Cyclopentenones reduction

As shown in Scheme 11.87, aldehyde 431 was transformed into sUylenol ether 432, which was treated with methylene triphenylphosphorane to give the expected cyclopentenone. Reduction of the keto group and protection of the resulting alcohol gave 433. As in Chiara s synthesis, epoxidation and opening of the latter with sodium azide completed the synthesis of 6-epi-trehazoline 434. 

The growing importance of cyclopropane derivatives (A. de Meijere, 1979), as synthetic intermediates originates in the unique, olefin-like properties of this carbocycle. Cyclopropane derivatives with one or two activating groups are easily opened (see. p. 69f.). Some of these reactions are highly regio- and stereoselective (E. Wenkert, 1970 A, B E. J. Corey, 1956 A, B, 1975 see p. 70). Many appropriately substituted cyclopropane derivatives yield 1,4-difunctional compounds under mild nucleophilic or reductive reaction conditions. Such compounds are especially useful in syntheses of cyclopentenone derivatives and of heterocycles (see also sections 1.13.3 and 4.6.4). 

Reaction of (T)-(-)-2-acetoxysuccinyl chloride (78), prepared from (5)-mahc acid, using the magnesiobromide salt of monomethyl malonate afforded the dioxosuberate (79) which was cyclized with magnesium carbonate to a 4 1 mixture of cyclopentenone (80) and the 5-acetoxy isomer. Catalytic hydrogenation of (80) gave (81) having the thermodynamically favored aH-trans stereochemistry. Ketone reduction and hydrolysis produced the bicycHc lactone acid (82) which was converted to the Corey aldehyde equivalent (83). A number of other approaches have been described (108). 

The intermediate enolate or enol ether from the initial reduction of an enone may be alkylated in situ (Eq. 281).455 / -Substituted cyclopentenones may be asymmetrically reduced and alkylated459 (see section on asymmetric reductions of enones). Enolates may also be trapped with an aldehyde in a reductive aldol condensation of an enone with an aldehyde,455 permitting a regioselective aldol condensation to be carried out as shown in Eq. 282.455 This class of reductive aldol condensation reactions can also occur in a cyclic manner (Eq. 283).460... 

The sequence of chiral 1,4-reduction of a fi-substituted cyclopentenone followed by electrophilic trapping of the intermediate enolate provides an efficient route to chiral 2,3-disubstituted cyclopentanones that generates two chiral centers in the process (Eq. 352)459... 

The relatively low percentage of ring substitution can be attributed to several side reactions 1,4-addition of Li to 2-cyclopentenone, incomplete dehydration of 4 as evidenced by the presence of a small hydroxyl absorption (3425 cm ) in the IR spectrum of 5, and reduction of the polymer-bound cyclopentadiene in its reaction with Co2(C0)8 (26,27,32). 

A total synthesis of functionalized 8,14-seco steroids with five- and six-membered D rings has been developed (467). The synthesis is based on the transformation of (S)-carvone into a steroidal AB ring moiety with a side chain at C(9), which allows the creation of a nitrile oxide at this position. The nitrile oxides are coupled with cyclic enones or enol derivatives of 1,3-diketones, and reductive cleavage of the obtained cycloadducts give the desired products. The formation of a twelve-membered ring compound has been reported in the cycloaddition of one of the nitrile oxides with cyclopentenone and as the result of an intramolecular ene reaction, followed by retro-aldol reaction. 

Cyclopentenones. Some time ago, Martin et al.1 reported that a,(3-unsaturated acid chlorides react with acetylene in the presence of 1 equiv. of A1C1, to give 5-chlorocyclopentenones. More recent research2 shows that this reaction is a convenient route to 4- and 5-substituted cyclopentenones after zinc reduction (equation... 

D-Ribonolactone is a convenient source of chiral cyclopentenones, acyclic structures, and oxacyclic systems, useful intermediates for the synthesis of biologically important molecules. Cyclopentenones derived from ribono-lactone have been employed for the synthesis of prostanoids and carbocyclic nucleosides. The cyclopentenone 280 was synthesized (265) from 2,3-0-cyclohexylidene-D-ribono-1,4-lactone (16b) by a threestep synthesis that involves successive periodate oxidation, glycosylation of the lactol with 2-propanol to give 279, and treatment of 279 with lithium dimethyl methyl-phosphonate. The enantiomer of 280 was prepared from D-mannose by converting it to the corresponding lactone, which was selectively protected at HO-2, HO-3 by acetalization. Likewise, the isopropylidene derivative 282 was obtained (266) via the intermediate unsaturated lactone 281, prepared from 16a. Reduction of 281 with di-tert-butoxy lithium aluminum hydride, followed by mesylation, gave 282. 

