2, 3-二氢蒽并(1, 2-b)(1, 4)恶嗪-7, 12-二酮的合成

2-溴-1, 4-二羟基蒽醌与氨基醇, 缩合可以生成2-取代氨基-1, 4-二羟基蒽醌, 但在较高温度下并延长反应时间, 部分产物可以进行分子内脱水而进一步环化为2, 3-二氢蒽并(1, 2-b)(1, 4)恶嗪-7, 12-二酮的衍生物。用MS和NMR确定其结构。     

Crystal Structure of Methyl 3- (2-chlorophenyl )-3- (5, 5-dimethyl-3-hydroxy-2-cyclohexene- 1-one-2-yl) propionate

1INTRODUCTIONInorganicsolidsupportsascatalystshavebeenwellstudied,becauseoftheirap-plicationsinorganicsynthese('~".Recently,wehavereportedtheKnoevenagelcon-densationcatalysedbyKF-Al,O,['i.Inthispaper,wediscussedthecrystalstruc-tureofthetitlecomPoundsynthesizedbythereactionof2-chlorobenzaldehydey5,5-dimethyl-1,3-cyclohexanedioneandisopropylidenemalonateinmethanolcatalyzedbyKF-Alzo,'Inordertoconfirmthestructureofthetitlecompound,theX-raycrys-tallOgraphicstudywascarriedout.2EXPER1MEN…     

Synthesis of 1-[6-Fluoro-(2S)-3H,4H-dihydro-2H-2-chromenyl]-(1R)-1,2- ethanediol and 1-[6-Fluoro-(2R)-3H,4H-dihydro-2H-2-chromenyl]- (1R)-1,2-ethanediol

Benzopyran compounds possess diverse pharmacological properties such as β-blockade, anticonvulsant and antimicrobial.[1,2] Our interest has been focused on the synthesis of 1-[6-Fluoro-2S]-3H,4H-dihydro-2H-2-chromenyl]-(1R)-1,2-ethanediol (6) and 1-[6-fluoro-(2R)-3H,4H-dihydro-2H-2-chromenyl]-(1R)-1,2-ethanediol (7) which are particularly convenient precursor to (S,R,R,R)-NE (8). 8 containing four asymmetrical carbon atoms was reported to be the most active isomer.[3] Chandrasekhar[4] has reported on the synthesis of 8. The key step to synthesize this compound is to obtain the chiral chromanone 6 and 7. 6 was accomplished in 8 steps by the Clasien rearrangement and a one-pot Sharpless asymmetric epoxidation, but the compound 7 was accomplished in 10 steps. Johannes[5] used Zr-catalytic kinetic resolution of allylic ethers and Mo-catalyzed chromene formation to synthesize 8 in 14 steps. However both of the methods request many synthetic steps and expensive reagents.     

Synthesis of 2-(3-hydroxy-2-methyl-1-alkenyl)-1-pyrrolines and 2-(3-hydroxybutyl)-1-pyrroline using α-lithiated 2-methyl-1-pyrroline

Condensation of 2-methyl-1-pyrroline with chloroacetone or 3-chloro-2-butanone using LDA in THF afforded novel 2-(3-hydroxy-2-methyl-1-alkenyl)-1-pyrrolines via a peculiar reaction mechanism instead of the anticipated 2-(3-oxobutyl)-1-pyrrolines. The intermediacy of 2-(2,3-epoxy-2-methylalkyl)-1-pyrrolines in the latter transformation was demonstrated by immediate reductive epoxide ring opening utilizing lithium aluminium hydride in diethyl ether. Furthermore, 2-(3-oxobutyl)-1-pyrroline was prepared via an alternative approach through alkylation of 2-methyl-1-pyrroline with 3-chloro-2-(methoxymethyloxy)-1-propene using LDA in THF, followed by acid hydrolysis. Reduction of 2-(3-oxobutyl)-1-pyrroline by sodium borohydride in methanol afforded the corresponding 2-(3-hydroxybutyl)-1-pyrroline in good yield.     

