Conjugate addition 474 Subject

Conjugate addition to acyclic enones is subject to chelation control when TiCl4 is used as the Lewis acid. Thus, whereas the A-enone 12 gives syn product 13 via an acyclic TS, the Z-isomer 14 reacts through a chelated TS to give 15.133... 

The polymerization of MMA has been shown to be subject to enantiomorphic site control when the Ci-symmetric a .va-lanthanocene complexes (196) and (197) are employed as initiators.463 When the (T)-neomenthyl catalyst (196) is used, highly isotactic PMMA is produced (94% mm at — 35 °C), whereas the (-)menthyl derived (197) affords syndiorich PMMA (73% rr at 25 °C). NMR statistical analysis suggests that conjugate addition of monomer competes with enolate isomerization processes, and the relative rate of the two pathways determines the tacticity. 

Greaney and coworkers have introduced the conjugate addition of thiols to Michael acceptors as an effective adaptive DCL strategy [46,47]. The reaction is well suited for biological DCL synthesis, taking place in water with no requirement for external reagents. As with disulfide bond formation, the reaction is subject to simple and effective pH control. Under mildly basic conditions, the thiolate anion adds rapidly to Michael acceptors under equilibrium conditions. Acidification effectively switches the reaction... 

Rhodium-catalyzed asymmetric conjugate addition has enjoyed uninterrupted prosperity since the first report by Hayashi and Miyaura [6]. Its high enantioselectivity and wide applicability are truly remarkable. However, some problems still remain, since the carbon atoms that can be successfully introduced by this rhodium-catalyzed reaction have been limited to sp carbons and the substrates employed have been limited mostly to the electron-deficient olefins free from sterically bulky substituents at a- and / -positions. These issues will be the subject of increasing attention in the future. 

The many uses of organocuprates have been the subject of numerous reviews,1 3 4 6-10 especially the conjugate addition reaction which has received the most attention1 and is the subject of this discussion. 

Since the previous review in this comprehensive book [1], the asymmetric catalytic conjugate additions of stabilized carbanions have made considerable advances. Publications between 1996 and early 2002 are summarized in this supplementary according to the same categorization as before. Several reviews have also appeared on this subject [2-4]. 

When subjected to the action of propanethiol under basic conditions (pH 9.2), jatrophone (2) undergoes a Michael reaction across its C8-C9 double bond, followed by facile transannular cyclization to give the tetracyclic diketone 3.2,9 The susceptibility of this enone part structure to conjugate addition has been proposed to constitute the event responsible for the pronounced biological activity of 2.9... 

When chiral acceptors are used, the initial alkoxymercuration step and consequently the overall conjugate addition of the O-nucleophile should be subject to substrate-induced diastereoselec-tion. Indeed, this approach could successfully be applied to the diastereoselective construction of open-chain carbon skeletons with consecutive stereogenic centers, bearing alternating oxy-... 

As already mentioned, the steric course of acid- or base-catalyzed conjugate additions is usually subject to thermodynamic control. An interesting example of how hydrogen bonding in the product(s) may affect the stereochemical outcome of the addition reaction is provided by ajmalicine (25). When the enoate 25 was treated with 5% aqueous sulfuric acid, the 17-hydroxy-derivative 26 was obtained as a single diastereomer in 40% yield20. The configuration of the... 

Dideoxynucleosides show potent anti-retroviral activity against HIV-specific reverse transcriptase80-83. In particular, 2, 3 -dideoxy-3 -C-cyano-2 -substituted thymidine derivatives (33 A and 33 B) with a free 5 -hydroxy function (R1 = H) are potential inhibitors of the HIV-reverse transcriptase-promoted c-DNA synthesis. As these compounds have yet to be prepared by another method, the 3 -ene-nitrile 3284 was subjected to conjugate addition reactions with ammonia, primary amines, secondary amines and carbon nucleophiles. Most of these nucleophilic amine addition reactions give either the trans-isomer 33 A as the sole product (e.g., reaction with pyrrolidine, piperidine, morpholine), or as the major product along with the c/s-isomer (e.g., reaction with methylamine, benzylamine), except for the reaction with ammonia where the cts-isomer 33B is formed as the major product84. 

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