聚苯乙炔/碳纳米管复合材料的导电性能研究

本文以无水A lC l3作催化剂合成聚苯乙炔(PPA),用H2SO4对其进行磺化改性,采用其混法制得了PPA/碳纳米管(CNTs)及磺化PPA/CNTs复合材料,对二者的常温电导率及变温电导率进行了测试。结果表明:磺化PPA的电导率较PPA的提高了3个数量级;随着CMTs含量增加,复合材料的电导率升高;PPA/CNTs导电的阈值是3%,达极限电导率(0.04S/m)所需CNTs含量为25%,而磺化PPA/CNTs导电的阈值是2%,达极限电导率所需CNTs(0.14 s/m)含量为25%。并分析了温度变化对复合材料电阻变化的影响因素。     

溴蒸气掺杂聚苯乙炔的导电机理

通过溴蒸气的吸附, 聚苯乙炔(PPA)的电导率比吸溴前提高近12个数量级. 采用固体紫外光谱、X光电子能谱研究了溴与PPA之间的p-π共轭效应, 探讨了掺溴PPA的导电机理. 研究表明, PPA掺溴产生了溴负离子和电子转移复合物, 促使导电率提高. 实验证明压力作用的增大有利于增强溴与PPA之间的共轭作用, 温度升高导致掺溴PPA中p-π共轭结构减少, 导致电导率降低.     

吡哌酸的固体表面-延迟荧光法研究

研究了吡哌酸(PPA)的同体表面-延迟荧光特征,实验表明Be(Ⅱ)、Mg(Ⅱ)、Ca(Ⅱ)、Sr(Ⅱ)、Ba(Ⅱ)及Zn(Ⅱ)、Cd(Ⅱ)、La(Ⅲ)等无机盐能显著增强PPA的固体表面-延迟荧光(SS-DF).pH值对PPA的SS-DF有显著影响。寿命测量结果表明,在固体表面PPA是以双指数衰减的,同时测量了PPA的低温光谱,在本文选择的条件下,PPA分析曲线的线性范围为1.8～1800ng/斑点。     

聚α,α-二甲基-β-丙内酯与聚(1,2-丙二醇-丁二酸酯)ABA型嵌段共聚物的合成

通过合成双羟端聚(1,2-丙二醇己二酸酯)(PPA),经丁二酸酐酰化得双羧端PPA,再经(Bu_4N)_2CO_3-THF铵化得铵化PPA,最后用铵化PPA与α,α-二甲基-β-丙内酯(PVL)嵌段共聚,首次合成了PPVL-PPA-PPVL的ABA型脂肪族聚酯嵌段共聚物。     

碳糊电极阳极吸附伏安法测定吡哌酸

吡哌酸（Pipmidic acid,简称PPA）,是吡喹酮类合成抗菌药物,目前的主要分析方法有分光光度法、交流示波滴定法、高效液相色谱法、阴极吸附溶出伏安法、单扫描示波极谱法、微分脉冲极谱法和循环伏安法。本文提出了在CPE上阳极吸附伏安法测定PPA的方法,并探讨了PPA在CPE上的伏安性质和电极反应机理。该法准确、简便、灵敏度高,应用于模拟尿样中痕量PPA的测定,得到满意的结果。     

聚苯乙炔包覆多壁碳纳米管的制备及其分散性

用苯乙炔合成聚苯乙炔(PPA), 对多壁碳纳米管进行纯化、氧化, 然后将多壁碳纳米管与PPA一起在甲苯中超声分散. 结果显示氧化多壁碳纳米管已被PPA包覆且能够稳定分散于甲苯溶液中, 一个多月不沉降. 分别采用傅立叶变换红外(FTIR)光谱、酸碱滴定、拉曼光谱分析氧化后多壁碳纳米管的结构变化. 利用高分辨透射电镜(HRTEM)分别观察纯化、氧化、PPA包覆多壁碳纳米管的分散情况.     

