Intramolecular cyclopropanation, chiral

In recent years, the variety of useful diazo substrates for asymmetric intramolecular cyclopropanation processes has really expanded. As another example, Charette and Wurz have reported the first example of an intramolecular cyclopropanation involving a-nitro-a-diazo carbonyl compounds.This reaction, catalysed by Rh2[(S)-DOSP]4, led to the formation of nine-membered nitrocyclopropyl lactones in good yields and enantioselectivities with extremely high diastereoselectivities (Scheme 6.17). This novel methodology constituted an efficient entry into chiral functionalised macrocyclic-fused cyclopropane oc-amino acids. 

The asymmetric synthesis of dihydrochrysanthemolactone 217 by intramolecular cyclopropanation of diazoacetate 216 in the presence of chiral salicylaldimine/... 

Intramolecular cyclopropanation has a noteworthy advantage. Unlike intermolecular asymmetric cyclopropanation, the intramolecular reaction produces only one diastereomer due to geometric constrains on the fused bicyclic products. Doyle has extensively studied the intramolecular enantioselective reactions of a variety of alkenyl diazoacetates catalyzed by chiral rhodium carboxamides 198 and 200 and has achieved excellent results. 

The inter- or intramolecular cyclopropanation of achiral alkenes with enantiome-rically pure diazoacetic esters [1016,1363,1364] or amides [1365,1366] does not usually proceed with high diastereoselectivity. A chiral auxiliary which occasionally gives good results is pantolactone (3-hydroxy-4,4-dimethyltetrahydro-2-furanone) [1016,1367,1368]. 

Since the first experiments with chiral copper complexes reported by Nozaki [650] and Aratani [1027] many different catalysts have been examined, both for intermolecular and intramolecular cyclopropanations (for a review, see [1369]). Syntheses of natural products [955,1370] and drugs [1371] using asymmetric cyclopropanation with chiral electrophilic carbene complexes have been reported. A selection of useful catalysts is given in Figure 4.20 (see also Experimental Procedure 4.1.1). 

For intermolecular cyclopropanations with unsubstituted diazoacetates the highest asymmetric inductions can be achieved with the copper(I) complexes of C2-symmetric, bidentate ligands developed by Pfaltz (e.g. 1) and Evans (2). The chiral rhodium(II) complexes known today do not generally lead to such high enantiomeric excesses as copper complexes in intermolecular cyclopropanations. For intramolecular cyclopropanations, however, chiral rhodium(II) complexes are usually superior to enantiomerically pure copper complexes [1374]. 

Chiral dirhodium(II) carboxamidates are preferred for intramolecular cyclopropanation of allylic and homoallylic diazoacetates (Eq. 2). The catalyst of choice is Rh2(MEPY)4 when R " and R are H, but Rh2(MPPIM)4 gives the highest selectivities when these substituents are alkyl or aryl. Representative examples of the applications of these catalysts are listed in Scheme 15.1 according to the cyclopropane synthesized. Use of the catalyst with mirror image chirality produces the enantiomeric cyclopropane with the same enantiomeric excess [33]. Enantioselectivities fall off to a level of 40-70% ee when n is increased beyond 2 and up to 8 (Eq. 2) [32], and in these cases the use of the chiral bisoxazoline-copper complexes is advantageous. 

Diazoacetamides undergo intramolecular cyclopropanation with similarly high enantios-electivities (Eq. 4) [33, 36, 37]. In these cases, however, competition from intramolecular dipolar cycloaddition can compHcate the reaction process. Therefore, the use of R = Me or Bu has been required to achieve good yields of reaction products. Representative examples of applications of chiral dirhodium(II) carboxamidates for enantioselective intramolecular cyclopropanation of diazoacetamides are compiled in Scheme 15.2. 

