17-β-雌二醇对心肌缺氧/复氧NF-κB及ICAM-1和VCAM-1表达的影响

利用乳鼠原代培养心肌细胞建立缺氧/复氧模型, 采用流式细胞术、Western blot、RT-PCR及Elisa等方法, 研究了17-β-雌二醇对缺氧/复氧诱导的ICAM-1和VCAM-1表达的影响, 分析雌激素在心肌缺氧/复氧损伤中的抗炎作用. 结果表明, 心肌缺氧/复氧使NF-κB p65活化, 雌激素对NF-κB活化有明显的抑制作用. 雌激素对NF-κB途径和对非NF-κB途径ICAM-1和VCAM-1的mRNA和蛋白表达都有抑制作用. 以上结果说明雌激素在心肌缺氧/复氧过程中的抗炎作用是通过多途径实现的.     

铬强化饲料喂养鸭的实验观察

用三氯化铬强化饲料喂养鸭,剂量从小到大。观察不同剂量所致器官性损害的效应关系及各脏器组织铬蓄积情况。对照组分别与实验组各组相比较,均有显著性差异（P＜0．05）;实验组1与实验组2也有显著性差异（P＜0．05）。鸭体各部位含铬量（10^-6)不同,其顺序是：脑（1．500）＞蛋（0．930）＞胸骨（0．880）＞大腿骨（0．440）＞肾（0．392）＞大腿肉（0．340）＞肠（0．290）＞胸肉（0．255）＞肝（0．180）。     

蛋鸡对日粮镁水平的反应

试验采用玉米-豆饼型试验日粮,高镁组（6000×10-6,MgO）鸡血液中镁含量显著高于中镁组（1200×10-6,MgO）和对照组（0．00×10-6,MgO）（P＜0．05）,中镁组与对照组间无显著差异（P＞0．05）,而血液中其他矿物元素含量三组间无显著差异（P＞0．05）。在肝脏中,高镁组的磷沉积量显著低于中镜组和对照组（P＜0.05）,而中镁组与对照组间无显著差异（P＞0．05）,其他矿物元素沉积量三组间无显著差异（P＞0.05）。在脾脏、肾脏、胰脏中镁、其他矿物元素的含量及沉积量三组间无显著差异（P＞0.05）。肝脏、脾脏、肾脏、胰脏的鲜重三组间无显著差异（P＞0．05）。     

发铅与缺铁性贫血关系的探讨

测定了40例缺铁性贫血患儿的发铅,并与健康对照组比较,结果表明,缺铁性贫血患儿发铅水平显著高于对照组（P＜0．01）,缺铁性贫血组发铅不高的9例平均血红蛋白量明显高于发铅高的31例（P＜0．05）,提示铅与缺铁性贫血有关。     

活细胞单分子力谱研究阿托伐他汀对ICAM-1与CD11b相互作用的影响

调节细胞黏附的整合素蛋白CD11b与其配体ICAM-1的相互作用在动脉粥样硬化的炎症进程中起至关重要的作用.阿托伐他汀(Atorvastatin,ATV)作为他汀类药物中的主要成员,以其良好的降脂作用广泛应用于动脉粥样硬化疾病的临床治疗,同时大量证据表明ATV还具有独立的抗炎作用,但其具体分子机制尚未完全明确.我们应用活细胞单分子力谱法研究了ATV干预对ICAM-1/CD11b相互作用的影响.结果表明原子力显微镜(AFM)在活细胞表面测得单对黏附分子ICAM-1/CD11b的相互作用力值约为40pN,ATV不能通过直接阻断ICAM-1或CD11b影响其单分子黏附力,而抗ICAM-1单克隆抗体则有效降低了此对黏附分子作用力.此外,流式结果表明ATV干预有效抑制了肿瘤坏死因子(TNF-α)诱导的人脐静脉内皮细胞(HUVEC)表面ICAM-1表达增加.本研究建立的方法模型可作为活细胞体系研究临床药物影响细胞黏附分子间相互作用及抗炎机制的重要手段.     