反式聚苯乙炔的光电导

聚苯乙炔(PPA)是一种共轭高分子材料,具有较好的光电导性能。因反式PPA比顺式具有较高的光暗比,本文研究了反式PPA的光导和暗导特性,得到的光、暗导曲线基本平行,说明本征载流子和光生载流子的输运机制是相似的。在欧姆区的光导和暗导的活化能分别为0.24±0.03eV和0.58±0.03eV。     

多聚磷酸催化合成阿斯匹林

自1950年Snyder第一次认识多聚磷酸(PPA)的催化活性以后,PPA在环化、缩合、水解、重排等反应中,迅速成为极为有用的催化剂。阿斯匹林(乙酰水杨酸)有多种合成方     

粉末状聚苯乙烯气凝胶的结构调控及其液相吸附性能初探

在成功合成粉末状聚苯乙烯气凝胶(PPA)的基础上,详细研究了高分子纳米球构筑单元的结构和Friedel-Crafts超交联条件对PPA纳米结构的影响,初步考察了PPA对甲基红和亚甲基蓝的液相吸附性能。实验结果表明,PPA呈现三维纳米网络结构,其纳米球网络单元粒径约为30nm,且纳米球之间的堆叠形成大孔和中孔,从而具有独特的微孔-中孔-大孔层次化分布的孔结构特征。通过控制反应条件,其BET比表面积和总孔容可分别在201m~2·g~(-1)~702m~2·g~(-1)和0.16cm~3·g~(-1)~1.29cm~3·g~(-1)范围内调控。PPA自身较强的疏水性和丰富的孔隙结构赋予其对正辛烷中的甲基红和水溶液中的亚甲基蓝良好的吸附性能。     

Sixteen capillary electrophoresis applications for viral vaccine analysis

A broad range of CE applications from our organization is reviewed to give a flavor of the use of CE within the field of vaccine analyses. Applicability of CE for viral vaccine characterization, and release and stability testing of seasonal influenza virosomal vaccines, universal subunit influenza vaccines, Sabin inactivated polio vaccines (sIPV), and adenovirus vector vaccines were demonstrated. Diverse CZE, CE-SDS, CGE, and cIEF methods were developed, validated, and applied for virus, protein, posttranslational modifications, DNA, and excipient concentration determinations, as well as for the integrity and composition verifications, and identity testing (e.g., CZE for intact virus particles, CE-SDS application for hemagglutinin quantification and influenza strain identification, chloride or bromide determination in process samples). Results were supported by other methods such as RP-HPLC, dynamic light scattering (DLS), and zeta potential measurements. Overall, 16 CE methods are presented that were developed and applied, comprising six adenovirus methods, five viral protein methods, and methods for antibodies determination of glycans, host cell-DNA, excipient chloride, and process impurity bromide. These methods were applied to support in-process control, release, stability, process- and product characterization and development, and critical reagent testing. Thirteen methods were validated. Intact virus particles were analyzed at concentrations as low as 0.8 pmol/L. Overall, CE took viral vaccine testing beyond what was previously possible, improved process and product understanding, and, in total, safety, efficacy, and quality.     

Spectrophotometric and fluorimetric determination of diazepam, bromazepam and clonazepam in pharmaceutical and urine samples

New spectrophotometric and fluorimetric methods have been developed to determine diazepam, bromazepam and clonazepam (1,4-benzodiazepines) in pure forms, pharmaceutical preparations and biological fluid. The new methods are based on measuring absorption or emission spectra in methanolic potassium hydroxide solution. Fluorimetric methods have proved selective with low detection limits, whereas photometric methods showed relatively high detection limits. Successive applications of developed methods for drugs determination in pharmaceutical preparations and urine samples were performed. Photometric methods gave linear calibration graphs in the ranges of 2.85-28.5, 0.316-3.16, and 0.316-3.16 microgml-1 with detection limits of 1.27, 0.08 and 0.13 microgml-1 for diazepam, bromazepam and clonazepam, respectively. Corresponding average errors of 2.60, 5.26 and 3.93 and relative standard deviations (R.S.D.s) of 2.79, 2.12 and 2.83, respectively, were obtained. Fluorimetric methods gave linear calibration graphs in the ranges of 0.03-0.34, 0.03-0.32 and 0.03-0.38 microgml-1 with detection limits of 7.13, 5.67 and 16.47 ngml-1 for diazepam, bromazepam and clonazepam, respectively. Corresponding average errors of 0.29, 4.33 and 5.42 and R.S.D.s of 1.27, 1.96 and 1.14 were obtained, respectively. Statistical Students t-test and F-test have been used and satisfactory results were obtained.     