The power of chiral C2-symmetric bis(oxazolines) in cyclopropanation reactions has also been exhibited in total synthesis. One example is Corey and co-workers synthesis of sirenin 63 using bis(oxazoline) ligand 8 (Fig. 9.19). They showed that the intramolecular cyclopropanation of diazo derivative 61 proceeded in 77% yield and with 90% ee. Shibasaki and co-workers constructed prostratin 67 through the intermediate cyclopropane 66, also shown in Figure 9.19. Using bis(oxazoline) ligand 64 and copper(I) triflate-derived catalyst, compound 66 was prepared in 70% yield and 92% ee from diazo derivative 65. ... 

Asymmetric ethylidene transfer has been achieved in the reactions of 1-cyclohexenyl ethers carrying a chiral auxiliary with 1,1-diodoethane/diethylzinc 39. Asymmetric induction in the reaction of diazofluorene with fumaric esters bearing chiral alcohol moieties has been investigated (equation 84)140,141. Kinetics of intramolecular cyclopropanation in... 

Chiral Rh(II) oxazolidinones Rh2(BNOX)4 and Rh2(IPOX)4 (25a,b) were not as effective as Rh2(MEPY)4 for enantioselective intramolecular cyclopropanation, even though the steric bulk of their chiral ligand attachments (COOMe versus i-Pr or CH2Ph) are similar. Significantly lower yields and lower enantioselectivides resulted from dinitrogen extrusion from prenyl diazoacetate catalyzed by either Rh2(4.S -lPOX)4 or Rh2(4S-BNOX)4. This difference, and those associated with butenolide formation [91], can be attributed to the ability of the carboxylate substituents to stabilize the carbocation form of the intermediate metal carbene (3b), thus limiting the Rh2(MEPY)4-catalyzed reaction to concerted carbene addition onto both carbon atoms of the C-C double bond. 

Once again, cis-disubstituted olefins lead to higher enantioselectivities than do trans-disubstituted olefins, but here the differences are not as great as they were with allyl diazoacetates. Both allylic and homoallylic diazoacetamides also undergo highly enantioselective intramolecular cyclopropanation (40-43) [93,94], However, with allylic a-diazopropionates enantiocontrol i s lower by 10-30% ee [95], The composite data suggest that chi ral dirhodium(II) carboxamide catalysts are superior to chiral Cu or Ru catalysts for intramolecular cyclopropanation reactions of allylic and homoallylic diazoacetates. 

Well-known is the cyclopropanation of various alkenes. As shown by 329, cyclopropanation starts by electrophilic attack to the alkene. Electron-rich alkenes have higher reactivity. Numerous applications of intramolecular cyclopropanation to syntheses of natural products have been reported. Optically active cyclopropanes are prepared by enantioselective cyclopropanation [100], As the first successful example, asymmetric synthesis of chrysanthemic acid (331) was carried out by cyclopropanation of 2,5-dimethyl-2,4-hexadiene (330) with diazoacetate, catalysed by the chiral... 

Dirhodium(II) tetrakis(carboxamides), constructed with chiral 2-pyrroli-done-5-carboxylate esters so that the two nitrogen donor atoms on each rhodium are in a cis arrangement, represent a new class of chiral catalysts with broad applicability to enantioselective metal carbene transformations. Enantiomeric excesses greater than 90% have been achieved in intramolecular cyclopropanation reactions of allyl diazoacetates. In intermolecular cyclopropanation reactions with monosubsti-tuted olefins, the cis-disubstituted cyclopropane is formed with a higher enantiomeric excess than the trans isomer, and for cyclopropenation of 1-alkynes extraordinary selectivity has been achieved. Carbon-hydro-gen insertion reactions of diazoacetate esters that result in substituted y-butyrolactones occur in high yield and with enantiomeric excess as high as 90% with the use of these catalysts. Their design affords stabilization of the intermediate metal carbene and orientation of the carbene substituents for selectivity enhancement. 

Intramolecular Cyclopropanation with Chiral Rhodium(II) 2-Pyrroli-done-5-carboxylates. Applications of chiral copper and cobalt catalysts, including... 

