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Enones enamine activation

The diflferent reactivity of aldehydes and ketones toward condensation with amines is also a differentiating element when using enals or enones as Michael donors under iminium activation. As in the enamine activation case, working with a,p-unsaturated aldehydes usually leads to faster reactions or better conversions but the same reaction with enones in many cases turns out to be a very slow or even non-existent reaction. Stereochemical control is also more problematic when a,p-unsaturated ketones are employed because the presence... [Pg.65]

It has to be pointed out that simple enolizable aldehydes and ketones, which are not acidic enough compounds to be directly used as pro-nucleophiles in this context, can nevertheless be employed as Michael donors in the reaction with enals or enones, which have been previously activated as the corresponding iminium ion, but their use requires prior activation via enamine activation. In these cases, it is usually proposed that the amine catalyst is involved in a dual activation profile interacting with both the Michael donor and the acceptor, although the enamine activation of the pro-nucleophile is mandatory for the reaction to occur, the activation of the acceptor being of less relevance in most cases. For these reasons, this chemistry has been covered in Chapter 2. [Pg.67]

One of the first synthetically useful organocatalytic C-N bond forming cycloaddition reaction came with the work of Yamamoto et al. [125] reported in 2004. Based on enamine activation, they developed the tandem 0-nitroso aldol/Michael reactions of cyclic enones to generate nitroso Diels-Alder adducts in moderate yields and high enantioselectivities (Scheme 11.44). [Pg.418]

Later, the same group expanded this chemistry further by developing a cascade Michael addition/cross-benzoin condensation sequence of enolizable aldehydes 43 and activated enones 44 [27]. The reaction proceeded by means of enamine activation of aliphatic aldehydes to induce an asymmetric Michael addition to activated enones followed by an intramolecular cross-benzoin condensation (Scheme 9.30). Compared with their previous work, complex cyclopentanones with complementary substitution patterns were observed. Screening of the reaction parameters revealed that the chiral triazolium catalyst was necessary to ensure a satisfactory stereochemical outcome. Further mechanistic insights indicated that the high diasteroselectivity observed attributed to the secondary amine-induced epimerizing of the a-position of intermediate aldehyde 89. [Pg.382]

The majority of the Michael-type conjugate additions are promoted by amine-based catalysts and proceed via an enamine or iminium intermediate species. Subsequently, Jprgensen et al. [43] explored the aza-Michael addition of hydra-zones to cyclic enones catalyzed by Cinchona alkaloids. Although the reaction proceeds under pyrrolidine catalysis via iminium activation of the enone, and also with NEtj via hydrazone activation, both methods do not confer enantioselectivity to the reaction. Under a Cinchona alkaloid screen, quinine 3 was identified as an effective aza-Michael catalyst to give 92% yield and 1 3.5 er (Scheme 4). [Pg.151]

The MacMillan catalysts (42, 45), the Jorgensen catalyst (51), and proline itself can promote Michael additions by iminium ion formation with the acceptor enal or enone (A, Scheme 4.22). Secondary amines can also activate a carbonyl donor by enamine formation (Scheme 4.22, B) [36, 37]. [Pg.64]

Small chiral organic molecules may catalyze the asymmetric addition of ketones, and aldehydes to electron-deficient olefins, such as vinylidene acetones, nitroole-fins, enones, and vinyl sulfones. In this chapter we will describe the inter- and intramolecular reactions in which activation of the carbonyl compound takes place via enamine formation. [Pg.77]

MacMillan s catalysts 56a and 61 allowed also the combination of the domino 1,4-hydride addition followed by intramolecular Michael addition [44]. The reaction is chemoselective, as the hydride addition takes place first on the iminium-activated enal. The enamine-product of the reaction is trapped in a rapid intramolecular reaction by the enone, as depicted in Scheme 2.54. The intramolecular trapping is efficient, as no formation of the saturated aldehyde can be observed. The best results were obtained with MacMillan s imidazolidinium salt 61 and Hantzsch ester 62 as hydride source. As was the case in the cyclization reaction, the reaction affords the thermodynamic trans product in high selectivity. This transformation sequence is particularly important in demonstrating that the same catalyst may trigger different reactions via different mechanistic pathways, in the same reaction mixture. [Pg.91]

Narasaka reported that the titanium compound generated from TiCl2(OiPr)2 and an optically active diol in the presence of 4 A molecular sieve promoted the asymmetric addition of enamine 69 to the activated fumarate 70 [72]. Cyclobutane derivatives were formed when p,p-disubstituted enamines were employed. Titanium oxide derived from (l )-BINOL and (iPr0)2Ti=0 catalyzed the asymmetric addition of silyl thioenol ether 71 to enones [73]. The sulfur derivative ex-... [Pg.1074]

A particularly difficult situation arises when combining in the same reaction the use of these rather unreactive acceptors such as enones with the incorporation of ketones as Michael donors in which the formation of the intermediate enamine by condensation with the amine catalyst is much more difficult. For this reason, the organocatalytic Michael addition of ketones to enones still remains rather unexplored. An example has been outlined in Scheme 2.22, in which it has been shown that pyrrolidine-sulfonamide 3a could catalyze the Michael reaction between cyclic ketones and enones with remarkably good results, although the reaction scope was exclusively studied for the case of cyclic six-membered ring ketones as nucleophiles and 1,4-diaryl substituted enones as electrophiles. In this system the authors also pointed toward a mechanism involving exclusively enamine-type activation of the nucleophile, with no contribution of any intermediate iminium species which could eventually activate the electrophile. Surprisingly, the use of primary amines as catalysts in this transformation has not been already considered. [Pg.47]

However, it is in this context where the use of primary amines as catalysts demonstrates the high performance of this concept. As has already been mentioned in Chapter 2, primary amines are much more efficient catalysts for the activation of ketones than the corresponding secondary amines due to the formation of a less sterically congested enamine or iminium ion and also because of the more efficient geometry control in their formation. For example, primary amine 28a was found to be able to activate a-enolizable enones toward... [Pg.249]

See other pages where Enones enamine activation is mentioned: [Pg.329]    [Pg.45]    [Pg.46]    [Pg.221]    [Pg.327]    [Pg.328]    [Pg.330]    [Pg.338]    [Pg.340]    [Pg.359]    [Pg.208]    [Pg.1062]    [Pg.1062]    [Pg.59]    [Pg.983]    [Pg.69]    [Pg.63]    [Pg.59]    [Pg.3913]    [Pg.285]    [Pg.285]    [Pg.112]    [Pg.362]    [Pg.838]    [Pg.3912]    [Pg.48]    [Pg.50]    [Pg.241]    [Pg.258]    [Pg.267]    [Pg.268]    [Pg.283]    [Pg.54]    [Pg.159]   
See also in sourсe #XX -- [ Pg.45 , Pg.46 , Pg.47 , Pg.48 , Pg.49 ]



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Enamine activation

Enones activation

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