含三唑二硫代膦酸酯类衍生物的研究

合成了四种含三唑二硫代膦酸酯衍生物；通过红外光谱、核磁共振氢谱、元素分析确证了化合物的结构，生物初筛结果表明，所有化合物均有一定的杀菌、除草和植物生长调节活性。     

含三氮唑的硫代(或二硫代)氨基磷酸酯类衍生物研究

合成了７种含三氮唑的硫代（或二硫代）氨基磷酸酯衍生物。通过元素分析、ＩＲ及１ＨＮＭＲ确证了化合物的结构。生物活性测试结果表明，这些化合物均有一定的杀菌、除草和植物生长调节活性。     

新型双缩硫代对称二氨基脲类衍生物的合成和生物活性测试

探讨了硫代对称二氨基脲与10种含三唑基或苯并三唑基的取代苯乙酮的缩合反应, 制得10种新的1,5-二取代苯乙酮双缩硫代对称二氨基脲类化合物, 产物经IR, ¹H NMR, ¹³C NMR和MS及元素分析确证. 并对这些化合物的抗真菌和抗病毒活性进行了测试.     

S-[(1,2,4-三唑-1-基)芳基(或烷基)甲羰]甲基二硫代磷酸酯衍生物的研究

探讨了S-[(1,2,4-三唑-1-基)芳基(或烷基)甲羰]甲基二硫代磷酸酯衍生物的合成方法,合成了12种含三唑有机磷新化合物,通过红外光谱分析,确定该类化合物P=S振动的吸收频率范围为640～680cm^-1,核磁共振氢谱证明,与磷原子相联的基团旋转部分受阻,生物初筛结果表明,部分化合物具有杀菌、除草及植物生长调节活性。     

三苯基锗二硫代氨基甲酸酯的合成及表征

近年来 ,人们相继合成了有机锗倍半硫化物、有机锗硫杂环戊酮、含硫的螺环有机锗等化合Scheme1　 Synthetic route of compound物[1,2 ] .但烃基锗二硫代氨基甲酸酯类化合物尚未见报道 .我们 [3,4 ] 发现 ,有机锡二硫代氨基甲酸酯类化合物有很强的生物活性 .鉴于有机锗化合物比有机锡化合物毒性低得多 ,且副作用小 ,我们以三苯基氯化锗和二硫代氨基甲酸盐为原料 ,合成了一系列新型的有机锗含硫衍生物 (反应式如Scheme1所示 ) ,并对其结构进行了表征 ,初步生物活性测试结果表明 ,部分化合物显示出较强的抗癌活性 .1　实　　验1 .1　仪器与…     

二苯基锗二硫代氨基甲酸酯的合成及表征

合成了10种二苯基锗二硫代氨基甲酸酯Ph2Ge(S2CNR2)2,用元素分析、IR、^1H NMR和MS表征了这些化合物的结构,体外实验表明,这些化合物对MCF－7,WiDr和EC癌细胞具有较的抑制活性。     

α，α＇-二氧代烯酮环二硫代缩酮类化合物的晶体结构研究

α，α＇-二氧代烯酮环二硫代缩酮类化合物是一类多官能团化合物。由于其结构上的特性，近年来，已成为有机合成研究的热点之一。多年来，我合成了一系列的α，α＇-二氧代烯酮环二硫代缩酮类化合物，对于这类特殊结构化合物的谱学性质研究，我们也曾有过详尽的报道。为了进一步了解和分析不同取代基对此类化合物的空间构象的影响，本文报道这类化合物中的两个化合物的晶体结构（结构通式如图1所示），以便更好的为进一步研究开发利用这类化合物积累有价值的参考信息。     

α—羰基烯酮式环二硫代缩醛类化合物的制备

从具有α-亚甲基的酮出发,利用溶液稀释的方法,提高了用Dieter法合成α-羰基烯酮式环二硫代缩醛类化合物的产率,并用改进方法合成了4个该类化合物。     

O-芳基苯基硫代膦酰肼与某些羧基化合物的反应

为探索 O-芳基苯基硫代膦酰肼的反应性能、测试所得产物的生物活性,寻找活性结构,本文研究了它与几种羰基化合物α-(1,2,4 三唑基)片呐酮、邻苯二甲酰氯,反式菊酰氯和原甲酸三乙酯的反应,合成了21个新的     