氟化石墨材料的改性及其电化学性能研究

本文以商用氟化石墨为原料,通过水合肼还原的方法对氟化石墨（CF_x）进行改性处理,系统研究了不同水合肼用量对材料电化学性能的影响. 采用XRD、SEM、EDS、XPS、交流阻抗（EIS）和恒流放电测试技术,对改性氟化石墨材料的物相及电化学性能进行了分析研究. 结果表明,采用改性氟化石墨材料制备的锂/氟化碳（Li/CF_x）电池的电压滞后现象得到明显改善,且不同水合肼用量对材料的电化学性能有重要影响. H-CF_x-2（CF_x：C₂H₆O：N₂H₄·H₂O 的比例为1：2：1）材料的综合性能最佳,在0.1C 倍率下,材料的克比容量达到794.5 mAh·g^-1,平台电压为2.53V,电压滞后现象的低波电压为2.37 V.     

17-β-雌二醇对心肌缺氧/复氧NF-κB及ICAM-1和VCAM-1表达的影响

利用乳鼠原代培养心肌细胞建立缺氧/复氧模型,采用流式细胞术、Western blot、RT-PCR及Elisa等方法,研究了17-β-雌二醇对缺氧/复氧诱导的ICAM-1和VCAM-1表达的影响,分析雌激素在心肌缺氧/复氧损伤中的抗炎作用.结果表明,心肌缺氧/复氧使NF-κB p65活化,雌激素对NF-κB活化有明显的抑制作用.雌激素对NF-κB途径和对非NF-κB途径ICAM-1和VCAM-1的mRNA和蛋白表达都有抑制作用.以上结果说明雌激素在心肌缺氧/复氧过程中的抗炎作用是通过多途径实现的.     

恩诺沙星分子印迹纳米纤维膜的制备及性能

通过沉淀聚合法制备了恩诺沙星（ENRO）分子印迹聚合物（MIPs）微球,将其添加到聚乙烯醇（PVA）溶液中,采用静电纺丝技术制备了恩诺沙星分子印迹纳米纤维膜（MINFMs）. 利用扫描电子显微镜（SEM）研究了纺丝液浓度、纺丝电压及接收距离对MINFMs纤维直径及表面形貌的影响,从溶胀性、孔隙率、吸附容量及吸附选择性等几个方面对印迹膜的性能进行了评价. 结果表明,在环境温度25 ℃、相对湿度 40%~50%、MIPs加入量8%（质量分数）、PVA质量分数7%、纺丝电压15 kV和接收距离25 cm的条件下,得到的MINFMs的纤维形态良好,纤维平均直径为180 nm. MINFMs的溶胀度和孔隙率分别为136.76%和33.42%,均大于非印迹纳米纤维膜（NINFMs）. 动力学吸附性能结果显示,MINFMs在300 min后吸附基本达到平衡,且明显高于NINFMs的吸附量;Scatchard分析结果表明,在所研究的浓度范围内MINFMs对模板ENRO的结合位点是等价的,其离解平衡常数（K_d）与最大表观结合量（Q_max）分别为505.817 mg/L和3.862 mg/g. 与环丙沙星（CIP）和氧氟沙星（OFL）相比,MINFMs对ENRO表现出更强的特异性吸附能力.     

溶液处理富锂锰基固溶体Li_1.2Mn_0.54Ni_0.13Co_0.13O_2

针对Li1.2Mn0.54Ni0.13Co0.13O2材料的首次效率过低和倍率性能差的缺陷,系统研究了中性去离子水、弱酸性的硫酸铵和强酸性的磷酸3种不同pH值的溶液处理对Li[Li0.2-Mn0.54Ni0.13Co0.13]O2综合性能的影响.ICP结果表明预处理液的pH值对Li的析出量有显著影响;XRD结果显示处理对材料的体相结构有影响;XPS证实处理对材料表面过渡金属元素的价态没有影响.充放电测试表明,硫酸铵处理后的样品具有最优的电化学性能,首次效率由64.6%提高到85.4%,1 C放电容量从149.5 mA h g?1提高到183.7 mA h g?1,中值电压呈缓和下降趋势.     

