An Efficient Synthesis of Highly Optically Active 4-Substituted-2（5H）-furanones from Chiral 3-Bromo-2（5H）-furanone

Highly optically active 4-substituted-2(5H)-furanones 6a-6j were obtained in good yields with de≥98% by the tandem Michael addition/elimination reaction of chiral 3-bromo-2(SH)-furanone (4a), which was conveniently prepared starting from 2-furaldehyde under mild conditions. The products were identified on the basis of their satisfactory elemental analysis and spectroscopic data of IR, UV, ^1H NMR, ^13C NMR and mass spectra. The stereochemistry and absolute configuration of this type of compounds were established by the X-ray crystallographic study. The reaction provided a short and efficient synthesis of the interesting highly optically active 4-subsdtuted-2(5H)-furanones containing an active pyrimidine and a purine base group.     

Synthesis of some isomeric 4-ethoxycarbonyl-3-and 5-(1- and 2-hydroxyalkyl)-1,3- and 1,5-dimethylpyrazoles from 3-(2H)furanones and 2,3-dihydro-4-pyrones

The title compounds were prepared by reaction of 3-(2H)furanones and 2,3-dihydro-4-pyrones with methylhydrazine or alternatively by methylation of the corresponding N-unsubstituted pyrazoles. ¹³C and ¹H nmr were used to assign the isomeric 3-methyl or 5-methyl structures.     

3(2H)Furanone derivatives. Ring-chain tautomerism in the 1,3,4,6-tetraketone series

Ring-chain tautomeric equilibria in the 1,3,4,6-tetraketone series 1 have been examined and the identification of the chain-form 2 and hydroxyfuranone 3 has been accomplished from ¹H-nmr spectra; the relative contribution of the two depends on the structure and also on the solvent. Conversions of 1 into 3(2H)furanones 4 and 5 involving the cyclic tautomer 3 are described.     

Synthesis of 4‐halo‐2 (5H)‐furanones and their suzuki‐coupling reactions with organoboronic acids. A general route to 4‐aryl‐2 (5 H) ‐furanones

4‐Halo‐2(5H)‐furanones were prepared by the halolactonization of 2,3‐allenoic acids. The subsequent Suzuki coupling reaction of 4‐halo 2(5H)‐furanones with aryl boronic acids was carried out to produce 4‐aryl‐2(5H)‐furanones in excellent yields.     

Facile Synthesis of 3(2H)‐Pyridazinones and 2(3H)‐Furanones of Anticipated Biological Activities

3‐Aroyl‐2‐arylpropionic acids 2a‐e were utilized to synthesize 3(2H)‐pyridazinones 3a‐e and 2(3H)‐furanones 6 through reaction with hydrazine hydrate and freshly distilled acetic anhydride, respectively, in the hope of obtaining new 3(2H)‐pyridazinones with no ulcerogenic side effect or with negligible general side effects as those currently used NSAID_S as well as biologically active 2(3H)‐furanones.     

General synthesis of: 5-substituted-3-acyl-4-carbethoxypyrazoles 3,6-subslituted-5-carbethoxy-4(h)pyridazinones and 3,7-substitutedpyrazoio[3,4-d] pyridazine-4(5h)ones via reactions between 2-hydroxy,methoxy, and acetoxy-3(2h)furanones and hydrazine

Synthesis of substituted 3-acyl-4-carbethoxypyrazoles, 5-earbethoxy-4(1H)pyridazinones and pyrazolo[3,4-d]pyridazine-4(5H)ones is described. They involve the reaction of the 2,5-substituted-4-earbelhoxy-2-hydroxy, methoxy and acetoxy-3(2H)furanones with hydrazine hydrate. The reaction was found to be dependent on the hydroxy, methoxy or acetoxy substituents of these furanones and proceeds with ring opening followed by cy clisation. Pyrazoles were formed with hydroxy or methoxy substituents while pyridazinones are afforded with acetoxy group. The pyrazoles so formed were readily converted to pyrazolo[3,4-d] pyridazinones by condensation with excess hydrazine.     

Behavior of 3(2‐pyridinylmethylene)‐5‐aryl‐2(3H)‐furanones and 3(3‐pyridinylmethylene)‐5‐aryl‐2(3H)‐furanones as alkylating agents: A comparative study

3(2‐pyridinylmethylene)‐5‐aryl‐2(3H)‐furanones and 3(3‐pyridinylmethylene)‐5‐aryl‐2(3H)‐furanones were prepared as a mixture of (E) and (Z) stereoisomers by condensing pyridine‐2‐carboxaldehyde and pyridine‐3‐carboxaldehyde with 3‐aroylpropionic acids. The reaction of the furanones 6 and 7 with anhydrous aluminium chloride in benzene led to the formation of 4,4‐diaryl‐1‐(2‐pyridinyl)but‐1,3‐diene ( 8 ) and 4,4‐diaryl‐1‐(3‐pyridinyl)but‐1,3‐diene ( 9 ) as mixtures of geometrical (E,E‐ and E,Z‐) stereoisomers via an intermolecular alkylation mode. When the reaction was carried out in tetrachloroethane as a solvent, the reaction of 6 gave 5‐arylquinoline‐7‐carboxylic acid via intramolecular alkylation mode. This may be considered as a novel method for the synthesis of quinoline derivatives. J. Heterocyclic Chem., (2011).     

