含氟吡啶羧酸酯类化合物的合成及生物活性

为了寻找具有生物活性的新化合物,以氟乙酸甲酯、氰乙酰胺和甲酸乙酯为起始原料,经环合、氯化、水解、酰氯化等反应合成了含氟吡啶酰氯中间体,再与醇类和酚类反应合成了一系列含氟吡啶羧酸酯类化合物,总收率约38%。其结构经1HNMR、13CNMR、IR、MS及元素分析测试技术确证。初步杀虫抑菌活性测试表明,部分化合物1e、1i、1j和1k在500mg/L浓度下,对淡色库蚊的杀死率在61.9%～100%之间,但对几种受试植物病菌的抑制活性很差。化合物1k活性最好,在500mg/L时对粘虫(armyworm)和淡色库蚊(culex mosquito)的杀死率均为100%。初步构效关系分析表明,芳杂环酚的该类化合物有较好的活性,而脂肪醇的该类化合物无活性。     

Heterocyclic benzoxazole-based liquid crystals

The synthesis, characterization, and mesomorphic properties of a new type of heteronuclear compounds 1a-c and a Pd complex 1d derived from benzoxazole as the core group are reported. These compounds were prepared by the ring closure reaction of 4-alkoxybenzoic acid 4-[(4-alkoxy-2-hydroxyphenylimino)methyl]phenyl esters 6 in the presence of lead(IV) acetate. All the compounds were characterized by ¹H and ¹³C NMR spectroscopies and elemental analysis. The phase behaviour of these mesogenic compounds was characterized and studied by differential scanning calorimetry and polarizing optical microscopy. All the compounds 1a exhibited nematic (N) and/or smectic C (SmC) phases, as expected for rod-like molecules; however, the compounds 1b and 1c exhibited crystal phases. For those compounds 1a having shorter carbon chains (n = 1, 3, 4) nematic phases were observed, whereas for compounds having longer carbon chains (n = 6, 7, 8, 10, 12, 14) smectic C behaviour was also observed at lower temperatures. The greater aspect ratio (l/d) of compounds 1a compared with 1b and 1c was found to be required for the observation of liquid crystallinity. The fluorescent properties of these compounds were also examined. All λ_max peaks of the absorption and photoluminescence spectra of compounds 1a-1c occurred at c. 316-322 nm and 371-382 nm, respectively. The quantum yields of some compounds were relatively low, and also slightly solvent-dependent.     

Magnesium-butadiene addition compounds: Isolation,structural analysis and chemical reactivity

The magnesium-butadiene 1 : 1 (1), 1 : 2 (II) and 1 : 3 addition compounds obtained by the direct metalation of butadiene with metallic magnesium were isolated. These compounds have a polymeric structure. Structural analysis of these compounds by NMR and IR methods was carried out. The process for the formation of II via I and III via II was investigated. The results of protolysis and alkylation of the above magnesium compounds corresponded well to those of crotylmagnesium compounds.     

STUDIES ON 1,2,3-DIAZAPHOSPHOLE Ⅳ REACTION OF 1,2,3-DIAZAPHOSPHOLE WITH ALCOHOLS

Rapid addition of alcohols to 1,2,3-diazaphosphole 1 easily gave tricoordinatedphosphorus compounds,which were sulfurized to tetracoordinated phosphorus compounds.When ethylene glycol and aminoethanol were used separately to react with 1,the tricoordinatedphosphorus compounds which formed,rearranged to pentacoordinated phosphorus compoundsand the substituents at N_2 affected the rearrangement significantly.     

