基于多羧酸烟酸配体的镝、钬、铒和铥配合物的合成及荧光、磁学性质的表征

以5-(4-羧基苯氧基)烟酸配体(H₂cpna)和稀土金属离子Dy³⁺、Ho³⁺、Er³⁺和Tm³⁺为原料,采用水热法合成了4种稀土金属配合物[M(Hcpna)(cpna)(H₂O)₃]_n,其中M=Dy(1)、Ho (2)、Er (3)、Tm (4)。单晶X射线衍射分析表明配合物1、2、3和4为同构配合物,均为一维链状结构。通过红外、元素分析以及粉末X射线衍射对所得配合物进行了表征,同时对配合物的荧光和磁学性质开展了研究。荧光测试结果表明,配合物1～4的荧光强度均低于配体H2cpna的荧光强度。在2～300 K温度范围内1 kOe直流电场下测试了配合物1～4的磁性,结果表明配合物1、2、3和4的χ_mT值分别为14.04、14.15、11.08和6.83 cm³·mol^-1·K,与文献理论值相符合。     

Synthesis and Antimicrobial Activity of Some New 1,3-Diphenylpyrazoles Bearing Pyrimidine,Pyrimidinethione, Thiazolopyrimidine,Triazolopyrimidine, Thio-and Alkylthiotriazolop-Yrimidinone Moieties at the 4-Position

1,3-diphenyl-1H-pyrazole-4-carboxaldehyde (1) reacted with ethyl cyanoacetate and thiourea to give the pyrimidinethione derivative 2. The reaction of 2 with some alkylating agents gave the corresponding thioethers 3a–e and 7. Thione 2 was cyclized to 5 and 6 upon a reaction with chloroacetic acid and with benzaldehyde, respectively. Thioether 3c was cyclized to 4 upon boiling with sodium acetate in ethanol, and 7 was cyclized to 8 upon boiling in an acetic anhydride-pyridine mixture. The hydrazino derivative 9 was prepared either by boiling 2 and/or 3a with hydrazine. The reaction of 9 with nitrous acid, acetylacetone, triethyl orthoformate, acetic anhydride, and carbon disulfide gave 10–14. The alkylation of 14 with ethyl iodide, phenacyl bromide, and ethyl chloroacetate afforded the alkythiotriazolo pyrimidinone derivatives 15a–c. The dialkyl derivative 16 was produced upon the treatment of 2 with two equivalents of ethyl iodide. Boiling 16 with hydrazine afforded the hydrazino 17. The reaction of 17 with nitrous acid, carbon disulfide, ethyl cyanoacetate, ethyl acetoacetae, and phenacyl bromide gave 18–22, respectively. Some of the newly obtained compounds were tested for their antibacterial and antifungal activities.     

ALKYLATIOIM,ACYLATION, AND ARYLATION PRODUCTS OF 1-CYANO-ISOTHIOCHROMANE

Abstract

1-Cyano-isothiochromane (1a) can be alkylated in position 1, using the carbanion that is formed from sodium amide, sodium hydride, or n-butyllithium. With methyl iodide or ethyl iodide 1c and 1d are formed; with α-halogenated ether or thioether, 1e and 1f; with propargyl bromide, 1h; with bromo acetophenone, li; and with ethyl chloroacetate, 1k. Similarly, acylation with benzoyl chloride leads to 11, and with 2,4-dinitrofluorobenzene to 1m. The alkylation products of 1a can be oxidized with peracids to the sulfones 2 and with LiAlH₄ reduced to 1-aminomethyl-isothiochroman (3): Acid hydrolysis of 1 gave isothiochromane-1-carboxylic acids, 4, whereas when 1 is treated with hydrogen peroxide in alkaline medium the S-dioxide and the S-oxide acid amides, 5 and 6 respectively, are formed.     

