利用碳碳叁键断裂重组反应合成2,4,4-三氯萘-1(4H)-酮衍生物

以炔烃-联烯酮为原料,水作为亲核试剂,通过N-氯代丁二酰亚胺(NCS)介导的[2+2]环加成和碳碳叁键断裂重组反应合成了18个2,4,4-三氯萘-1(4H)-酮衍生物,产率为55%～88%.所得产物的结构经NMR和IR以及HRMS等表征,其中目标产物2e的结构经X单晶分析确认.该反应条件温和、操作简单、无需金属催化剂且产率良好,为合成官能化的1-萘酮衍生物提供了一种新的高效的合成策略.     

利用自由基引发的1,2-炔基迁移实现非活性烯烃的炔膦酰化

研究了1,4-烯炔衍生物与二芳基膦氧化物在银介导下发生的炔酰化反应.该反应利用自由基引发的1,2-炔基迁移策略合成了一系列γ-酮膦氧化物,产率适中.该反应机理可能涉及膦中心自由基与乙烯基的加成、3-exo-dig环化和1,2-炔基迁移等连续的过程,一步形成了C-P、C-C键等化学键,实现了非活性烯烃的双官能化.     

自由基促进硫甲基取代的炔酮的环化反应

硫代吡喃酮是一种重要的结构骨架, 广泛存在于天然产物、潜在药物及生物活性分子中. 因此, 发展简洁、高效构建硫代吡喃酮的合成方法具有重要意义. 发展了一种自由基促进的硫甲基取代炔酮的加成环化反应来构建硫代吡喃酮环的新方法. 该方法具有底物适用性广, 一系列自由基前体如二苯基膦氧、硫酚、醛等都可以在该反应体系中实现转化. 机理研究表明, 自由基前体对炔酮的选择性加成得到C(sp ²)自由基中间体, 该中间体促进的C(sp ²)—S键构建及C(sp ³)—S键断裂是关键步骤.     

膦、胂叶立德的化学与应用(ⅩⅩⅠⅩ)——含全氟烷基胂叶立德水解合成2-吡喃酮衍生物

在无水碳酸钾存在下,以无水二氯甲烷作溶剂,室温下将溴化(2-萘甲酰基)甲基三苯基(1)与2-全氟炔酸甲酯(2)反应,高产率地得到加合产物4-(2-萘甲酰基)-2-三苯基胂基-3-全氟烷基-3-丁烯酸甲酯(3)和少量4-(2-萘甲酰基)-4-三苯基胂基-3-全氟烷基-2-丁烯酸甲酯(4). 加合产物3在9∶1的甲醇-水溶液中在一定温度下反应,高产率地得到4-全氟烷基-6-(2-萘基)-2-吡喃酮(5). 研究发现硅胶对该反应具有催化作用. 提出并讨论了反应机理.     

邻醌与噁唑的光化[4+4]环加成反应

虽然[2+2]和[4+4]环加成反应都是光化学允许的,但[4+4]环加成远不及[2+2]反应普遍.已知的[4+4]环加成主要为蒽、萘、吡啶-2-酮和吡喃-2-酮衍生物的光化二聚以及它们与某些1,3-二烯的环加成.羰基化合物与烯烃一般发生[2+2]环加成(Peterno-B點hi反应).邻醌和α-二羰基化合物与富电子烯烃则已知可进行[2+2]或[4+2]的光化环加成反应,分别得到α-羰基氧杂环丁烷和1,4-二氧杂环己烯.但未知有光化[4+4]环加成反应.     

有机小分子催化的β-酮酯不对称α-官能化反应

有机小分子催化的不对称反应是目前有机化学的研究热点之一。β-酮酯是一类具有活泼次甲基的"软"亲核试剂,可以在有机碱或者金属路易斯酸的催化下进行α-官能化反应。本文详细介绍了有机催化的β-酮酯不对称α-官能化反应的最新研究进展,并对不同亲电试剂参与β-酮酯的α-官能化反应进行了简要评述。     

一种新型呋喃香豆素类似物: 呋喃并萘并吡喃酮的合成及DNA嵌入活性

1,5-萘二酚经Pechmann缩合，烯丙基醚化，Claisen重排，乙酰化，溴加成，闭环六步反应，合成了一个新型的呋喃香豆素类似物，2H-4,8-二甲基呋喃并[2',3':5,6]萘并[1,2-b]吡喃-2-酮(6)。所得2～6的5个新化合物的结构均经^1H NMR，MS，IR，元素分析确证，测试了化合物6的紫外及荧光光谱。在DMSO-Tris HCl体系中，用荧光淬灭技术考察了6和7的DNA嵌入活性，求取了Scatchard表观嵌入常数，发现6和7都能有效地嵌入小牛胸腺DNA中，6的嵌入活性小于7。     

