微量热法研究过氧化氢酶反应

利用微量热法和热动力学方程研究了过氢化氢酶反应.该反应遵循Michaelis-Menten动力学,298.15K和pH7.0时,其米氏常数、酶转换数以及摩尔反应焓分别为2.36×10^-2mol/L、1.20×10⁴s^-1和-83.67kJ·mol^-1.过氧化氢酶反应后期对底物是一级反应,其总反应速度常数和一级速度常数分别为k_o=6.31×10⁵L·mol^-1·s^-1和k₁=6.31×10⁵/[E_o]s^-1.该反应服从Ogura机理,其酶-底物三元复合物的分解速度常数为6.00×10³s^-1.     

溶剂对脂肪酶降解高分子量PBS及改性共聚物的影响

采用固定化脂肪酶分别在四氢呋喃(THF)、甲苯及THF和甲苯的混合溶剂体系中, 对高分子量的PBS及PBS/CHDM共聚物进行了催化降解, 用GPC测定了降解产物的分子量, 用质谱(MS)对降解产物进行了分析, 用FTIR表征了产物化学结构. 研究结果表明, 在脂肪酶的作用下, 对M_n在10⁵以上的PBS, 在THF体系中可降解到1.4×10⁴, 而在甲苯体系中可降解到4×10⁴; 但在THF和甲苯的混合体系中, 可将M_n 10⁵以上的PBS和PBS/CHDM共聚物都可降解为0.1×10⁴以下的原料单体、一至四环状低聚物及少量线型低聚物. 分析了水含量对酶解反应的影响.     

取代基效应对N-4-取代苯亚甲基苯胺与N-4-取代苯亚甲基环己胺NMR和UV光谱影响的差异性

合成了N-4-取代苯亚甲基苯胺(1)与N-4-取代苯亚甲基环己胺(2)两个系列化合物, 测定其¹³C和¹H 核磁共振(NMR)化学位移以及紫外(UV)吸收光谱. 定量对比了取代基效应对两个系列化合物CH=N键的¹³CNMR化学位移δ_C(C=N)和¹H NMR化学位移δ_H以及UV吸收光谱最大波长能量(v_max)的影响差异. 研究结果表明,对于分子骨架相似的化合物(1)和(2), 取代基效应的作用方式存在多样性: (i)化合物(1)的δ_C(C=N)、δ_H以及v_max受到基团的特殊交叉相互作用(Δσ²)的影响显著, 而Δσ²对化合物(2)相应性能的影响很小; (ii)无论化合物(1)还是化合物(2), 取代基场/诱导效应σ_F和共轭效应σ_R对δ_C(C=N)的影响为负相关, 而对δ_H的影响为正相关, 它们对δ_C(C=N)和δ_H的影响正好相反. 另一方面, 场/诱导效应σ_F对(1)和(2)的δ_C(C=N)影响重要, 而对它们的δ_H影响很小; (iii)化合物(1)和(2)的δ_C(C=N)、δ_H以及v_max的变化规律, 可分别建立通用方程表达, 其中与CH=N的N原子键连苯基的影响可由指示变量(I)表示, 该苯基对三种性能分别有固定的贡献.     

二茂铁-酞菁-富勒烯超分子三元体系的构筑及光物理和电化学性质

采用富勒吡咯烷衍生物中的吡啶或咪唑基与二茂铁修饰的金属酞菁轴向配位构筑了二茂铁-酞菁-富勒烯超分子三元体系, 通过紫外-可见光谱滴定法测定了其配位稳定性(K_assoc约为8.58×10⁴ L/mol). 稳态和时间分辨荧光光谱研究结果表明, 在该超分子三元体系中发生了快速的光诱导电子转移(k_CS约为10⁹ s^-1), 并具有较高的电荷分离态量子产率(Ф_CS=0.88). 循环伏安法数据表明, 其电荷分离驱动力ΔG_CS为负值(-0.60 eV), 说明酞菁和富勒烯之间容易形成电荷分离态.     