Nouvelle Synthese Des 2-Thioxoethylphosphonates, 2- mercaptovinylphosphonates, 2-Phosphoryl-3-thioxopropanoates, 2-Thiomethylvinylphosphonates, 2-Thioethoxycarbonylmethylvinylphosphonates

The cyanomethylphosphonates 1 and the ethyl phosphoacetates 2 were reacted with some fluorophenylisothiocyanates to give the 2-thioxoethylphosphonates 3 in tautomeric equilibrium with the corresponding 2-mercaptovinylphosphonates 3 ′ and the 2-phosphoryl-3-thioxopropanoates 4 , respectively. Reaction of the cyanomethylphosphonates 1 with fluorophenylisothiocyanates in presence of methyliodide furnished the 2- thiometylvinylphosphonates 5 . The 2-mercaptovinylphosphonates 3 ′ reacted with ethyl chloroacetate in refluxing ethanol in the presence of triethylamine to give S-substitued derivatives 6 .     

Synthesis of new triazoloquinoxalines,pyrroloquinoxalines, and pyrimidopyrroloquinoxalines

Summary When 2-hydroxyquinoxaline-3-carboxamide (1) was reacted with POCl₃ inDMF, 2-chloro-3-dimethylaminomethylenecarboxamide (2) was obtained. The chloro compound2 was reacted with thiourea and hydrazine hydrate to give the corresponding mercapto and hydrazino derivatives3 and8, respectively. On the other hand, 2-chloroquinoxaline-3-carbonitrile (13) reacted with ethyl glycinate to the glycinate derivative14 which was cyclized to pyrroloquinoxaline15 by heating with sodium ethoxide. Pyrimidopyrroloquinoxaline derivatives16 and17 were obtainedvia the reaction of15 with formamide and phenyl isothiocyanate, respectively.

---

Synthese neuer Triazolochinoxaline, Pyrrolochinoxaline und Pyrimidopyrrolochinoxaline

Zusammenfassung Wenn man 2-Hydroxychinoxalin-3-carboxamid (1) mit POCl₃ inDMF reagieren läßt, erhält man 2-Chlor-3-dimethylaminomethylencarboxamid (2). Die Chlorverbindung2 wurde mit Thioharnstoff und Hydrazinhydrat zu den entsprechenden Mercapto- und Hydrazinderivaten3 und8 umgesetzt. Aus 2-Chlorchinoxalin-3-carbonsäurenitril (13) und Ethylglycinat erhält man14, das durch Erhitzen mit Natriumethylat zum Pyrrolochinoxalin15 cyclisiert wurde. Die Pyrimidopyrrolochinoxalinderivate16 und17 wurden durch Reaktion von15 mit Formamid bzw. Phenylisothiocyanat erhalten.

     

Prearranged Glycosides,Part 10. Intramolecular Glycosylation with Cellobiosyl,Lactosyl, and Maltosyl Donors

ABSTRACT

Acetyl protected 1,2-O-(1-methoxyethylidene)-disaccharides 1 of maltose, cellobiose, and lactose, respectively were converted via the corresponding benzyl protected couterparts 2, the benzyl protected phenyl 2-O-acetyl- 3 and 2-O-unprotected 1-thio-glycoside disaccharides 4 into 2-O-succinoylated disaccharides 5. The latter were esterified with benzyl 2-O-benzoyl-4,6-di-O-benzylidene-α-D-glucopyranoside (6) to afford succinyl linked derivatives 7 the benzylidene groups of which were regioselectively opened to give prearranged glycoside trisaccharides 8. Intramolecular glycosylation of the latter with N-iodosuccinimide resulted in exclusive formation of the corresponding α-(1→4)-linked trisaccharides 9. No influence of the donor moiety on the diastereoselectivity of the intramolecular glycosylation was observed.     

A Convenient Route to 1,3,4-Thiadiazoles,Thiazolidinone, Thiazoles,Pyridones, Coumarins,Triazolo[5,1-c]triazines,and Pyrazolo[5,1-c]triazines Incorporating Pyrazolone Moiety and Their Use as Antimicrobial Agents

Condensation of 4-acetyl-5-methyl-2-phenyl-2,4-dihydropyrazol-3-one (1) with hydrazine derivatives (2a–d) afforded hydrazone derivatives (3a–d), which reacted with alkyl halides 4a–c to give bis(alkylthio)methylene derivatives (5a–e). Also, 3a,b reacted with hydrazonyl halides 6a–d to give 1,3,4-thiadiazole (7a–d). Cyclization of 3c with ethyl bromoacetate and haloketones gave thiazolidinone and thiazole derivatives (8, 10a,b) respectively. Treatment of hydrazone (3d) with benzylidine malononitrile 13a,b gave pyridine (14a,b). In addition, cyclocondensation of 3d with phenolic aldehydes furnished coumarin derivatives (16a–c). Coupling of 3d with heterocyclic diazonium salts gave triazol[5,1-c]triazine (20) and pyrazolo[5,1-c]triazine (22). Some of the prepared products showed potent antimicrobial activity.     

