Diastereoselective homoallyl alcohols

Allylboron compounds have proven to be an exceedingly useful class of allylmetal reagents for the stereoselective synthesis of homoallylic alcohols via reactions with carbonyl compounds, especially aldehydes1. The reactions of allylboron compounds and aldehydes proceed by way of cyclic transition states with predictable transmission of olefinic stereochemistry to anti (from L-alkene precursors) or syn (from Z-alkene precursors) relationships about the newly formed carbon-carbon bond. This stereochemical feature, classified as simple diastereoselection, is general for Type I allylorganometallicslb. 

Allylboronates are attractive reagents for the highly diastereoselective ally-lation of carbonyl compounds. A sequential cross-metathesis-allylation reaction has recently been developed by Grubbs et al. [88c] and by Miyaura et al. [103]. The sequence is illustrated in Scheme 23 for the formation of homoallylic alcohol 114 from allylboronate 112, acetal 113, and benzaldehyde [88c]. 

Sulfonic peracids (66) have also been applied recently to the preparation of acid sensitive oxiranes and for the epoxidation of allylic and homoallylic alcohols, as well as relatively unreactive a, p - unsaturated ketones. These reagents, prepared in situ from the corresponding sulfonyl imidazolides 65, promote the same sense of diastereoselectivity as the conventional peracids, but often to a higher degree. In particular, the epoxidation of certain A -3-ketosteroids (e.g., 67) with sulfonic peracids 66 resulted in the formation of oxirane products (e.g., 68) in remarkably high diastereomeric excess. This increased selectivity is most likely the result of the considerable steric requirements about the sulfur atom, which enhances non-bonded interactions believed to be operative in the diastereoselection mechanism <96TET2957>. 

B. Potassium allyl- and crotyltrifluoroborates undergo addition to aldehydes in biphasic media as well as water to provide homoallylic alcohol in high yields (>94%) and excellent diastereoselectivity (dr >98 2). The presence of a phase-transfer catalyst (e.g., B114NI) significantly accelerates the rate of reaction, whereas adding fluoride ion retards the reaction (Eq. 8.70).165 The method was applied to the asymmetric total synthesis of the antiobesity agent tetrahydrolipstatin (orlistat).166... 

Iridium-catalyzed transfer hydrogenation of aldehyde 73 in the presence of 1,1-dimethylallene promotes tert-prenylation [64] to form the secondary neopentyl alcohol 74. In this process, isopropanol serves as the hydrogen donor, and the isolated iridium complex prepared from [Ir(cod)Cl]2, allyl acetate, m-nitrobenzoic acid, and (S)-SEGPHOS is used as catalyst. Complete levels of catalyst-directed diastereoselectivity are observed. Exposure of neopentyl alcohol 74 to acetic anhydride followed by ozonolysis provides p-acetoxy aldehyde 75. Reductive coupling of aldehyde 75 with allyl acetate under transfer hydrogenation conditions results in the formation of homoallylic alcohol 76. As the stereochemistry of this addition is irrelevant, an achiral iridium complex derived from [Ir(cod)Cl]2, allyl acetate, m-nitrobenzoic acid, and BIPHEP was employed as catalyst (Scheme 5.9). 

This regio- and stereochemistry in these reactions can be accounted for as shown in Scheme 17.26 When coordinating electrophiles like ketones and aldehydes are used, the equilibrium between ij1- and 3-allyl complexes shifts to rj1, resulting in the formation of the least substituted -complex 52 preferentially. Carbon-carbon bond formation takes place via a six-membered ring transition state 53, leading to the formation of the branched homoallylic alcohols 54 with //-diastereoselectivity. 

Allylplatinum intermediates generated in the course of silaboration of dienes readily react with aldehydes to give homoallylic alcohols (Equation (125)).484 The observed high diastereoselectivity is explained by a chair-like cyclic transition state. 

In the case of tri-substituted alkenes, the 1,3-syn products are formed in moderate to high diastereoselectivities (Table 21.10, entries 6—12). The stereochemistry of hydrogenation of homoallylic alcohols with a trisubstituted olefin unit is governed by the stereochemistry of the homoallylic hydroxy group, the stereogenic center at the allyl position, and the geometry of the double bond (Scheme 21.4). In entries 8 to 10 of Table 21.10, the product of 1,3-syn structure is formed in more than 90% d.e. with a cationic rhodium catalyst. The stereochemistry of the products in entries 10 to 12 shows that it is the stereogenic center at the allylic position which dictates the sense of asymmetric induction... 