苹果酸酶结合域定点突变对烟酰胺腺嘌呤二核苷酸类似物催化性能的影响

通过对苹果酸酶(ME)辅酶结合域L310、Q401、L404饱和位点突变库与辅酶烟酰胺腺嘌呤二核苷酸(NAD⁺)类似物库的高通量筛选,研究了苹果酸酶结合域位点对NAD⁺及其类似物(B1~B7)催化活性的影响。 结果表明,突变后酶ME-Q401H/L404T对类似物B4的k_cat/K_m是野生型酶的50倍;突变后酶ME-L310M/Q401N对类似物B4的k_cat/K_m是野生型酶的16倍,对类似物B3的k_cat/K_m是野生型酶的5倍,因此通过对结合域定点突变,NAD⁺类似物的催化活性得到提高。     

pH法研究UO2+2与甘氨酰替甘氨酸、白氨酸和四咪噻唑的络合物

本文应用pH法测定了UO₂⁺²与甘氨酰替甘氨酸、白氨酸和d,l-2,3,5,6-四氢-6-苯基咪唑[2,1-6]噻唑的络合物的逐级稳定常数,分别得出,UO₂⁺²-甘氨酰替甘氨酸体系:β₁=5.7×10³和β₂=1.4×10¹⁰;UO₂⁺²-白氨酸体系:β₁=4.0×10⁵和β₂=1.6×10¹³,以及UO₂⁺²-d,l-2,3,5,6-四氢-6-苯基咪唑(2,1-6)噻唑体系:β₁=6.5×10⁴和β₂=2.0×10¹⁰(25℃,μ=0.1,KCl维持)。同时,将徐光宪的溶液中络合物吸附平衡理论引入pH法研究络合物稳定常数中。     

具有cGPX活力的含硒抗体酶的酶学及动力学性质研究

通过单克隆抗体制备技术得到三株特异结合半抗原4(GSH-S-DNP二苄酯)的单克隆抗体HB4,HB5和HB7.抗体经两步化学诱变得到具有细胞谷胱甘肽过氧化物酶(cGPX)活性的含硒抗体酶mHB4,mHB5和mHB7,活力分别为170,1867,32U/μmol.其中mHB5的活力是天然兔肝cGPX的0.32倍,m4A4的1.51倍.等离子体-质谱(ICP/MS)测得每分子含硒抗体酶分子中大约存在2个硒原子.mHB5的最适pH为8.6～8.8.在pH值范围为7.0和37℃条件下,mHB5催化GSH和H₂O₂或t-ROOH反应的二级速率常数为:_k+1(H₂O₂)9.71×10⁶L/(mol·min),_k+1(t-ROOH)5.99×10⁵L/(mol·min).mHB5使非酶催化反应速率提高了9.8×10⁶和3.7×10⁵倍.     

具有GPX活力的抗体片段Fv的制备和性质

具有谷胱甘肽(GSH)结合部位的鼠抗体3H₄(IgM)经胃蛋白酶水解,产生分子量为25000的抗体Fv片段,用荧光滴定法测定了它与GSH的亲和常数K_a=1.17×10₇L/mol.该片段经苯甲基磺酰氟活化,再经NaHSe作用,其结合部位的丝氨酸被突变为谷胱甘肽过氧化物酶(GPX)的催化基团硒代半胱氨酸.突变后的Fv片段表现出很高的GPX活性,其活力高达2500U/μmol,称为Fv抗体酶.动力学分析表明,Fv酶的最适温度为55℃,最适pH为7.0,催化机制为乒乓机制,米氏常数分别为:K_m(GSH)=4.16×10^-3mol/L,K_m(H₂O₂)=2.8×10^-4mol/L.     

三种不同碳桥联双核茂钛配合物的合成及催化乙烯聚合研究

合成了3种不同结构的CnH₂n桥联双核茂钛配合物(CH₃)₂C[(C₅H₄)TiCl₂(C₅H₅)]₂(3),(CH₂)_n[(C₅H₄)TiCl₂(C₅H₅)]₂(6,n=3;7,n=4),并用1HNMR进行了表征.发现以甲苯为溶剂时,不仅提高了产率,而且有效地避免了副产物Cp₂TiCl₂的生成.研究了化合物7/MAO(甲基铝氧烷)催化乙烯聚合的反应,考察了反应条件对催化体系的影响.结果表明,催化活性随着n(Al)/n(Cat.)比的增大而提高,聚乙烯的分子量在n(Al)/n(Cat.)=500和50℃时达到最高值9.0102×10⁴;随着聚合时间的延长,催化活性下降,而产物分子量不断升高;随着温度的上升,50℃时催化活性和聚乙烯的分子量最高,分别为2.4074×10⁵gPE/(molTi·h)和6.8679×10⁴.随着桥联双核茂钛配合物碳桥的增长,催化活性增加,所得聚乙烯的分子量降低.     

