Studies on arylhydrazonoisoxazolinethiones. Behaviour of 4-arylhydrazono-3-phenyl-2-isoxazoline-5-thiones toward hydrazines,grignard reagents and alkylating agents

The 4-arylhydrazono-3-phenyl-2-isoxazoline-5-thiones 2 react with hydrazines to yield the 5-hydrazones 3 and 5 . The reaction of 2 with Grignard reagent resulted in addition of the reagent to the thiocarbonyl group to yield 7 . Treatment of 2 with diazomethane effected S - and N -methylation beside 1,2,3-triazole derivative 11 obtained through isomerisation. The potassium salt of 2 react with alkyl halides to yield the S-alkyl derivatives 12 .     

The reaction of 4-(p-nitrobenzyl)pyridine with some electrophiles

The nucleophile 4-(p-nitrobenzyl)pyridine was allowed to react with four carcinogenic alkylating agents, chloromethyl methyl ether, bis(chloromethyl) ether, glycol sulfate and propane sultone, one carcinogenic acylating agent, N,N-dimethylcarbamyl chloride, and one noncarcinogenic electrophile, perchlorocyclobutenone. The structures of the major products formed, which are substituted pyridinium salts or 1,4-dihydropyridines, were determined.     

REACTIONS OF DITHIOLETHIONES WITH N,N-DICHLOROAMIDES

Abstract

Dependent on the starting materials and the reaction conditions N,N-dichloroamides Cl₂N-X (X = COaryl, CO₂alkyl, SO₂aryl, SO₂N(alkyl)₂) react with dithiolethiones 1 and 5 to N-(dithiolyliden)amides 2, 6, S-(dithiolylidene)sulfimides 3, thionoxides 7 and dithiolones 4, 8. The mechanisms have been studied.     

Synthesis of trichloromethylpyrimidines and trichloromethylpyrimido [4,5-<Emphasis Type="Italic">d</Emphasis>]pyrimidines from alkyl 2-(diaminomethylidene)-3-oxobutyrates and trichloroacetonitrile

Heterocyclization of alkyl 2-(diaminomethylidene)-3-oxobutyrates with trichloroacetonitrile yields alkyl 4-mino-6-methyl-2-trichloromethylpyrimidine-5-carboxylates. The latter compounds react with aryl isocyanates to produce the corresponding pyrimidinylureas, which undergo cyclization to 3-aryl-5-methyl-7-trichloromethylpyrimido[4,5- d]pyrimidine-2,4(1H,3H)-diones under the action of MeONa in MeOH.     

Regio‐ and stereoselective synthesis of isoxazolidine derivatives by asymmetric 1,3‐dipolar cycloaddition reaction of chiral nitrones with 1‐propene‐1,3‐sultone

Asymmetric 1,3‐dipolar cycloadditions of chiral nitrones to 1‐propene‐1,3‐sultone ( 1 ) were investigated. Chiral nitrones 6a‐e reacted with sultone 1 in toluene at 90 °C for 24‐36 h to give the corresponding isoxazolidines in moderate yields with high regioselectivities and stereoselectivities. The diastereoselectivity of this reaction varied with the choice of dipolarophile and the steric demands of nitrones. When sultone 1 was allowed to react chiral nitrone 6e , a much better diastereoselectivity of up to 5.1:1 was observed.     

Reactions of Alkyl 1H,1H-Perfluoroalkyl Sulfones with Ammonia, Amines, and Hydrazines

2,2,3,3-Tetrafluoropropyl and 2,2,3,3,4,4,5,5-octafluoropentyl alkyl sulfones react with ammonia, primary and secondary amines, hydrazine hydrate, phenylhydrazine, and N,N-dimethylhydrazine to afford, depending on the length of the polyfluoroalkyl chain and reaction conditions, the corresponding enamines, imines, or mono- and bis-hydrazones. The bis-hydrazone obtained from phenylhydrazine and 2,2,3,3,4,4,5,5-octafluoropentyl benzyl sulfone is capable of undergoing further dehydrofluorination to give 5-difluoromethyl- or 5-unsubstituted 1-phenylpyrazole.     

