Aziridination catalyzed

Nakagawa devised a concise synthetic route to physostigimine (169) where the key step involves the alkylative cyclization of 1,3-dimethylindole (167) with (Z)-aziridine catalyzed by Sc(OTf)3 and TMSC1 to give 168, which, in turn, can be converted into 169 . A similar asymmetric approach to this natural product was also developed by these authors via treatment of tryptophan carbamates with the Corey-Kim reagent so as to induce intramolecular cyclization to the pyrrolo-indole skeleton . 

Scheme 46 Ring opening of aziridines catalyzed by NHCs...

Aziridination Catalyzed by Iron, Manganese and Copper Salts Simple and Substrate-Induced Diastereoselectivity... 

Enantioselective Aziridination Catalyzed by Chiral Diimine-CnOTf124 ... 

Table 11. Enantioselectivc Aziridination Catalyzed by Diimine-Copper Triflate Complexes 24...

Cycloaddition, Diels-Alder reactions, epoxidation of aromatic aldehydes, isomerization of aryl-substituted epoxides, and aziridination catalyzed by the iron Lewis acid [(j 5-C5H5)Fe(CO)2(THF)] 03ACA3. 

Antilla and co-workers reported desymmetrization of meso-aziridines catalyzed by the (R)-VAPOL-derived phosphoric acid 26 (Equation 10.50, Figure 10.22) [96],... 

The carbonylation of several classes of aziridines have been reported. In general, the carbonylation of aziridines containing alkyl or benzyl substituents on the two carbon atoms occurs to insert the CO into the C-N bond containing the less-substituted carbon. Equation 17.53 shows a series of these reactions catalyzed by Co2(CO)g. In contrast, the carbonylation of aziridines containing aryl groups on one of the two carbons occurs at the benzylic position. Examples of these reactions are shown in Equation 17.54. Carbonylation of these phenyl-substituted aziridines catalyzed by [Rh(CO)2Cl]j has also been reported by Alper, and a representative example is shown in Equation 17,55. ... 

Ring opening of aziridines catalyzed by In(III) salts was studied by Yadav et al. and the results showed the same trend as above. InBrs was used for addition of amines to N-tosyl aziridines [86], In(OTf)3 for carboxylic acids [87], and InCh for trimethylsilyl azide [88] (Figure 8.45). 

Oxidative cleavage of P-aminoacyl complexes can yield P-amino acid derivatives (320,321). The rhodium(I)-catalyzed carbonylation of substituted aziridines leads to P-lactams, presumably also via a P-aminoacyl—metal acycHc compound as intermediate. The substituent in the aziridine must have 7T or electrons for coordination with the rhodium (322,323). 

P-chlorocarbamates which can be converted to aziridines and alkyloxazoUdones (93,115). A/-Chloro-A/-sodiourethane reacts with organoboranes forming A/-alkylcarbamates (114), and with olefins, catalyzed by Os, forming vicinal hydroxy carbamates (116). 

There are at least two mechanisms available for aziridine cis-trans isomerism. The first is base-catalyzed and proceeds via an intermediate carbanion (235). The second mechanism can be either thermally or photochemically initiated and proceeds by way of an intermediate azomethine ylide. The absence of a catalytic effect and interception of the 1,3-dipole intermediate provide support for this route. A variety of aziridinyl ketones have been found to undergo equilibration when subjected to base-catalyzed conditions (65JA1050). In most of these cases the cis isomer is more stable than the trans. Base-catalyzed isotope exchange has also been observed in at least one molecule which lacks a stabilizing carbonyl group (72TL3591). 

Thus, in contrast to benzothiepins, dibenzo compounds can be synthesized by direct acid-catalyzed elimination of water from hydroxy derivatives, or of amines from amino derivatives, at elevated temperatures due to their thermal stability. As in the case of benzothiepins, dibenzo derivatives can also be prepared by base-catalyzed elimination from the corresponding halo derivatives however, the yields are somewhat lower compared to the acid-catalyzed reactions. As a special case, an aziridine derivative was deaminated by palladium-catalyzed hydrogenation to afford the corresponding dibenzothiepin.69... 

Jorgensen has recently reported similar enantioselective reactions between N-tosylimines 107 and trimethylsilyldiazomethane (TMSD) catalyzed by chiral Lewis acid complexes (Scheme 1.32) [57, 53]. The cis-aziridine could be obtained in 72% ee with use of a BINAP-copper(i) catalyst, but when a bisoxazoline-copper(i) complex was used the corresponding trans isomer was fonned in 69% ee but with very poor diastereoselectivity. 

Catalysts prepared either from VAPOL (109) or from VANOL (110) ligands and triphenylborate were found to catalyze the asymmetric aziridination efficiently. Good to high yields, excellent enantioselectivities, and cis diastereoselectivities were observed with all the reported substrates, which included aromatic, heteroaromatic and aliphatic imines (Table 1.14). 

