Theoretical and experimental study of imine-enamine tautomerism of condensation products of propanal with 4-aminobenzoic acid in ethanol

The tautomerism of the reaction products of propanal with 4-aminobenzoic acid in ethanol was studied by J-modulated spin-echo (JMOD) ¹³C NMR spectroscopy and gradient-enhanced heteronuclear (ge-2D) ¹H–¹³C HSQC spectroscopy. The existence of imine and enamine tautomeric forms of the reduced compounds in solution was established. The tautomeric equilibrium of the condensation product of propanal with 4-aminobenzoic acid in ethanol was found to be shifted toward the imine form. Quantum chemical calculations by the density functional theory (DFT) method demonstrated that the 4-(N-propylidene)aminobenzoic acid molecule forms a stronger hydrogen bond with an ethanol solvent molecule compared to the enamine molecule, resulting in a higher stability of the ethanol adduct of azomethine compared to the adduct of enamine.     

DFT study on the isomerization in vitamin B6

Isomerization and tautomerism reactions of the active form of vitamin B6, pyridoxal phosphate, are studied at B3LYP level of theory using 6-311++G(2df,p) basis set in gas and aqueous phases. Twenty-three transition state (TS) structures for vitamin B6 isomerization are optimized, including 13 TS structures for O–H and C–C rotations, 8 TS structures for imine–enamine tautomerism, and 2 TS structures for keto–enol tautomerism. Activation energy (E _a), imaginary frequency (υ), and Gibbs free energy of activation (ΔG ^#) for the isomerization reactions are calculated. The activation energies of the imine–enamine tautomerism are in the range of 190–280 kJ/mol and of O–H and C–C rotations are mainly less than 60 kJ/mol. Also, our calculation shows that the imine forms of B6 are mainly more stable than the enamine forms. Effect of microhydration on the TS structures and activation energies is also investigated. It is found that the presence of water molecules catalyzes only the imine–enamine tautomerism.     

The oxidation of compounds capable of imine-enamine tautomerism with lead tetraacetate

Compounds capable of imine-enamine tautomerism react preferentially via their enamine tautomer giving a 2-acetoxyaldehyde which equilibrates with the starting imine. This derives from the extra nucleophilicity of the β-carbon of the enamine tautomer. The reaction of the imine isomer to form an aryl- or an alkylnitrenoid species is a minor pathway.     

Imine-enamine tautomerism of tropanone Schiff's bases

Using PMR spectroscopy, we have demonstrated the existence of an imine-enamine tautomerism and optically active forms in tropanone Schiff's bases. We have studied the effect of solvents and substituents on the tautomeric equilibrium of the system. By reaction with acid chlorides, we obtain the N-acylation products of the enamine form of the Schiff's bases.Translated from Khimiya Geterotsiklicheskikh Soedinenii, Vol. 34, No. 3, pp. 381–386, March, 1994.     

Resolution of the enantiomers of tetrahydrozoline by chiral HPLC. The racemization of the enantiomers via an imine–enamine tautomerism

Resolution of the enantiomers of the sympathomimetic drug tetrahydrozoline was obtained by chiral HPLC. The isolated enantiomers racemize easily and chiral HPLC experiments allowed the determination of the racemization rate constant. This process occurs via an imine–enamine tautomerism which was studied by UV and ¹H NMR spectroscopies.     

How to drive imine–enamine tautomerism of pyronic derivatives of biological interest – A theoretical and experimental study of substituent and solvent effects

An investigation of the tautomerism of five series of aminated pyronic compounds of pharmacological interest was carried out using NMR experiments and standard quantum mechanical B3LYP/6-311+G** calculations. The obtained results indicate that among four possible tautomers, imine and enamine forms are the two predominating ones in the gas phase as well as in solution. Depending on the nature of the substituting group, the enamine or the imine form is the most stable tautomer, the calculations being in agreement with experiment. The calculated equilibrium constants in the gas phase and in solution show that the enamine form is stabilized by polar solvents, in all cases. NBO analysis explains well the predominance of a form over another one when changing a substituting group. We give indications on how to favour the imine form which is preferred for synthesis purposes.     