Synthesis of some 3-acetyl-5-arylmethyl- or arylaminomethyltetronic acids from 4-ethoxycarbonyl-3-(2H)furanone precursors

The synthesis of a series of tetronic acids was accomplished by ring opening of new 4-ethoxycarbonyl-3(2H) furanones.     

Synthesis of some 3-EthoxycarbonyI-5-hydroxy-4-oxo-2-pyrroline derivatives from 3(2H)furanones

A number of 3-ethoxycarbonyl-5-hydroxy-2-methyl-5-or-1,5-substituted 4-oxo-2-pyrrolines have been prepared, respectively, by the action of ammonium hydroxide or primary aliphatic amines on 2-arylidene or 2-N-acetyl-N-arylaminomethylene-4-ethoxycarbonyl-5-methyl-3(2H)furanones. The structures of these prepared compounds have been determined by spectroscopic data and chemical means.     

Behavior of 3‐benzylamino‐5‐aryl‐2(3H)‐furanones towards some nitrogen nucleophiles

Ring closure of 2‐N‐benzylamino‐3‐aroylpropionic acids ( 3 ) with acetic anhydride afforded 3‐N‐benzylamino‐5‐aryl‐2(3H)‐furanones ( 4 ). The reaction of the furanones ( 4 ) with benzylamine in benzene was found to be time dependent. Thus refluxing the reaction mixture for 1 h only afforded the open‐chain amides ( 5a‐c ). When the reaction was conducted for 3 h the 2(3H)‐pyrrolones ( 6 ) were obtained. Hydrazine hydrate affected ring opening of the furanones to give the hydrazides ( 5d‐f ). Also, semicarbazide converted ( 4 ) into the corresponding semicarbazide derivatives ( 5g‐i ). The hydrazides ( 5d‐f ) were reacted with benzoyl chloride to give the corresponding diaroylhydrazines ( 5j‐l ). The open‐chain derivatives ( 5 ) were converted into a variety of heterocycles: isothiazolones ( 7 ), dihydropyridazinones ( 8 ), 1,3,4‐oxadiazoles ( 9 ) and 1,2,4‐triazole derivatives ( 10 ) via cyclization reactions.     

Substituted-γ-lactones. XXIX. N-heterocycles via photolysis or thermolysis of 3-(2-azidophenylmethylene)-4,5-dihydro-2-(3H)furanone

The thermolysis and/or photolysis of 3-(2-azidophenylmethylene)-4,5-dihydro-2-(3H)furanone offers a preparatively useful way towards the synthesis of indoles and quinolines. This method is superior over previously published methods which afforded these heterocycles in poor yields by the deoxygenative cyclization of 3-(2-nitrophenyImethylene)-4,5-dihydro-2-(3H)furanones. J. Heterocyclic Chem., 15 , 703 (1978)     

Synthesis of 2(5H)‐Furanone Derivatives with Bis‐1,2,3‐triazole Structure

A series of new chiral 2(5H)‐furanone derivatives containing bis‐1,2,3‐triazole moiety were designed and synthesized from (5S)‐5‐alkoxy‐3,4‐dihalo‐2(5H)‐furanones 1 , dicarboxyl amino acids 2 , propargyl bromide, and organic azides 5 under mild conditions via the sequential three steps, including asymmetric Michael addition‐elimination, substitution and no‐ligand click reaction. Twelve new intermediates, including N‐[5‐alkoxy‐2(5H)‐furanonyl] dicarboxyl amino acids 3 and their corresponding propargyl esters 4 , and twelve target molecules 6 were characterized by FTIR, ¹H NMR, ¹³C NMR, MS and elemental analysis. The influences of different synthetic conditions and substrates in each step were investigated. The research provides a new method and idea for the synthesis of 2(5H)‐furanone compounds with polyheterocyclic structure due to the diversities of four basic unit molecules.     

