Pyrans, unsaturated

Clerodanes involve a (C61C6) group variously linked to furan (unsaturated C40), pyran (unsaturated C50), methyleneoxy and methylenedioxy rings. Clerodanes include bitter tastants and antifeedants as exemplified by the extremely bitter component columbin of the bitter tonic made from roots of Jateorhiza columba (columba root) (Menispermaceae). 

Vinyl ethers and a,P unsaturated carbonyl compounds cyclize in a hetero-Diels-Alder reaction when heated together in an autoclave with small amounts of hydroquinone added to inhibit polymerisation. Acrolein gives 3,4-dihydro-2-methoxy-2JT-pyran (234,235), which can easily be hydrolysed to glutaraldehyde (236) or hydrogenated to 1,5-pentanediol (237). With 2-meth5lene-l,3-dicarbonyl compounds the reaction is nearly quantitative (238). 

Hydroqulnollnes. Pyrans formed by reactions of a,P-unsaturated aldehydes with 1-ethoxycyclohexene and treated with hydroxjiamine are converted ia good yield to 5,6,7,8-tetrahydroquiQolines (117). These compounds can be dehydrogenated to the corresponding quiaolines. The parent reduced product has been prepared by heating O-aHylcyclohexanone oxime (118). 

Despite the increasing information on the photochemistry of 2,4-dienones and other unsaturated ketones, as well as on the ring-chain valence isomerism of halogen-substituted pyran and dihydi opyran systems,the data are still very scarce. The intermediate formation of pyrans valence-isomeric with unsaturated carbonyl compounds in the pyridine syntheses based on reactions of ammonia with aldehydes or ketones, advocated by various authors (cf. Section II,B,2,f), is still rather speculative. (See also Section II,B,2,e for the valence isomerism of 5-chloro-2,4-dienones with pyrylium chlorides.)... 

A simple approach for the formation of 2-substituted 3,4-dihydro-2H-pyrans, which are useful precursors for natural products such as optically active carbohydrates, is the catalytic enantioselective cycloaddition reaction of a,/ -unsaturated carbonyl compounds with electron-rich alkenes. This is an inverse electron-demand cycloaddition reaction which is controlled by a dominant interaction between the LUMO of the 1-oxa-1,3-butadiene and the HOMO of the alkene (Scheme 4.2, right). This is usually a concerted non-synchronous reaction with retention of the configuration of the die-nophile and results in normally high regioselectivity, which in the presence of Lewis acids is improved and, furthermore, also increases the reaction rate. 

If the carbonyl and the hydroxyl group are in the same molecule, an intramolecular nucleophilic addition can take place, leading to the formation of a cyclic hemiacetal. Five- and six-membered cyclic hemiacetals are relatively strain-free and particularly stable, and many carbohydrates therefore exist in an equilibrium between open-chain and cyclic forms. Glucose, for instance, exists in aqueous solution primarily in the six-membered, pyranose form resulting from intramolecular nucleophilic addition of the -OH group at C5 to the Cl carbonyl group (Figure 25.4). The name pyranose is derived from pyran, the name of the unsaturated six-membered cyclic ether. 

The intramolecular Michael addition11 of a nucleophilic oxygen to an a,/ -unsaturated ester constitutes an attractive alternative strategy for the synthesis of the pyran nucleus, a strategy that could conceivably be applied to the brevetoxin problem (see Scheme 2). For example, treatment of hydroxy a,/ -unsaturated ester 9 with sodium hydride furnishes an alkoxide ion that induces ring formation by attacking the electrophilic //-carbon of the unsaturated ester moiety. This base-induced intramolecular Michael addition reaction is a reversible process, and it ultimately affords the thermodynamically most stable product 10 (92% yield). 

Synthesis of highly functionalized 3,4-dihydro-2H-pyrans by high-pressure Lewis-acid-catalyzed cycloaddition of enol ethers and a,/i-unsaturated aldehydes [83]... 

Dihydro-2H-pyran-2-ones (e. g., 4-195) are valuable intermediates in the synthesis of several natural products [67]. Hattori, Miyano and coworkers [68] have recently shown that these compounds can be easily obtained in high yield by a Pd2+-catalyzed [2+2] cycloaddition of ct, 3-unsaturated aldehydes 4-192 with ketene 4-193, followed by an allylic rearrangement of the intermediate 4-194 (Scheme 4.42). In this reaction the Pd2+-compound acts as a mild Lewis acid. a,(3-unsaturated ketones can also be used, but the yields are below 20%. 

Increasing use is being made of pyran syntheses based upon [4 + 2] cycloadditions of carbonyl compounds. The appropriate unsaturated aldehyde with ethyl vinyl ether yields 53 with peracids this affords an epoxide that undergoes ring contraction to the aldehyde 54 (Scheme 23) and rhodium catalyzed decarbonylation affords the required 3-alkylfuran with the optical center intact.116 Acetoxybutadiene derivatives add active carbonyl compounds giving pyrans that contract under the influence of acids to give... 

An interesting feature of the cyclization of y, -unsaturated alcohols is the marked effect on product isomer distribution by the nature of substituents remote from the double bond (cf. 42 and Scheme 59).98 Complete stereospecificity is observed for the phenyl derivative 42a in contrast to 42b and c, and the isomer ratio is reversed for 42d. The suggested mechanism98 is shown in Scheme 60 the trisubstituted alkene (45) is mainly converted into a pyran (46) rather than a tetrahydrofuran derivative (Scheme 61). 