Similarly, a double functionalization can be reached when an activating group is present in close vicinity to the triple bond. Tsuji et al. have discovered that with a diphosphine palladium(O) complex, a carbonate function in the a-position of the alkyne provides by decarboxylation a palladium methoxy species on which the alkyne moiety can be isomerized into an al-lenyl a -bonded group. CO insertion in the Pd - C bond, reductive elimination with the methoxy group and further cyclization with incorporation of a second CO molecule give rise to the corresponding cyclopentenone as shown in Scheme 21 [127]. 

A proposed mechanism of this reaction was reported by Magnus and Principle [10], which is nowadays widely accepted (Scheme 1). Recently, negative-ion electrospray collision experiments have confirmed this mechanism in detail [11]. Starting with the formation of the alkyne-Co2(CO)6 complex 2, olefin 3 coordination and subsequent insertion takes place at the less hindered end of the alkyne. The in situ formed metallacycle 4 reacts rapidly under insertion of a CO ligand 5 and reductive elimination of 6 proceeds to liberate the desired cyclopentenone 7. It is important to note that all the bond-forming steps occur on only one cobalt atom. The other cobalt atom of the complex is presumed to act as an anchor which has additional electronic influences on the bond-forming metal atom via the existing metal-metal bond [12]. 

Conversion of a Co2(CO)6-alkyne complex into a cyclopentenone is the Pauson-Khand reaction. It proceeds by loss of CO from one Co to make a 16-electron complex, coordination and insertion of the C6=C7 K bond into the C2-Co bond to make the C2-C6 bond and a C7-Co bond, migratory insertion of CO into the C7-Co bond to make the C7-C8 bond, reductive elimination of the C1-C8 bond from Co, and decomplexation of the other Co from the C1=C2 k bond. The mechanism is discussed in the text (Section B.l.f). 

Racemic diquinane enone rac-6 was prepared by Piers and Orellana starting from cyclopentenone (Scheme 6) [11]. After the preparation of the heterocuprate from stannane 20, conjugate addition to cyclopentenone in the presence of BF3 Et20 provided carbonyl compound 21. It was expected that conversion of 21 by intramolecular alkylation and subsequent hydrogenation should provide the desired endo-substituted diquinane rac-13. While other hydrogenation methods proved to be rather unselective, reduction in the presence of Wilkinson s catalyst finally resulted in the formation of rac-13 with good facial diastereoselectivity [11]. 

Reduction of unsaturated ketones to saturated alcohols is achieved by catalytic hydrogenation using a nickel catalyst [49], a copper chromite catalyst [50, 887] or by treatment with a nickel-aluminum alloy in sodium hydroxide [555]. If the double bond is conjugated, complete reduction can also be obtained with some hydrides. 2-Cyclopentenone was reduced to cyclopentanol in 83.5% yield with lithium aluminum hydride in tetrahydrofuran [764], with lithium tris tert-butoxy)aluminium hydride (88.8% yield) [764], and with sodium borohydride in ethanol at 78° (yield 100%) [764], Most frequently, however, only the carbonyl is reduced, especially with application of the inverse technique (p. 21). 

The alkyne-cobalt carbonyl complex 3 formed from the alkyne 1 and dicobalt octacarbonyl 2 should lose at least one of the GOs on the metal to provide the vacancy for the incoming olefins. Subsequently, an olefin-bound complex 5 rearranged oxidatively to yield a metallacyclic intermediate 6. Migratory insertion of GO of 6 would provide the homologated ring intermediate 7, and the following two successive reductive eliminations afford the cyclopentenone... 

The 2-methylenecyclopentanone initially formed presumably rearranges into 2-methyl-2-cyclopentenone under the reaction conditions. The final step of the mechanism, elimination of the cobalt carbonyl group, is not well understood but the same kind of elimination and reduction reactions occur with known 3-ketocobalt complexes. As mentioned above, crotonaldehyde, acrolein (27), and glyddaldehyde (38) react rapidly with cobalt hydrocarbonvl under similar conditions to give reduction products, rather than forming stable alkyl- or acyl-cobalt tetracarbonyl derivatives. 

Mechanistic studies are consistent with photochemical electron transfer from the carbyne complex to chloroform followed by H atom abstraction. Ring expansion then occurs to give a metallacyclopentene, which undergoes carbonyl insertion. Finally, reductive elimination yields the cyclopentenone complex that slowly releases the free enone (equation 119)158. 

Chiral 4,4-dialkyl-l-cyclopentenones.1 The chiral bicyclic lactam 2, derived from levulinic acid and 1, on monoalkylation exhibits slight if any selectivity regardless of the electrophile. However, a second alkylation exhibits high endo-selectivity. This product (3), after reductive cleavage, furnishes a keto aldehyde that is cyclized by base to a chiral 4,4-disubstituted-2-cyclopentenone (4). Either antipode of 4 can be prepared by the sequence of alkylation. 

---