α-溴代二硫缩烯酮的制备及其反应

α-羰基二硫缩烯酮 ( 1 )是一类重要的有机合成中间体 ,作为 1 ,3-亲核体用于酯环、苯系芳烃及芳杂环化合物的合成[1～ 4 ] .Hosomi等 [5～ 7] 用有机铜试剂或二碘化钐和 α-羰基与二甲硫缩烯酮反应 ,将与硫相连的缩烯酮碳原子转化为亲核中心 .用不同的烷硫基作为调控基团将该类中间体用于二萜 pseu-dopterosins的合成 [8～ 10 ] ,并作为替代 Peterson法合成 1 ,1 -二烷硫基 - 1 ,3-丁二烯或 1 ,1 -二烷硫基 - 1 ,3,5 -己三烯 [11,12 ] ,从不同的角度对 α-羰基二硫缩烯酮在合成上的应用进行了新的探索 .Junjappa等 [13,14 ] 曾用 NBS和 …     

Evaluation of the antioxidant potential of Salvia miltiorrhiza ethanol extract in a rat model of ischemia-reperfusion injury

The present study was undertaken to evaluate the protection potential of ethanol extract of Salvia miltiorrhiza (SMEE) against oxidative injury in the ischemia-reperfusion (I/R) model of rats in vivo. Rats were divided into six groups of 10 rats each. Group I/R model and sham were fed with a standard rat chow, groups SMEE I and SMEE II were fed with a standard rat chow and 400 or 800 mg/kg b.w. ethanol extract for 12 days before the beginning of I/R studies. Positive control group was fed with a standard rat chow and salvianolic acid B (55 mg/kg b.w.) or tanshinone II-A (55 mg/kg b.w.) for 12 days before the beginning of I/R studies. To produce I/R, the left anterior descending artery (LAD) was occluded in anesthetized rats for 15 min, followed by 120 min reperfusion. Infarct sizes were found significantly decreased in SMEE-treated and positive control groups compared to I/R model group. Serum AST, LDH and CK-MB activities were significantly reduced and myocardium Na+-K+ ATPase, Ca2+-Mg2+ ATPase activities and antioxidant enzyme activities (SOD, CAT, GSH-Px) were markedly increased in SMEE-treated and salvianolic acid B or tanshinone II-A positive control groups compared to the I/R model group. Pretreatment of S. miltiorrhiza ethanol extract and salvianolic acid B or tanshinone II-A dose-dependently reduced significantly myocardium MDA level, ROS and NOS activities and enhanced myocardium GSH level in I/R rats compared to I/R rats model. In conclusion, we clearly demonstrated that S. miltiorrhiza ethanol extract pretreatment can decrease oxidative injury in rats subjected to myocardial I/R.     

Synthesis of N-substituted C-normorphinans and their pharmacological properties.

Several N-substituted C-normorphinans (VIII and IX) were synthesized and tested for their analgetic and narcotic antagonist activities and physical dependence capacity. Treatment of N-formyl- octahydro-2-pyrindine (IIIc) with polyphosphoric acid readily gave N-formyl-C-normorphinan (IV). The N-nor bases (V and VII) obtained from IV were converted to VIII and IX. The N-methyl derivative (I), which was previously reported to be inactive by Haffner's method, exhibited potent analgetic activity by the hot plate method and the AcOH-induced writhing test. Compounds VIII and IX showed pharmacological properties similar to those of N-substituted morphinans and exhibited agonist (analgetic) and/or narcotic antagonist activities. The C-nor analogue (IXa) of cyclorphan (IIc) exhibited potent analgetic and antagonist activities with no physical dependence capacity in the single-dose suppression tests both in rats and monkeys.     

开链冠醚类似物的合成与研究I

Antipyrine derivatives I (Z = O, S; Z1 = CH2, CH2OCH2; n = 0, 1, 2, 3) were prepared as open-chain crown ether analogs. Thus, refluxing diethylene glycol ditosylate with 4-hydroxyantipyrine and K2CO3 in acetone for 15 h gave I (Z = O, Z1 = CH2OCH2). The activities of I as phase-transfer catalyst for iodination of 1-bromoctane with NaI, or KI were reported.     