New functionalized pyrazolines from 1-aroyl-2-phenylacetylenes and thiocarbonohydrazides

The reaction of 1-aroyl-2-phenylacetylenes with thiocarbonohydrazide and benzaldehyde thiocarbohydrazone in acetic acid-water or ethanol-water systems with the reagents in an equimolar ratio leads to the selective formation of 1-carbothiohydrazinoyl-5-hydroxy-3-phenyl-5-R-2-pyrazolines. Ring-chain tautomerism involving the enamine and hydrazone forms was detected for solutions of the pyrazolines (with R = 2-thienyl) in DMSO. Dedicated to Academician M. G. Voronkov on his 85th birthday. __________ Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 11, pp. 1655–1661, November, 2006.     

Tautomerism in bis(oxazolines): an experimental and theoretical study of proton transfer in 1,1-bis(4,4-dimethyl-1,3-oxazolin-2-yl)-ethane

The serendipitous isolation of an unusual protonated bis(oxazoline) prompted us to discuss the role of H⁺ on the kinetics and thermodynamics of the equilibrium between its ketimine and enamine forms. X-ray diffraction analysis revealed that the protonated bis(oxazoline) is in the Z-enamine form, the unipositive charge is counterbalanced by [(FeCl₃)₂O]²⁻ and [FeCl₄]⁻ anions. DFT calculation at the BP86/TZVP level showed that relative stability of enamine tautomer versus ketimine tautomer increases with the protonation of the nitrogen atom of the oxazolidine ring. At the same time, the barrier energy of tautomerism decreases.     

Nitrogen bridgehead compounds. Part 35. Structures of α-formyl-2,3-polymethylene-3,4-dihydroquinazolin-4-ones

The structures of the title compounds bearing a five-, six- or seven-membered A ring have been investigated by uv and ¹H and ¹³C nmr spectroscopy. The imine-enol-enamine (I-II-III) tautomerism of these compounds depends greatly on the ring size. A significant solvent-dependence is observed only for the five-membered-ring compounds 1 and 2 , which in ethanolic solution exist predominantly in the imine form I, and in chloroform solution in the enol form II. The compounds with a six-membered A ring, 3 and 4 , are mainly in the enamine form III. On protonation, 3 and 4 change into the E and Z isomeric mixture of the enol tautomer II. The seven-membered-ring compound 5 is a mixture of the imine I and the enamine III tautomers.     

Synthesis of novel 3-(α-arylhydrazono-1,3,4-oxadiazol-2-ylmethyl)-2-oxo-1,2-dihydroquinoxalines and their characteristic tautomerism between the hydrazone imine and diazenyl enamine forms

The reactions of 3-(α-arylhydrazono)hydrazinocarbonylmethyl-2-oxo-1,2-dihydroquinoxalines 1a,b with triethyl orthoesters resulted in the intramolecular cyclization to give the 3-(α-arylhydrazono-1,3,4-oxadiazol-2-ylmethyl)-2-oxo-1,2-dihydroquinoxalines 4a–d , but not the 1,2,4,5-tetrazepinylquinoxalines 5a–d . The cyclization mode into the 1,3,4-oxadiazole ring was confirmed by the alternate syntheses of 4a,c from the reactions of 3-(1,3,4-oxadiazol-2-ylmethylene)-2-oxo-1,2,3,4-tetrahydroquinoxalines 6a,b with o-chlorophenyl diazonium salts, respectively. Moreover, 4a–d exhibited an interesting tautomerism between the hydrazone imine form A and diazenyl enamine form B.     

3-乙氧羰基-2,3/2,5-二氢-1,5-苯并硫氮杂卓的互变异构及其热行为

用核磁共振法研究了3-乙氧羰基-2,3/2,5-二氢-1,5-苯并硫氮杂卓（亚胺型杂卓4/烯胺型杂卓5）在氘代甲醇（CD3OD）、苯（C6D6）、三氯甲烷（CDCl3）和二甲基亚砜（DMSO-d6）四种不同极性溶剂中的互变异构.结果表明,无水条件下,亚胺型杂卓4和烯胺型杂卓5在非质子溶剂中不发生相互转化,而在质子溶剂中,亚胺型杂卓4不稳定,部分转化成其异构体—烯胺型杂卓5;基于杂卓4和5在DMSO和CHCl3中的紫外光谱有良好的区分度,用紫外光谱法研究了在DMSO及CHCl3（低温时）中溶液的温度、酸碱度对其互变异构的影响,发现上述异构体在不同温度下均很稳定,并且对弱酸、弱碱稳定.然而,随着溶液酸性的增强,杂卓4向杂卓5快速转化,而在强碱中两种异构体均发生分解.用TG/DSC技术、Kissinger法和Ozawa-Doyle法考察了上述异构体的热稳定性以及第一步分解过程的非等温动力学,确定了分解反应动力学参数（活化能E和指前因子A）及DTG峰温处的热力学参数（△G≠,△H≠,△S≠）.     