α-(1H-1,2,4-三唑-1-基)-β-芳硫基取代苯酮的合成及生物活性研究

利用 2 (1H 1,2 ,4 三唑 1 基 ) 2 丙烯 1 酮 (2 )与取代硫酚或含巯基的杂环化合物进行 1,4 亲核加成 ,得到目标化合物 3,其结构经元素分析、核磁和红外光谱所证实 ,并对其进行了生物活性的测试 ,发现大部分化合物具有很好的抑菌活性 .结构与活性的关系表明不同的R1取代对其生物活性有较大的影响 ,当R1=(CH3 ) 3 C时 ,对小麦锈病的抑制活性要高于R1=Ar的活性 ,而Ar上不同的取代基对其活性影响不大     

α-(1H-1,2,4-三唑-1-基)-β-芳硫基取代苯酮的合成及生物活性研究

利用2-（1H-1,2,4-三唑-1-基）-2-丙烯-1-酮（2）与取代硫酚或含巯基的 杂环化合物进行1,4-亲核加成,得到目标化合物3,其结构经元素分析、核磁和红 外光谱所证实,并对其进行了生物活性的测试,发现大部分化合物具有很好的抑菌 活性。结构与活性的关系表明不同的R~1取代对其生物活性有较大的影响,当R~1 = （CH_3）_3C时,对小麦锈病的抑制活性要高于R~1 = Ar的活性,而Ar上不同的 取代基对其活性影响不大。     

Synthesis,Chemistry and Applications of Heterocyclic Cage Compounds (V)

The synthesis and chemistry of polycyclic cage compounds have attracted considerable attention in recent years.¹ The vast majority of the work reported in this area has dealt with caybocyclic cage compounds. On the other hand, the synthesis and chemistry of heterocyclic cage compounds have received less attention. Recently, we have accomplished the synthesis of a series of oxa-cage compounds and performed the chemical transformations of these oxa-cage compounds.² As part of a program that involves the synthesis,chemistry and applications of heterocyclic cage compounds we report here the synthesis of heterocyclic cage compounds 1-12. We also wish to report the applications of compounds 7-12 on the π-facial selectivities. Studies on the cation-binding properties of compounds 1 and 2 and other oxa-cages are undertaken.     

反相薄层色谱法测定1-1,2,4-三唑类杀菌剂的疏水性

1-1 ,2 ,4-三唑类农药是本世纪 60年代初期发展起来的新型杀菌剂 ,具有广谱、高效和内吸等优点 ,一直是农药研究的热门课题 [1] .多年的研究表明 ,其疏水性与活性有很好的相关性 ,因此快速准确地测定其疏水性显得十分重要 .与传统的振荡方法测定化合物的疏水性相比 ,反相高效液相色谱法( RP-HPLC) [2～ 4 ] 和反相薄层色谱法 ( RP-TL C) [5,6 ] 简单、快速、经济 ,所需样品量很少 ,对样品纯度要求也不高 .尤其是薄层色谱法所需仪器简单 ,耗时更短 .本文以甲醇 -水混合物为展开剂测定了我们合成的 2 3种新型三唑类化合物在 C2高效薄层板…     

Research on the Synthesis and Optical Properties of Isomeric Bichromophoric Compounds --3-or 4- Phenyl 7-Coumarin ω-9-Anthracene-Poly-methene Carboxylate

Six bichromophoric compounds-substituted coumarin ω -9-anthra-cene-poly-methene carboxylate and five model compounds were synthesized. Among them, eight compounds are new ones. Intramolecular singlet energy transfer has been demonstrated in the bichromophoric compounds 1? and studied in some detail. The absorption spectra of the compounds 1-6 bear evidence that the π-electron systems of coumarin and anthracene ring do not overlap appreciably. The coumarin moiety of the bichromophoric compounds molecule was excited at 314nm and the resulting fluorescence was characteristic of the anthracene group. The efficiency of transfer of singlet excitation from coumarin moiety to the anthracene grou is about 100% in both calculation and observation and the rate of the singlet energy transfer is about 1014 sec in the compounds 4-6. A possible mechanism of intramolecular energy transfer was suggested. The difference between 4-phenyl compounds 1-3 and 3-phenyl compounds 4-6 in spectra was com -pared.     

