder-... 

Jacobsen demonstrated that the (salen)Cr system used to effect intermolecular, cooperative asymmetric azidolysis of meso-epoxides (Schemes 7.3 and 7.5) could be applied to sulfur-centered nucleophiles (Scheme 7.13). In order to overcome moderate enantioselectivity (<60% ee), a dithiol nucleophile was employed as part of a double resolution strategy in which the minor enantiomer of the monoaddition product reacts preferentially to form the meso- bis-addition product, thereby increasing the ee of the C2-symmetric bis-addition product. Enantiopure 1,2-mer-capto alcohols (>99% ee) were obtained from the meso-epoxide in ca. 50% overall yield by a burdensome (though effective) multistep sequence, [23]. 

Subsequent to the development of the (salen)Cr-catalyzed desymmetrization of meso-epoxides with azide (Scheme 7.3), Jacobsen discovered that the analogous (salen)Co(n) complex 6 promoted the enantioselective addition of benzoic acids to meso-epoxides to afford valuable monoprotected C2-symmetric diols (Scheme 7.15) [26], Under the reaction conditions, complex 6 served as a precatalyst for the (salen) Co(iii)-OBz complex, which was fonned in situ by aerobic oxidation. While the enantioselectivity was moderate for certain substrates, the high crystallinity of the products allowed access to enantiopure materials by simple recrystallization. 

From the standpoints of both cost and atom economy, water is the ideal nucleophile for synthesis of enantioenriched C2-symmetric 1,2-diols from meso-epoxides. 

The highest ee s reported to date for the addition of achiral organometallic reagents in the presence of aprotic chiral additives were observed with the C2-symmetric diamines 10, 11 and 12 (Table 25)13 — 15. Enantioselectivities as high as 89% ee were observed with chiral auxiliary 1012. Addition of phenyllithium to pentanal proceeds with lower enantioselection that the analogous addition of butyllithium to benzaldehydeu. Generally, the enantioselcctivity in-... 

Furthermore, both (E)- and (Z)-enolborinates add to aldehydes in a stereoconvergcnt manner, giving predominantly, syn-/J-hydroxycarbonyl compounds49. In contrast, only moderate induced diastereoselectivity is obtained in the reaction of achiral aldehydes with C2-symmetric enolborates, whereby the chiral information is located in the ligand at the metal atom50. The ee of the product /1-hydroxy ketones ranges from 4 to 72%. 

The following C2-symmetric bis-sulfonamide is a more efficient controller of stereoselectivity in aldol additions. The incorporation of this ligand into the bromodiazaborolane, subsequent generation of the boron enolate derived from 3-pentanone, and addition to achiral aldehydes preferentially leads to the formation of ijn-adducts (synjanti 94 6 to >98 2) with 95-98% ee. Chemical yields of 85-95% are achieved51. 

Boron enolates containing the chiral information in C2-symmetric ligands of the metal atom, also provide rmt/-/ -hydroxycarboxylic acid derivatives of high optical purity34 -64-70. When 5-(3-cthylpent-3-yl) thiopropanoate is treated with (5,5)-2,5-dimethyl-l-(trifluoromethylsul-... 

The latter is estimated to be at least 50 1. Unfortunately, the C2-symmetric borolane reagent is not readily available34. 

With C2-symmetric reagents (5,5)-2,5-dimethyl-l-trifluoromethylsulfonylborolane34 and (R,R)-l-chloro-2,5-diphenylborolane , (S)-(3-ethylpent-3-yl) thiopropanoate is added, via the corresponding enolates, to aldehydes with remarkable auxiliary-induced stereoselectivity. Thus, /1-hydroxy thioestcrs arc obtained with 87-94% ee when the borolanyl triflate auxiliary reagent is used. These ee values do not exactly reflect the enantiofacial selectivity since the borolane is not available in enantiomerically pure form (see Section 1.3.4.2.2.2.). Use of the chiral chloroborolane auxiliary gives the thioestcrs with 95-96% cc70,11. o... 