2-氨基-3-氰基-4-芳基-6-甲氧基-1,4,9,10-四氢萘并[2,1-b]吡喃衍生物的一步合成

以芳醛、丙二腈和7-甲氧基-1,2,3,4-四氢萘-2-酮为原料,在六氢吡啶催化下以乙醇为溶剂,在室温合成了一系列新的2-氨基-3-氰基-4-芳基-6-甲氧基-1,4,9,10-四氢萘并[2,1-b]吡喃衍生物,反应条件温和,产率较高,并通过IR,1H NMR和元素分析表征产物的结构,还通过单晶X射线衍射分析确证产物的构象.     

铜催化苯甲酰胺与烷基偶氮试剂环化合成含α-取代季碳中心异喹啉二酮

发展了一种苯甲酰胺自由基自由基环化制备α-官能化叔烷基取代的异喹啉二酮的新反应。此环化反应以偶氮试剂为α-取代叔烷基自由基源物质,利用碘化亚铜/空气体系催化N-烷基-N-甲基丙烯酰基苯甲酰胺发生环化,经过串联自由基加成/环化/碳-碳键形成过程,一步构建了三重碳-碳键,以41%~71%的产率合成了一系列异喹啉二酮及其衍生物。特别值得提出得是,此研究发展了一种新型α-官能叔烷基自由基源物质,发现了一种同时引入两个α-官能叔烷基片段的串联新反应。反应底物适应范围广,反应高效,催化体系廉价实用,为具有潜在药用价值的含α-取代季碳中心的异喹啉二酮及衍生物的合成提供了一条廉价、简单、快捷的新途径。     

无溶剂条件下合成2-[3-氧代-1,3-二(未)取代苯基丙基]-1,2,3,4-四氢萘-1-酮

以3,4-二氢-1-萘酮和查尔酮为原料,在K2CO3-NaOH存在下,无溶剂室温研磨反应,方便地得到2-[3-氧代-1,3-二(未)取代苯基丙基]-1,2,3,4-四氢萘-1-酮.该方法具有反应条件温和、操作简单和产率较高等优点,并通过IR,1HNMR,元素分析确定了产物的结构,3b晶体结构通过X衍射测定.     

Simultaneous chiral separation of leucovorin and its major metabolite 5-methyl-tetrahydrofolate by capillary electrophoresis using cyclodextrins as chiral selectors: Estimation of the formation constant and mobility of the solute-cyclodextrin complexes

Summary Capillary electrophoresis with an electrolyte containing cyclodextrin was investigated for the simultaneous separation of the diastereoisomers of 6R,S-leucovorin and its active metabolite 6R,S-5-methyl-tetrahydrofolate. , and -cyclodextrin separated the diastereoisomers of 5-methyl-tetrahydrofolate, while only -cyclodextrin was found to be effective for the chiral separation of leucovorin. The effect of -cyclodextrin concentration was investigated, and subsequently a curve-fitting analysis for the quantitative estimation of the binding constants was attempted. The binding constants were found to be very small, in the range 2–4 M^–1. Although the interaction between -cyclodextrin and the tetrahydrofolates is weak, the high efficiency of capillary electrophoresis and the use of high concentrations of -cyclodextrin allow baseline chiral separation of the diastereoisomers of leucovorin and 5-methyl-tetrahydrofolate. Changes in temperature exert differing effects on the separations of leucovorin and 5-methyl-tetrahydrofolate; higher temperatures improved the separation of leucovorin diastereoisomers but reduced the resolution of 5-methyl-tetrahydrofolate diastereoisomers. The effects of urea and buffer salt concentrations and of buffer pH were also investigated. Capillary electrophoresis with -cyclodextrin was used to analyse plasma samples spiked with clinically-relevant levels of leucovorin and 5-methyl-tetrahydrofolate. Resolution of these compounds in ultrafiltered plasma was demonstrated, but detection sensitivity was not adequate for the routine use of this method for the determination of leucovorin and 5-methyl-tetrahydrofolate in plasma. In addition, a simple technique to reverse the elution order of ionic stereoisomers was demonstrated. By adding a cationic surfactant into the buffer and reversing the separation potential, the elution order of the diastereoisomers of leucovorin and 5-methyl-tetrahydrofolate was reversed.     

