Subject allyl formate

The idea enabled a domino process by combining copper-catalyzed C-O bond formation and thermal Claisen rearrangement. Subjecting allylic alcohol and vinyl iodide to the reaction conditions led to the clean formation of the desired rearrangement product in 55% yield with high stereochemical purity (Eq. 3.1.15). The preparation of two adjacent quartemary stereocenters from geraniols is successfully prepared using the aforementioned reaction conditions (Eq. 3.1.16). 

Enone formation-aromatization has been used for the synthesis of 7-hydro-xyalkavinone (716)[456]. The isotlavone 717 was prepared by the elimina-tion[457]. The unsaturated 5-keto allyl esters 718 and 719, obtained in two steps from myreene. were subjected to enone formation. The reaction can be carried out even at room temperature using dinitriles such as adiponitrile (720) or 1,6-dicyanohexane as a solvent and a weak ligand to give the pseudo-ionone isomers 721 and 722 without giving an allylated product(458]. 

The allylic position of olefins is subject to attack by free radicals with the consequent formation of stable allylic free radicals. This fact is utilized in many substitution reactions at the allylic position (cf. Chapter 6, Section III). The procedure given here employs f-butyl perbenzoate, which reacts with cuprous ion to liberate /-butoxy radical, the chain reaction initiator. The outcome of the reaction, which has general applicability, is the introduction of a benzoyloxy group in the allylic position. 

As mentioned in an earlier section (cf. Chapter 1, Section III), allylic positions are subject to attack by free radicals resulting in the formation of stable allyl radicals. A-Bromosuccinimide (NBS) in the presence of free-radical initiators liberates bromine radicals and initiates a chain reaction bromination sequence by the abstraction of allylic or benzylic hydrogens. Since NBS is also conveniently handled, and since it is unreactive toward a variety of other functional groups, it is usually the reagent of choice for allylic or benzylic brominations (7). 

Trifluoromethanesulfonates of alkyl and allylic alcohols can be prepared by reaction with trifluoromethanesulfonic anhydride in halogenated solvents in the presence of pyridine.3 Since the preparation of sulfonate esters does not disturb the C—O bond, problems of rearrangement or racemization do not arise in the ester formation step. However, sensitive sulfonate esters, such as allylic systems, may be subject to reversible ionization reactions, so appropriate precautions must be taken to ensure structural and stereochemical integrity. Tertiary alkyl sulfonates are neither as easily prepared nor as stable as those from primary and secondary alcohols. Under the standard preparative conditions, tertiary alcohols are likely to be converted to the corresponding alkene. 

Nucleophilic Substitution of xi-Allyl Palladium Complexes. TT-Allyl palladium species are subject to a number of useful reactions that result in allylation of nucleophiles.114 The reaction can be applied to carbon-carbon bond formation using relatively stable carbanions, such as those derived from malonate esters and (3-sulfonyl esters.115 The TT-allyl complexes are usually generated in situ by reaction of an allylic acetate with a catalytic amount of fefrafcz s-(triphenylphosphine)palladium... 

Asymmetric Allylation. One of the recent new developments on this subject is the asymmetric allylation reaction. It was found that native and trimethylated cyclodextrins (CDs) promote enantiose-lective allylation of 2-cyclohexenone and aldehydes using Zn dust and alkyl halides in 5 1 H2O-THF. Moderately optically active products with ee up to 50% were obtained.188 The results can be rationalized in terms of the formation of inclusion complexes between the substrates and the CDs and of their interaction with the surface of the metal. 

Novel alkenylphosphonium salts were subjected to the Wittig reaction (Scheme 12). Allylic deprotonation took place for phosphonium salts possessing such protons, and the olefination proceeded after double bond migration. In cases where such protons were absent, allene formation was observed. 

Ester-tethered enyne systems cycloisomerized to give lactone products (Eq. 11) [24]. Eor example, enyne 6 reacted under the Alder-ene conditions of [Rh(COD)Cl]2/BlNAP/ AgSbEg to give the corresponding lactone (Eq. 11). Once again free hydroxyl groups on the allylic terminus were incorporated into the cyclization precursors and subjected to the Alder-ene conditions, which led to the exclusive formation of the tautomerized products in good yields and enantioselectivities (Eq. 12). 

In the second approach, allylboronation of 9 with 10 led to the predominant formation of 8a which was transformed to 6a (R = H). The allylic alcohols 5a and 5b prepared from 6a and 6b, respectively, were subjected to asymmetric epoxidations307, each with (-f)-DET and (—)-DET, to provide four diastereomers. One of them, 4b, was identical with degradation product 2. Note that in these reactions double stereodifferenlialion (see Section A.2.3.5.4.) is operating (for configurational assignment at C-15, see p431)244. 

We also discovered the ability of 2-azadienes of this sort to cycloadd to unactivated carbon—carbon double and triple bonds in an intramolecular fashion (89CC267) (Scheme 50) such a process appears to be one of the first examples of intramolecular [4 + 2] cycloadditions of simple 2-azadienes. Azadiene 216 was made from O-allyl salicylaldehyde 215 (R = allyl) and heated at 120°C in toluene to furnish the trans-fused tricyclic adduct 217 in excellent yield further dehydrogenation of 217 with DDQ afforded 5H-[ 1 ]-benzopyran[4,3-6]pyridine 218. On the other hand, when 0-(2-butynyl) salicylaldehyde 215 (R = 2-butynyl) was transformed into azadiene 219 and subjected to heating in a sealed tube at 150°C, pyridine 222 was isolated in very high yield. Its formation can be rationalized to occur via the expected Diels-Alder intermediate 220 thus, [1,5]-H shift in 220 would give rise to tautomer 221, which would suffer electro-cyclic ring-opening and aromatization to pyridine derivative 222. 

The exact mechanism of lattice oxygen incorporation and second hydrogen abstraction, and the precise sequence of elementary events is still a subject of speculation. Several authors assume that two distinct active sites are involved in the acrolein formation. The first, presumably a cation, participates in the formation of the initial allyl complex, while the second, which may contain a different cation and reactive oxygen anions, is the place where further hydrogen abstraction and oxygen incorporation take place. 

The modification of [T-amino acids by a-selenylation and then free radical allylation leads to the formation of (A-amino acids bearing an a-allyl group (Scheme 12). Hanessian and co-workers 22 initially used this approach to produce p2 3-amino acids which were then subjected to suitable coupling procedures. Interestingly, the coupling method chosen made use of PyBOP and hence demonstrates that other peptide coupling procedures can be used in the synthesis of (3-peptides. 

Treatment of ethacrylate esters 1 with nitronium tetrafluoroborate in acetonitrile has been shown to give cyclopropanes 2 and the products of allylic nitration 3. Formation of 2 was postulated to proceed via an a-carbonyl cation. In an attempt to obtain evidence for the possible intermediacy of a-carbonyl cations in these reactions in terms of Wagner-Meerwein derived products, the more highly substituted substrates 4a, b were subjected to the same reaction conditions of NC>2BF4/MeCN followed by aqueous work-up. This gave 5a, b and 6a, b as shown. 

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