Isocyanates hydantoin ring

Mass spectral fragmentation patterns of alkyl and phenyl hydantoins have been investigated by means of labeling techniques (28—30), and similar studies have also been carried out for thiohydantoins (31,32). In all cases, breakdown of the hydantoin ring occurs by a-ftssion at C-4 with concomitant loss of carbon monoxide and an isocyanate molecule. In the case of aryl derivatives, the ease of formation of Ar—NCO is related to the electronic properties of the aryl ring substituents (33). Mass spectrometry has been used for identification of the phenylthiohydantoin derivatives formed from amino acids during peptide sequence determination by the Edman method (34). 

Scheme 16 shows parallel syntheses of cyclic and acyclic amide compounds. Fluorous benzaldehydes were first subjected to reductive amination reactions. The resulting amines were then reacted with isocyanates to form substituted hydantoin rings 14 or with benzoyl chlorides to form amides 15. Purified F-sulfonates were used for palladium-catalyzed cross-coupling reactions to form corresponding biaryl 16 [31] and arylsulfide 17 [32] products, respectively. 

Monosubshtuted hydantoins are a-amino acids cyclically protected at both the carboxyl- and the a-amino group. They can be easily prepared from an aldehyde and isocyanate or by the Bucherer-Bergs synthesis and similar methods. Indeed, the hydantoin synthesis is also a prachcal method for the preparahon of the racemic amino acid. Enzymes belonging to the dihydro-pyrimidinase family hydrolyze hydantoins to the carbamoyl amino acid. The latter can be hydrolyzed in turn to the amino acid by a second enzyme, a carbamoylase. Both enzymes can discriminate between enantiomers and, if their action is cooperative, either the L- or the D-amino acid can be obtained (Scheme 13.10) [36]. What makes the system of special interest is that the proton in the 5-position of the hydantoin ring (it will become the a-hydrogen in the a-amino acid) is considerably more acidic than conventional protons in amino acid esters or amides and much more acidic than the amino acid itself. Thus, the hydantoin can be often racemized in situ at slightly basic pH where the enzymes are stiU stable and active. If these condihons are met. 

A typical way to synthesize a hydantoin core starting from a resin-bound amino acid is shown in Scheme 9.10. Fmoc-amino acid loaded polystyrene resin 77 was deprotected in 20% piperidine in NMP, which then underwent a reductive alkylation process in an NMP solution of 6 equiv of isocyanate (78) and 1 equiv of DIEA for 3 h, affording the urea derivatives 79. Cyclocleavage of 79 was carried out in 10% triethylamine in methanol, shaking for 3h, to give the desired hydantoin ring 80. 

A novel reaction of pyroglutamate (6) and an isocyanate promoted by NaH in THF leads to functionalized hydantoins (7) in good yields. The reaction involves the ring closure of intermediate (8) by a nucleophilic attack on the carbonyl of the ester function followed by expulsion of an alkoxide anion resulting in the formation of the bicyclic intermediate (9). The alkoxide anion in turn can open this bicyclic intermediate with formation of anions (10) and (11) leading to the final racemic hydantoins (7) (Scheme 3).8... 

Moreover, the isocyanate photoproduct was found to undergo hydrolysis at both the isocyanate and adjacent carbonyl groups, producing urea and amide derivatives, respectively.381 The exact position of ring opening at the C-4—C-5 bond was evidenced by the formation of 137 during photolysis of 136 (R = Et, Ph) but the formation of hydantoin derivative 138 by an elimination... 

Addition of 2,5-dihydro-2,2-dimethyl-5,5-bis(propylthio)-l,3,4-oxadiazole in refluxing benzene and an aryl isocyanate releases the bis(propylthio)carbene in situ which then adds easily to the aryl isocyanate to yield a substituted isatin with the ketone functionality protected as a thioacetal (eq 4)7 Ring closure also occurred when the 2,5-dihydro-2,2-dimethyl-5,5-bis(propylthio)-1,3,4-oxadiazole carbene precursor was added to 1-naphthyl isocyanate in refluxing acetonitrile (eq 5)7 Formation of thioacetal protected isatin products are unique to the bis(propylthio)carbene as other nucleophilic carbenes added to aryl isocyanates afforded only modest yields of hydantoin products. ... 

---