Solid-Phase Extraction with Slurry Injection of the Resin Into ETAAS for Trace Determination of Thallium in Natural Water

Thallium in natural water samples was determined by electrothermal atomic absorption spectrometry after 1000-fold enrichment by mini solid-phase extraction from a 100-mL sample solution. A Tl-pyrrolidine-1-carbodithioate complex formed in a sample solution of pH 1.6 was extracted on fine particles of a cellulose nitrate resin dispersed in the sample solution. The cellulose nitrate resin was then collected on a membrane filter (25mm^ø) by filtration under suction using a glass funnel with an effective filtration area of 0.64cm². As a result, a circular thin layer of the resin phase with a diameter of 9mm was obtained. Then the resin phase was carved out by an acrylate resin puncher with a 10-mm^ø hole to put it into a sample cup containing 100µL of 10mM HNO₃ containing 0.5mM NaCl. The resin phase was suspended in the solution by ultrasonication. 1000-fold enrichment was thus attained within 15min, and the suspension was delivered to electrothermal atomic absorption spectrometry. The linear calibration graph was obtained in the range of 0–4ng of Tl in 100mL of a sample solution. The detection limit obtained by 3 method was 0.19ng. The proposed method was applied to the determination of Tl in natural water samples. The results showed the concentration of Tl in seawater was 12.1±1.8pgmL^–1 for the calibration graph method and 12.6±1.4pgmL^–1 for the standard addition method. A snowmelt sample contained 20.7±1.0pgmL^–1 of Tl.     

Molecular inclusion complexation of tolbutamide with permethyl-β-cyclodextrin

The formation of a stable inclusion complex between tolbutamide and permethyl- cyclodextrin was systematically studied. It shows that permethyl--CD forms a 1 : 1 complex with tolbutamide. Its molecular structure was elucidated by physicochemical methods including IR and high field NMR analysis. The influence of pennethyl--cyclodextrin on the hypoglycemic effect of tolbutamide was evaluated by measuring the blood glucose level. The reduction in plasma glucose was significantly greater when the rabbits were treated with the complex than with tolbutamide alone. The enhancement of the bioavailability of tolbutamide by permethyl--cyclodextrin is likely attributed to the molecular inclusion effect.     

A technique for capillary joining in capillary electrophoresis

Summary Aspects of cracking and joining capillaries have been investigated. Capillary coupling was achieved using various methods. The most successful used hydrofluoric acid-etched capillaries to form male and female ends which were then joined together. This type of joint was used to connect sections of capillary of similar and different internal diameters with minimal loss in resolution, peak width and number of theoretical plates. (Uridine and hypoxanthine was used as a test mixture). For hypoxanthine on a 50 m/50 m etched joined capillary 10 cm from the detector window the number of theoretical plates was 96.6% of that for hypoxanthine on an unbroken capillary. Following the relative success of capillary joining, a coupled capillary flowcell (50 m/200 m) was produced and evaluated.     

反相高效液相色谱法测定3种中成药中的葛根素

 建立了测定小儿清感灵片、步长新脑心通胶囊和感冒清热颗粒 3种中成药中葛根素含量的反相高效液相色谱方法。采用APEXODS色谱柱 ,以醋酸铵缓冲液 (10 0mmol/L ,pH 5 0 ) 甲醇 (体积比为 75∶2 5 )的混合溶液为流动相 ,检测波长为 2 5 0nm ,流速为 0 8mL/min。葛根素在 2mg/L～ 2 0mg/L时其色谱峰面积与质量浓度的线性关系良好 (r =0 9999) ;上述 3种中成药中的葛根素含量分别为 3 48mg/g ,1 0 8mg/ g及 1 5 2mg/ g(蔗糖型 ) ;其加样回收率分别为 99 0 % ,93 4%和 97 5 %。该法简便、快速、专属性强 ,可以作为多种中药制剂中葛根素含量的测定方法。     

Effect of β-cyclodextrin on disposition of hexobarbital and phenobarbital in mice

The effect of -cyclodextrin (-CD) on the disposition of hexobarbital (HBA) and phenobarbital (PhBA) after intravenous administration, with the simultaneous administration with -CD, was investigated in mice.In the case of HBA, the whole blood concentration was slightly heightened, the brain and liver concentrations were significantly lowered, and the kidney concentration was significantly heightened. Moreover, -CD also influenced the disposition and formation of 3-hydroxy- and 3-keto-HBA. On the other hand, in the case of PhBA, the whole blood concentration was slightly lowered, the time at maximum brain concentration (t-max) was prolonged about 30 to 60 min, the kidney concentration was significantly heightened at the initial stage, while the liver concentration did not show a clear difference by the simultaneous administration with -CD. These results suggest that the disposition of drugs might be modified by the use of CD.     