Syntheses of highly fluorescent GFP-chromophore analogues

Eight B-containing compounds, i.e., 1a-h, were prepared as mimics of the green fluorescent protein (GFP) fluorophore. The underlying concept was that synthetic GFP chromophore analogues are not fluorescent primarily because of free rotation about an aryl-alkene bond (Figure 1b). This rotation is not possible in the beta-barrel of GFP; hence, the molecule is strongly fluorescent. In compounds 1a-h, radiationless decay via this mechanism is prevented by complexation of the BF2 entity. The target materials were prepared via two methods; most were obtained according to the novel route shown in Scheme 1b, but compound 1f was made via the procedure described in Scheme 2. Both syntheses involved formation of undesired compounds E-4a-h that formed simultaneously with the desired isomeric intermediates Z-4a-h. Both compounds form BF2 adducts, i.e., 1a-h and 5a-h, respectively. Methods used for spectroscopic characterization and differentiation of compounds in the series 1 and 5 are discussed, and these are supported by single-crystal X-ray diffraction analyses for compounds 1c, 5c, 1f, and 5f. Electronic spectra of compounds 1a-h and 5a-h were studied in detail. Those in the 5 series were shown to be only weakly fluorescent, but the 1 series were strongly fluorescent compounds (comparable to the boraindacene, BODIPY, dyes). Compounds 1g and 1h are water soluble, and 1h has particularly significant potential as a probe, since it also has a carboxylic acid group for attachment to biomolecules.     

Determination of phenolic compounds in water using membrane inlet mass spectrometry

Two membrane inlet mass spectrometric (MIMS) methods for determining phenolic compounds in water are described and compared, namely direct analysis and analysis after acetylation of the phenolic compounds. Direct analysis of phenolic compounds in water is a very simple and rapid method and detection limits are relatively low (from 30 mug 1(-1) for phenol to 1000 mug 1(-1) for 4-nitrophenol). Analysis of phenolic compounds after aqueous acetylation is also a very simple and rapid method, and the detection limits are even two orders of magnitude lower than in the direct analysis. For example the detection limit of phenol acetate is 0.5 mug 1(-1) and that of 4-nitrophenol is 10 mug 1(-1). The acetylation method was also tested in the analysis of phenolic compounds from contaminated surface water samples.     

Synthesis and biological evaluation of novel isopropanolamine derivatives as non-peptide human immunodeficiency virus protease inhibitors

Novel potential human immunodeficiency virus (HIV) protease inhibitors were designed by a combination of nelfinavir and amprenavir motifs. The designed compounds were prepared by a facile synthetic route and their stereochemistry was further confirmed by a stereospecific synthesis from commercially available (S)-2-oxiranylmethyl m-nitrobenzenesulfonate. All compounds were tested for their ability in inhibiting HIV type 1 protease activity with the published method of reference 19. Derivatives 1a--u exhibited moderate to significant inhibitory activities in preliminary bioassay. The best compound 1a has IC50 value of 0.02 microM, comparable to that of amprenavir. A docking study on compounds 1a--u was performed using the published X-ray crystal structure of HIV type 1 protease, all compounds bound to the HIV type 1 protease in an extended conformation and the scaffoldings of the binding conformations could be aligned quite well. Comparative molecular field analysis (CoMFA) study was performed to explore the specific contributions of electrostatic and steric effects in the binding of these new compounds to HIV type 1 protease and a predictive CoMFA model was built with thirteen compounds as training set. Test analysis of other five compounds as test set demonstrated that the CoMFA model has strong predictive ability to this series of compounds. It will be very useful to further optimize the designed inhibitors.     

含(1-芳乙酰胺基-2-叔胺基)乙烷结构的六氢-1H-1,4-二氮(艹卓)类化合物的合成与镇痛活性

2-或5-取代的六氢-1H-1,4-二氮(艹卓)类化合物(1～3)经单酰化及酰化反应后,合成了16个带有(1-芳乙酰胺基-2-叔氨基)乙烷结构的六氢-1H-1,4-二氮(艹卓)类目标化合物(5～9,11～13,15～17,19～23),经元素分析、IR、MS和¹H NMR确证了其组成和结构。对所有目标化合物都进行了豚鼠回肠试验,初步药理试验表明,16个化合物对受试标本显示不同程度的抑制作用,对抑制率较高的两个化合物5和7测试了IC₅₀值。对在豚鼠回肠试验中显示较强激动作用的4个化合物进行了小鼠扭体法镇痛活性试验,测得了其ED₅₀值。     