Determination of carbamazepine and its impurities iminostilbene and iminodibenzyl in solid dosage form by column high-performance liquid chromatography

An accurate and precise RP-HPLC method was developed and validated for the determination of carbamazepine and its impurities iminostilbene and iminodibenzyl in a tablet formulation with fluphenazine as an internal standard. Buffer-methanol (50 + 50, v/v) was used as the mobile phase. During validation, specificity, linearity, precision, accuracy, LOD, LOQ, and robustness of the method were tested. The method was proven to be specific against placebo interference. Linearity was evaluated over the concentration range of 100-500, 0.05-0.25, and 0.1-0.5 microg/mL, and the r values were 0.9994, 0.9997, and 0.9979 for carbamazepine, iminostilbene, and iminodibenzyl, respectively. Intraday precision of the method was good, and RSD was below 2% for all analytes. The accuracy of the method ranged from 100.69 to 102.10, 99.76 to 102.66, and 99.26 to 100.08% for carbamazepine, iminostilbene, and iminodibenzyl, respectively. LOD was 0.0125, 0.025, and 0.05 microg/mL and LOQ was 0.05, 0.05, and 0.1 microg/mL for carbamazepine, iminostilbene, and iminodibenzyl, respectiviely. Robustness of the method was proven by using a chemometric approach. The method was successfully applied to the analysis of commercially available carbamazepine tablets and showed good repeatability, with RSD below 2%.     

Stress-induced increase in the amounts of maysin and maysin derivatives in world premium natural compounds from centipedegrass

The red leaves of centipedegrass are known to produce compounds with stronger antibiotic effects than those produced by green leaves. Therefore, the aim of this study was to identify if stress methods (e.g., gamma irradiation, UV-B irradiation, and wounding) could effectively convert green leaves to red leaves, and thereby increase the production of maysin and maysin derivatives that have been known for antibiotic properties. Our results showed differential concentration changes for different compounds using these stress methods. The concentrations of luteolin increased from 0.014% to 0.019%, 0.022%, and 0.028% following gamma irradiation, UV-B irradiation, and wounding, respectively. The concentration of isoorientin increased from 0.898% to 1.938% and 2.538%, while the concentration of mixed rhamnosylisoorientin and orientin increased from 0.303% to 0.474% and 0.690%, following UV-B irradiation and wounding, respectively. Gamma irradiation produced concentrations of isoorientin, rhamnosylisoorientin, and orientin similar to those found in red leaves. The concentrations of derhamnosylmaysin increased from 0.004% to 0.009%, 0.015%, and 0.024% by gamma irradiation, UV-B irradiation, and wounding, respectively. The concentration of maysin increased from 0.515% to 0.714%, 0.583%, and 0.777% by gamma irradiation, UV-B irradiation, and wounding, respectively, while the concentration of luteolin-6-C-boivinopyranoside increased from 0.324% to 0.834%, 0.979%, and 1.493% by gamma irradiation, UV-B irradiation, and wounding, respectively. According to these results, wounding and gamma irradiation are promising methods for increasing the concentrations of maysin and maysin derivatives.     

Polymer-surfactant and protein-surfactant interactions

The phase behavior and some physicochemical properties of homopolymers (HP) and hydrophobically modified (HMP) polymers, as well as of polyelectrolytes (PE) and proteins (PR), in the presence of aqueous surfactants, or their mixtures, are discussed. Mixing the above components gives rise to the formation of organized phases, whose properties are controlled by polymer and/or surfactant content, temperature, pH, and ionic strength. Depending on the nature, concentration, and net charge of both solutes, molecular solutions, polymer-surfactant complexes, adsorption onto micelles and vesicles, gels, liquid crystalline phases, and precipitates are observed. Such rich polymorphic behavior is the result of a complex balance between electrostatic, excluded volume, van der Waals, and other contributions to overall system stability. It is also modulated by the molecular details and architecture of both the polymer and the surfactant. Different experimental methods allow investigation of the above systems and getting information on the nature of polymer-surfactant interactions (PSI). Surface adsorption and thermodynamic methods, together with investigation of the phase diagrams, give information on the forces controlling PSI and on the existence of different phases. Conductivity, QELS and viscosity allow estimating the size and shape of polymer-surfactant (protein-surfactant) complexes. Optical microscopy, cryo-TEM, AFM, NMR, fluorescence, and relaxation methods give more information on the above systems. Use of the above mixtures in controlling gelation, surface covering, preparing dielectric layers, and drug release is suggested.     

