Alkylation stereocontrolled

Trost, B. M., and T. R. Verhoeven New Synthetic Reactions. Catalytic vs. Stoichiometric Allylic Alkylation. Stereocontrolled Approach to Steroid Side Chain. J. Amer. Chem. Soc. 98, 630 (1976). 

This remarkable alkylation stereocontrol has been exploited in a number of syntheses, including a concise synthesis of homochiral (5,5)-captopril and (S,/ )-epi-captopril. The example given in Protocol 3 is for the key step in the synthesis of (S)-(+)-2-methylhept-4-ynoate 9 (Scheme 4.5), the sidechain of prostacyclin. ... 

Lavilla et al. have reported several stereocontrolled oxidative electrophilic additions to A-alkyl-l,4-dihydropyridines 34 leading to the synthesis of 3-halo-2-substituted-l,2,3,4-tetrahydropyridines 67 (98JOC2728). Adding a stoichiometric amount of iodine or NIS (A-iodosuccinimide) to a methanolic solution of 1 -methy 1-... 

An important task remaining is the stereocontrolled introduction of a methyl group at C-8. When a cold (-78 °C) solution of 14 in THF is treated successively with LDA and methyl iodide and then warmed to -45 °C, intermediate 24 admixed with minor amounts of the C-8 epimer is formed in a yield of 95 %. The action of LDA on 14 generates a lactone enolate which is alkylated on carbon in a diastereoselective fashion with methyl iodide to give 24. It is of no consequence that 24 is contaminated with small amounts of the unwanted C-8 epimer because hydrolysis of the mixture with lithium hydroxide affords, after Jones oxidation of the secondary alcohol, a single keto acid (13) in an overall yield of 80%. Apparently, the undesired diastereoisomer is epimerized to the desired one under the basic conditions of the saponification step. 

Stereocontrol in the formation of spiroketals has been achieved in the alkylation of 2-(benzenesulfonyl)pyrans with allylsilanes <96JOC7860> and using a double carbonyl cycUsation strategy <96SL1065>. Spirocyclisation of protected dihydroxydiketones yields cis- and trans- l,7,9-trioxadispiro[5.1.5.3]hexadecanes the latter isomer is the thermodynamically more stable <96TL5461>. 

This homoenolate methodology has been extended to the use of nitrones 170 as electrophiles [72]. Scheldt and co-workers have shown that enantiomerically enriched y-amino esters 172 can be prepared with excellent levels of stereocontrol from an enal 27 and a nitrone 170 using the NHC derived from triazolium salt 164 (Scheme 12.37). The oxazinone product 171, formally a result of a [3-1-3] cycloaddition, is cleaved to afford the y-amino ester product 172. The reaction shows broad substrate scope, as a range of substituted aryl nitrones containing electron donating and withdrawing substituents are tolerated, while the enal component is tolerant of both alkyl and aryl substituents. 

The facile isomerization of alkyl and vinyl zirconocenes complicates the stereocontrol in the transformations of internal acyclic aikenes and allenes, and so further studies are certainly needed to circumvent this problem. 

The synthesis in Scheme 13.21 starts with a lactone that is available in enantiomer-ically pure form. It was first subjected to an enolate alkylation that was stereocontrolled by the convex shape of the cis ring junction (Step A). A stereospecific Pd-mediated allylic substitution followed by LiAlH4 reduction generated the first key intermediate (Step B). This compound was oxidized with NaI04, converted to the methyl ester, and subjected to a base-catalyzed conjugation. After oxidation of the primary alcohol to an aldehyde, a Wittig-Horner olefination completed the side chain. 

The first example of an intermolecular radical addihon/intermolecular trapping domino reactions of an acyclic system in a stereocontrolled fashion to build stereo-genic centers at the a- and 3-carbons was described by Sibi and coworkers [59]. Enantioselective addition of in-sitw-prepared alkyl radical to crotonate or cinnamate,... 

Dipolar addition to nitroalkenes provides a useful strategy for synthesis of various heterocycles. The [3+2] reaction of azomethine ylides and alkenes is one of the most useful methods for the preparation of pyrolines. Stereocontrolled synthesis of highly substituted proline esters via [3+2] cycloaddition between IV-methylated azomethine ylides and nitroalkenes has been reported.147 The stereochemistry of 1,3-dipolar cycloaddition of azomethine ylides derived from aromatic aldehydes and L-proline alkyl esters with various nitroalkenes has been reported. Cyclic and acyclic nitroalkenes add to the anti form of the ylide in a highly regioselective manner to give pyrrolizidine derivatives.148... 

Fu and Dosa139 report the enantioselective addition of diphenylzinc to a range of aryl-alkyl and dialkyl ketones with good to excellent stereocontrol. Addition of 1.5 eq. of MeOH in the presence of a catalytic amount of (+)-DAIB 135 results in enhanced enantioselectivity and improved yield (Scheme 2-53). Table 2-16 gives the results of this reaction. 

Typical electrophiles that attack olefins like Br+ (Eq. 64)105) and (OH)+ (Eq. 65) 105) do lead to electrophilic addition with ring enlargement101 a). Most interesting is the ability for electrophiles that normally do not attack olefins to also react. Thus, an oxycarbonium ion generated from an acetal smoothly alkylates the double bond of this composite functional group in an overall highly stereocontrolled 1,1,2-trialkylation of a simple ketone as illustrated in Eq. 66 106). The chemo- and... 

The sequences of spiroannulation-secobromination or, better, spiroannulation-secosulfenylation offer great versatility for geminal alkylation as summarized in Eq. 123. The fact that spiroannulation of carbonyl compounds proceeds with stereocontrol converts these transformations into stereocontrolled carbonyl group elaborations. 

This reaction can also be used for exocyclic intramolecular alkylation of an allylic silane, such as the cyclization of 3 to trarts-4 with complete stereocontrol. 

Aryl and alkenyl groups undergo this anft -migration more easily than an alkyl group. This rearrangement in combination with Sharpless asymmetric epoxidation affords a stereocontrolled route to aldols and 1,3-diols (second example). 

C-Alkylation has also been observed in intramolecular reactions where the O-alkylation is not favoured.76 This property has been recently exploited in a stereocontrolled intramolecular cyclization of nitronate of nitro sugar 101 (Scheme 32), that provided the novel bicyclic nitrolactone 102, a synthetic precursor of tripeptide 103, that includes the first reported polyhydroxylated cyclopentane (3-amino acid.77... 

Toru has investigated the stereoselectivity of the conjugate addition of trialkylboranes to 2-arylsulfinylcyclopentenones. Excellent stereocontrol is achieved with different alkyl radicals (Scheme 27) [73-76]. In the acyclic series, the lack of diastereoselectivity in the addition step and a competitive Pummerer rearrangement have limited the synthetic potential of this reaction [77]. 

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