Esters as Radical Acceptors: β‐NHC‐Borylalkenyl Radicals Induce Lactonization by C−C Bond Formation/Cleavage on Esters

Substituted propargyl acetates are converted into 4‐boryl‐2(5H)‐furanones upon thermolysis in the presence of an N‐heterocyclic carbene borane (NHC‐borane) and di‐tert‐butyl peroxide. The acetyl methyl group is lost during the reaction as methane. Evidence suggests that the reaction proceeds by a sequence of radical events including: 1) addition of an NHC‐boryl radical to the triple bond; 2) cyclization of the resultant β‐borylalkenyl radical to the ester carbonyl group; 3) β‐scission of the so‐formed alkoxy radical to provide the 4‐boryl‐2(5H)‐furanone and a methyl radical; and 4) hydrogen abstraction from the NHC‐borane to return the initial NHC‐boryl radical and methane.     

Phenyliodine(III) Triflate Mediated Synthesis of 5‐Benzoyldihydro‐2(3H)‐furanones

A direct and efficient method for the preparation of 5‐benzoyldihydro‐2(3H)‐furanones was realized by cyclization of 4‐benzoylbutyric acids in the presence of phenyliodine(III) triflate.     

Réactions de Friedel et Crafts de dérivés aromatiques sur les composés dioxo-1,4,2,3-non saturés. IV. Réactions des hydroxy-5-ouchloro-5-diméthyl-3,5- ou diméthyl-4,5-dihydro-2,5-furannones-2

Friedel-Crafts reactions of aromatic derivatives with 1,4-dicarbonyls 2,3-éthylenic compounds. Part IV. Reactions of 5-hydroxy or 5-chloro 3,5-dimethyl or 4,5-dimethyl 2 (5 H) furanones We studied the Friedel-Crafts reactions of 2-(5H)-furanones. In the presence of sulfuric acid and of an aromatic derivative, 5-hydroxy- or 5-chloro-5-methyl-2-(5H)-furanones with one methyl group either in the 3 position, or in the 4 position generally give the corresponding 5-aryl-2-(5H)-furanones, while with aluminium chloride, it is possible to obtain, when a reaction takes place, isomeric 1H-indenecarboxylic acids. However, in a particular case, an addition to the substrate's double bond is observed. The 3-aryl-5-hydroxy-tetrahydrofuran-2-one obtained is methylated in two ways and gives either a cyclic product, or a linear one. In two cases tautomerism between 1H-1-indenecarboxylic acid and 1H-3-indenecarboxylic has been shown by ¹H-NMR.     

Two tetranuclear zinc clusters, [Zn4(μ3‐OEt)2(μ2‐MalO)4Et2] and [Zn4(μ3‐GueO)2(μ2‐GueO)2(μ2‐MalO)2(MalO)2]·2C7H8, containing defective dicubane core geometries (MalOH is maltol and GueOH is guethol)

The zinc alkoxide molecules in di‐μ₃‐ethanolato‐diethyltetrakis(μ₂‐2‐methyl‐4‐oxo‐4H‐pyran‐3‐olato‐κ³O³,O⁴:O³)tetrazinc(II), [Zn₄(C₂H₅)₂(C₂H₅O)₂(C₆H₅O₃)₄], (I), and bis(μ₃‐2‐ethoxyphenolato‐κ⁴O¹,O²:O¹:O¹)bis(μ₂‐2‐ethoxyphenolato‐κ³O¹,O²:O¹)bis(μ₂‐2‐methyl‐4‐oxo‐4H‐pyran‐3‐olato‐κ³O³,O⁴:O³)bis(2‐methyl‐4‐oxo‐4H‐pyran‐3‐olato‐κ²O³,O⁴)tetrazinc(II) toluene disolvate, [Zn₄(C₆H₅O₃)₄(C₈H₉O₂)₄]·2C₇H₈, (II), lie on crystallographic centres of inversion. The asymmetric units of (I) and (II) contain half of the tetrameric unit and additionally one molecule of toluene for (II). The Zn^II atoms are four‐ and six‐coordinated in distorted tetrahedral and octahedral geometries for (I), and six‐coordinated in a distorted octahedral environment for (II). The Zn^II atoms in both compounds are arranged in a defect dicubane Zn₄O₆ core structure composed of two EtZnO₃ tetrahedra and ZnO₆ octahedra for (I), and of four ZnO₆ octahedra for (II), sharing common corners. The maltolate ligands exist mostly in a μ₂‐bridging mode, while the guetholate ligands prefer a higher coordination mode and act as μ₃‐ and μ₂‐bridges.     