含有手性和发光官能团侧基的聚1-苯基-1-辛炔的合成与性能研究

设计并合成了一系列含手性和发光生色团侧基的聚（1-苯基-1-辛炔）衍生物{-[（C6H13）C=C（C6H4-p-CO2-R）]n-,R=[（1S）-endo]-（-）-冰片基（P3）,（1R,2S,5R）-（-）-薄荷基（P4）,-C6H4-p-（1R,2S,5R）-（-）-薄荷基（P5）,2-萘基（P6）,4-联苯基（P7）}.用WCl6-Ph4Sn作催化剂,成功地制备了这些具有中等产率和高分子量（Mw高达64000）的聚合物.聚合物的结构和性能通过NMR,TGA,UV,CD,PL和EL等分析方法进行了表征.所有聚合物都表现出良好的热稳定性,在N2保护条件下,其失重5%的温度在300～416℃之间.所有聚合物的带隙约为3.0eV.聚合物P4和P5表现出与聚合物链段螺旋性相对应的CD吸收.在UV辐照下,P3～P7的THF溶液均发射强烈蓝光,其最大发射波长位于485nm左右,量子效率均高于20%.聚合物薄膜发射与其溶液发射在相同的光谱区域,并表现出轻微的聚集诱导猝灭.制备了ITO/聚合物：PVK/BCP/Alq3/LiF/Al多层聚合物EL器件,其最大发射波长为487nm.随着侧基的改变,器件的最大亮度和外量子效率也随之发生变化,其中P6表现出最高的外量子效率（0.16%）.EL器件均具有良好的光谱稳定性,其EL最大发射峰几乎不随外加电压的变化而改变.     

Identification and X‐ray Co‐crystal Structure of a Small‐Molecule Activator of LFA‐1‐ICAM‐1 Binding

Stabilization of protein–protein interactions by small molecules is a concept with few examples reported to date. Herein we describe the identification and X‐ray co‐crystal structure determination of IBE‐667, an ICAM‐1 binding enhancer for LFA‐1. IBE‐667 was designed based on the SAR information obtained from an on‐bead screen of tagged one‐bead one‐compound combinatorial libraries by confocal nanoscanning and bead picking (CONA). Cellular assays demonstrate the activity of IBE‐667 in promoting the binding of LFA‐1 on activated immune cells to ICAM‐1.     

不同液体介质的高压静电雾化试验研究

自行设计、组装高压静电雾化试验装置,研究同一环境下煤油、乳化剂和酒精3种不同液体介质在高压静电场中的雾化过程.结果表明:液体介质的表面张力和粘性力越小、电导率越大,静电雾化效果越好.煤油、乳化剂和酒精分别在40 V,10 kV和25 kV时达到最佳的雾化效果.     

Photochemically inactivated hepatitis B virus promotes upregulation of Th1-type cytokines

Photochemical virus inactivation technology is widely used to improve the safety of blood products. However, the process by which this inactivation occurs and the resulting immunogenicity of treated viruses remain to be elucidated. This study aimed to explore the effects of two photochemical inactivation methods (methylene and riboflavin, MP and RP) on hepatitis B virus (HBV) immunogenicity. Inactivated HBV were incubated with PBMC from six healthy donors. Culture supernatants were collected at 0, 24 and 72 h for the analysis of HBsAg and HBeAg expression using ELISA. Cytokine expression was analyzed at 72 h using ELISA. Costimulatory and cell adhesion molecule mRNA expression was analyzed at 24 h by RT–PCR. No significant changes in HBsAg and HBeAg were detected following MP. However, the secretion of TNF‐α and IFN‐γ was upregulated. Expression of CD80, CD86, ICAM2 and LFA3 mRNA was also upregulated. In contrast, although RP did not significantly alter HBsAg expression, a reduction in HBeAg expression was observed. Furthermore, no upregulation of cytokines and intracellular molecule expression was observed following RP. These data indicate that the immunogenicity of HBV is retained following MP, and the inactivation of HBV could upregulate the Th1‐type cellular immune responses, which may play significant roles in the antiviral process.     

