Allyl carbamates, secondary

An efficient kinetic resolution of racemic secondary allyl carbamates was accomplished by the jw-butyllithium-(-)-sparteine complex76 131. Whereas the R-enantiomer (80% ee) is recovered unchanged, the 5-enantiomer is deprotonated preferentially. 

Pd(0)/phosphine complexes, or their precursors, in the presence of a suitable co-base, have also been shown to promote, in good yields (66-100%), the formation of allylic carbamates from various primary and secondary aliphatic amines, pressurized C02 and allylic chlorides, in THF, at ambient temperature [87a]. The choice of the added co-base (Base), used for generating the carbamate salt RR NC02 (BaseH)+, was found to be critical for high yields of O-allylic urethanes. The use of a guanidine (CyTMG) or amidine (DBU) base was optimal for this system (see also Section 6.3.1). ft is assumed that this chemistry passes catalytically through a mechanism similar to that illustrated in Scheme 6.19. This involves nucleophilic attack by carbamate anion on a (tt-allyl) palladium species, formed by the oxidative addition of the allylic chloride to a palladium(O) intermediate. 

Following a first report by Kunz and WaldmannP l secondary amines such as diethylamine, piperidine, and in particular the less basic morpholineP l have been extensively used for the deprotection of allyl esters. As the allylammonium species formed in this process (Scheme 14) may also behave as an allyl donor towards palladium zerovalent complexes, the use of an excess of scavenger is highly recommended in order to totally displace the equilibrium towards deprotection. Secondary amines can also be used in the deprotection of allyl carbamates. Here again an excess of scavenger is necessary to avoid kineticaUy competitive allylation of the liberated amine. 

The double inversion mechanism that operates in the Ir-catalyzed decarboxylative decomposition of secondary allylic carbamates effectively converts allylic alcohols into the corresponding amine derivatives with complete retention of configuration. ... 

The deprotonations are complete within a few hours at -78 °C and afford the lithium car-benoid sparteine complexes (5)-l-(-)-3 with excellent enantioselectivities. [6-12] Whereas sparteine complexes of lithiated secondary allyl and primary alkyl carbamates are configurationally stable below -30 °C, those of primary allyl carbamates such as 4 (-)-3 are not configurationally stable even at -70 °C. It is, however, possible to use these reagents in synthesis, since the preferential crystallization of the S diastereomer in pentane/cyclohexane drives the equilibrium completely to one side. After a low-temperature transmetalation of (5 )-4-(-)-3 with an excess of tetraisopropo-xytitanium, the allylic titanium reagent (Ji)-S is obtained with inversion of configuration. The addition of various aldehydes to (R)-5 furnishes homoaldol adducts of type 6 with... 

Sulfides can be oxidized to sulfoxides by reaction with NCS in methanol (0°C, 1 h). Similarly, selenides couple with amines when activated by NCS to form selenimide species. These have been generated from allylic selenides in order to prepare allylic amines and chiral secondary allylic carbamates by [2,3]-sigmatropic rearrangement (eq 8). ... 

The chiral information of stereogenic centers in the allyl moiety of the precursor is destroyed on deprotonation. While an i/3-bound ion pair with a planar carbon frame is a chiral compound, usually rapid racemization takes place by intra- or intermolecular migration of the cation from one face to the opposite one. The sole exceptions known at present are secondary 2-alkenyl carbamates with X = dialkylaminocarbonyloxy21, in which the cation is tied by the chelating ligand, see Section 1.3.3.3.1.2. 

Allylsilanes are available by treatment of allyl acetates and allyl carbonates with silyl cuprates17-18, with antarafacial stereochemistry being observed for displacement of tertiary allyl acetates19. This reaction provides a useful asymmetric synthesis of allylsilanes using esters and carbamates derived from optically active secondary alcohols antarafacial stereochemistry is observed for the esters, and suprafacial stereochemistry for the carbamates20,21. 

An efficient chemoenzymatic route for the synthesis of optically active substituted indolines has been recently developed (Scheme 7.27), and also the alkoxycarbonyla-tion process is more efficient than the acylation reaction. Different lipases have been tested in the alkoxycarbonylation of these secondary amines, GALA being found to be the best biocatalyst for 2-substituted-indolines, and CALB for 3-methylindoline. The combination of lipases with a variety of allyl carbonates and TBME as solvent has allowed the isolation of the carbamate and amine derivatives in a high level of enantiopurity [51]. 

The cyclohexene 121, which was readily accessible from the Diels-Alder reaction of methyl hexa-3,5-dienoate and 3,4-methylenedioxy-(3-nitrostyrene (108), served as the starting point for another formal total synthesis of ( )-lycorine (1) (Scheme 11) (113). In the event dissolving metal reduction of 121 with zinc followed by reduction of the intermediate cyclic hydroxamic acid with lithium diethoxyaluminum hydride provided the secondary amine 122. Transformation of 122 to the tetracyclic lactam 123 was achieved by sequential treatment with ethyl chloroformate and Bischler-Napieralski cyclization of the resulting carbamate with phosphorus oxychloride. Since attempts to effect cleanly the direct allylic oxidation of 123 to provide an intermediate suitable for subsequent elaboration to ( )-lycorine (1) were unsuccessful, a stepwise protocol was devised. Namely, addition of phenylselenyl bromide to 123 in acetic acid followed by hydrolysis of the intermediate acetates gave a mixture of two hydroxy se-lenides. Oxidative elimination of phenylselenous acid from the minor product afforded the allylic alcohol 124, whereas the major hydroxy selenide was resistant to oxidation and elimination. When 124 was treated with a small amount of acetic anhydride and sulfuric acid in acetic acid, the main product was the rearranged acetate 67, which had been previously converted to ( )-lycorine (108). 

N-Allyl tertiary amides 72 can be lithiated with r-BuLi and, like the secondary amides 54 and 57 they react y to nitrogen to give cis acylenamine products 74, with the intermediate organolithium adopting a structure approximating to 72.152 The stereochemistry of the reactions of lithiated allyl amides and carbamates in the presence of (-)-sparteine53 is discussed further in chapter 6. 

A fourth type of product, a carbamate RNHCOOR , can be obtained from primary or secondary amines, if these are treated with CO, O2, and an alcohol R OH in the presence of a catalyst. " Primary amines react with dimethyl carbonate in supercritical CO2 (see p. 414) to give a carbamate. " Carbamates can also be obtained from nitroso compounds, by treatment with CO, R OH, Pd(OAc)2, and Cu(OAc)2, " and from nitro compounds. " When allylic amines (R2C=CHRCHRNR 2) are treated with CO and a palladium-phosphine catalyst, the CO inserts to produce the p,y-unsa-turated amides (R2C=CHRCHRCONR 2) in good yields. " Ring-expanded lactams are obtained from cyclic amines via a similar reaction (see also, 16-22). Silyloxy carbamates (RNHC02SiR 3) can be prepared by the reaction of a primary amine with carbon dioxide and triethylamine, followed by reaction with triisopropylsilyl triflate and tetrabutylammonium fluoride. ... 

The analogous reactions of acetates of primary and secondary allyl alcohols normally lead to equilibrium mixtures only slightly favoring primary allyl acetates. The equilibration of allyl alcohols by the Pd-catalyzed equilibration of derived esters or carbamates has some advantages in comparison with the... 

The Overman rearrangement has been extended to the synthesis of secondary allyl aryl ethers and allylic thiol carbamates, using a palladized oxazolinylcobaltocene-type complex (187)." The former reaction could very well be considered as an SN2 process. 

---