Synthesis and cytotoxicity of dinuclear platinum(Ⅱ) complexes of (1S, 3S)-1, 2, 3, 4-tetrahydroisoquinolines

A series of novel dinuclear platinum(Ⅱ) complexes with (1S, 3S)-1,2,3,4-tetrahydroisoquinolines as the ligands were synthesized as potential anticancer agents in several steps starting from commercially available L-DOPA. The cytotoxicities of the series of dinuclear platinum(Ⅱ) complexes of tetrahydroisoquinoline were tested against HCT-8, BEL-7402, A2780, MCF-7, Hela, A549 and BGC-823 cell lines by the MTT test. These complexes showed selective inhibition activity against cisplatin-insensitive cell line Skov3.     

CRYSTAL AND MOLECULAR STRUCTURE OF 1-(4-DIMETHY-LAMINOPHENYL)-2- (3, 4-METHYLENE-DIOXYPHENYL ) ACRY-LONITRILE, C_(18)H_(16)N_2O_2

<正> C18H16N2O2, Mr = 292. 34, monoclinic space .group P21/c, a= 7.972(6), b = 6. 446(3), c=28.906(4)(?); β=95.59(8)°, V = 1478. 3(7)(?)3, Z = 4, Dx =1. 313 g/cm3, R = 0. 049. The non-hydrogen atoms of the title molecule are nearly co-planar forming a conjugation system.     

Synthesis of propyl O-(α-L-rhamnopyranosyl)-(1→3)-[2,4-di-O-(2s-methylbutyryl)-α-L-rhamno-pyranosyl]-(1→2)-(3-O-acetyl-β-D-glucopyranosyl)-(1→2)-β-D-fucopyranoside,the tetrasaccharide moiety of Tricolorin A

Propyl O-(α-L-rhamncpyranosyl)-(1→3)-[2,4-di-O-(2s-methylbutyryl)-α-L-rham-nopyranosyl]-(1→2)-(3-O-acetyl-β-D-glucopyranosyl)-(1→2)-β-D-fucopyranoside (1), the tetrasac-charide moiety of Tricolorin A, was synthesized in total 23 steps with a longest linear sequence of 10 steps, and overall yield of 3.7% from D-Glucose. The isomerization of the dioxolane-type berzyli-dene in the presence of NIS/AgOTf was observed. Tetrasaccharide 1 exhibited no activity against the cultured P388 cell as Tricolorin A did.     

Synthesis of Two Isomeric Tetrasaccharides 0-α-L-Fucopyranosyl-(1→3) and (1→4)-0-(2-Acetamido-2-Deoxy-β-D-Glucopyranosyl)-(1→3)-0-(β-D-Galactopyranosyl)-(1→4)-D-Glucopyranose and a Related Tetrasaccharide 0-α-L-Fucopyranosyl-(1→3)-0-(2-Acetamido-2-Deoxy-β-D-Glucopyranosyl-(1→6)-0-(β-D-Galactopyranosyl)-(1→4)-D-Glucopyranose

ABSTRACT

Synthesis of three tetrasaccharides, namely, 0-α-L-fucopyranosyl-(1→3)-0-(2-acetamido-2-deoxy-β-D-glucopyranosyl)-(1→3)-0-(β-D-galactopyranosyl)-(1→4)-β-D-glucopyranose (7), 0-α-L-fucopyranosyl-(1→4)-0-(2-acetamido-2-deoxy-β-D-glucopyranosyl)-(1→3)-0-(β-D-galactopyranosyl)-(1→4)-D-glucopyranose (9), and 0-α-L-fucopyransoyl-(1→3)-0-(2-acetamido-2-deoxy-β-D-glucopyransoyl)-(1→6)-0-(β-D-galactopyranosyl)-(1→4)-D-glucopyranose (15) has been described. Their structures have been established by ¹³C NMR spectroscopy.     