苯乙酸对肝癌细胞系SMMC-7721的增殖抑制作用及与RNA编辑酶ADAR1表达的相关性

为探讨苯乙酸(PA)对肝癌细胞系SMMC-7721的增殖抑制作用及其与RNA编辑酶ADAR1表达的相关性, 应用细胞计数及MTT法检测了不同浓度(0.5, 1.0, 2.0和4.0 mmol/L)PA对肝癌细胞系SMMC-7721的增殖抑制作用, 通过流式细胞术(FCM)分析了各细胞周期的细胞百分比, 应用半定量逆转录-聚合酶链式反应(RT-PCR)及免疫印迹杂交分析使用不同浓度(0.5, 1.0, 2.0 mmol/L)PA作用后肝癌细胞系SMMC-7721中RNA编辑酶ADAR1 mRNA及蛋白表达的变化. 结果表明, 肝癌细胞系SMMC-7721经不同浓度PA作用后, 增殖抑制率随作用时间延长及PA浓度增加而明显提高(P<0.05), 但2.0和4.0 mmol/L PA作用72 h后组间差异比较无统计学意义(P>0.05). 肝癌细胞系SMMC-7721中RNA编辑酶ADAR1 mRNA及蛋白表达随PA浓度增加而明显降低(P<0.05). 通过沉默SMMC-7721细胞中ADAR1的表达发现, ADAR1表达下调可有效抑制肝癌细胞增殖. 结果表明, PA可阻抑肝癌细胞系SMMC-7721细胞增殖, 且存在时间及剂量的依赖性, 作用机制与PA下调ADAR1表达相关.     

A high resolving power multiple reflection matrix-assisted laser desorption/ionization time-of-flight mass spectrometer

Two electrostatic mirrors, mounted symmetrically on the same optical axis facing each other, are used to increase the time-of-flight of molecular ions produced in matrix-assisted laser desorption/ionization (MALDI). The mirrors, which are used in the non-compensating mode, are located between a MALDI ion source and a stop detector. The source is operated at 10.5 kV acceleration voltage using the delayed extraction technique. The high voltage for the mirror arrangement is switched on after the desorption event when the molecular ions have drifted into the region between the mirrors. The ions are trapped by successive reflections of the opposite electrostatic fields in the mirrors until the electric fields are switched off. The number of reflections depends on the speed of the ions when they enter the mirror trap and the ontime of the mirrors. When the electric fields are removed during the motion of the ions towards the stop detector, the ions penetrate the grids of the mirror and reach that detector. The extension of the flight path due to the number of reflections is used to increase the resolving power in time-of-flight spectra. Values of 55,000 for substance-P (MW 1346.7) and 31,000 for bovine insulin (MW 5734) were obtained for single laser shot spectra.     

Comparison of azacyclic urea A-98881 as HIV-1 protease inhibitor with cage dimeric N-benzyl 4-(4-methoxyphenyl)-1,4- dihydropyridine as representative of a novel class of HIV-1 protease inhibitors: A molecular modeling study

The functional groups of cage dimeric N-alkyl substituted 3,5-bis(hydroxymethyl)-4-(4-methoxyphenyl)-1,4-dihydropyridines are similar to those of cyclic and azacyclic ureas that are potent inhibitors of HIV-1 protease of the dihydroxyethylene- and hydroxyethylene type, respectively. In the following study the conformity of common functional groups is investigated concerning their orientation in space as well as in the enzyme HIV-1 protease. Starting from X-ray crystal data of the centrosymmetric cage dimeric N-benzyl derivative with ester groups, the derivative with hydroxymethylene groups was built and a systematic conformational search was performed for the conformationally important torsion angles considering electrostatic and van der Waals interactions. From the huge number of conformations those comprising centrosymmetrical and C2-symmetrical energy minima were selected and minimized. The three remaining conformers were fitted to the azacyclic urea A-98881 selected from the HIV-1 protease enzyme- inhibitor complex using the centroids of the corresponding aromatic residues and additionally by the field fit option of the Advanced CoMFA module of SYBYL. Interestingly, the energetically most favourable one, which, additionally, possesses C2-symmetry like the active site cavity of HIV-1 protease, showed the best fit. Comparing the electrostatic potential (EP) of the latter with the EP of A-98881 the aromatic residues show excellent accordance. Slight differences in the extent of the EP were found in the areas of the hydroxymethylene groups of the cage dimer and the single hydroxy group as well as the urea carbonyl group of A- 98881, respectively. In order to compare the binding possibilities to the enzyme HIV-1 protease for the cage dimer and A-98881, their interaction fields with certain probes (CH3 for alkyl, NHamide, and carbonyl, O– of COO–), representing the decisive functional groups of the active site, have been calculated using GRID and projected into the enzyme placing the structures according to the position of A-98881 in the enzyme- inhibitor complex. The strongest calculated fields of the O– probe were found near Asp 25 for both structures. Another respective conformity consists in the overlap of the fields for the NHamide probe near Ile 50 and 50 for the investigated cage dimer and A-98881.     