A-Cu,N-Co, and P-Cu to carbenoid transformations have been limited to intermolecular reactions, for which they remain superior to chiral dirhodium(II) catalysts for intermolecular cyclopropanation reactions. Few examples other than those recently reported by Dauben and coworkers (eq 1) (35) portray the effectiveness of these chiral catalysts for enantioseleetive intramolecular cyclopropanation reactions, and these examples demonstrate their limitations. However, with Rh2(5S-MEPY)4 intramolecular cyclopropanation of 3-methyl-2-buten-1 -yl diazoacetate (eq 2) occurs in high yield and with 92% enantiomeric excess (36). 

Several iodonium ylides, thermally or photochemically, transferred their carbene moiety to alkenes which were converted into cyclopropane derivatives. The thermal decomposition of ylides was usually catalysed by copper or rhodium salts and was most efficient in intramolecular cyclopropanation. Reactions of PhI=C(C02Me)2 with styrenes, allylbenzene and phenylacetylene have established the intermediacy of carbenes in the presence of a chiral catalyst, intramolecular cyclopropanation resulted in the preparation of a product in 67% enantiomeric excess [12]. 

Other terminal olefins were transformed to the corresponding cyclopropane esters with Z-menthyl and d-menthyl diazoacetates with high stereoselectivity up to 98% ee (Scheme 3). Intramolecular reaction of the phenyl-allyl ester 9 was carried out to give the bicyclic compound 10 with 86% ee and 93% yield. The enantioselectivity for intramolecular cyclopropanation of the 3-methylbutenyl ester 11 was compared with chiral Cu(I), Rh(II), and Ru Pybox catalysts Rh>Ru>Cu [26]. 

Intramolecular cyclopropanation of allyl diazoacetates gives rise to interesting cyclopropane-fused y-butyrolactones. A chiral ruthenium bis(oxa-zolinyl)pyridine complex 85 was employed for the catalytic cyclization of trans-cinnamyl diazoacetate 83 at room temperature to obtain an optically active lactone 84 in 93% yield with 86% ee (Eq. 34, Fig. 2) [85]. Chiral porphyrin and salen complexes of ruthenium 86 [86] and 87 [87] also catalyzed the asymmetric intramolecular cyclopropanation of 83 to afford 84 in similar yields and enantiomeric excess. 

The mechanism of the [3 + 2] cycloaddition is summarized in Scheme The first intermediate results from charge transfer interaction between the eli tronically excited aromatic compound at its singlet state S1 with the alkene w] leads to the formation of the exciplexes K. A more stable intermediate is generated by the formation of two C-C bonds, leading to the intermediates These intermediates have still singlet multiplicity and therefore possess zwii ionic mesomeric structures mainly of type M. In most cases and especially intramolecular reactions, chiral induction occurs during the formation of L. final products are then obtained by cyclopropane formation in the last step. 

A review about the rearrangement and cycloaddition of carbonyl ylides generated from a-diazo compounds is available <2001CSR50>. Enantioselective intramolecular cyclopropanations of allyl 2-diazo-3-silanyloxybut-3-enoates to yield cyclopropyl 7-butyrolactones have been investigated with a variety of chiral rhodium catalysts. The best results were obtained with Rh2(PTTL)4, where enantioselectivity culminated at 89% ee (Equation 99) <2005TA2007>. 

This is the first detailed procedure for the synthesis of a chiral dirhodium(ll) carboxamide catalyst and its application to intramolecular cyclopropanation. The preparation of the ligand, methyl 2-pyrrolidone-5(R)-carboxylate, is adapted from the procedure of Ackermann, Matthes, and Tamm.2 The method for ligand displacement from dirhodium(ll) tetraacetate is an extension of that reported for the synthesis of dirhodium(ll) tetraacetamide.6 The title compound, (1 R,5S)-(-)-6,6-dimethyl-3-oxabicyclo[3.1.0]hexan-2-one, is a synthetic precursor to (1 R,3S)-(+)-cis-chrysanthemic acid.5... 