DiastereoselectiveandEnantioselectiveSynthesisof(1S,2S)-2-Ethyl-1-aminocyclopropaneCarboxylicAcid

During the last decade, 1-aminocyclopropanecarboxylic acid and its derivatives (ACCS) have attracted increasing attention of organic and bioorganic chemists due to their outstanding biological properties, ranging from antimicrobial, insecticidal, plant growth and fruit ripening controls, etc.1. Moreover, the three-membered carbocycle provides building blocks of unprecedented synthetic potential because it undergoes selective ring opening, ring enlargement or cycloaddition reactions2. The mo…     

SYNTHESIS, CHARACTERIZATION OF 2-[2-(3-NITRO-4-METHOXYLPHENYL) VINYLI-1-ME

ＳＹＮＴＨＥＳＩＳ，ＣＨＡＲＡＣＴＥＲＩＺＡＴＩＯＮＯＦ２－［２－（３－ＮＩＴＲＯ－４－ＭＥＴＨＯＸＹＬＰＨＥＮＹＬ）ＶＩＮＹＬＩ－１－ＭＥＴＨＹＬＰＹＲＩＤＩＮＩＵＭＰＥＮＴＡＡＮＤＨＥＸＡＮＩＴＲＡＴＯＲＡＲＥＥＡＲＴＨ（Ⅲ）ＣＯＭＰＬＥＸＥＳＨ...     

Synthesis of 2[(1R,2R)-2-(2,4-Difluorophenyl)-2-hydroxy-1-methyl-3-(1H-1,2,4-triazol-yl)propyl]-4-[4-tetrafluoropropoxy)phenyl]-3-(2H,4H)-1,2,4-triazol-3-thione—A Novel and Potent Azole Antifungal Agent

A simple approach involving refluxing appropriately disubstituted thiosemicarbazide 8 in presence of formic acid for the synthesis of 1, a potent azole antifungal agent, has been described.     

Asymmetric Synthesis of (-)-(2R,3R,6S)-Irnigaine

Introduction　　Asarelativelynewmemberofnaturalalkaloidswith2 ,6 disubstituted 3 piperidinolskeleton ,irnigaine 1wasisolatedfromthetubersofArisarumVulgare (Araceae)in1995byMelhaouiandBode .1Itsstructureandrelativeconfigurationswereelucidatedby1HNMRstudiesandtheabsoluteconfigurationwasproposedonthebasisofitsopti calrotation .1Soonafterthen ,Meyerandhisco workersreportedthefirstsynthesisof (- ) (2R ,3R ,6S) irni gaineandtheconfigurationconfirmation .Althoughtheirsynthesisroutewasshortan…     

Syntheses,Structure and Biological Activities of 2-(1H-Benzo [1,2,3]triazole-1-yl)-1-(3-methyl-4-bromobiphenyl)-2-(1H-1,2,4-triazole-1-yl)ethanone

Introduction1,2,4-Triazole derivatives represent an interesting class of heterocyclic compounds[1]and have become the most rapidly expanding group of antifungal compounds with the advantages of toxicity, high oral bioavailabi-lity, and broad spectrum of a…     

A Novel Fused Phosphorus Heterocycle: 4-(1'''',2'''',3'''',4-Tetrahydro-1, 3, 2-benzodiazaphosphorin-2''''-sulfide)-3, 4b, 4a-thiazphosphaphenanthridine Derivative

Organophosphorus compounds are ubiquitous in nature and they have broad applications in the fields of agriculture and medicine1-4. There has been a considerably growing interest in heterocyclic compounds due to their pharmaceutical importance and extensive application in organic synthesis, and the application of heterocycles is suggested to enhance the biological activity and/or offer other diverse properties5-7. In the previous work8, we have reported that 11-ethoxycarbonylmethyl-6-oxo-3, 4…     

X@(HAINH)_(12)和X(HAINH)_(12)(X=F~-,Cl~-,Br~-,O~(2-),S~(2-),Se~(2-))复合物的结构和稳定性

用DFT的B3LYP方法在6-31G(d)基组的水平上,对闭式多面体簇合物(HA1NH)12及其内含式X@(HA1NH)12外接式X(HA1NH)12(X=F-,Cl-,Br-,O2-,S2-,Se2-)复合物的结构进行了构型优化和能量计算,并讨论了几何构型、自然键轨道(NBO)、振动频率、能量参数及NMR数据与结构的关系,最后得到复合物结构的稳定性信息,具有Th对称性的X@(HA1NH)12(X=F-,Cl-,Br-,S2-,Se2-)复合物和具有C3对称性的O2-@(HA1NH)12复合物为内含式的基态结构,从能量角度分析,内含式复合物比外接式复合物的结构稳定.     