3D-QSAR and molecular modeling of HIV-1 integrase inhibitors

Three-dimensional quantitative structure-activity relationship (3D QSAR) methods were applied on a series of inhibitors of HIV-1 integrase with respect to their inhibition of 3-processing and 3-end joining steps in vitro.The training set consisted of 27 compounds belonging to the class of thiazolothiazepines. The predictive ability of each model was evaluated using test set I consisting of four thiazolothiazepines and test set II comprised of seven compounds belonging to an entirely different structural class of coumarins. Maximum Common Substructure (MCS) based method was used to align the molecules and this was compared with other known methods of alignment. Two methods of 3D QSAR: comparative molecular field analysis (CoMFA) and comparative molecular similarity indices analysis (CoMSIA) were analyzed in terms of their predictive abilities. CoMSIA produced significantly better results for all correlations. The results indicate a strong correlation between the inhibitory activity of these compounds and the steric and electrostatic fields around them. CoMSIA models with considerable internal as well as external predictive ability were obtained. A poor correlation obtained with hydrophobic field indicates that the binding of thiazolothiazepines to HIV-1 integrase is mainly enthalpic in nature. Further the most active compound of the series was docked into the active site using the crystal structure of integrase. The binding site was formed by the amino acid residues 64-67, 116, 148, 151-152, 155-156, and 159. The comparison of coefficient contour maps with the steric and electrostatic properties of the receptor shows high level of compatibility.     

Inhibition of immediate type hypersensitivity reaction by combined irradiation with ultraviolet and visible light

Recently we found that ultraviolet B (UVB) irradiation in erythematous doses significantly inhibited the immediate type hypersensibility reaction in the skin. In the present study we investigated the effects of different wavelengths on the skin prick test reaction (SPT). The forearm of ragweed allergic patients was irradiated with increasing doses of ultraviolet A (UVA), visible light (VIS) or combined UVB, UVA and VIS light, referred to as mUV/VIS. SPTs were performed 24 h after irradiation both on irradiated and non-irradiated control skin areas using ragweed extract. UVA and VIS irradiation led to a slight, not significant inhibition of allergen-induced wheal formation. Mixed irradiation with mUV/VIS light resulted in a dose-dependent inhibition of the allergen-induced wheal formation. The inhibition was significant already at suberythematous doses. As there is a good correlation between SPT and the nasal symptoms in patients with hay fever these data suggest that phototherapy with mUV/VIS light might be an effective and safe treatment modality for immediate type hypersensibility reactions in the skin and nasal mucosa.     

毛细管区带电泳测定D1蛋白酶的活性及其抑制剂先导化合物的筛选

建立了毛细管区带电泳技术快速测定D1蛋白酶活性及其抑制剂先导化合物的筛选方法。实验选用未涂层熔融石英毛细管(43 cm 5mm)和磷酸盐缓冲溶液(50 mmol/L, pH 3.0)作为分离介质,运行电压18 kV,测定了D1蛋白酶的活性并对部分抑制剂先导化合物进行了筛选。结果表明, ITP26和ITP21两种异噁唑噻唑哌啶类先导化合物对蛋白酶活性具有抑制作用,抑制率分别为26%和13%。     

荔枝中水溶性维生素的毛细管电泳快速分离分析

本研究通过双模对接高压电源实现了毛细管电泳中0～40 kV及以上的超高电压。通过考察电压、缓冲溶液浓度、pH等对分离的影响,确定了优化的实验条件。结果表明,在40 kV的超高电压下,缓冲液为25 mmol/L硼砂-H3BO3溶液(pH 8.8),8种水溶性维生素(VB1、VB2、VB6、VC、D-泛酸钙、D-生物素和烟酸、叶酸)在2.2 min内获得了较好的基线分离。同时对荔枝中的水溶性维生素进行定量分析得到了令人满意的结果。