Phosphorus-Nitrogen Compounds: Part 25. Syntheses,Spectroscopic, Structural and Electrochemical Investigations,Antimicrobial Activities,and DNA Interactions of Ferrocenyldiaminocyclotriphosphazenes

Abstract

The condensation reactions of hexachlorocyclotriphosphazene (N₃P₃Cl₆) with mono (1 and 2) and bisferrocenyldiamines (3–5 and 7) resulted in the formation of tetrachloro mono- (8 and 9) and bisferrocenylspirocyclotriphosphazenes (10–13). In addition the tetramorpholino mono- (8a and 9a) and bisferrocenylphosphazenes (10a–12a) were obtained from the reactions of the corresponding tetrachlorophosphazenes (8–12) with excess morpholine. The structures of all the phosphazenes were determined using FTIR, MS, ¹H, ¹³C, and ³¹P NMR and 2-dimensional NMR techniques. The structures of 9a and 13 were determined by single crystal X-ray diffraction techniques. Cyclic voltammetric investigations of compounds 8a, 9a, and 11a revealed that ferrocene redox centers undergo reversible oxidation. These ferrocenylphosphazenes appear to be quite robust electrochemically. Interactions between the compounds 8a, 9a, 11a, and 12a and pBR322 plasmid DNA were investigated by agarose gel electrophoresis.

[Supplementary materials are available for this article. Go to the publisher's online edition of Phosphorus, Sulfer, and Silicon and the Related Elements for the following free supplemental files: Additional text and figures.]     

SOME NEW S-, S,S- AND N,S-SUBSTITUTED 2-NITRODIENES AND BUTADIENYL-SUBSTITUTED PIPERAZINES

Nitrodiene 1 reacted with 2a, b and gave the novel compounds 3a, b, 4a, b, and 5a. Monosubstituted diene compound 3a gave the compounds 9a with morpholine, 11a with piperidine, and 13a with homopiperazine. Compound 3a gives the thioether compound 15 by the reaction with the dithiol (HS─(CH₂)₂─O─(CH₂)₂─SH) in ethanol containing sodium hydroxide.     

New Route for the Synthesis of Pyrazole,Triazole, Triazine,and Triazepine Derivatives

N,N′‐Diphenylpiperidine‐1‐carbohydrazonamide 1 was prepared and treated with halo compounds, active nitriles, diethylhy malonate, ketones, CS₂, phenylisocyanate, phenylisothiocyanate, LR, ethyl 2‐cyano‐3,13‐dithiomethylacetate, and benzylidenenitriles to give the corresponding triazines 2–4, pyrazoles 5 and 6, triazoles 7, 8, and 10, triazaphosphole 11, and triazepines 12 – 14, respectively.     

Mono-, di-, and trinuclear phosphonate oxygen-bridged copper(II) complexes: syntheses,structures, and properties

Reactions of copper salts, zoledronic acid, and 2,2′-bipyridine/1,10-phenanthroline in aqueous ethanolic solutions afforded four phosphonate oxygen-bridged copper complexes, Cu(bipy)(H₄zdn)(HSO₄) (1), [Cu₂(bipy)₂(H₂zdn)(H₂O)(Cl)]·4H₂O (2), [Cu₂(phen)₂(H₂zdn)(H₂O)(Cl)]·2.5H₂O (3), and [Cu₃(bipy)₃(H₄zdn)(H₂zdn)(SO₄)]·5H₂O (4) (H₅zdn = zoledronic acid, bipy = 2,2′-bipyridine, phen = 1,10-phenanthroline). The copper centers of 1–4 have square pyramidal coordination geometries. The Cu(II) ions are coordinated to bipy/phen, zoledronate, and HSO₄^?/Cl^? forming mononuclear units for 1, dinuclear for 2 and 3, and trinuclear for 4. These building units are further extended into 3-D supramolecular networks via multiple hydrogen bond interactions. Temperature-dependent magnetic properties of 2 and 4 suggest weak antiferromagnetic coupling (J = ?4.53(8) cm^?1 for 2, J = ?1.69(4) cm^?1 for 4). The antitumor activity of 2 was evaluated against the human lung cancer cell line and indicates effective time- and dose-dependent cytotoxic effects.     