Chiral amide and imide enolates are amongst the most effective reagents providing. yv -3-hy-droxycarboxylic acids in both high simple diastereoselectivity and induced stereoselectivity, e.g., the amides 1 and 2, and especially, the imides 3 and 4 (derived from (S(-valine and (l/ ,2S)-norephedrine, respectively)93 and the C2-symmetric amide 594 are highly effective systems ... 

The amide 33l06b and the cyclic sulfamide 34106c, both C2-symmetric, and the borneol derived amide 3510bd provide further ways to xyn-aldols with remarkable induced diastereoselectivity. 

Use of the valine derived (4S )-3-acetyl-4-isopropyl-1,3-oxazolidine (8)92, the C2-symmetric reagents (2.5,55)-l-acetyl-2,5-bissubstituted pyrrolidine 994, or the doubly deprotonated acetyl urea /V-acetyl- V..V -bis[(.S)-l-phcnylethyl]urea (10), also does not lead to sufficient induced stereoselectivity combined with acceptable chemical yield. When the acetyl urea enolate is reacted with aliphatic and aromatic aldehydes, the diastereomeric adducts (ratios ranging from 1 1 to 3 1) may be separated by column chromatography to give ultimately both enantiomers of the 3-hydroxy acids in 99% ee110. 

The reaction of butyllithium with 1-naphthaldehyde cyclohexylimine in the presence of (/C )-l,2-diphenylethane-1,2-diol dimethyl ether in toluene at —78 °C, followed by treatment with acetate buffer, gave 2-butyl-1,2-dihydronaphthalene-l-carbaldehyde, which was then reduced with sodium borohydride in methanol to afford (1 R,2.S)-2-butyl-1 -hydroxymcthyl-1,2-dihydronaphthalene in 80% overall yield with 91 % ee83. Similarly, the enantioselective conjugate addition of organolithium reagents to several a,/J-unsaturated aldimines took place in the presence of C2-symmetric chiral diethers, such as (/, / )-1,2-butanediol dimethyl ether and (/, / )- ,2-diphenylethane-1,2-diol dimethyl ether. 

A remarkably high enantioselectivity of 81 % is achieved using the simple C2-symmetric chiral crown ether 6 derived from (2,S ,3b )-butanediol263. 

Zirconocene dichloride 121 derived from (l-phenylethyl)cyclopentadienyl ligand is formed as a mixture of diastereomers from which the racemic form can be isolated by fractional crystallization. This complex was studied by X-ray diffraction methods and revealed a virtually chiral C2-symmetrical conformation in which the chiral ring-substituents are arranged in a synclinal position relative to the five-membered ring. It was proposed that this conformation is preserved in solution. Using 121 as catalyst the influence of double stereodifferentiation during isospecific polymerization of propylene (Eq. 32) was demonstrated for the first time [142],... 

The problem of tr-facial differentiation, i.e. diastereomer formation, encountered in the metal complexation of the above mentioned annulated cyclopentadienyl ligands is avoided when C2-symmetrical ligands [153] are utilized. Since in such ligands both sides of the five-membered rings are homotopic, only one isomer is... 

Inverse electron-demand Diels-Alder reaction of (E)-2-oxo-l-phenylsulfo-nyl-3-alkenes 81 with enolethers, catalyzed by a chiral titanium-based catalyst, afforded substituted dihydro pyranes (Equation 3.27) in excellent yields and with moderate to high levels of enantioselection [81]. The enantioselectivity is dependent on the bulkiness of the Ri group of the dienophile, and the best result was obtained when Ri was an isopropyl group. Better reaction yields and enantioselectivity [82, 83] were attained in the synthesis of substituted chiral pyranes by cycloaddition of heterodienes 82 with cyclic and acyclic enolethers, catalyzed by C2-symmetric chiral Cu(II) complexes 83 (Scheme 3.16). 

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