含希夫碱侧基聚酯及其锌配合物的合成和性能

经多步反应合成2种新型含希夫碱侧基聚酯(P5,P6),进一步与醋酸锌反应得到2种聚酯锌配合物(P5-Zn,P6-Zn)。 采用元素分析、FT-IR、UV-Vis、¹H NMR、GPC、TG、DSC和荧光光谱等技术手段对其结构和性能进行表征。 P5和P6均溶于四氢呋喃(THF)、氯仿(CHCl₃)、N,N-二甲基甲酰胺(DMF)、N,N-二甲基乙酰胺(DMAc)、二甲基亚砜(DMSO)、N-甲基吡咯烷酮法(NMP)等有机溶剂,P5-Zn和P6-Zn部分溶于THF及CHCl₃,溶于DMF、DMAc、DMSO、NMP等有机溶剂。 P5和P6的重均相对分子质量M_w及相对分子质量分布指数PDI分别为4164、6148 g/mol和1.42、1.43。 P5、P6、P5-Zn和P6-Zn的5%失重温度分别为339、348、367和358℃。 P5、P6、P5-Zn和P6-Zn的玻璃化转变温度T_g分别为88.8、123.3、39.8和63.8 ℃。 P5和P6的DMF溶液(5×10^-5 mol/L)在418和416 nm处发射弱紫色荧光,P5-Zn和P6-Zn的DMF溶液(5×10^-5 mol/L)在505和506 nm处发射强绿色荧光,固体P5-Zn和P6-Zn在527和532 nm处发射强绿色荧光。     

Determination of carbohydrates and sweeteners in foods and biologically active additives by high-performance liquid chromatography

A method for the determination of large amounts of carbohydrates (glucose, lactose, maltose, mannose, sucrose, and fructose) and sweeteners (xylitol and sorbitol) by reversed-phase liquid chromatography with refractive index detection without derivatization has been developed. The limits of determination for glucose, fructose, and sucrose in liquid samples were 0.1 g/L, and for xylite, lactose, maltose, mannose, and sorbite, 1 g/L. In solid samples the limits of determination for glucose, fructose, and sucrose were 0.1%, and for xylite, lactose, maltose, mannose, and sorbite, 0.6%. The method is applicable to the analysis of samples of wine, juice, honey, cookies, dairy products, and biologically active additives. The developed method for the determination of carbohydrates and sweeteners in foods and biologically active additives was certified in the Mendeleev Institute for Metrology (St. Petersburg).     

Analysis of selected phytotoxins and mycotoxins in environmental samples

Natural toxins such as phytotoxins and mycotoxins have been studied in food and feed for decades, but little attention has yet been paid to their occurrence in the environment. Because of increasing awareness of the presence and potential relevance of micropollutants in the environment, phytotoxins and mycotoxins should be considered and investigated as part of the chemical cocktail in natural samples. Here, we compile chemical analytical methods to determine important phytotoxins (i.e. phenolic acids, quinones, benzoxazinones, terpenoids, glycoalkaloids, glucosinolates, isothiocyanates, phytosterols, flavonoids, coumestans, lignans, and chalcones) and mycotoxins (i.e. resorcyclic acid lactones, trichothecenes, fumonisins, and aflatoxins) in environmentally relevant matrices such as surface water, waste water-treatment plant influent and effluent, soil, sediment, manure, and sewage sludge. The main problems encountered in many of the reviewed methods were the frequent unavailability of suitable internal standards (especially isotope-labelled analogues) and often absent or fragmentary method optimization and validation.     

Density,viscosity, and surface tension of binary liquid systems: Ethanoic acid,propanoic acid,and butanoic acid with nitrobenzene

Density, viscosity, and surface tension of three binary liquid systems: ethanoic acid+nitrobenzene, propanoic acid+nitrobenzene, and butanoic acid+nitrobenzene have been determined at 25, 35, and 45°C, over the whole composition range. The excess molar volumes, viscosities, Gibbs energies for the activation of flow, and surface tension were evaluated and fitted to a Redlich-Kister type of equation. The Grunberg-Nissan parameter d was also calculated. Binary viscosity data were fitted to the models of McAllister, Heric, Krishnan, and Laddha, Auslander, and Teja and Rice. Surface tension data were fitted to the models of Zihao and Jufu, Rice, and Teja, and an empirical two-constant model.