细胞色素P450 Kemp消除酶的改造及新型催化机制解析（英文）

传统的Kemp消除反应可以通过氢氧化钾和三烷基胺等碱性物质,催化底物苯并异恶唑开环生成产物2-氰基苯酚.三十年来, Kemp消除反应一直被用作模式反应来设计或定向进化新型生物酶催化剂,从而揭示未知的酶催化机制的复杂性,增强对酶催化机制的理解.目前科研人员使用不同的蛋白作为骨架设计能够高效催化Kemp消除反应的人工酶.例如Hilvert及Mayo等基于人工酶HG3.17,设计获得了Kemp消除酶,可以催化5-硝基苯并异恶唑生成产物2-氰基-4-硝基苯酚.通过17轮定向进化获得的最终突变体展现出与天然酶相近的催化活性(k_cat/K_m=230000 L mol^-1 s^-1; k_cat=700 s^-1).该研究不仅表明蛋白质工程可以进化出高效的生物酶,量子力学/分子力学(QM/MM)分析还揭示了突变体催化活性提高的分子机制.与酸碱催化的Kemp消除反应不同,最近Korendovych等报道以肌红蛋白作为骨架基于氧化还原机制的Kemp消除反应,通过开发一种独特的基于...     

CdTe/CdS量子点与丝裂霉素的相互作用及其应用

在水相中合成了硫普罗宁(Tiopronin,TP)修饰的CdTe/CdS量子点(TP-CdTe/CdS QDs).利用紫外-可见吸收光谱、荧光光谱研究了TP-CdTe/CdS QDs与丝裂霉素(mitomycin C,MMC)的相互作用机理.在pH=7.6的tris-HCl缓冲溶液介质中,TP-CdTe/CdS QDs与MMC相互作用,使TP-CdTe/CdS QDs的荧光发生猝灭,并且QDs的荧光强度与MMC的浓度有良好的线性关系(r=0.9991),线性范围4.7×10-9～1.2×10-8g/mL,检出限(3σ)为1.4×10-g/mL.此方法快速简便,用于尿样中丝裂霉素的测定,实验结果令人满意.     

胃蛋白酶对CdTe纳米粒子的表面修饰及分析应用

以巯基乙酸为稳定剂和表面修饰剂, 在有机相中合成了平均粒径为3 nm左右的CdTe纳米粒子, 用胃蛋白酶改变纳米粒子的表面修饰状态并研究其系列特性. CdTe纳米粒子在320 nm处有强的紫外吸收, 在524.8 nm处有荧光发射. 经胃蛋白酶对其表面修饰后, 紫外吸收峰位不变, 但吸光强度升高, 荧光峰位蓝移至467.2 nm, 荧光强度降低. 温度、pH值及离子强度均对表面修饰产生影响. 在最佳实验条件下, 胃蛋白酶质量浓度在4—40 mg/L范围内与荧光降低值之间呈线性关系, 检测限(3σ)为0.28 mg/L(n=10), 该方法已被用于人体胃液胃蛋白酶的测定.     

香豆素/Betti碱主体合成及其对铷、钡离子的选择性响应(英文)

合成了一个新型香豆素/Betti碱主体化合物1,并对其进行了结构表征。在乙腈/水溶液中进行主体1和碱金属、碱土金属相关离子(Li+,Na+,K+,Rb+,Cs+,Be2+,Mg2+,Ca2+,Sr2+,Ba2+)的相互作用研究时,发现仅Rb+,Ba2+离子对主体1有敏感的紫外光谱及荧光光谱响应,而其它的碱金属、碱土金属离子无敏感性光响应。紫外光谱显示,Rb+,Ba2+离子使主体1产生明显的红移(ε=4.66×102L·(mol·cm)-1,Δ=91nm),肉眼可观察到明显的由浅黄向橙红色的颜色变化,并使主体1的荧光光谱发生一定程度的猝灭。     

1,10-Phenanthrolines with tunable luminescence upon protonation: a spectroscopic and computational study

