Enantiomeric boranes

Among chiral dialkylboranes, diisopinocampheylborane (8) is the most important and best-studied asymmetric hydroborating agent. It is obtained in both enantiomeric forms from naturally occurring a-pinene. Several procedures for its synthesis have been developed (151—153). The most convenient one, providing product of essentially 100% ee, involves the hydroboration of a-pinene with borane—dimethyl sulfide in tetrahydrofuran (154). Other chiral dialkylboranes derived from terpenes, eg, 2- and 3-carene (155), limonene (156), and longifolene (157,158), can also be prepared by controlled hydroboration. A more tedious approach to chiral dialkylboranes is based on the resolution of racemates. /n j -2,5-Dimethylborolane, which shows excellent enantioselectivity in the hydroboration of all principal classes of prochiral alkenes except 1,1-disubstituted terminal double bonds, has been... 

The milder metal hydnde reagents are also used in stereoselective reductions Inclusion complexes of amine-borane reagent with cyclodexnins reduce ketones to opucally active alcohols, sometimes in modest enantiomeric excess [59] (equation 48). Diisobutylaluminum hydride modified by zmc bromide-MMA. A -tetra-methylethylenediamme (TMEDA) reduces a,a-difluoro-[i-hydroxy ketones to give predominantly erythro-2,2-difluoro-l,3-diols [60] (equation 49). The three isomers are formed on reduction with aluminum isopropoxide... 

When /V-arenesulfonyl-a-amino acid derived boranes 13 and 14 are used in substoichiometric amounts in order to mediate enantioselective aldol additions of a,a-dimethyl substituted ketcnc acetal 15, /J-hydroxycarboxylic esters 16 are obtained in enantiomeric excess of 84 to > 99 %3fi. 

Alkyldimethylphosphine-boranes 74 underwent enantioselective deprotonation employing (-)-sparteine/s-BuLi, followed by oxidation with molecular oxygen [91, 92] in the presence of triethyl phosphite (Scheme 12) to afford moderate yields of enantiomerically enriched alkyl(hydroxymethyl)methylphosphine-bo-ranes 76, with 91-93% ee in the case of a bulky alkyl group and 75-81% ee in the case of cyclohexyl or phenyl groups [93]. Except for the adamantyl derivative (in which the ee increased to 99%), no major improvement in the ee was observed after recrystallization. 

The same phosphine-borane used for the synthesis of BisP acted as the starting materials of the construction of MiniPHOS, the next smaller analogue to BisP (Scheme 13). The chirally induced lithium salt was treated with alkylphos-phorus dichloride, methylmagnesium bromide, and borane-THF complex to afford enantiomerically pure MiniPHOS-borane 82a. Recrystallization enabled elimination of a small amount of corresponding raeso-diastereomer formed [29]. Yields were generally low, ranging from 13 to 28%. 

We further synthesized unsymmetrical MiniPHOS derivatives 13b (Scheme 13) [30]. Thus, enantioselective deprotonation of l-adamantyl(dimethyl)phos-phine-borane (74, R = 1 -Ad), followed by treatment with ferf-butyldichlorophos-phine or 1-adamantyldichlorophosphine, methylmagnesium bromide and bo-rane-THF complex afforded the optically active diphosphine-boranes 82b as a mixture with the corresponding raeso-diastereomer. Enantiomerically pure unsymmetrical MiniPHOS-boranes 82b were obtained by column chromatography on silica gel or separation by recycling preparative HPLC. 

Similarly to the P-CHj group, secondary phosphine-boranes react smoothly in the presence of a base (BuLi, NaH) under mild conditions to afford other kinds of functionalized phosphine-boranes in good to high yields, without racemi-zation. Yet the success of deprotonation/treatment with an electrophile process to afford substituted phosphine derivatives without any loss in optical purity may depend on the deprotonation agents employed. Use of butyllithium usually provides the products with high enantiomeric excess in good to high yields [73]. 

P-Chirogenic diphosphine 19, which rhodium-chelate complex forms a seven-membered ring (rare case for P-stereogenic ligand), was also prepared in reasonable yield (68%) using the wide chemistry of secondary phosphine borane [37]. Deprotonation of the enantiomerically enriched ferf-butylmethylphos-phine-borane 88 (Scheme 15) followed by quenching with a,a -dichloro-o-xylene and recrystallization afforded optically active diphosphine-borane 89 (precursor of free phosphine 19). 

As mentioned in Sect. 2.2, phosphine oxides are air-stable compounds, making their use in the field of asymmetric catalysis convenient. Moreover, they present electronic properties very different from the corresponding free phosphines and thus may be employed in different types of enantioselective reactions, m-Chloroperbenzoic acid (m-CPBA) has been showed to be a powerful reagent for the stereospecific oxidation of enantiomerically pure P-chirogenic phos-phine-boranes [98], affording R,R)-97 from Ad-BisP 6 (Scheme 18) [99]. The synthesis of R,R)-98 and (S,S)-99, which possess a f-Bu substituent, differs from the precedent in that deboranation precedes oxidation with hydrogen peroxide to yield the corresponding enantiomerically pure diphosphine oxides (Scheme 18) [99]. 

Several alkylboranes are available in enantiomerically enriched or pure form and can be used to prepare enantiomerically enriched alcohols and other compounds available via organoborane intermediates.196 One route to enantiopure boranes is by hydroboration of readily available terpenes that occur naturally in enantiomerically enriched or pure form. The most thoroughly investigated of these is bis-(isopinocampheyl)borane (Ipc)2BH), which can be prepared in 100% enantiomeric purity from the readily available terpene a-pinene.197 Both enantiomers are available. 