Theoretical calculation of nitro-1-(2,4,6-trinitrophenyl)-1H-azoles energetic compounds

In order to study the properties of new energetic compounds formed by introducing nitroazoles into 2,4,6-trinitrobezene, the density, heat of formation and detonation properties of 36 nitro-1-(2,4,6-trinitrobenzene)-1H-azoles energetic compounds are studied by density functional theory, and their stability and melting point are predicted. The results show that most of target compounds have good detonation properties and stability. And it is found that nitro-1-(2,4,6-Trinitrophenyl)-1H-pyrrole compounds and nitro-1-(2,4,6-trinitrop-enyl)-1H-Imidazole compounds have good thermal stability, and their weakest bond is C NO₂ bond, the bond dissociation energy of the weakest bond is 222–238 kJ mol⁻¹ and close to 2,4,6-trinitrotoluene (235 kJ mol⁻¹). The weakest bond of the other compounds may be the C NO₂ bond or the N N bond, and the strength of the N N bond is related to the nitro group on azole ring.     

Isolation of toxic compounds from wild Phaeocystis globosa

Two new compounds, namely taenialactam C and globorin A (1 and 2), as well as six known compounds, cornoside (3), 2-phenylethyl-b-D-glucoside (4), 3-isopropyl-5-acetoxycyclohexene-2-one-1 (5), 4-methyl-phenol (6), 5-[(2S)-2-aminobutyl]-2-methyl-phenol (7), and 1-(4-methylphenyl)-1-propanone (8) were isolated from wild Phaeocystis globosa. The structures of the new compounds were established by detailed spectroscopic analysis and by comparison with spectral data of related known compounds. The structures of the known compounds were identified by comparing their spectroscopic data with those reported in the literature. This paper also reports toxicity properties of the eight compounds against the brine shrimp Artemia salina and juvenile Epinephelus akaara fish. Some of these compounds showed significant lethality on the brine shrimp A. salina and the juvenile E. akaara fish.     

Activation mechanisms of butyrylcholinesterase by 2,4,6-trinitrotoluene, 3,3-dimethylbutyl-N-n-butylcarbamate, and 2-trimethylsilyl-ethyl-N-n-butylcarbamate

The goal of this work was to propose a possible mechanism for the butyrylcholinesterase activation by 2,4,6-trinitrotoluene (TNT), 3,3-dimethylbutyl-N-n-butylcarbamate (1), and 2-trimethylsilyl-ethyl-N-n-butylcarbamate (2). Kinetically, TNT, and compounds 1 and 2 were characterized as the nonessential activators of butyrylcholinesterase. TNT, and compounds 1 and 2 were hydrophobic compounds and were proposed to bind to the hydrophobic activator binding site, which was located outside the active site gorge of the enzyme. The conformational change from a normal active site gorge to a more accessible active site gorge of the enzyme was proposed after binding of TNT, and compounds 1 and 2 to the activator binding site of the enzyme. Therefore, TNT, and compounds 1 and 2 may act as the excess of butyrylcholine in the substrate activator for the butyrylcholinesterase catalyzed reactions.     

顺,反式环丙烷衍生物异构体的区分

在化学电离条件下，研究了４种顺、反式环丙烷衍生物与丙酮和醋酸乙烯酸乙烯酯的分子离子反应。异构体１，２的丙酮ＣＩ谱及其加合离子「Ｍ＋Ｈ＋Ａ」的ＣＩＤ谱都 可以区分该对异构体。化合物２，３和４可以和质子化丙酮及质子化二聚体发生加合反应，但化合物１仅能与质子化丙酮发生加合反应。在醋酸乙烯酯的ＣＩ谱中，观察到４个化合物的质子化二聚体，其中异构体１，２的质子化二聚体的ＣＩＤ谱也能反映它们立体结构的差异。     

A μ(1,1)- or μ(1,3)-carboxylate bridge makes the difference in the magnetic properties of dinuclear Mn(II) compounds