Zeolite Catalyzed Alkylation of Biphenyl. Where Does Shape-Selective Catalysis Occur?

Liquid-phase alkylation of biphenyl (BP) was studied over large-pore zeolites. Selective formation of the least bulky products, 4,4-diisopropylbiphenyl (4,4-DIPB) occurred only in the isopropylation of BP over one- or two-dimensional zeolites, H-mordenite (HM), ZSM-12, SSZ-24, SAPO-5, SSZ-31, and CIT-5. These shape-selective catalyses are ascribed to steric restriction of transition state and to easiness of the substrates to enter into the pores. HM gave the highest selectivity among them. The dealumination of HM enhanced catalytic activity and the selectivity for 4,4-DIPB because of the decrease of coke deposition. Non-regioselective catalysis occurs on external acid sites over HM with the low SiO₂/Al₂O₃ ratio because severe coke deposition deactivates the acid sites inside the pores by blocking pore openings. The selectivity of DIPB isomers was changed with propylene pressure and/or with reaction temperature. Selective formation of 4,4-DIPB was observed at moderate temperatures such as 250°C, whereas the decrease of the selectivity of 4,4-DIPB occurred at higher temperatures as 300°C. 4,4-DIPB yielded selectively under high propylene pressure (<0.3 MPa) at 250°C, while the selectivity of 4,4-DIPB decreased under low propylene pressure as 0.2 MPa. However, 4,4-DIPB was almost exclusive isomer in the encapsulated DIPB isomers inside the pores under every temperature and pressure. The decrease of the selectivity of 4,4-DIPB is due to the isomerization of 4,4-DIPB on the external acid sites. The deactivation of external acid sites of HM was examined by the modification with cerium and other rare earth metal oxide on HM. Selectivities of 4,4-DIPB were improved over modified HM even at high temperatures because of the suppression of non-regioselective alkylation and isomerization at the external acid sites. The ethylation of BP to ethylbiphenyls (EBPs) and diethylbiphenyls (DEBPs) was non-regioselective. The ethylation of BP to EBPs was controlled kinetically. However, there was difference in reactivities of EBPs and DEBPs for their further ethylation. 4-EBP was ethylated preferentially among the isomers, although the formation of 4,4-DEBP was less selective. 4-EBP and 4,4-DEBP have the highest reactivities among EBPs and DEBPs for the ethylation to polyethylbiphenyls (PEBPs). These results show that the environments of HM pores are too loose for shape-selective formation of the least bulky isomers, 4-EBP and 4,4-DEBP, in the ethylation of BP, and that HM pores have enough space for the further ethylation of 4,4-DEBP.     

FT-Raman Spectra of o-, m-, and p-Nitrophenol Included in Cyclodextrins

FT-Raman spectra of o-, m-, and p-nitrophenol included in -cyclodextrin (CD), -CD, hydroxypropyl (HP) -CD, andsulfated -CD were recorded. The phenyl (C=C) band of o- and p-nitrophenol in the CD inclusion complexes was shifted to higher wavenumber thanthat of pure o- and p-nitrophenol,whereas the phenyl (C=C) band of m-nitrophenol in the CD inclusion complexes was shifted to lower wavenumber than that of pure m-nitrophenol. The ring CH peak of o-nitrophenol in the CD complexes was shifted to higher wavenumber than that of pure o-nitrophenol, whereas the ring CH peak of m- and p-nitrophenol in the CD complexes was shifted to lower wavenumber than that of pure m- and p-nitrophenol.     

Photochemical Synthesis and Magnetic Property Investigation of a Mixed-valence 11-Tungstophosphate

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Stability of Ibuprofen in its Inclusion Complex with β-Cyclodextrin

The ibuprofen--cyclodextrin inclusion complex was prepared by theco-precipitation method. The identity of the obtained product was verified by X-ray and thermogravimetric techniques. The effect of -cyclodextrin on the stability of ibuprofen was analysed.