Reduction stereoselective synthesis

Despite the progress made in the stereoselective synthesis of (R)-pantothenic acid since the mid-1980s, the commercial chemical synthesis still involves resolution of racemic pantolactone. Recent (ca 1997) synthetic efforts have been directed toward developing a method for enantioselective synthesis of (R)-pantolactone by either chemical or microbial reduction of ketopantolactone. Microbial reduction of ketopantolactone is a promising area for future research. 

Solanesol and other prenyl alcohols are important as metabolites in mulberry and tobacco leaves and in the synthesis of isoprenoid quinones. Hence, Sato and collaborators107 have developed a stereoselective synthesis of all-trans-polyprenol alcohols up to C50. Construction of the requisite skeletons was accomplished by the alkylation of a p-toluenesulphonyl-stabilized carbanion, followed by reductive desulphonylation of the resulting allylic sulphonyl group. This was achieved most efficiently by the use of a large excess of lithium metal in ethylamine (equation (43)), although all reaction conditions led to mixtures. The minor product results from double bond rearrangement. 

These topics are discussed in more detail in other chapters of this text. Formally, the pyrolytic elimination of sulphur dioxide from a sulphone, with the concomitant formation of a new carbon-carbon bond, constitutes a reduction at sulphur. These reductions have been valuable in the formation of new molecules, especially macrocycles and cyclophanes, and have been reviewed by Vogtle and Rossa205. Pyrolytic elimination of sulphur dioxide has been used by Julia and co workers in the formation of mixtures of isoprenoids206, and by Takayama and collaborators in the stereoselective synthesis of vitamin D, 19-alkanoic acids207. 

This procedure illustrates a general method for the stereoselective synthesis of ( P)-disubstitnted alkenyl alcohols. The reductive elimination of cyclic /3-halo-ethers with metals was first introduced by Paul3 and one example, the conversion of tetrahydrofurfuryl chloride [2-(chloromethyl)tetrahydrofuran] to 4-penten-l-ol, is described in an earlier volume of this series.4 In 1947 Paul and Riobe5 prepared 4-nonen-l-ol by this method, and the general method has subsequently been applied to obtain alkenyl alcohols with other substitution patterns.2,6-8 (I )-4-Hexen-l-ol has been prepared by this method9 and in lower yield by an analogous reaction with 3-bromo-2-methyltetra-hydropyran.10... 

Kaneko C., Katagiri N., Nomura M., Sato H. A New Method for the Stereoselective Synthesis of Nucleosides by Means of Sodium Borohydride Mediated Reductive C-C or C-N Bond Cleavage Reaction Isr. J. Chem. 1991 31 247-259 Keywords carbohydrates... 

There can be significant differences in the rates of elimination of the stereoiso-meric (3-hydroxysilanes. Van Vranken and co-workers took advantage of such a situation to achieve a highly stereoselective synthesis of a styryl terpene. (The lithiated reactant is prepared by reductive lithiation see p. 625). The syn adduct decomposes rapidly at -78° C but because of steric effects, the anti isomer remains unreacted. Acidification then promotes anti elimination to the desired /i-isomer.275... 

Since the seminal contributions by Nugent and RajanBabu the field of reductive C - C bond formation after epoxide opening via electron transfer has developed at a rapid pace. Novel catalytic methodology, enantio- and stereoselective synthesis and numerous applications in the preparation of biologically active substances and natural products have evolved. In brief, a large repertoire of useful and original reactions is available. These reactions are waiting to be applied in a complex context ... 

An intramolecular nitrone 1,3-dipolar cycloaddition reaction to give 46 from 45 followed by reductive N-O bond cleavage afforded a stereoselective synthesis of the tetrahydro 177-1-benzazepines 47 the nitrone precursors 44 were prepared in turn by a Claisen rearrangement from an IV-allylamine <06SL2275>. 

Scheme 4.40 Stereoselective synthesis ofcholesteryl allene 154 by LiAIH4 reduction.

Scheme 4.41 Stereoselective synthesis of camphor-based allenes byAIH3 reduction.

A stereoselective synthesis of the enantiomerically enriched allenic hydrocarbons was described in 2001 (Scheme 18.11) [37]. For example, hydrostannylation of the chiral propargylic alcohol 28 (obtained with 82% ee by enantioselective reduction of... 

Complex hydrides have been used rather frequently for the conjugate reduction of activated dienes92-95. Just and coworkers92 found that the reduction of a,ft-unsaturated ketene 5,5-acetals with lithium triethylborohydride provided mixtures of 1,4- and 1,6-reduction products which were transformed into enals by treatment with mercuric salts (equation 27). Likewise, tetrahydro-3//-naphthalen-2-ones can be reduced with L-Selectride to the 1,6-reduction products93 -95 this reaction has been utilized in the stereoselective synthesis of several terpenes, e.g. of (/ )-(—)-ligularenolide (equation 28)95. Other methods for the conjugate reduction of acceptor-substituted dienes involve the use of methylcopper/diisobutylaluminum hydride96 and of the Hantzsch ester... 