The synthesis of P-chiral optically pure phosphorothioates,phosphorotrithioates, phosphoroselenothioates,methanephosphonothioates, and methylphenylphosphinothioates

Enantiomers of representative alkyl esters of phosphorothioic ( 7 ), phosphorodithioic ( 6 ), phosphorotrithioic ( 11 ), phosphoroselenothioic ( 9 ), methanephosphonothioic ( 28 ), methanephosphonodithioic ( 25 ), and methylphenylphosphinothioic ( 31 ) acids were prepared from corresponding pure diastereoisomers of N-[R(+)- or S(-)-α-methylbenzyl] phosphamidochalcogenates (e.g. 2 , 3 , 12 , 17 , 23 , 26 , and 30 ) via PN → PX conversion, which has been proved to proceed with full retention of configuration at phosphorus.     

Reactions with 1.3 propane sultone for the synthesis of cation-exchange membranes

For several reasons it is interesting for membrane technology to introduce strongly anionic groups in membranes. Therefore the possibilities of 1.3 propane sultone were studied to modify cellulose, cellulose acetate and polyacrylonitrile.The results showed that cellulose and cellulose acetate could be modified by a direct reaction of 1.3 propane sultone with the available hydroxyl groups. The nitrile groups in polyacrylonitrile had to be reacted first with hydrogen sulphide to give reactive thioamide groups, able to react with the sultone. These results give evidence for 1.3 propane sultone being a useful chemical for modification of polymers, its carcinogenic properties will however prevent applications.     

Study on 1,3,5‐Triazine Chemistry in Dehydrocondensation: Gauche Effect on the Generation of Active Triazinylammonium Species

The reaction of 2‐chloro‐4,6‐dimethoxy‐1,3,5‐triazine (CDMT) with various nitrogen‐containing compounds, particularly tertiary amines (tert‐amines), has been studied for the preparation of 2‐(4,6‐dimethoxy‐1,3,5‐triazinyl)trialkylammonium salts [DMT‐Am(s)]. DMT‐Ams derived from aliphatic tert‐amines exhibited activity for the dehydrocondensation between a carboxylic acid and an amine to form an amide in a model reaction. Based on a conformational analysis of DMT‐Ams and tert‐amines by NMR and X‐ray diffraction methods, we concluded that a β‐alkyl group maintained in a gauche relationship with the nitrogen lone pair of tert‐amines significantly hinders the approach of CDMT to the nitrogen. Thus, trimethylamine and quinuclidine without such alkyl groups readily react with CDMT whereas triethylamine, possessing two or three such gauche β‐alkyl groups in the stable conformations, does not react at all. The theory of “gauche β‐alkyl group effect” proposed here provides useful guidelines for the preparation of DMT‐Ams possessing various tertiary amine moieties. An investigation of the dehydrocondensation activity of tert‐amines in a CDMT/tert‐amine system that involves in situ generation of DMT‐Am, showed that the gauche effect of the β‐alkyl group becomes quite pronounced; the yield of the amide decreases significantly with tert‐amines possessing an unavoidable gauche β‐alkyl group. Thus, the tert‐amine/CDMT systems are useful for judging whether tert‐amines can readily react with CDMT without isolation of DMT‐Ams.     

Alkylative amination of non-enolizable aldehydes with alkyl (dialkyl-amino)titanium derivatives Preliminary Communication

The readily available tris (diethylamino)methyltitanium and related compounds (see 1 in Scheme 2) react with non-enolizable aldehydes to give tertiary amines 2 ; these amines result from direct replacement of the carbonyl O-atom by an alkyl and an amino group (Scheme 3). A tentative mechanism is proposed, according to which the amino group is transferred to the carbonyl C-atom prior to the alkyl group (Scheme 4).     

