Stereoselectivity anions

Zheng, Z. Knobler. C.B. Hawthorne. M.F. Stereoselective anion template effects Syntheses and molecular structures of tetraphenyl [12]mercuracarborand-4 complexes of halide ions. J. Am. Chem. Soc. 1995. 117 (18), 5105-5113. 

Differentiation of the prochiral cyclopentadienyl system in 310 by intramolecular AHR generates 7r-allylpalladium 312, which was trapped intermolecularly with the malonate 311 in regio- and stereoselective maimer to provide the bicyclic system 313 with 87 % ee in the presence of NaBr in DMSO. The regio- and stereoselective anion capture can be understood by considering the steric effect as shown by 312. The total synthesis of c nellene 314 has been achieved from 313 [128],... 

Very recently, we have disclosed the stereoselective anionic polymerization of dibutylamino-substituted masked disilenes 1 [12]. The stereochemistry of the polymers is analyzed based on diad and triad sequences. Under the appropriate conditions, the polymerization produced a polymer rich in syndiotacticity up to 89 % in diad. Typical examples of the analysis are shown in Table 2. A high r content in the diad tacticity as well as a high rr fraction in the triad tacticity indicates clearly that the polysilane is rich in syndiotacticity. 

A transannular ene-reaction was featured in the reaction cascade that was used by Paquette and co-workers in their synthesis of the [5.9.5] tricyclic diterpenes jatrophatrione and citlalitrione. This reaction cascade involved initiating the stereoselective anionic oxy-Cope reaction of 43 by treatment with KOf-Bu and 18-crown-6 followed by trapping the enolate 44 with methyl iodide to give intermediate 45 (Scheme 20.13). This was followed by the spontaneous transannular ene-reaction to give 46 in 70% overall yield. It was converted to jatrophatrione and citMitrione after additional transformations. 

If alkyl groups are attached to the ylide carbon atom, cis-olefins are formed at low temperatures with stereoselectivity up to 98Vo. Sodium bis(trimethylsilyl)amide is a recommended base for this purpose. Electron withdrawing groups at the ylide carbon atom give rise to trans-stereoselectivity. If the carbon atom is connected with a polyene, mixtures of cis- and rrans-alkenes are formed. The trans-olefin is also stereoseiectively produced when phosphonate diester a-carbanions are used, because the elimination of a phosphate ester anion is slow (W.S. Wadsworth, 1977). 

A classical reaction leading to 1,4-difunctional compounds is the nucleophilic substitution of the bromine of cf-bromo carbonyl compounds (a -synthons) with enolate type anions (d -synthons). Regio- and stereoselectivities, which can be achieved by an appropiate choice of the enol component, are similar to those described in the previous section. Just one example of a highly functionalized product (W.L. Meyer, 1963) is given. 

Silyl ethers serve as preeursors of nucleophiles and liberate a nucleophilic alkoxide by desilylation with a chloride anion generated from CCI4 under the reaction conditions described before[124]. Rapid intramolecular stereoselective reaction of an alcohol with a vinyloxirane has been observed in dichloro-methane when an alkoxide is generated by desilylation of the silyl ether 340 with TBAF. The cis- and tru/u-pyranopyran systems 341 and 342 can be prepared selectively from the trans- and c/.y-epoxides 340, respectively. The reaction is applicable to the preparation of 1,2-diol systems[209]. The method is useful for the enantioselective synthesis of the AB ring fragment of gambier-toxin[210]. Similarly, tributyltin alkoxides as nucleophiles are used for the preparation of allyl alkyl ethers[211]. 

Carboxylate anions are better nucleophiles for allylation. The monoepoxide of cyclopentadiene 343 is attacked by AcOH regio- and stereoselectively via tt-aliylpalladium complex formation to give the m-3,5-disubstituted cyclopen-tene 344[212]. The attacks of both the Pd and the acetoxy anion proceed by inversion (overall retention) to give the cis product. 

Meyers has demonstrated that chiral oxazolines derived from valine or rert-leucine are also effective auxiliaries for asymmetric additions to naphthalene. These chiral oxazolines (39 and 40) are more readily available than the methoxymethyl substituted compounds (3) described above but provide comparable yields and stereoselectivities in the tandem alkylation reactions. For example, addition of -butyllithium to naphthyl oxazoline 39 followed by treatment of the resulting anion with iodomethane afforded 41 in 99% yield as a 99 1 mixture of diastereomers. The identical transformation of valine derived substrate 40 led to a 97% yield of 42 with 94% de. As described above, sequential treatment of the oxazoline products 41 and 42 with MeOTf, NaBKi and aqueous oxalic acid afforded aldehydes 43 in > 98% ee and 90% ee, respectively. These experiments demonstrate that a chelating (methoxymethyl) group is not necessary for reactions to proceed with high asymmetric induction. 

The foregoing examples do not represent useful chiral formyl anion equivalents in a direct sense since the stereoselectivity of the initial addition to aldehydes is poor, although as has been explained, the situation is salvaged by oxidation and re-reduction. On the other hand, by lithiation at the 2 position of the achiral oxazo-lidine 53 in the presence of (-)-sparteine followed by addition of benzaldehyde, useful levels of d.e. and e.e. are achieved directly (98TA3125). For example, by adding MgBr2 before the benzaldehyde, the major product obtained is 54 in 80% d.e. and 86% e.e. 

There has been recent interest in naphtho-fused dithiepines as chiral acyl anion equivalents, particularly since the starting dithiol 128 can be obtained in enan-tiomerically pure form (89TL2575). This is transformed using standard methods into the dithiepine 129, but showed only moderate diastereoselectivity in its addition to carbonyl compounds. On the other hand, as we have seen previously for other systems, formation of the 2-acyl compound 130 and reduction or addition of a Grignard reagent gave the products 131 with much better stereoselectivity (91JOC4467). 

The elaboration of the polyunsaturated side chain of asteltoxin requires a stereoselective coupling of aldehyde 2 with a suitable synthetic equivalent for the anion of 4-formyl-1,3-butadiene (see intermediate 3 in Scheme 4). Acid-induced skeletal reorganization of the aldehyde addition product, followed by an intermolecular... 

The strategy for the construction of 13 from aldehyde 16 with two units of phosphonate 15 is summarized in Scheme 12. As expected, aldehyde 16 condenses smoothly with the anion derived from 15 to give, as the major product, the corresponding E,E,E-tri-ene ester. Reduction of the latter substance to the corresponding primary alcohol with Dibal-H, followed by oxidation with MnC>2, then furnishes aldehyde 60 in 86 % overall yield. Reiteration of this tactic and a simple deprotection step completes the synthesis of the desired intermediate 13 in good overall yield and with excellent stereoselectivity. 

Florio et al. demonstrated that the lithiation/electrophile trapping of enantio-pure styrene oxide, as well as the (3-substituted styrene oxides 180 and 182, is totally stereoselective (Scheme 5.42) [66]. These results demonstrate that the intermediate benzylic anions are configurationally stable within the timescale of depro-tonation/electrophile trapping. 

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