Stannanes reactions with acetals

The Stille reaction has been successfully applied to a number of macrocyclic ring closures.207 In a synthesis of amphidinolide A, the two major fragments were coupled via a selective Stille reaction, presumably governed by steric factors. After deprotection the ring was closed by coupling the second vinyl stannane group with an allylic acetate.208... 

The product possesses a homoallylic stannane moiety, which can be utilized as a useful synthon for cyclopropane formation (Scheme 68). Upon treatment of the homoallylstannane with HI, destannative cyclization takes place to give cyclopropylmethylsilane.271,272 A Lewis acid-catalyzed reaction with benzaldehyde dimethyl acetal affords vinylcyclopropane.273... 

Crich and Rumthao reported a new synthesis of carbazomycin B using a benzeneselenol-catalyzed, stannane-mediated addition of an aryl radical to the functionalized iodocarbamate 835, followed by cyclization and dehydrogenative aromatization (622). The iodocarbamate 835 required for the key radical reaction was obtained from the nitrophenol 784 (609) (see Scheme 5.85). lodination of 784, followed by acetylation, afforded 3,4-dimethyl-6-iodo-2-methoxy-5-nitrophenyl acetate 834. Reduction of 834 with iron and ferric chloride in acetic acid, followed by reaction with methyl chloroformate, led to the iodocarbamate 835. Reaction of 835 and diphenyl diselenide in refluxing benzene with tributyltin hydride and azobisisobutyronitrile (AIBN) gave the adduct 836 in 40% yield, along with 8% of the recovered substrate and 12% of the deiodinated carbamate 837. Treatment of 836 with phenylselenenyl bromide in dichloromethane afforded the phenylselenenyltetrahydrocarbazole 838. Oxidative... 

In the presence of Lewis acids allyl silanes and stannanes react with epoxides generally at the sterically less demanding carbon atom. Other electron-rich alkenes, such as ketene acetals, can also be used as nucleophiles. The strong Lewis acids required might, however, also lead to rearrangement of the epoxide before addition of the nucleophile can occur (last reaction, Scheme 4.72). 

Analogous to the allylation with allylsilanes and -stannanes, the transformations, vinylallylation, propargylation, allenylation, alkenylation, alkynylation, and arylation, are viable by the use of an appropriate reagent in the presence of a titanium Lewis acid these are surveyed in the review articles cited both in the Introduction and in this section. The stereochemistry of the reaction of a (vinylallyl)silane in the presence of TiCU has been reported [234]. Equation (113) shows that the major reaction of this silane and isobutyraldehyde occurred mainly in the anti sense with a ratio of anti to syn attack of 90 10 at the terminus remote from the silyl group. Essentially the same stereochemical outcome was observed for the same reaction with the corresponding trimethylsilyl derivative. The intramolecular reaction with an acetal, however, proceeded less selectively the anti syn ratio was 60 40 (Eq. 114) [234]. 

Allenylsilanes and -stannanes combined with a titanium salt are versatile reagents for propargylation of aldehydes (Eq. 115) [297], ketones (Eq. 116) [298], (A,0)-acetals (Eq. 117) [299], and a,/ -unsaturated ketones in a conjugate fashion (Eq. 118) [300]. Intramolecular reaction has also been reported (Eq. 119) [301] in which a Bu3Sn-carbon bond was cleaved exclusively in the presence of a TBS-carbon bond. That the isomeric starting material, propargylstannane, did not give the desired product (Eq. 120) demonstrates that the direct scission of the carbon-Sn bond by the electrophile under these reaction conditions is not a feasible path [301]. 

Much more promising and synthetically versatile is the use of the bifunctional acetal stan-nane12. In this case, both reactive centers are activated under the same conditions and lead to clean [3 + 2] reactions with silyl enol ethers. The acetal stannane is readily available by Gri-gnard reaction of trimethylchlorostannane with the corresponding bromoacetal to afford the product in 76% yield. 