Synthesis,characterization, crystal structures,enzyme inhibition,DNA binding,and electrochemical studies of zinc(II) complexes

Five zinc(II) complexes, [Zn(L¹)₂] (1), [Zn(L¹)₂(phen)H₂O]·H₂O (2), [Zn(L¹)₂(bipy)] (3), [Zn(L²)₂] (4), and [Zn(L²)₂(phen)] (5) (where L¹?=?4-nitrophenylacetate, L²?=?phenylacetate, phen?=?1,10-phenanthroline and bipy?=?2,2′-bipyridine), have been synthesized and characterized by elemental analysis, FT-IR, and multinuclear NMR. Complexes 2, 3, and 4 have been confirmed by single-crystal X-ray diffraction. In 2 and 3, zinc is bonded monodentate to two carboxylates exhibiting distorted trigonal bipyramidal and tetrahedral geometries, respectively, whereas in 4, the carboxylates are bridging bidentate in distorted tetrahedral geometry. The complexes have been screened for electro- and biological activities, including DNA interaction and enzyme inhibition studies. The effect of concentration of 1–5 on the activity of enzyme, alkaline phosphatase, showed that an increase in concentration of complex decreased the activity of the enzyme. Electrochemical behavior of HL¹, 2, and 3 was investigated by cyclic voltammetry and it was observed that ligand-centered electro-activity exhibits a proportionate change on complexation. The UV–visible spectroscopic and viscometric data indicate electrostatic and groove binding of the complexes with DNA. The binding constant and Gibb’s free energy values indicate the feasibility of the complex–DNA interaction and show potent biological activity of the complexes.     

SYNTHESES,STRUCTURES AND REACTIONS OF NEW AND NOVEL FOUR-, FIVEAND SIX-MEMBERED UNSATURATED N,P-HETEROCYCLE COMPLEXES

Metal-assisted heterocyclic ligand syntheses are reported using 2-H-azaphosphirene complex 1 or 7-phosphanorbornadiene complex 7 as starting material. Thermal decomposition of complex 1 led to 1,2dihydro-1,2,3-azadiphosphete complex 2, which was transformed into 2,6-dihydro-1,3,2,6-diazadiphosphinines 5a, b via ring expansion with carbonitriles 3a, b. Insertion of tert-butyl isonitrile into the P─ P bond of 2 at ambient temperature furnished the first Δ ¹ -1,3,5-azadi-phospholene complex 6─P bond of 2 using 7 failed. The 1,2,3,4-azatriphospholene complexes 9a, b were obtained by thermolysis of complex 2 in the presence of functionalized carbonitriles 8a, b.     

Synthesis,characterization, and catalytic oxidation of styrene,cyclohexene, allylbenzene,and cis-cyclooctene by recyclable polymer-grafted Schiff base complexes of vanadium(IV)

