Tautomerism and Stereodynamics of Indophenols,Amidines, and Their Derivatives and Analogs: XV.1 Cyclization of N-Benzylidene-N'-R-sulfonyl-o-phenylenediamines to Tetrahydroquinoxalines

Alkylation of N-benzylidene-N'-R-sulfonyl-o-phenylenediamines with phenacyl bromides is accompanied by diastereoselective cyclization to afford tetrahydroquinoxaline derivatives. No cyclization occurs in the alkylation of the same compounds with p-nitrobenzyl bromide or chloroacetamide derivatives because of reduced reactivity of the N-methylene protons.     

Regio- and Stereoselective Synthesis of γ-Alkylidenebutenolides by Cyclization of Dilithiated 1,3-Dicarbonyl Compounds with N,N′-Dimethoxy-N,N′-dimethylethane- diamide

The remarkably simple synthesis of γ-alkylidenebutenolides 3 is achieved by cyclization of the dilithiated 1,3-dicarbonyl compounds 1 with N,N′-dimethoxy-N,N′-dimethylethanediamide ( 2 ). This regio- and stereoselective cyclization provides a route to a wide range of butenolides, which are of pharmacological relevance and of importance for natural product synthesis.     

Quantum chemical study of the transformation of 2-(N-alkylamino)-3-(indol-1-yl)-and 2-(N-alkylamino)-3-(indol-3-yl)maleimides by protic acids: Tandem hydride transfer/cyclization mechanism

The geometric parameters, the charge distribution, and the energetics of N-methyl-2-(N-ethylanilino)-3-(indol-1-yl)-and N-methyl-2-(N-ethylanilino)-3-(indol-3-yl)maleimides and their conjugated acids were studied by density functional theory calculations at the B3LYP/6-31G(d) level. The mechanism of the tandem hydride transfer/cyclization sequence, which occurs after protonation of N-methyl-2-(N-ethylanilino)-3-(indol-1-yl)-and N-methyl-2-(N-ethylanilino)-3-(indol-3-yl)maleimides, was analyzed. The investigation of the potential energy surface for the tandem hydride transfer/cyclization of the iminium cation that formed upon protonation revealed that the hydride transfer followed by intramolecular cyclization at position 7 of the indole fragment in N-methyl-2-(N-ethylanilino)-3-(indol-1-yl)maleimide is the preferable process, unlike alternative intramolecular cyclization involving the cationic center at the C(2) atom of the indole fragment and the benzene ring of the N-ethylaniline fragment of the indoleninium cation in N-methyl-2-(N-ethylanilino)-3-(indol-3-yl)maleimide. A study of the key intermediates of the assumed reaction mechanism demonstrated that these intermediates are actually stationary points on the potential energy surface (minima and transition states). Published in Russian in Izvestiya Akademii Nauk. Seriya Khimicheskaya, No. 12, pp. 2069–2073, December, 2006.     

2,3,5,6-tetramethylmorpholine. VI. Cyclization of N-substituted 3,3′-iminobis-2-butanols

The cyclization of N-substituted 3,3′-iminobis-2-butanols to N-substituted 2,3,5,6-tetramethylmorpholines in sulfuric acid is studied. The ring closure seems to be exclusively a normal S_N2-type substitution with partial inversion of configuration before the cyclization. The steric influence of the N-substituents on the S_N2-reaction and on the inversion is discussed.     

Preparation and characterization of Cu(II)-N-salicylideneanthranilic acids,their reduction products and hydrolysis of the Schiff base

Copper (II) complexes ofN-salicylideneanthranilic acid (I) and its derivatives (II, III) as well as their NaBH₄ reduction products, namelyN-(2-hydroxybenzyl) anthranilic acids (IV–VI) have been prepared and their structures have been determined analytically. Tetracoordinated planar structures of the Cu(II) complexes of the Schiff bases and distorted tetrahedral structures of the Cu(II) complexes of compoundsV–VI have been elucidated by ESR and other spectral methods. During the preparation of the complex the hydrolysis of the Schiff base often takes place in the presence of water giving anthranilates and salicylaldehydates of metals to some extent along with the complexes of the Schiff base. The kinetic data for the hydrolysis ofN-salicylideneanthranilic acid (I) in methanol-water solution also are reported.Presented at the Sixth International Seminar on Inclusion Compounds, Istanbul, Turkey, 27–31 August, 1995.     