Enol stannanes of cyclohexanone and propiophenone have been indicated to take part in r/treo-selective aldol reactions with benzaldehyde at low temperatures e.g. —78 °C), but to be erythro-seAsciiwe at higher temperatures ca 45 °C). Two complementary methods have been described for stereoselection in aldol-type reactions. Whilst a-mercurio-ketones show eryr/wo-selection in their reactions with aldehydes in the presence of boron trifluoride diethyl etherate, pre-formed lithium enolates and aldehydes, in the presence of simple trialkyl-boranes, lead to mixtures that are rich in the more stable threo-d do product. Aldol-type products arise from 1,3-alkyl migrations of alk-l-enyl alkyl acetals and ketals, in a reaction that is catalysed by boron trifluoride diethyl etherate (Scheme 52). Diastereoselection is possible, since (.E)-alkenyl acetals give the... 

Addition of tributylstannyl-lithium to crotonaldehyde and protection of the resulting alcohol with chloromethyl methyl ether gives the stannane (192), which reacts with both alkyl and aryl aldehydes RCHO to form specifically the t/rr o-hydroxy-enol ethers (193). These latter compounds have been used to prepare tra/i5-4,5-disubstituted butyrolactones by hydrolysis and subsequent oxidation. Palladium-catalysed carbonylation of RX in the presence of organotin species constitutes a useful synthesis of unsymmetrical ketones, and in the example reported this year RX is an arenediazonium salt. The reaction, which is basically an aromatic acylation, proceeds in good to excellent yield. Another Pd-catalysed reaction of aromatics, this time aryl bromides, is their reaction with acetonyltributyltin (194), prepared from methoxytributyltin and isopropenyl acetate, to give the arylacetones (195). ... 

Dialkoxydialkyl stannanes cross-couple with derivatives of chiral tartaric acid, preserving the original chirality, as shown in reaction 32. The dialkylstannylene acetals produced in this reaction are useful reagents for synthesis of chiral compounds28611. 

Two important classes of reactions use labelled tin compounds to prepare labelled compounds for mechanistic and analytical purposes. In the first type of reaction, labelled trialkyl- or triaryl tin hydrides (stannanes) are used to reduce (replace) several different groups such as halogen, —N02, —N=C, —N=C=Se, —COOR, —SR or an acetal group with a deuterium or a tritium atom. 

Alkylation of allylic acetates. Rcgioselccti ve monoalkylation of allylic acetates is possible by use of enol stannanes (prepared by reaction of lithium enolates with chlorotri-n-butyltin) in the presence of this Pd complex. The less substituted end of the allyl group is alkylated with formation of the (E)-isomer.4 Examples ... 

Initial reports on the use of simple enolates as nucleophiles in TT-allylpalladium chemistry met with only limited success.77 106 The enolate of acetophenone reacted with allyl acetate in the presence of Pd(PPh3)4, but gave predominantly dialkylated product.106 The use of the enol silyl ether of acetophenone gave only monoalkylated product with allyl acetate and Pd° catalysis, but substituted allyl acetates did not function in this reaction.106 Enol stannanes, however, have been found to give monoalkylated products with a wide variety of allyl acetates (equation 19).106 In situ generation of enol stannanes from lithium enolates and trialkylstannyl trifluoroacetates followed by Pd°-catalyzed allylation has been demonstrated.107... 

Yamamoto has recently described a novel catalytic, asymmetric aldol addition reaction of enol stannanes 19 and 21 with aldehydes (Eqs. 8B2.6 and 8B2.7) [14]. The stannyl ketones are prepared solvent-free by treatment of the corresponding enol acetates with tributyltin methoxide. Although, in general, these enolates are known to exist as mixtures of C- and 0-bound tautomers, it is reported that the mixture may be utilized in the catalytic process. The complexes Yamamoto utilized in this unprecedented process are noteworthy in their novelty as catalysts for catalytic C-C bond-forming reactions. The active complex is generated upon treatment of Ag(OTf) with (R)-BINAP in THF. Under optimal conditions, 10 mol % catalyst 20 effects the addition of enol stannanes with benzaldehyde, hydrocinnamaldehyde, or cinnamaldehyde to give the adducts of acetone, rerf-butyl methyl ketone (pinacolone), and acetophenone in good yields and 41-95% ee (Table 8B2.3). 

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