Schiff base-functionalized chloromethylated polystyrenes, PS-[Ae-Eol] (I), PS-[Hy-Eda] (II) and PS-[HyP-Eda] (III), were synthesized by reacting 2-(2-aminoethoxy)ethanol (Ae-Eol), N-(2-hydroxyethyl)ethylenediamine (Hy-Eda), and N-(2-hydroxpropyl)ethylenediamine (HyP-Eda) with oxidized chloromethylated polystyrene. Oxidized chloromethylated polystyrene (PS-CHO) was prepared by oxidation of chloromethylated polystyrene (PS) with sodium bicarbonate in DMSO. By reacting DMSO solution of [VO(acac)₂] with polymer-anchored Schiff base ligands I, II, and III, vanadium(IV) complexes PS-[V^IVO(Ae-Eol)] (1), PS-[V^IVO(Hy-Eda)] (2), and PS-[V^IVO(HyP-Eda)] (3) were prepared. Structure and bonding of I, II, and III as well as corresponding vanadium complexes 1, 2, and 3 were confirmed by FT-IR, UV–vis spectroscopy, SEM, EDX, AAS, TGA, EPR, etc. Polymer-anchored vanadium(IV) complexes 1, 2, and 3 show, efficient catalysis toward oxidation of styrene, cyclohexene, allylbenzene, and cis-cyclooctene in the presence of hydrogen peroxide. Optimized reaction conditions for the oxidation of these alkenes was achieved by changing various reaction parameters (like amount of catalyst, amount of oxidizing agent, volume of solvent, etc.). Polymer-grafted 1, 2, and 3 can be reused multiple times without depletion of their activity.     

Cyanothioacetamide in Heterocyclic Chemistry: Synthesis of Thiopyran,Pyridinethione, Thienopyridine,Pyridothienotriazine and Pyridothienopyrimidine Derivatives

Abstract

Cyanothioacetamide (1) reacted with α- and β-naphthaldehyde 2a,b to afford the corresponding 3-naphthyl-2-thiocarboxamidopropenonitriles 3a,b. Compounds 3a,b structures could be elucidated via their reactions with acrylonitrile, ethyl acrylate (4a,b). N-arylmaleimides 6a-c and ethyl acetoacetate (8). The isolated products could be represented as the thiopyran, thiopyranopyrrolidine and pyridinethione derivatives 5a-d, 7a-f and 9a,b respectively. Pyridinethiones 9a,b had been used as the starting materials in the present study in addition to the next ones to synthesize several new thienopyridines, pyridothienotriazine and pyridothienopyrimidines 12a-f, 15a,b, 16b, 17–19a,b respectively through their reactions with the corresponding reagents.

All structures of the newly synthesized heterocyclic compounds were established on the basis of the data of IR, ¹H NMR and elemental analyses.     

Dapson in Heterocyclic Chemistry,Part II: Antimicrobial and Antitumor Activities of Some Novel Sulfone Biscompounds Containing Biologically Active Thioureido,Carbamothioate, Quinazoline,Imidazolidine, and Thiazole Moieties

The reaction of 4,4′-diisothiocyanato-1,1-diphenylsulfone 2 with aromatic amines and phenol derivatives afforded the corresponding thioureio derivatives 3–9 , respectively. Also, the reaction of 2 with catechol gave the corresponding carbamothioate derivative 11. Quinazoline derivatives 14 and 15 were obtained in good yield via reaction of 2 with anthranlic acid derivatives. Imidazolidine biscompounds 16 and 17 were readily synthesized from the reaction of 2 with N-(4-substituted-phenyl)cyanothioformanilides. The structure of the products was confirmed from elemental analysis as well as spectral data. Most of the synthesized compounds showed remarkable antimicrobial activity compared with chloramphenicol and Grisofluvine as positive controls. Compound 6 was almost as active an antitumor agent as the reference drug Doxorubicin.     

Reaction of 2-Thioxo-4-Thiazolidinones Toward Lawesson's Reagent,Phosphorus Pentasulfide,Dialkylaminophosphines, and Phosphorus Ylides

Abstract

2-Thioxo—3-allyl-4-thiazolidinone 1a reacts with Lawesson's reagent (LR, 2) to give the ethylenic product 5 through a coupling reaction along with the dithioxo compound 6. Coupling reaction products of types 8 and 9 are also produced upon reacting thiazolidinones 1 and with the appropriate tris(diallkylamino) phosphine reagent (3 a,b). Reaction of the thiazolidinone 1a with the ylidenetriphenylphosphorane reagents 4 a–c proceeds according to the Wittig mechanism yielding ethylenes 10a–c, respectively. Structural elucidations for the new products were based upon compatible analytical and spectroscopic measurements as well a confirmatory single crystal X-ray structure for 5.

Supplemental materials are available for this article. Go to the publisher's online edition of Phosphorus, Sulfur, and Silicon and the related elements to view the free supplemental file.     