Both natural and non-natural compounds with a 2ff,5ff-pyrano[4,3-fc]pyran-5-one skeleton are of interest in medicinal chemistry. Several natural products, such as the pyripyropenes, incorporate this bicyclic ring system. The group of Beifuss has described an efficient microwave-promoted domino synthesis of the 2ff,5H-pyr-ano[4,3-fo]pyran-5-one skeleton by condensation of a,/3-unsaturated aldehydes with 4-hydroxy-6-methyl-2]-f-pyran-2-one (Scheme 6.244) [428]. It is assumed that in the presence of an amino acid catalyst a Knoevenagel condensation occurs first, which is then followed by a 6jr-electron electrocyclization to the pyran ring. While the conventional thermal protocol required a reaction time of up to 25 h (refluxing ethyl... 

A typical reaction is the formation of 2-substituted 3,6-divinyltetrahydro-pyranes (108) by the reaction of butadiene with aldehydes (97-100). In this reaction, unsaturated noncyclized alcohols 109 are also formed. The selectivity to the pyranes and alcohols can be controlled by the ratio of Pd and PPh3 in the catalyst system. When the ratio was higher than 3, pyranes were formed exclusively. On the other hand, with the lower ratio of Pd and PPh3, the unsaturated alcohols were formed as the main product. 

Compounds are generally classified according to their fully unsaturated parent compound (but see below). Thus substituted, partially saturated, and fully saturated derivatives of, for example, pyrrole are all indexed under pyrrole. Benzo and similar derivatives are included under the most unsaturated parent system (e.g., quinoline, thienofuran, etc.). For any given heterocyclic parent only one indicated hydrogen isomer appears in the text, typically the most stable or the lowest numbered form thus all instances of pyran, whether of the 2H- or 4H-form, are indexed under 2H-pyran. The charges and additional valences for any heterocyclic parent structure are not indicated. 

The high levels of enantioselectivity obtained in the asymmetric catalytic carbomagnesa-tion reactions (Tables 6.1 and 6.2) imply an organized (ebthi)Zr—alkene complex interaction with the heterocyclic alkene substrates. When chiral unsaturated pyrans or furans are employed, the resident center of asymmetry may induce differential rates of reaction, such that after -50 % conversion one enantiomer of the chiral alkene can be recovered in high enantiomeric purity. As an example, molecular models indicate that with a 2-substituted pyran, as shown in Fig. 6.2, the mode of addition labeled as I should be significantly favored over II or III, where unfavorable steric interactions between the (ebthi)Zr complex and the olefmic substrate would lead to significant catalyst—substrate complex destabilization. 

The synthetic versatility and significance of the Zr-catalyzed kinetic resolution of exocyc-lic allylic ethers is demonstrated by the example provided in Scheme 6.9. The optically pure starting allylic ether, obtained by the aforementioned catalytic kinetic resolution, undergoes a facile Ru-catalyzed rearrangement to afford the desired chromene in >99% ee [20], Unlike the unsaturated pyrans discussed above, chiral 2-substituted chromenes are not readily resolved by the Zr-catalyzed protocol. Optically pure styrenyl ethers, such as that shown in Scheme 6.9, are obtained by means of the Zr-catalyzed kinetic resolution, allowing for the efficient and enantioselective preparation of these important chromene heterocycles by a sequential catalytic protocol. 

Cycloaddition reactions of electron-rich allenes with some heterodienes take place at the C1-C2 bond of the allene to yield heterocycles, a,Unsaturated carbonyl compounds 185 react with the internal C=C bond of ethoxyallene to afford dihydro-pyrans in moderate yields [150]. 

We have studied the anodic oxidation of unsaturated alcohols using the controlled potential electrolysis (E = 1.9V vs SCE) in CH3CN-O.I mol/1 Et4NC104 solution in a divided cell [110]. The oxidation of 4-pentenol after consumption of 0.8 F/mol gave 2-methyltetrahydrofuran and tetrahydropyran as the major products. The oxidation of 5-pentenol gave 2-methyltetrahydro-pyran and oxepam, while the oxidation of 3-butenol under the same reaction conditions did not give the cyclic products. We rationalized this reaction as the electrongenerated acid (EGA) catalyzed intramolecular cyclization (Scheme 44). 

The catalytic enantioselective ring-closing metathesis of various polyenes affords unsaturated furans, pyrans, and siloxanes efficiently ... 

Inverse type hetero-Diels-Alder reactions between p-acyloxy-a-phenylthio substituted a, p-unsaturated cabonyl compounds as 1-oxa-1,3-dienes, enol ethers, a-alkoxy acrylates, and styrenes, respectively, as hetero-dienophiles result in an efficient one step synthesis of highly functionalized 3,4-dihydro-2H-pyrans (hex-4-enopyranosides). These compounds are diastereospecifically transformed into deoxy and amino-deoxy sugars such as the antibiotic ramulosin, in pyridines having a variety of electron donating substituents, in the important 3-deoxy-2-gly-culosonates, in precursors for macrolide synthesis, and in C.-aryl-glucopyranosides. 

Aiming at the pyranose form of sugars, normal type hetero-Diels-Alder reactions were extensively used for the synthesis of functionally substituted dihydropyran and tetrahydropyran systems (5-10) (see routes A - D in the general Scheme 1) which are also important targets in the "Chiron approach" to natural product syntheses (2.) Hetero-Diels-Alder reactions with inverse electron demand such as a, p-unsaturated carbonyl compounds (l-oxa-1,3-dienes) as heterodienes and enol ethers as hetero-dienophiles, are an attractive route for the synthesis of 3,4-dihydro-2H-pyrans (11). 

The rhodium-catalyzed asymmetric conjugate addition is applicable to a,yS-unsaturated esters (Scheme 3.8). Hayashi reported [20] that the reachon of 5,6-dihydro-2H-pyran-2-one 19a with phenylboronic acid gave a 94% yield of phenylated lactone (S)-20am with 98% enanhomeric excess. For the linear enoates, organoboronic acids did not give... 

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