1-(4-ANTIPYRINYL)-3-(2, 4-DINITROPHENYL)-TRIAZENE AND ITS COLOUR REACTION WITH CADMIUM

A new reagent,1(4 antipyriny1) 3(2,4-dinitropheny1)triazene(APDNBT), was synthesized in this lab and its analytical properties and its colour reaction with cadmium were studied.     

杂芳基乙烯光化学反应的研究 2: r-1, c-2, t-3, t-4-1, 3-二(4-甲基苯基)-2, 4-二(4-吡啶基)环丁烷的结构及光解反应

通过反-1-(4-甲基苯基)-2-(4-吡啶基)乙烯(E-MEP)在稀盐酸中的光二聚反应得到了接近定量的标题化合物(DMDPC)。用元素分析,IR, UV, 1H NMR和MS表征了其结构, 并用X射线衍射法测定了DMDPC的晶体结构。DMDPC属单斜晶系, 空间群为P21/c, 晶胞参数a=1.1376(6), b=1.7379(8), c=1.1590(5)nm, β=106.16(4)ⅲ, Z=4。由于四元环同侧苯环和吡啶环的相互排斥作用, DMDPC采取蝶式构象。研究发现, DMDPC在短波紫外光照射下易发生开环反应; 同时还发现,E-MEP与其顺式异构体(Z-MEP)间的反-顺异构化平衡受照射光波长控制。     

Crystal Structure of 1, 1-Dichloro-la, 3-diphenyl-1, la, 2, 3-tetrahydro-azirino [2, 1-d ] [1, 5]benzothiazepine (C_(22),H_(17)Cl_2NS )

1INTR0DUCTI0NBenzoheteroazepinecompoundsareimportantpharmaceuticalagents"-".Inre-centyears,ithasbeenfoundthatbenzoheter0azepinetricyclicderivatives,especiallythosefusedwithotherfiveorsix-memberedheterocycle,area1soofpotentialphar-maceuticalinterestst4-6j.Hence,muchattentionhasbeenpaidtothesynthesesofthem,suchasl,3-oxazino[3,2-djt1,5jbenzothia/diazepin-l-onet"'J,1,2,4-tria-zolo[4,3-dj[1,5jbenzothia/diazepine"',1,2,4-oxadiazolo[4,5-dj[l,5jbenzothia/diazepine',',andsoon.Meanwhiletheirstructur…     

Reactions of 1,4-difeffocenylbuta-1,3-diyne and 1,4-diphenylbut-l-en-3-yne with Ru3(CO)12. Crystal structure of Ru3(CO)8(μ3-η-1-η1-η4-η2-C4Ph2(CH=CHPh)2)

Diyne FcCmCC.CFc (Fc is ferrocenyl) reacts with Ru₃(CO)₁₂ in boiling hexane to yield binuclear complexes Ru₂ and Ru₂(CO)₆(C₄Fc₂(C=CFc)₂C=O) containing ruthenacyclopentadiene and diruthenacycloheptadienone rings, respectively. The isomerism of the complexes is due to the different ways of coupling of the alkyne fragments of the diyne, namely, head-to-head, head-to-tail or tail-to-tail. The reaction of enyne PhC=CCH=CHPh with Ru₃(CO)₁₂ under similar conditions gives isomeric binuclear complexes Ru₂(CO)₆(C₄Ph₂(CH=CHPh)₂) and trinuclear clusters Ru₃(CO)₆(w-CO)₂(C₄Ph₂(CH=CHPh)₂) and Ru₃(CO)₈(₃-,¹-¹-⁴-² C₄Ph₂(CH=CHPh)₂). The structure of the latter was determined by X-ray diffraction analysis. The Ru₃ triangle coordinates eight terminal CO groups and the organic ligand resulting from the head-to-head dimerization of enyne molecules; the ruthenacyclopentadiene moiety is ⁴-coordinated to the Ru(CO)₂ group, and the third ruthenium atom is 2-bound to one of the PhCH=CH groups.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 5, pp. 1261–1267, May, 1996.