Lewis acid assisted cyclization of arylcyanoguanidines to 2,4-diaminoquinazolines

The mild preparation of N-cyano-N-(1-H-indol-5-yl)guanidine and its cyclization to 1,3-diamino-7H-pyrrolo[3,2-f]quinazoline is described. Whereas previously reported methods of cyclization employed high temperatures to effect ring closure, we found that certain Lewis acids, such as boron trifluoride etherate, induce cyclization at moderate temperatures.     

Model Construction for the A–B–C Ring System of Lysergic Acid via Vilsmeier–Haack‐Type Cyclization of 1H‐Indole‐4‐propanoic Acid Derivatives

Vilsmeier–Haack‐type cyclization of 1H‐indole‐4‐propanoic acid derivatives was examined as model construction for the A–B–C ring system of lysergic acid ( 1 ). Smooth cyclization from the 4 position of 1H‐indole to the 3 position was achieved by Vilsmeier–Haack reaction in the presence of K₂CO₃ in MeCN, and the best substrate was found to be the N,N‐dimethylcarboxamide 9 (Table 1). The modified method can be successfully applied to an α‐amino acid derivative protected with an N‐acetyl function, i.e., to 27 (Table 2); however, loss of optical purity was observed in the cyclization when a chiral substrate (S)‐ 27 was used (Scheme 5). On the other hand, the intramolecular Pummerer reaction of the corresponding sulfoxide 20 afforded an S‐containing tricyclic system 22 , which was formed by a cyclization to the 5 position (Scheme 3).     

Unusual Loss of Substituents in the Course of Cyclization of Tetrahydrobilines to Dihydroporphyrins

Metallo‐tetrahydrobiline rac‐ 8 was prepared to investigate its cyclization directed to the formation of N‐confused chlorins. To achieve the site‐directed selectivity of the cyclization, the 2‐position of rac‐ 2 was activated by an electron‐withdrawing cyano function and its 1‐position was blocked by a methyl group. In spite of this provision, the cyclization occurred at the apparently blocked 1‐position with loss or migration of the methyl substituent.     

New Highlights in the Synthesis of 4‐Aryl‐1,4‐dihydropyrazines

The 4‐aryl‐1,4‐dihydropyrazines were prepared via the cyclization of N,N‐bisalkylated anilines with ammonium acetate. These reactions were aided by improvements in the synthesis of N,N‐bisalkylated anilines which were alkylated with anilines using ethyl 2‐diazo acetoacetate in a reaction catalyzed by rhodium acetate in the absence of oxygen. A possible mechanistic route is postulated on the basis of the isolation of the N‐alkylation intermediates, which were determined to be N‐aryloxamates by ¹H NMR data and X‐ray diffraction.     

A Study on the Intramolecular Mitsunobu Reaction of N6‐(ω‐Hydroxyalkyl)adenines

The cyclization of N ⁶‐(ω‐hydroxyalkyl)adenines with a N⁶H‐group leads to N⁶,N1 ring closure regardless of the method of the cyclization that was used. Five‐membered to eight‐membered rings were obtained using NBS/PPh₃; however, under Mitsunobu conditions, the eight‐membered fused purine was not formed. Surprisingly, the cyclization of N ⁶‐methyl‐N ⁶‐(4‐hydroxybutyl)adenine only leads to N⁶,N7 ring closure using both methods.     