Stereoselectivity) is observed however, for ethylidene complexes of Fe(CO)(PR3)Cp (69) the products reflect trans selectivity. This difference in stereoselectivity has been suggested to be dependent upon which conformer is more reactive. The reaction of a chiral-at-iron cationic carbene complex (70) with styrene or vinyl acetate affords optically active cyclopropane products with high enantioselectivity (Scheme 24). h >3 intramolecular cyclopropanation, as in the case of (71), proceeds moderately well for the formation of norcarane-type ring systems however, intramolecular C-H insertion is a competing pathway when the alkene is highly... 

Synthesis of Cyclopropanes. Chiral imide enolates which contain y-halide substituents undergo intramolecular displacement to form cyclopropanes. Halogenation of y,5-unsamrated acyl imides occurs at the y-position in 85% yield with modest stereoinduction. The (Z) sodium enolates of these compounds then cyclize through an intramolecular double stereodifferentiating reaction (eq 61). 

Semicorrinato)copper catalysts have also been used for intramolecular cyclopropanation reactions of alkenyl diazo ketones (eq 9 and eq 10). In this case the (semicorrinato)copper catalyst derived from complex (5) proved to be superior to related methylene-bis(oxazoline)copper complexes. Interestingly, analogous allyl diazoacetates react with markedly lower enantioselectivity under these conditions, in contrast to the results obtained with chiral Rh complexes which are excellent catalysts for intramolecular cyclopropanations of allyl diazoacetates but give poor enantioselectivities with alkenyl diazo ketones (see Dirhodium(II) Tetrakis(methyl 2-pyrrolidone-5(S -carboxylate ) Moderate enantioselectivities in the reactions... 

Metal Carbene TVansformations. The effectiveness of Rh2(55 -MEPY)4 and its 5R-form, Rh2 5R-MEPY)4, is exceptional for highly enantioselective intramolecular cyclopropanation and carbon-hydrogen insertion reactions. Intermolecular cyclopropanation occurs with lower enantiomeric excesses than with alternative chiral copper salicylaldimine or C2-symmetric semicorrin or bis-oxazoline copper catalysts, but intermolecular cyclopropenation exhibits higher enantio-control with Rh2(MEPY)4 catalysts. The methyl carboxylate attachment of Rh2(55-MEPY)4 is far more effective than steri-cally similar benzyl or isopropyl attachments for enantioselective metal carbene transformations. The significant enhancement in enantiocontrol is believed to be due to carboxylate carbonyl stabilization of the intermediate metal carbene and/or to dipolar influences on substrate approach to the carbene center. 

A double diastereotopic differentiation strategy on a phosphonoacetate template has been described. The approach utilizes Rh2(OAc)4-catalysed intramolecular cyclopropanation (ICP) employing the (R)-pantolactone auxiliary in the ester functionality of the phosphonoacetate (328).The olefinic diastereofacial selectivity is governed by inherent electronic and steric interactions in the reacting carbene intermediate, while the group selectivity is dictated by the chiral auxiliary. This approach is an effective method to access bicyclic P-chiral phos-phonates (329) (Scheme 87). ... 

The use of chiral additives with a rhodium complex also leads to cyclopropanes enantioselectively. An important chiral rhodium species is Rh2(5-DOSP)4, which leads to cyclopropanes with excellent enantioselectivity in carbene cyclopro-panation reactions. Asymmetric, intramolecular cyclopropanation reactions have been reported. The copper catalyzed diazoester cyclopropanation was reported in an ionic liquid. ° It is noted that the reaction of a diazoester with a chiral dirhodium catalyst leads to p-lactones with modest enantioselectivity Phosphonate esters have been incorporated into the diazo compound... 

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