Cyanothioacetanilide Intermediates in Heterocyclic Synthesis,Part 1: Synthesis and Biological Evaluation of Some Novel Thiazole,Thiophene, Pyrazole,and Pyrazolo[1,5-a]Pyrimidine Derivatives

Some novel thiophenes (4a,b, 5, and 9a,b) were obtained from the cycloalkylation of the thiocarbamoyl group in the cyanothioacetanilide derivative (1) with α-halocarbonyl compounds. Also, the reaction of cyanothioacetanilide derivative with phenyl isothiocyanate in the presence of potassium hydroxide followed by in situ heterocyclization of the resulting adduct with α-halocarbonyl compounds furnished the corresponding thiazole (12, 14, and 15), pyrazole (19), and pyraozlo[1,5-a]pyrimidine (22, 25, and 26) derivatives. Compounds (4b, 5, 9a, 12, 13, 18, 22, 25, and 26) were tested to evaluate their antimicrobial activity.

Supplemental materials are available for this article. Go to the publisher's online edition of Phosphorus, Sulfur, and Silicon and the Related Elements to view the free supplemental file.     

SYNTHESIS OF NEW ANTHRACYCLINE DERIVATIVES CONTAINING PYRUVIC,ASPARTIC, OR N-ACETYLASPARTIC ACID MOLECULE

ABSTRACT

The new anthracycline analogues (2–10) as potential anticancer agents were synthesized from daunomycin (1a) and doxorubicin (1b). Compounds 2, 6, and 7 were prepared by the nucleophilic displacement type esterification of a 14-bromodaunomycin (1c) with a sodium pyruvate, aspartate, and N-acetylaspartic acid, respectively. Whereas compounds (3, 8) and (4, 9) were prepared by the reaction of daunomycin (1a) or doxorubicin (1b) with one equivalent of the corresponding acids in the presence of EDCI/PP, compounds (5, 10) were obtained from 1b by reaction with two equivalents of the corresponding acids in the same manner.     

Chromatographic and electrophoretic determination of thioamides based on thiazole, 1,3,4-thiadiazole, 1,2,4-triazole,and tetrazole

A procedure was developed for the determination of the following thioamides based on thiazole, 1,3,4-thiadiazole, 1,2,4-triazole, and tetrazole: 2-mercaptothiazole (I), 2-mercapto-1,3,4-thiadiazole (II), 2-mercapto-5-methyl-1,3,4-thiadiazole (III), 3-mercapto-1,2,4-triazole (IV), 3-mercapto-4-methyl-1,2,4-triazole (V), and 5-mercapto-1-methyltetrazole (VI). The determination was performed by reversed-phase HPLC on a column (150 × 4 mm) packed with Diaspher-110-C18 (5 μm) using elution with an acetonitrile-acetate buffer solution (pH 4.70) mixture (5: 95). Detection was performed at the light absorption maximums of compounds I (320 nm), II (305 nm), III (310 nm), IV (260 nm), V (254 nm), and VI (245 nm). The calibration graphs were linear over the following concentration ranges (μg/mL): 0.47–11.72 (I), 0.47–11.82 (II), 0.53–13.22 (III), 0.40–10.11 (IV), 0.46–11.52 (V), and 0.46–11.62 (VI). The limits of detection were 0.45, 0.43, 0.50, 0.37, 0.41, and 0.42 μg/mL for compounds I–VI, respectively. Conditions for the separation of a mixture of compounds I and III–V and for the quantitative determination of compounds I–VI by capillary zone electrophoresis (CZE) were optimized. CZE was performed on a quartz capillary of size 60 cm (effective length of 50 cm) × 75 μm at a voltage of 20 kV with a borate buffer solution (pH 9.18). The procedure allowed us to evaluate the concentrations of substances in the ranges of 1.17–93.75 (I), 1.18–94.54 (II), 1.32–105.76 (III), 1.01–101.13 (IV) 1.15–115.16 (V), and 1.16–116.15 (VI) μg/mL with the detection limits of 1.10, 1.11, 1.20, 0.96, 1.01, and 1.02 μg/mL for compounds I–VI, respectively.