Theoretical study of the structure and unimolecular decomposition pathways of ethyloxonium, [CH3CH2OH2]+

Ab initio molecular orbital calculations with split-valence plus polarization basis sets and incorporating valence-electron correlation have been performed to determine the equilibrium structure of ethyloxonium ([CH₃CH₂OH₂]⁺) and examine its modes of unimolecular dissociation. An asymmetric structure (1) is predicted to be the most stable form of ethyloxonium, but a second conformational isomer of C_s symmetry lies only 1.4 kJ mol^?1 higher in energy than 1. Four unimolecular decomposition pathways for 1 have been examined involving loss of H₂, CH₄, H₂O or C₂H₄. The most stable fragmentation products, lying 65 kJ mol^?1 above 1, are associated with the H₂ elimination reaction. However, large barriers of 257 and 223 kJ mol^?1 have to be surmounted for H₂ and CH₄ loss, respectively. On the other hand, elimination of either C₂H₄ or H₂O from ethyloxonium can proceed without a barrier to the reverse associations and, with total endothermicities of 130 and 160 kJ mol^?1, respectively, these reactions are expected to dominate at lower energies. A second important equilibrium structure on the surface is a hydrogen-bridged complex, lying 53 kJ mol^?1 above 1. This complex is involved in the C₂H₄ elimination reaction, acts as an intermediate in the proton-transfer reaction connecting [C₂H₅]⁺ +H₂O and C₂H₄ + [H₃O]⁺ and plays an important role in the isotopic scrambling that has been observed experimentally in the elimination of either H₂O or C₂H₄ from ethyloxonium. The proton affinity of ethanol was calculated as 799 kJ mol^?1, in close agreement with the experimental value of 794 kJ mol^?1.     

Synthesis of 3-(3-Methyl-1-aryl-1H-pyrazol-5-yl)-2H-2-chromen-2-one Derivatives via a One-Pot,Three-Component Reaction

An efficient synthesis of 3-(3-methyl-1-aryl-1H-pyrazol-5-yl)-2H-2-chromen-2-one derivatives by the reaction of salicylaldehydes, 4-hydroxy-6-methyl-2H-pyran-2-one, and arylhydrazine in acetonitrile under reflux condition and in the presence of piperidine is reported. This three-component reaction has some advantages such as ease of handling, good yields, and easy purification. All structures were confirmed by infrared, mass, ¹H NMR, and ¹³C NMR spectroscopy.     

Ringerweiterungen und Ringverengungen bei der Umsetzung von 1, 3-Oxazolidin-2, 4-dionen und 1, 3-Thiazoiidin-2, 4-dion mit 3-Amino-2H-azirinen

Ring Enlargements and Ring Contractions in the Reaction of 1, 3-Oxazolidine-2, 4-diones and l, 3-Thiazolidine-2, 4-dione with 3-Amino-2H-azirines The reaction of 3-amino-2H-azirines 1 and 1, 3-oxazolidine-2, 4-diones 2 in MeCN at room temperature leads to 3, 4-dihydro-3-(2-hydroxyacetyl)-2H-imidazol-2-ones 3 in good yield (Scheme 2, Table 1). A reaction mechanism proceeding via ring enlargement of the bicyclic zwitterion A to give B, followed by transannular ring contraction to C, is proposed for the formation of 3 . This mechanism is in accordance with the result of the reaction of 2a and the ¹⁵N-labelled 1a *: in the isolated product 3a *, only N(3) is labelled (Scheme 1). The analogous reaction of 1 and 1, 3-thiazolidine-2, 4-dione ( 5 ) is more complex (Schemes 4 and 5, Table 2). Besides the expected 3, 4-dihydro-3-(2-mercaptoacetyl)-2H-imidazol-2-ones 7, 5-amino-3, 4-dihydro-2H-imidazol-2-ones of type 8 and/or N-(1, 4-thiazin-2-ylidene)ureas 9 are formed. In the case of 2-(dimethylamino)-1-azaspiro[2. 3]hex-1-ene ( 1d ), the postulated eight-membered intermediate 6d could be isolated. Its structure as well as that of 9f has been determined by X-ray structure analysis. A reaction mechanism for the formation of the 1, 4-thiazine derivatives of type 9 is proposed in Scheme 6.     

Synthesis and Evaluation of 2-{[(2-Oxo-1H-quinolin-8-yl)oxy]methyl}-Substituted α-Methylidene-γ-butyrolactones

O-Alkylation of 8-hydroxy-1H-quinolin-2-one ( 1 ) afforded 8-(2-oxopropoxy)-1H-quinolin-2-one ( 2 ) which was immediately cyclized to form the tricyclic 2,3-dihydro-3-hydroxy-3-methyl-5H-pyrido[1,2,3-de][1,4]benzoxazine,-5-one ( 3). The Reformatsky-type condensation of 3 furnished antiplatelet 8-[(2,3,4,5-tetrahydro-2-methyl-4-methylidene-5-oxofuran-2-yl)melhoxy]-1H-quinolin-2-one ( 4 ). Its counterparts 7a – f , Ph-substituted at C(2) of the furan ring, were obtained from 1 via alkylation and the Reformatsky-type condensation. Although compound 4 was less active against platelet aggregation than 7a – f , it was the only compound which exhibited significant inhibitory activity on high-K⁺ medium, Ca²⁺-induced vasoconstriction and was more active than most of its Ph-substituted counterparts against norepinephrine-induced vasoconstrictions.