A Multicontrolled Enamine Configurational Switch Undergoing Dynamic Constitutional Exchange

A multiresponsive enamine‐based molecular switch is presented, in which forward/backward configurational rotation around the C=C bond could be precisely controlled by the addition of an acid/base or metal ions. Fluorescence turn‐on/off effects and large Stokes shifts were observed while regulating the switching process with Cu^II. The enamine functionality furthermore enabled double dynamic regimes, in which configurational switching could operate in conjunction with constitutional enamine exchange of the rotor part. This behavior was used to construct a prototypical dynamic covalent switch system through enamine exchange with primary amines. The dynamic exchange process could be readily turned on/off by regulating the switch status with pH.     

Thermal sigmatropic rearrangements of isopyrazoles and pyrazolenines to pyrazoles

Thermal rearrangement of 4-allyl-, 4-dimethylallyl-, and 4-propargyl-isopyrazoles proceed by [3,3]-sigmatropic processes to pyrazoles. The migration terminus is the C(3) Me group, if present, and the rearrangement is preceded by imine-enamine tautomerism. When enamine formation is not possible the rearrangment is diverted to nitrogen. Thermal rearrangements of 4-alkyl- and 4-benzyl-isopyrazoles also occur although at higher temperatures and evidence is presented suggesting [1,5]-sigmatropic processes are involved. Some pyrazolenine to pyrazole rearrangements involving migration of ester and phenyl groups are also reported.     

Nitrogen bridgehead compounds. Part 51 Autoxidation of 9-aminotetrahydro-4H-pyrido[1,2-a]pyrimidin-4-ones. Synthesis and stereochemistry of 9-amino- and 9-hydroxy-6,7-dihydro-4H-pyrido[1,2-a]-pyrimidin-4-ones

In solution the 9-phenylaminotetrahydro-4H-pyrido[1,2-a]pyrimidin-4-ones 1-5 were oxidized into the 9-aminodihydro compounds 15-19 by atmospheric oxygen at ambient temperature. Autoxidation is most probably a free-radical chain process, which takes place with ground-state triplet oxygen via the radical cation of the enamine form. The 9-aminodihydro derivatives were also prepared from 9,9-dibromo compounds 10 and 11 and from 9-hydroxydihydro compounds 12-14 . The 9-hydroxydihydro derivatives, obtained from the 9-amino compounds 16, 19 and 21 by acidic hydrolysis, showed a solvent-dependent and R¹ substituent-dependent oxo-enol tautomerism. The enol form was stabilized by electron-withdrawing R¹ groups and a polar solvent. However, for the 9-aminodihydropyrido[1,2-a]pyrimidines 15-26 only the enamine tautomer (E) could be identified independently of the substituent and the solvent. The chemical structures of the synthesized products were studied by uv, ir, ¹H- and ¹³C-nmr spectroscopy.     

Configurational stability of 9-hydroxyrisperidone. Kinetics and mechanism of racemization

The configurational stability of 9-hydroxyrisperidone, an atypical antipsychotic, was studied under acidic, basic and physiological conditions. The analysis of 9-hydroxyrisperidone was performed using a recently validated chiral capillary electrophoretic method developed using a dual cyclodextrin mode (hydroxypropylated-β-CD and sulfated-α-CD). The kinetic parameters (rate constants, half-lives, and apparent free energy barriers) of the racemization were calculated through a mathematical model of the first-order reaction. The influences of the pH, the temperature, the nature and the concentration of the buffer, and the presence of an organic co-solvent were investigated. The fastest racemizations were observed under acidic conditions with high phosphate buffer concentrations and high temperatures. Under these conditions, the cyclodextrins (β-CD, methyl- β-CD, or hydroxypropylated-β-CD) added to both enantiomers in various molar ratios were not able to retard the racemization. Finally, the mechanism of racemization was investigated using nuclear magnetic resonance (NMR) and the proton–deuterium exchange of the proton H₉ borne by the chiral carbon has proven the presence of an imine–enamine tautomerism.     

Phototransformation products of the alkaloid lappaconitine: Multinuclear NMR study

The NMR technique has been applied to characterize the phototransformation products of the natural alkaloid lappaconitine. It was demonstrated that the photolysis of lappaconitine 1 results in cleavage of the ester bond with elimination of N-acetylanthranilic acid. The final reaction product was found to be an immonium salt 4 of N-acetylanthranilic acid and enamine 3. An equilibrium between the imine cation and the enamine 3 was detected.     