Six new dinuclear Mn(II) compounds with carboxylate bridges have been synthesized and characterized by X-ray diffraction: [{Mn(phen)(2)}(2)(μ-RC(6)H(4)COO)(2)](ClO(4))(2) with R = 2-Cl (1), 2-CH(3) (2), 3-Cl (3), 3-CH(3) (4), 4-Cl (5) and 4-CH(3) (6). Compounds 1 and 2 show two μ(1,3)-carboxylate bridges in a syn-anti mode while compounds 3-6 present a very uncommon coordination mode of the carboxylate ligand: the μ(1,1)-bridge. The magnetic properties of these compounds are very sensitive to the bridging mode of the carboxylate ligands. While compounds 1 and 2 (μ(1,3)-bridge) display antiferromagnetic interactions, with J values of -1.41 and -1.66 cm(-1), respectively, compounds 3-6 (μ(1,1)-bridge) show ferromagnetic interactions, with J values of 1.01, 0.98, 1.04 and 1.06 cm(-1), respectively. It is worth noting that compounds 3-6 are the first of their class to be magnetically characterized. The EPR spectra at 4 K for compounds with antiferromagnetic coupling (1 and 2) are more complex than those for compounds with a ferromagnetic interaction (3-6). Quite good simulations can be obtained with the ZFS parameters of the Mn(II) ion D(Mn) ~ 0.095 cm(-1) and E(Mn) ~ 0.025 cm(-1) for compounds 1 and 2 and D(Mn) ~ 0.060 cm(-1) and E(Mn) ~ 0.004 cm(-1) for compounds 3-6.     

Nucleophilic additions of arylzinc compounds to aldehydes mediated by CrCl(3): efficient and facile synthesis of functionalized benzhydrols, 1(3H)-isobenzofuranones, benzyl alcohols, or diaryl ketones

In the presence of a stoichiometric amount of CrCl(3) and trimethylchlorosilane (TMSCl), nucleophilic addition of arylzinc compounds 1c-h to arylaldehydes 2a,b,g smoothly proceeded at room temperature to yield corresponding benzhydrols 4a-f in good yields. From arylzinc compounds 1a,b, 3-aryl-1(3H)-isobenzofuranones 3a-f were given by the CrCl(3)-mediated reaction with arylaldehydes 2a-f. Diaryl ketones 5a-e were obtained in good yields by the addition of excess amount of benzaldehyde as an oxidant to the resulting solution after the CrCl(3)-mediated reaction between arylzinc compounds 1c-g and arylaldehydes 2b,g was completed. In the nucleophilic additions of arylzinc compounds 1a,d,f to alkyladehydes 6b-f, the treatment of arylzinc compounds with CrCl(3) was required prior to the addition of the aldehydes in order to prevent the fast protodezincation of arylzinc compounds by the enolizable aldehydes. In these CrCl(3)-mediated nucleophilic additions of arylzinc compounds to aldehydes, arylchromium(III) species are probably reactive intermediates.     

Syntheses of New Multisubstituted 1-Acyloxyindole Compounds

The syntheses of novel 1-acyloxyindole compounds 1 and the investigations on reaction pathways are presented. Nitro ketoester substrate 2, obtained in a two-step synthetic process, underwent reduction, intramolecular addition, nucleophilic 1,5-addition, and acylation to afford 1-acyloxyindoles 1 in one pot. Based on the systematic studies, we established the optimized reaction conditions for 1 focusing on the final acylation step of the intermediate 1-hydroxyindole 8. With the optimized conditions, we succeeded in synthesizing 21 examples of new 1-acyloxyindole derivatives 1 in modest yields (Y = 24 − 35%). Among the 1-acyloxyindole compounds, 1-acetoxyindole compounds 1x were generally unstable, and their yields were relatively lower than the other 1-acyloxyindoles. We expect that a bulkier alkyl or aromatic group on R² could stabilize the 1-acyloxyindole compounds. Significantly, one-pot reactions of a four-step sequence successfully generated compounds 1 that are all new and might be difficult to be synthesized otherwise.