With the aid of BF3 OEt2, methoxyborolane (R,R)-114 reacts with (.E)- or (Z)-crotylpotassium to provide (is,R,R)-115 and (Z,R,R)-115, respectively. After adding the aldehyde to a solution of crotyl-borolane in THF at —78°C for 4 hours, 2-aminoethanol is added. The solution is warmed to room temperature, and oxidative cleavage at this point gives the homoallylic alcohols with high stereoselectivity. The borolane moiety can be recovered by precipitating it as an amino alcohol complex and can be reused without any loss of enantiomeric purity. As shown in Scheme 3-43, the (.E)- and (Z)-crotyl compounds lead to anti- and -products 116, respectively. The diastereoselectivity is about 20 1, and the ee for most cases is over 95% (Table 3-11). 

Diastereoselective reaction with fl-alkoxy-a-methylpropionaldehydes.1 The reaction of (R,R)-1 with the chiral aldehyde 2a provides the syn-homoallylic alcohol... 

As demonstrated in recent work by Obora and Ishii, alkynes serve as allyl donors in carbonyl allylations from the alcohol oxidation level [277]. Specifically, upon exposure to an iridium catalyst generated in situ from [lr(OH)(cod)]2 and P( -Oct)3, l-aryl-2-methylalkynes couple to primary alcohols to furnish homoallylic alcohols with complete branched regioselectivity and excellent levels of diastereoselectivity (Scheme 17). 

This chelation-controlled addition generated the homoallylic alcohols 86 with a diastereoselectivity of syn anti=S6ll4 , In contrast to the other syntheses described so far, the ring closing reaction was a 5 2 reaction but not a... 

Aldehyde 13, readily prepared by a four step synthesis from L-threonine,3a-i5 was treated with the known (Z)-7-methoxyallylboronate 1412a,c. This reaction, as with other reactions of pinacol allylboronates, was relatively slow and required 24-48 h at room temperature to reach completion. It was, however, extremely selective ana provided homoallyl alcohol 15 in 70% yield with greater than 95% diastereoselectivity. The stereochemistiy of this compound was quickly verified by conversion to 3 as shown in Figure 7.3a We now believe that this reaction proceeds by way of the Conforth-like transition state depicted in Figure 7, and not by way of a Felkin transition state as suggested in our original ublication, since a serious nonbonded interaction exists between the (Z)-methoxyl group and the C(3) substituents of 13 in the Felkin transition state. A... 

The tandem silylformylation/allylsilylation reaction is particularly well suited to the synthesis of skipped polyol motifs such as are found in the oxopolyene macroHdes. The synthesis of protected triol 43 (an intermediate in the mycoticin A formal synthesis described above see Scheme 5.18) relied on an application of this methodology. Thus, homoallylic alcohol 76 was transformed into triol 77 in 55% overall yield and >10 1 diastereoselectivity (Scheme 5.27) [23]. Selective protection of the triol to give 43... 

Ab initio calculations also confirm that the use of an allyl magnesium alkoxide in place of the alcohol functionality will lead to high or complete stereoselectivity (138). When homoallylic alcohols are used, the Kanemasa protocol afforded the respective isoxazolines with poor stereoselectivity ( 55 45) in the case of terminal aUcenes, but with very high diastereoselectivity (up to 96 4) in the reaction of cis-1,2-disubstituted olefins (136). Extension of this concept to the reaction of a-silyl allyl alcohols also proved feasible and produced the syn (threo) adducts as nearly pure diastereomers (>94 6) (137). Thus, the normal stereoselectivity of the cycloaddition to the Morita-Baylis-Hillman adducts (anti > syn, see above) can be reversed by prior addition of a Grignard reagent (176,177). Both this reversal... 

Reaction of the bis (allyl) titanium complexes -16 with saturated and unsaturated aldehydes at -78 °C in the presence of 1.1 equiv of ClTi(OiPr)3 afforded the corresponding Z-anti-configured homoallyl alcohols 4 with >98% regioselectivity and >98% diastereoselectivity in good yields (Scheme 1.3.6) [14]. 

The treatment of the lithiated allyl sulfoximines E-15 with 1.1-1.2 equiv of ClTi(NEt2)3 at -78 to 0°C in THF or ether afforded the corresponding mono (allyl) titanium complexes E-19 in practically quantitative yields (Scheme 1.3.7) [14, 16]. Similarly the Z-configured complexes Z-19 were obtained from the Z-configured allyl sulfoximines Z-15. Reaction of the titanium complexes E-19 with aldehydes at -78 °C took place at the a-position and gave the corresponding homoallyl alcohols 6 with >98% diastereoselectivity in medium to good yields (Scheme 1.3.8) [14, 16]. 

However, a more detailed study of the reaction of the mono(allyl)titanium complexes -19 carrying different alkyl groups at the double bond with different aldehydes revealed in some cases the highly diastereoselective (>98%) formation of significant amounts of the isomeric homoallyl alcohols 4 besides 6 (Table 1.3.1). 

As one might expect, the diastereoselectivities with homoallylic alcohols are quite substrate-dependent. One successful example involves the cyclopropanation of allyl silanes which could be cyclopropanated with a high level of diastereocontrol (equations 65 and 66). 

---