Interaction of zinc enolates prepared from 1-aryl-2,2-dibromoalkanones and zinc with alkyl 3-oxo-1,3-dihydrobenzo[<Emphasis Type="Italic">c</Emphasis>]oxepine-4-carboxylates

Zinc enolates obtained from substituted 1-aryl-2,2-dibromoalkanones and zinc react with alkyl 3-oxo-1,3-dihydrobenzo[c]oxepine-4-carboxylate to give the alkyl 1-alkyl-1-aroyl-2-oxo-4,8b-dihydro-1H-3-oxabenzo[a]cyclopropa[c]cycloheptene-1a-carboxylate.     

Reactions of Zinc Enolates of Substituted 1-Aryl-2,2-dibromobutanones with Alkyl Esters of 3-Oxo-3H-benzo[f]chromene-2-carboxylic Acid

Zinc enolates derived from substituted 1-aryl-2,2-dibromobutanones react with alkyl 3-oxo-3H-benzo[f]chromene-2-carboxylates to form alkyl 1-aroyl-1-ethyl-2-oxo-1,9c-dihydro-3-oxacyclopropa[c]phenanthrene-1a-carboxylate as a single geometric isomer.     

1H, 13C and 15N NMR observations on the protonation of 1- and 3-deazapurine

Using ¹H, ¹³C and ¹⁵N NMR it has been concluded that 3-deazarpurine protonates exclusively at N-1 with a pK of about 5.6. The base exhibits rapid tautomerism with proportions of 70:30, with the N–7-H tautomer in the majority. The salt exists predominantly as the N-7-H tautomer. 1-Deazapurine protonates essentially in a 1:1 ratio at N-3 and at the imidazole ring, with a pK of about 3.1. This base also exhibits rapid tautomerism with proportions of 30:70, this time with the N-9-H in the majority. The salt also exists in a tautomcric mixture with approximately equal proportions. One form has N-3 and N-9 bearing hydrogens and the other has N-7 and N-9 bearing hydrogens.     

Alkyl 3-fluoroalkyl-3-oxopropionates in reactions with azolyldiazonium salts

Alkyl 3-fluoroalkyl-3-oxopropionates react with antipyrinyldiazonium chloride to form 2-antipyrinylhydrazono-3-fluoroalkyl-3-oxopropionates. The use in these reactions of hetaryldiazonium salts, containing NH group in the α position, leads to alkyl 7-fluoroalkyl-7-hydroxy-4,7- dihydroazolo[5,1-c]triazine-6-carboxylates. 3-Amino-1H-1,2,4-triazole, 3-amino-4-ethoxycar- bonyl-1H-pyrazole, and 5-amino-4-ethoxycarbonyl-1H-imidazole were used as the heterocyclic component. Published in Russian in Izvestiya Akademii Nauk. Seriya Khimicheskaya, No. 3, pp. 599–603, March, 2008.     

Stereospecific Synthesis of 2-Oxazinyl-4-oxoazetidinecarbamates Starting from a 1,2-Diazepine. A new type of intramolecular transbenzoylation

Azeitidinodiazepines 4b and 4c react with acylnitroso dienophiles 5a–c , specifically from their convexe α-side, but in a non-regiospecific way, leading thereby stereospecifically to the expected adducts 6a–d and 7a–d . The three-dimensional structures of 6a and 7a were determined by X-ray analyses which corroborated their NMR data. OsO₄ cis-glycolization occurred in good yield with the inverse adducts 7a and 7e and led to the rearranged products 10 . These latter ones result from an intramolecular N- to O-transbenzoylation of the short-lived intermediates 9 followed by fragmentation of the animal function. X-Ray analysis of 7a showed the N(10) atom to be pyramidal, a result which demonstrates that it does not have any pronounced benzamide character; otherwise no such N- to O-transbenzoylation would have taken place. Structure and relative configuration of 10a were ascertained by X-ray analysis which confirmed its NMR data as well as the stereochemical outcome of its formation.     