Tautomerism of diazepines fused with pyrimidine rings

The tautomerism of 1,4‐diazepines fused with pyrimidine rings was studied by means of nmr spec‐troscopy, X‐ray analysis and quantum chemical calculations. It was found that in the case of 6,8‐diphenyl‐pyrimido[4,5‐b][1,4]diazepin‐4‐ols (7a ‐ e) the enamine form is more stable than the diimine form. This result is rationalized with the electron‐withdrawing effect of the 4‐hydroxypyrimidine ring and with the formation of intermolecular hydrogen bonds. In contrast to 7a ‐ e , the 6,8‐diaryl‐2,3,4,7‐tetrahydro‐1,3‐dimethyl‐1H‐pyrimido[4,5‐b][1,4]diazepine‐2,4‐diones (9a, c, f) exist in the diimine form.     

Theoretical study of the reaction from 7-alkylidenecephalosporin sulfone to bicyclic intermediates in inhibiting β-lactamase

Density functional theory (DFT) calculations have been performed on the 7-alkylidenecephalosporin sulfone in order to study the mechanism of producing the bicyclic intermediate. The solvent effect was considered via polarizable continuum model (PCM) computations. The results show that in the acyl-enzyme intermediate, the side chain pyridine nitrogen atom attacks the C6 atom, which is followed by cleavage of the C6–S1 bond. The unsaturated C7 is attacked by the leaving sulfinate, and a tricyclic structure yields. This structure is unstable, and the proton is transferred from C6 to the sulfone to yield the bicyclic end product. Besides, the reactant can undergo enamine–imine tautomerism. This suggests the end products have two forms, viz. imine and enamine. Electronic supplementary material  The online version of this article (doi:) contains supplementary material, which is available to authorized users.     

Solvent-assisted catalysis mechanism on Keto–enol tautomerism of cyameluric acid

The keto–enol tautomerism of cyameluric acid, both in gas phase and in water and methanol solution, has been studied at the B3LYP/6-31++g(d,P) level of theory in this paper. The harmonic frequencies of all the structures are calculated. The results show that the transition states of the tautomerism are 4-membered ring conformations in gas phase, whereas 6-membered ring conformations in solution. In the first proton transfer, activation energy ΔE^# is 56.4 and 50.9 kJ/mol for water and methanol solution, respectively, which is much lower than that in gas phase (163.2 kJ/mol). Solvent molecules (water and methanol) produce an important catalytic effect in the tautomerism, especially for methanol-solvated system. NBO analysis shows that there is a strong interaction between cyameluric acid and solvent molecules in transition states. AIM charge analysis indicates that the keto–enol tautomerism shows a certain degree of proton transfer character. From the reaction enthalpy and reaction rate point of view, keto–enol tautomerism in water-solvated and methanol-solvated system is easier than that in gas phase. The keto–enol tautomerisms are endothermic both in gas phase and in solution, so the enol forms are less stable than the keto ones.     

Formaldehyde oxime <--> nitrosomethane tautomerism

Formaldehyde oxime <--> nitrosomethane tautomerism, isomeric nitrone, and their common cations and anions are studied with Gaussian-2 theory using MP2(full)/6-31G geometries and with density functional theory using B3LYP/6-311+G**. Geometrical parameters, harmonic vibrational frequencies, relative stabilities, conformational stabilities, and ionization energies are compared with experimental gas-phase data when available. The formaldehyde oxime <--> nitrosomethane tautomerism is compared with the amide <--> imidol, imine <--> enamine, keto <--> enol, and nitro <--> aci-nitro tautomeric processes. Solvent effects are estimated by the self-consistent isodensity polarizable continuum model (SCIPCM). The influence of hydrogen bonding interactions with the solvent is addressed by including two water molecules. In the final evaluation, formaldehyde oxime is 15.8 kcal/mol more stable than nitrosomethane when the aqueous solvation correction of 3.8 kcal/mol is applied to the G2 energies. Unsolvated formaldehyde oxime is estimated to be 11.1 kcal/mol more stable than nitrone. The estimated gas-phase ionization energies (G2) are 362.5 kcal/mol for formaldehyde oxime, 350.6 kcal/mol for nitrosomethane, and 351.4 kcal/mol for nitrone.