In 1995, aziridination with 1,3-dienes 10 by treatment with PhI=NTs 9 was developed (Scheme 2.4) [10] on the foundation of pioneering works by Jacobsen and Evans on copper-catalyzed asymmetric aziridination of isolated alkenes [11]. 

Scheme 2.20 Palladium(0)-catalyzed aziridination of a-amino allene 66.

As described in Section 2.3.2, vinylaziridines are versatile intermediates for the stereoselective synthesis of (E)-alkene dipeptide isosteres. One of the simplest methods for the synthesis of alkene isosteres such as 242 and 243 via aziridine derivatives of type 240 and 241 (Scheme 2.59) involves the use of chiral anti- and syn-amino alcohols 238 and 239, synthesizable in turn from various chiral amino aldehydes 237. However, when a chiral N-protected amino aldehyde derived from a natural ot-amino acid is treated with an organometallic reagent such as vinylmag-nesium bromide, a mixture of anti- and syn-amino alcohols 238 and 239 is always obtained. Highly stereoselective syntheses of either anti- or syn-amino alcohols 238 or 239, and hence 2,3-trans- or 2,3-as-3-alkyl-2-vinylaziridines 240 or 241, from readily available amino aldehydes 237 had thus hitherto been difficult. Ibuka and coworkers overcame this difficulty by developing an extremely useful epimerization of vinylaziridines. Palladium(0)-catalyzed reactions of 2,3-trons-2-vinylaziri-dines 240 afforded the thermodynamically more stable 2,3-cis isomers 241 predominantly over 240 (241 240 >94 6) through 7i-allylpalladium intermediates, in accordance with ab initio calculations [29]. This epimerization allowed a highly stereoselective synthesis of (E) -alkene dipeptide isosteres 243 with the desired L,L-... 

The BF3 Et20-catalyzed aziridination of compounds 47 (Scheme 3.15) with a diazo ester derived from (R)-pantolacetone gave aziridine-2-carboxylates 48 [59]. The reaction exhibited both high cis selectivity (>95 <5) and excellent diastereose-lectivity. Treatment of a-amino nitrile 49 (Scheme 3.16) with ethyl diazoacetate in the presence of 0.5 equivalent of SnCl4 afforded aziridines 50 and 51 in 39% yield in a ratio of 75 25 [60]. 

With Sulfur Nucleophiles N-Carboxy-protected aziridine-2-carboxylates react with thiols to give P-mercapto-ot-amino acid derivatives. The reaction is usually catalyzed by BF3 and the yields range from fair to excellent [15, 16, 108-111]. With N-unprotected 3-substituted aziridine-2-carboxylates, the ring-opening with thiols usually takes place with anti stereoselectivity, especially in the case of the C-3 aliphatic substituted substrates. In cases in which C-3 is aromatic, however, the stereoselectivity has been found to be a function of the substitution pattern on the aromatic ring 3-p-methoxy ph eri yl-su bs li In led aziridines 143a (Scheme 3.51) and... 

Bromamine-T can also be utilized as a nitrene source, as reported by Zhang et al. [27]. Fe(in) porphyrins such as Fe(TPPC)Cl (Figure 4.2) thus catalyze the aziridination of alkenes when bromamine-T is used, whereas chloramine-T was inactive and iodinanes were inefficient reagents. 

Jacobsen has utilized [(salen)Co]-catalyzed kinetic resolutions of tenninal epoxides to prepare N-nosyl aziridines with high levels of enantioselectivity [72], A range of racemic aryl and aliphatic epoxides are thus converted into aziridines in a four-step process, by sequential treatment with water (0.55 equivalents), Ns-NH-BOC, TFA, Ms20, and carbonate (Scheme 4.49). Despite the apparently lengthy procedure, overall yields of the product aziridines are excellent and only one chromatographic purification is required in the entire sequence. 

Two recent reports described addition of nitrogen-centered nucleophiles in usefully protected fonn. Jacobsen reported that N-Boc-protected sulfonamides undergo poorly selective (salen) Co-catalyzed addition to racemic epoxides. However, by performing a one-pot, indirect kinetic resolution with water first (HKR, vide infra, Table 7.1) and then sulfonamide, it was possible to obtain highly enantiomer-ically enriched addition products (Scheme 7.39) [71]. These products were transformed into enantioenriched terminal aziridines in straightforward manner. 

Two methods that are particularly convenient for large-scale synthesis of aziridines are discussed below. Both utilize readily available chloramine salts, such as chloramine-T, as sources of nitrogen. The first method involves direct olefin azir-idination catalyzed by phenyltrimethylammonium tribromide (PhNMe3+Br3 PTAB) [42]. In the second method, 1,2-hydroxysulfonamides, conveniently obtained by osmium-catalyzed aminohydroxylation of olefins, are converted into aziridines by one-pot cyclodehydration. 

Bromine-catalyzed Aziridination of Olefins with Chloramines... 

Table 12.4 Bromine-catalyzed aziridination of allylic alcohols with anhydrous TsNCINa. a]...

Table 12.5 PTAB-catalyzed aziridinations with BusN(CI)Na.

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