Cyclopolymerization. XIX. Effect of N-substituents on cyclopolymerizability of N-allylmethacrylamides

The effect of bulky N-substitutents of N-t-butyl- and N-phenyl-N-allylmethacrylamides (BAMA and PAMA, respectively) on their cyclopolymerizability was investigated. BAMA yielded an almost completely cyclized polymer while the degree of cyclization of poly (PAMA) was about 95%. The latter value indicates that the effect of phenyl group is comparable with that of methyl group, since N-methyl-N-allylmethacrylamide was reported to give a polymer with a degree of cyclization of 93%. Structural investigation on telomerization products of BAMA and PAMA permitted the assignment of the repeating cyclic units of these polymers to that of a five-membered ring. This structural characteristic was also supported by the observation of five-membered cyclized radicals on ESR measurements of these monomers. Rotation around amide C? N bonds of these monomers and related compounds studied by ¹³C-NMR was found to be strongly dependent on N-substitutents. The mechanism of the cyclization was discussed in terms of the structure of the ring formed and rotation around amide C? N bonds of these monomers. The reactivity of the methacryloyl and allyl groups involved in these monomers were compared based on the information obtained by structural investigation of polymers and telomerization products and by ESR studies. © 1993 John Wiley & Sons, Inc.     

Cu–N‐heterocyclic carbene‐catalysed synthesis of 2‐aryl‐3‐(arylethynyl)quinoxalines from one‐pot tandem coupling of o‐phenylenediamines and terminal alkynes

A series of new benzimidazolium chlorides bearing N,N′‐benzyl, 2,4,6‐trimethylbenzyl and 2,4,6‐triisopropylbenzyl substituents have been designed and synthesized from various o‐phenylenediamines. Subsequently, corresponding Cu‐based N‐heterocyclic carbenes (NHCs) were generated in situ in the reaction medium which represents a new application of NHCs exploiting distinct catalytic property towards intermolecular cyclization reaction cascade for the synthesis of 2‐aryl‐3‐(arylethynyl)quinoxalines from o‐phenylenediamines and terminal alkynes. The outcome of the cyclization reaction product depends upon the N,N′‐substituents present on the benzimidazolium chlorides.     

Effects of introduction of α‐carboxylate,N‐methyl,and N‐formyl groups on intramolecular cyclization of o‐quinone amines: Density functional theory‐based study

o‐Quinone amines, which are relevant to various biological processes, can undergo spontaneous intramolecular cyclization (ring closure reaction by amino‐terminated hydrocarbon side chain) that deactivates them toward another possible reactions, that is, thiol binding. Density functional theory‐based calculation is employed for obtaining the potential energy curves along the C? N bond formation in the intramolecular cyclization of various o‐quinone amines, viz., dopaminequinone, dopaquinone, N‐methyl‐dopaminequinone, N‐formyl‐dopaminequinone, and the corresponding methylene‐inserted analogues. The activation barrier is decreased by introduction of α‐carboxylate and N‐methyl group whereas increased by introduction of N‐formyl group. A negative correlation between the activation barriers and the level of highest occupied molecular orbital is pointed out. Furthermore, the methylene‐inserted analogues show decreased activation barriers. This is explained by reduction of steric repulsion in the transition state.     

Synthesis of 1H-imidazo[1,2-a]imidazole

The synthesis and structure analysis of the unknown 1H-imidazo[1,2-a]imidazole ( 1 ) is described. The preparation involves alkylation of 2-aminoimidazole with bromoacetaldehyde diethyl acetal and subsequent hydrolysis and cyclization with hydrochloric acid. The structure was characterized by mass spectrometry and by ¹H-, ¹⁵N- and ¹³C-nmr of 1 and by ¹H-nmr of its 1-benzyl derivative 8 . An independent synthesis of 8 was accomplished via cyclization of 2-(N-dichloroethyl-N-benzyl)aminoimidazole ( 11 ).     

Reactivity of 2‐Methyl‐4H‐3,1‐benzoxazin‐4‐ones and 2‐Methyl‐4H‐pyrido[2,3‐d][1,3]oxazin‐4‐one under Microwave Irradiation Conditions

The reactivity of variably substituted 2‐methyl‐4H‐3,1‐benzoxazin‐4‐ones and 2‐methyl‐4H‐pyrido[2,3‐d][1,3]oxazin‐4‐one towards carbon and oxygen nucleophiles under microwave irradiation conditions was investigated. Optimization of the reaction conditions of oxazinones with carbon nucleophiles led to the synthesis of a series of 4‐hydroxy‐quinolin‐2‐ones and 4‐hydroxy‐1,8‐naphthyridin‐2‐ones in high yields, whereas reaction with a variety of alcohols proceeded smoothly to the formation of the corresponding N‐acetyl‐anthranilates and nicotinates.     