Oxygen binding and activation by the complexes of PY2- and TPA-appended diphenylglycoluril receptors with copper and other metals

The copper(I) complexes of diphenylglycoluril basket receptors and , appended with bis(2-ethylpyridine)amine (PY2) and tris(2-methylpyridine)amine (TPA), respectively, and their dioxygen adducts were studied with low-temperature UV-vis and X-ray absorption spectroscopy (XAS). The copper(I) complex of, [.Cu(I)2] or, forms a micro-eta2:eta2 dioxygen complex, whereas the copper(I) complex of, [.Cu(I)2] or, does not form a well defined dioxygen complex, but is oxidized to Cu(II). Dioxygen is bound irreversibly to and the formed complex is stable over time. The coordination geometries of the above complexes were determined by XAS, which revealed that pyridyl groups and amine N-donors participate in the coordination to Cu(I) ions in the complexes of both receptors. The catalytic activities of various metal complexes of and , that were designed as mimics of dinuclear copper enzymes that can activate dioxygen, were investigated. Phenolic substrates that were expected to undergo aromatic hydroxylation, showed oxidative polymerization without insertion of oxygen. The mechanism of this polymerization turns out to be a radical coupling reaction as was established by experiments with the model substrate 2,4-di-tert-butylphenol. In addition to Cu(II), the Mn(III) complex of and the Fe(II) complex of were tested as oxidation catalysts. Oxidation of catechol was observed for the Cu(II) complex of receptor but the other metal complexes did not lead to oxidation.     

alpha-N-benzoylarginine-2-naphthylamide hydrolase (cathepsin B1 ?) from rat skin. II. Purification of the enzyme and demonstration of two inhibitors in the skin.

A thiol-activated, alpha-N-benzoylarginine-2-naph-thylamide (BANA) hydrolyzing enzyme was purified from rat skin by ammonium sulfate precipitation, gel filtration, and DEAE cellulose chromatography. In DEAE cellulose chromatography the enzyme was fractionated into two multiple forms (preparations I and II). The activity of undiluted preparation II, but not that of preparation I, was increased, when the enzyme was preincubated at pH 4, at 55 degrees C. Simultaneously, the isoelectric point of preparation II was shifted to that of preparation I, i.e., from 6.2 to 7.5. Activated preparation II behaved in DEAE cellulose chromatography as preparation I. Molecular weights of the enzymes of both preparations were 27 000, and pH optima were at pH 5.8 and 7.0, for BANA and leucine-2-napthylamide (Leu-NA), respectively. The BANA and Leu-NA hydrolyzing enzymes could not be separated by gel filtration, DEAE, CM, or Amberlite IRC-50 chromatography, isoelectric focusing, or analytical polyacrylamide gel electrophoresis. Two inhibitors of BANA hydrolase were demonstrated by gel filtration in the salt precipitated skin extract. The activities of the BANA hydrolase preparations did not increase linearly with increasing enzyme concentration, with the exceptions of activities of preparation I and acid-activated preparation II. The role of the inhibitors in the nonlinearity of the activity/enzyme concentration curves is discussed.     

含氮或碳中心原子的窝穴体开链类似物的合成与研究

本文合成了十种含氮或碳中心原子的窝穴体开链类似物(1a～e, 2a～e). 通过三乙醇胺, 季戊四醇及4-羟基安替比林的O-烷基化和用季戊四溴对2-巯基苯并咪唑, 2-巯基苯并噻唑的S-烷基化方法. 以它们作为液膜(CHCl~3)离子载体对Ag(I)迁移实验表明, 化合物1a～e迁移能力较强.     

Synthesis and characterization of water-soluble silver(I) complexes with L-histidine (H2his) and (S)-(-)-2-pyrrolidone-5-carboxylic acid (H2pyrrld) showing a wide spectrum of effective antibacterial and antifungal activities. Crystal structures of chiral helical polymers [Ag(Hhis)]n and ([Ag(Hpyrrld)]2)n in the solid state