Several catalysts are used in the field of microbial reductions. The common features of these catalysts are the high selectivity and their use only on a laboratorial scale. They are applied, for example, in the stereoselective synthesis of pharmaceutical intermediates. The reductions are exclusively selective either in the hydrogenation of the C=C double bond or in that of other reducible groups. One of the most widely used catalysts is baker s yeast. In the following hydrogenations, which are catalyzed by Saccharomyces cerevisiae, high enantioselectivities were achieved (equations 35-38)105-108. 

The stereoselective synthesis of tetrahydronaphthalenones was carried out via homogeneous hydrogenation. The reduction at 2 bar hydrogen pressure gave the saturated product in good yield (equation 69)165. 

Another stereoselective synthesis (Scheme 11) is based on sugar aldehyde 35 and intermediate 36 subsequent 1,2-O-isopropylidine deprotection, N,0-debenzylation/olefin reduction/reductive cyclization in a single pot, and O-acetylation result in the formation of bicyclic aza sugar 37 (09TA1217). 

Acid treatment of a 3 1 mixture of murrayafoline A (7) and koenoline (8) led to chrestifoline A (192) in 70% yield. Addition of murrayafoline A (7) to a mixture of 1057 and lithium aluminum hydride in ether and dichloromethane afforded bismurrayafoline-A (197) in 19% yield (662) (Scheme 5.166). In addition to the aforementioned methods, the same group also reported a stereoselective synthesis of axially chiral bis-carbazole alkaloids by application of their "lactone concept" (663) and a reductive biaryl coupling leading to 2,2 -bis-carbazoles (664). 

In addition, stereoselective synthesis of solenopsin A has been reported by four research groups. An approach utilizing the stereoselective reductive de-cyanation (596) starts with aminonitrile 229, prepared from 2-picoline. It was selectively hydrogenated in the presence of Pd-C, followed by alkylation with undecyl bromide, affording 231. Reductive decyanation of 231 with NaBH4 in MeOH led to predominant (8 2) formation of the trans isomer (232) which was then debenzylated to ( )-solenopsin A (Id). The cis product (Ic) was in turn prepared by treatment of 231 with sodium in liquid ammonia followed by de-benzylation (Scheme 10). 

Strategies centered on reductive introduction of the fluoroolefin via a geminal difluoro allylic array have been reviewed [66]. In an introductory example to this synthetic approach, Okada et al. [67] developed a completely stereoselective synthesis of Z)-2,5-syn 2-alkyl-4-fluoro-5-hydroxy-3-alkenoic acids through the Cu(l)-mediated allylic substitution reaction of trialkylaluminum with the (E)-4,4-difluoro-5-hydroxyallylic alcohol derivative (61) (Scheme 21). Reaction... 

S. Sano, K. Saito, Y. Nagao, Tandem reduction-olefination for the stereoselective synthesis of (Z)-ot-fluoro-ot, -unsaturated esters. Tetrahedron Lett. 44 (2003) 3987-3990. 

The other stereoselective synthesis/281 shown in Scheme 8, foresees conversion of Boc-L-Asp-OtBu 20 into the related (3-aldehyde 22 via the Weinreb amide 21 and its reduction with diisobutylaluminum hydride (DIBAL-H). Wittig condensation of 22 with the ylide derived from (3-carboxypropyl)triphenylphosphonium bromide using lithium hexamethyldisilaza-nide at —78 to 0°C, produces the unsaturated compound 23 which is catalytically hydrogenated to the protected L-a-aminosuberic acid derivative 24. Conversion of the co-carboxy group into the 9-fluorenylmethyl ester, followed by TFA treatment and reprotection of the M -amino group affords Boc-L-Asu(OFm)-OH (25). 

Highly enantioenriched 4-alken-l-yn-3-ol moieties present in many bioactive acetylenic metabolites from sponges have been efficiently obtained by reduction of the parent 1-trimethylsilyI-4-alken-l-yn-3-one 18 with Alpine-borane or with BH3-SMe2 in the presence of chiral oxazaborolidines, followed by desilylation of the resulting alcohol. This strategy has been applied to the first stereoselective synthesis of petrofuran 19 <99SL429>. 

M. Tramontini, Synthesis 1982, 605-644 . .Stereoselective Synthesis of Diastereomeric Amino Alcohols from Chiral Aminocarbonyl Compounds by Reduction or by Addition of Organometallic Reagents". 

The enzyme-catalyzed regio- and enantioselective reduction of a- and/or y-alkyl-substituted p,5-diketo ester derivatives would enable the simultaneous introduction of up to four stereogenic centers into the molecule by two consecutive reduction steps through dynamic kinetic resolution with a theoretical maximum yield of 100%. Although the dynamic kinetic resolution of a-substituted P-keto esters by chemical [14] or biocatalytic [15] reduction has proven broad applicability in stereoselective synthesis, the corresponding dynamic kinetic resolution of 2-substituted 1,3-diketones is rarely found in the literature [16]. 

A HIGHLY STEREOSELECTIVE SYNTHESIS OF 3a-AMINO-23,24-BISNOR-5a-CHOLANE VIA REDUCTIVE AMINATION... 

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