Studies on pyrrolidinones. Synthesis of 1,2,3,5,11,11a-hexahydroindolizino[7,6-b]indole-3,11-dione

Condensation of N-trimethylsilylindole with methyl N-trimethylsilyloxymethylpyroglutamate is the best method to obtain methyl N-indolylmethylpyroglutamate. Friedel-Crafts cyclization of the corresponding acid yields a new ketone (1,2,3,5,11,11a-hexahydroindolizino[7,6-b] indole-3,11-dione).     

A [4+1] Cyclative Capture Approach to 3H‐Indole‐N‐oxides at Room Temperature by Rhodium(III)‐Catalyzed C?H Activation

The rhodium(III)‐catalyzed [3+2] C H cyclization of aniline derivatives and internal alkynes represents a useful contribution to straightforward synthesis of indoles. However, there is no report on the more challenging synthesis of pharmaceutically important N‐hydroxyindoles and 3H‐indole‐N‐oxides. Reported herein is the first rhodium(III)‐catalyzed [4+1] C H oxidative cyclization of nitrones with diazo compounds to access 3H‐indole‐N‐oxides. More significantly, this reaction proceeds at room temperature and has been extended to the synthesis of N‐hydroxyindoles and N‐hydroxyindolines.     

A [4+1] Cyclative Capture Approach to 3H‐Indole‐N‐oxides at Room Temperature by Rhodium(III)‐Catalyzed CH Activation

The rhodium(III)‐catalyzed [3+2] C? H cyclization of aniline derivatives and internal alkynes represents a useful contribution to straightforward synthesis of indoles. However, there is no report on the more challenging synthesis of pharmaceutically important N‐hydroxyindoles and 3H‐indole‐N‐oxides. Reported herein is the first rhodium(III)‐catalyzed [4+1] C? H oxidative cyclization of nitrones with diazo compounds to access 3H‐indole‐N‐oxides. More significantly, this reaction proceeds at room temperature and has been extended to the synthesis of N‐hydroxyindoles and N‐hydroxyindolines.     

Cyclopolymerization. II. Mechanism of the free-radical polymerization of N-n-propyldimethacrylamide

The mechanism of cyclopolymerization was investigated by using N-n-propyldimethacrylamide (PDMA). Completely cyclized polymers were formed on polymerization of PDMA by a radical initiator. Moreover, those copolymers of PDMA and various monomers, such as styrene, methyl methacrylate, and vinyl acetate, obtained did not contain any detectable pendent double bonds. The kinetic investigation showed that the termination reaction proceeded between the cyclized radicals. The attempted polymerization of N-n-propyl-N-isobutyrylmethacrylamide, the monofunctional counterpart of PDMA, was failed. These results appear to confirm that cyclopolymerization of PDMA proceeds through a concerted mechanism which has been proposed for the mechanism of the cyclopolymerization of various difunctional monomers. Measurement of the ESR spectra of propagating radical has, however, revealed that the rate-determining step of the cyclopolymerization of PDMA is not intermolecular propagation but intramolecular cyclization, which indicates that the cyclization reaction proceeds in a stepwise way. This apparent contradiction was explained based upon thermodynamic considerations.     

Electrophilic amination reactions with 1H-indazole-3-carboxylates: Synthesis of amino acid frameworks and 3-amino-2-oxindoles

Reaction of 1-sulfonylindazole-3-carboxylates with various Grignard reagents effects the N-N bond cleavage of the hydrazone moiety with the first nucleophile and the subsequent N-alkylation gives N,N-dialkylation products in good yields. A new strategy for the synthesis of α-(2-arylsulfonamide)phenylglycine, a precursor to tissue factor/factor VIIa inhibitors is also described. Moreover, the synthesis of quaternary 3-aminooxindoles is developed, utilizing this N,N-dialkylation reaction, followed by intramolecular cyclization/nucleophilic addition reaction.