Monoisocampheylborane (IpcBH2) can be prepared in enantiomerically pure form by purification of a TMEDA adduct.202 When this monoalkylborane reacts with a prochiral alkene, one of the diastereomeric products is normally formed in excess and can be obtained in high enantiomeric purity by an appropriate separation.203 Oxidation of the borane then provides the corresponding alcohol having the enantiomeric purity achieved for the borane. 

The trialkylborane can be transformed to a dialkyl(ethoxy)borane by heating with acetaldehyde, which releases the original chiral a-pinene. Finally application of one of the carbonylation procedures outlined in Scheme 9.1 gives a chiral ketone.17 The enantiomeric excess observed for ketones prepared in this way ranges from 60-90%. 

The allylation reaction has been extended to enantiomerically pure allylic boranes and borinates. For example, the 3-methyl-2-butenyl derivative of (Ipc)2BH reacts with aldehydes to give carbinols of greater than 90% e.e. in most cases.39... 

P-Allyl-to-(isopinocampheyl)borane exhibits high stereoselectivity in reactions with chiral a-substituted aldehydes.40 The stereoselectivity is reagent controlled, in that there is no change in stereoselectivity between the two enantiomeric boranes in reaction with a chiral aldehyde. Rather, the configuration of the product is determined by the borane. Both enantiomers of (Ipc)2BH are available, so either enantiomer can be prepared from a given aldehyde. 

Show how the following compounds could be prepared in high enantiomeric purity using enantiopure boranes as reactants. 

Treatment of the optically active gem-borazirconocene alkanes with deuterium oxide followed by alkaline oxidation affords the corresponding optically active 1-deuterio primary alcohols. The enantiomeric excess of the resulting primary alcohols represents the diaster-eoselectivity of the asymmetric hydrozirconation (Scheme 7.13). Based on the cost and availability of optically active ligands, three types were explored monoterpenes, 1,2-diols, and 1,2-amino alcohols. Hydrozirconation of optically pure 1-alkenyl boranes 39 provided optically active 1,1-bimetallics 40. 

Nonmetallic systems (Chapter 11) are efficient for catalytic reduction and are complementary to the metallic catalytic methods. For example lithium aluminium hydride, sodium borohydride and borane-tetrahydrofuran have been modified with enantiomerically pure ligands161. Among those catalysts, the chirally modified boron complexes have received increased interest. Several ligands, such as amino alcohols[7], phosphino alcohols18 91 and hydroxysulfoximines[10], com-plexed with the borane, have been found to be selective reducing agents. 

In 1969, Fiaud and Kagan[U1 tested ephedrine boranes but achieved only 3.6-5% enantiomeric excess in the reduction of acetophenone. Itsuno et a/.[121 reported in 1981 an interesting enantioselective reduction of a ketone using an amino alcohol-borane complex as a catalyst. Buono[131 investigated and developed the reactivity of phosphorus compounds as ligands in borane complexes for asymmetric hydrogenation. 

To obtain a good enantiomeric excess, the ligand synthesis and the reduction reaction need to be carried out under strictly anhydrous conditions. The addition of the substrate needs to be as slow as possible. Table 11.3 gives some examples of the different substrates that can be reduced by the hydro-xysulfoximine-borane catalyst described. Other examples are given in the comparative Table 11.4. Concerning the synthesis of the catalyst, the yield can dramatically decrease if the reaction conditions are not strictly anhydrous. 

This procedure has been developed through the evaluation of several reaction parameters (catalyst, temperature, borane source, additives) and has been successfully used on large scale. The chemical purity of the product is excellent and the enantiomeric purity of the product can be increased by crystallizing from toluene/heptane. 

Fig. 2.1-20. Valence bond structure of the calculated ground state for n/ do-tetra-borane(8) and a suggested mechanism for the enantiomerization of B4H3R4- (R = H or alkyl).

In the asymmetric reduction of ketones, stereodifferentiation has been explained in terms of the steric recognition of two substituents on the prochiral carbon by chirally modified reducing agents40. Enantiomeric excesses for the reduction of dialkyl ketones, therefore, are low because of the little differences in the bulkiness of the two alkyl groups40. In the reduction of ketoxime ethers, however, the prochiral carbon atom does not play a central role for the stereoselectivity, and dialkyl ketoxime ethers are reduced in the same enantiomeric excess as are aryl alkyl ketoxime ethers. Reduction of the oxime benzyl ethers of (E)- and (Z)-2-octanone with borane in THF and the chiral auxiliary (1 R,2S) 26 gave (S)- and (R)-2-aminooctane in 80 and 79% ee, respectively39. 

Reduction of a, -acetylenic ketones with chiral borane NB-Enanthrane prepared by addition of 9-borabicyclo[3.3.1]nonane to the benzyl ether of nopol yielded optically active acetylenic alcohols in 74-84% yields and 91-96% enantiomeric excess [770]. Another way to optically active acetylenic alcohols is reduction with a reagent prepared from lithium aluminum hydride and (2S, 3R)-( -I- )-4-dimethylamino-3-methy 1-1,2-dipheny 1-2-butanol. At —78° mainly R alcohols were obtained in 62-99% yield and 34-90% enantiomeric excesses [893]. 

The reaction of 7-oxabenzonorbomadiene 95 with (-)-diisopinocamphenyl-borane (96) gave the corresponding trialkylborane which, on treatment with acetaldehyde, followed by oxidation with H202/Na0H, afforded (+)-(lR,2S,4R)-7-oxabenzonorbom-5-en-2-exo-ol (97) in 80 % yield and 100 % enantiomeric purity. ... 

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