Two water-soluble, silver(I) complexes showing a wide spectrum of effective antibacterial and antifungal activities, i.e., ([Ag(Hhis)].0.2EtOH)2 (1; H2his = L-histidine) and [Ag(Hpyrrld)]2 (3; H2pyrrld = (S)-(-)-2-pyrrolidone-5-carboxylic acid) were prepared. In aqueous solution 1 and 3 were present as dimers, whereas in the solid state they were polymers. Crystallization of 1 by slow evaporation and/or vapor diffusion gave water-insoluble crystals of [Ag(Hhis)]n (2) showing modest antimicrobial activities. The complex 1 in the solid state is a polymer formed by intermolecular hydrogen-bonding interactions between dimeric [Ag(Hhis)]2 cores, while 2 is a different polymer without a core complex. X-ray crystallography revealed that 2 was a left-handed helical polymer consisting of a bent, 2-coordinate silver(I) atom bonding to the Namino atom of one Hhis- ligand and the N pi atom of a different Hhis- ligand. Of particular note is the fact that Ocarboxyl atoms do not participate in the coordination. X-ray crystallography also revealed that 3 was a left-handed helical polymer formed by self-assembly of dimeric [Ag(Hpyrrld)]2 cores with an intramolecular metal(I)-metal(I) interaction (Ag-Ag distance, 2.9022(7) A). The FT-IR and the solid-state 13C and 15N NMR spectra showed that the dimeric core of 1 was formed through Ag-N bonds, while that of 3 was formed through Ag-O bonds. The molecular ions of 1 and 3 were detected by the positive-ion electrospray ionization (ESI) mass spectrometry. For 1-3, characterization by elemental analysis, TG/DTA, FT-IR, and variable-temperature solid-state 13C NMR and room-temperature 15N NMR measurements was performed, and for 1 and 3, that by solution molecular weight measurements and solution (109Ag, 1H, and 13C) NMR spectroscopies was also carried out. The antibacterial and antifungal activities of 1 and 3 were remarkable and comparable to those of the previous silver(I)-N-heterocycle complexes.     

5-取代氨基-12-取代苯并[c]菲啶衍生物的合成、晶体结构及生物活性

为了寻找新的高活性农药, 利用2-甲基苯甲腈与不同的醛反应, 再通过2,3-二氯-5,6-二氰基-1,4-苯醌(DDQ)脱氢或NaH和CH3I氮甲基化, 合成了3个系列共18个5-取代氨基-12-取代苯并[c]菲啶衍生物, 其中15个是未见文献报道的化合物. 它们的结构均经1H NMR, 13C NMR, IR和高分辨质谱表征; 用X射线衍射测定了化合物5-氨基-12-(4-二乙氨基苯基)-11,12-2H-苯并[c]菲啶盐酸盐(3c)的晶体结构. 初步的生物活性测试结果表明, 部分化合物具有一定的杀菌活性和促进黄瓜子叶生根活性.     

Synthesis of 1,4-disubstituted mono and bis-triazolocarbo-acyclonucleoside analogues of 9-(4-hydroxybutyl)guanine by Cu(I)-catalyzed click azide-alkyne cycloaddition

A series of novel mono-1,2,3-triazole and bis-1,2,3-triazole acyclonucleoside analogues of 9-(4-hydroxybutyl)guanine was prepared via copper(I)-catalyzed 1,3-dipolar cycloaddition of N-9 propargylpurine, N-1-propargylpyrimidines/as-triazine with the azido-pseudo-sugar 4-azidobutylacetate under solvent-free microwave conditions, followed by treatment with K(2)CO(3)/MeOH, or NH(3)/MeOH. All compounds studied in this work were screened for their antiviral activities [against human rhinovirus (HRV) and hepatitis C virus (HCV)] and antibacterial activities against a series of Gram positive and negative bacteria.     

Synthesis and fungicidal activity study of novel daphneolone analogs with 2,6-dimethylmorpholine

A series of novel daphneolone analogs was designed and synthesized on the basis of natural product 1,5-diphenyl-2-penten-1-one(I) from Stellera chamaejasme L. as lead compound, whereby 2,6-dimethylmorpholine moiety was introduced to replace 1-phenyl group. Their structures were confirmed by IR,1H NMR, and HRMS(ESI) or elemental analysis,13 C NMR for some representative compounds. The two isomers of target compounds were separated and identified by NOESY technique and chemical method.All of the synthesized compounds have been evaluated for anti-plant pathogenic fungi activities. The results showed that some compounds exhibited moderate to good antifungal activities against tested fungi at the concentration of 50 mg/L. Among them, compound 7d, with a 4-bromine-substituted phenyl group and cis-2,6-dimethylmorpholine moiety, displayed best activity with an EC50 of 23.87 mmol/L against Valsa mali, superior to lead compound I. In addition, preliminary structure–activity relationship analysis indicated that, between two isomers of target compounds, the antifungal activities of the isomer with cis-2,6-dimethylmorpholine were better than the trans-isomer.