Über Reaktionen von Alkylbiguaniden mit Benzoin beimpH der Biguanidbasen

Summary Alkylbiguanides2 a–e react with benzoin (1) at thepH of the base in different ways.1 undergoes in presence of2 a, c oxidation to benzoic acid which reacts with the bases2 a, c to yield 4-phenyl-1,3,5-triazinamines3 c, 4 c; in presence of2 b 1 is transformed to benzil, which reacts with2 b under rearrangement to yield 1-(4-oxo-5,5-diphenyl-2-imidazolin-2-yl)-3,3-dimethylguanidine (5 b). However, the cycloalkylbiguanides2 d, e, react in presence of nitrogen as well as oxygen with1 to yield piperidine-1-[N-(4,5-diphenylimidazol-2-yl)-carboxamidine] (7 d), resp. morpholine-4-[N-(4,5-diphenylimidazol-2-yl)-carboxamidine] (7 e). The structure of7 e was established by means of an X-ray structure analysis. All proton- and carbon resonances were assigned on the basis of 2-dimensional NMR data.

     

Nitrene insertion reactions. Part III. The steric effect of the Isopropyl and t-butyl groups. 1,6 Type cycloaddition of tetracyanoethylene to 1H-azepines

Various alkyl and aryl carboxynitrenes generated thermally from the azidoformates react with para-di-t-butylbenzene with a high degree of selectivity to yield predominantly, or exclusively, 3,6-di-t-butylazepine-N-carboxylates. 3,6-Dialkylazepines react readily with tetracyanoethylene to afford the first known TCNR-1H-azepine cycloadducts of the 1,6 type.     

Zur Synthese 3,5,6-substituierters-Triazin-2,4-dione

The reaction of N-(2-pyridyl)-carbaminates (3), 1-phenyl-3-(2-pyridyl)-urea (5 a) or alkyl and aryl substituted pyridopyrimidinediones (2) synthesized from 2-amino-pyridine with arylisocyanates (4 a, b) yields 3-aryl substituted pyrido-[1,2-a]-s-triazine-2,4-diones (1). 2-Aminopyridine and azamalonic derivatives (ethoxycarbonyl isocyanate, ethyl iminodicarboxylate) react to give the 3-unsubstituted triazine system (1 c). The isolation of monocyclic triazinediones obtained from the reaction of N-phenylbenzamidine (9) with aryl isocyanate (4 a) or ethoxycarbonyl isocyanate failed because of hydrolytic ring opening. The mechanism of the reaction of 3-substituted pyrido-pyrimidinediones (2) and phenyl isocyanate (4 a) is discussed.     

SYNTHESIS,SPECTRAL STUDIES,AND ANTIMICROBIAL ACTIVITIES OF [N-(UN)ALKYLATED-2-ARYLINDOL-3-YL]THIOCARBOXAMIDES

A series of [N-(un)alkylated-2-arylindol-3-yl]thiocarboxamides(6) have been synthesized by the condensation of alkyl [N-(un)alkylated-2-arylindol-3-yl]dithiocarboxylates (5) with appropriate secondary amines in absolute alcohol. Compound 5 was prepared by the reaction of N-(un)alkylated-2-arylindoles with carbon disulphide in the presence of potassium-t-butoxide followed by alkyl iodide under nitrogen atmosphere. All of the compounds have been characterized on the basis of their elemental and spectral data and have been screened for their antibacterial and antifungal activities. Some of the synthesized compounds have shown promising activity.     

Reactions of 1-Aryl-2,2-dibromobutan-1-ones with Zinc and Alkyl 6-Bromo-2-oxo-2-H-chromen-3-carboxylate

Zinc enolates formed from 1-aryl-2,2-dibromobutan-1-ones and zinc react with alkyl 6-bromo-2-oxo-2-H-chromen-3-carboxylates affording alkyl 1-aroyl-6-bromo-2-oxo-1-ethyl-1,7b-dihydrocyclopropa[c]-chromen-1a(2H)-carboxylates as a single isomer.