We have synthesized nine 2,9-aryl-substituted 1,10-phenanthrolines (1-9) with the aim of rationalizing their electronic absorption and luminescence properties in both the basic and acid form. The latter are generated upon addition of trifluoroacetic acid to CH2Cl2 solutions of 1-9 and their formation is unambiguously evidenced by UV-vis absorption and 1H NMR spectroscopy. 1-9 can be subdivided into three groups, depending on their chemical structure and luminescence behavior. 1-3 are symmetrically substituted p-dianisylphenanthrolines which exhibit relatively intense violet fluorescence in CH2Cl2 (lambda(max) ca. 400 nm, Phi(fl) = 0.12-0.33) and are strongly quenched and substantially red-shifted upon protonation (lambda(max) ca. 550 nm, Phi(fl) = 0.010-0.045). 4-5 are 2,6-dimethoxyphenylphenanthrolines with faint luminescence in both the basic and acid form. 6-9 are various unsymmetric aryl-substituted-phenanthrolines and their relatively strong fluorescence (lambda(max) ca. 400 nm, Phi(fl) = 0.08-0.24) is red-shifted and substantially enhanced following protonation (lambda(max) ca. 475 nm, Phi(fl) = 0.16-0.50). The markedly different trends in the electronic absorption and fluorescence spectra are rationalized by means of both time-dependent Hartree-Fock and density functional theory by using hybrid functionals to assign the excited states. Interestingly, protonation of 1-9 also occurs in spin-coated films simply exposed to vapors of acid, and the reaction can be signaled by the color tuning of the emission signal (vapoluminescence). This observation makes substituted phenanthrolines potential candidates as proton sensors also in the solid phase.     

Yb3+敏化宽波带掺Er3+氟磷酸盐玻璃的发光性质及Judd-Ofelt理论研究

采用高温熔融法制备了一种新的Er3+/Yb3+共掺氟磷酸盐玻璃,测试和分析了其密度、吸收光谱以及荧光光谱,讨论了Er3+离子和Yb3+离子对光谱性质的影响.根据Judd-Ofelt理论计算了玻璃中Er3+离子的强度参数Ωt(t=2,4,6),分别为Ω2=4.36×10-20cm2,Ω4=1.35×10-20cm2,Ω6=0.79×10-20cm2,以及Er3+离子4I13/2能级荧光寿命τm=8.26ms.主发射峰1.53μm处半高宽(FWHM)为68nm.根据McCumber理论计算了Er3+的受激发射截面σe=8.5×10-21cm2.比较了不同玻璃基质中Er3+离子的光谱特性,结果表明:Er3+/Yb3+双掺氟磷酸盐玻璃在1.53μm附近具有较宽的半高宽和较大的受激发射截面,是一种高增益掺铒光纤放大器的理想介质材料.     

Synthesis of homoveratric acid-imprinted polymers and their evaluation as selective separation materials

A bulk polymerization method was used to easily and efficiently prepare homoveratric acid (3,4-dimethoxyphenylacetic acid)-imprinted polymers from eight basic monomers: 2-vinylpyridine, 4-vinylpyridine, 1-vinylimidazole, N-allylaniline, N-allylpiperazine, allylurea, allylthiourea, and allylamine, in the presence of homoveratric acid as a template in N,N-dimethylformamide as a porogen. The imprinted polymer prepared from allylamine had the highest affinity to the template, showing an imprinting factor of 3.43, and allylamine polymers MIP8/NIP8 were selected for further studies. Their binding properties were analyzed using the Scatchard method. The results showed that the imprinted polymers have two classes of heterogeneous binding sites characterized by two pairs of K(d), B(max) values: K(d)(1) = 0.060 μmol/mL, B(max)(1) = 0.093 μmol/mg for the higher affinity binding sites, and K(d)(2) = 0.455 μmol/mL, B(max)(2) = 0.248 μmol/mg for the lower affinity binding sites. Non-imprinted polymer has only one class of binding site, with K(d) = 0.417 μmol/mL and B(max) = 0.184 μmol/mg. A computational analysis of the energies of the prepolymerization complexes was in agreement with the experimental results. It showed that the selective binding interactions arose from cooperative three point interactions between the carboxylic acid and the two methoxy groups in the template and amino groups in the polymer cavities. Those results were confirmed by the recognition studies performed with the set of structurally related compounds. Allylamine polymer MIP8 had no affinity towards biogenic amines. The obtained imprinted polymer could be used for selective separation of homoveratric acid.     

卡维地洛的电化学测定及与牛血清白蛋白相互作用的研究

建立了测定卡维地洛(CAR)新的电化学方法.结合紫外、红外光谱分析,研究了CAR与牛血清白蛋白(BSA)的相互作用.实验发现,在pH4.0Britton-Robinson(B-R)缓冲溶液中,CAR在碳糊电极上产生3个不可逆的氧化峰.以0.92V处的氧化峰为研究对象,结果发现峰电流Ipa,1与CAR浓度在2.45×10-5～1.19×10-3mol/L范围呈良好的线性关系,CAR的检出限为5.6×10-6mol/L.当BSA加入CAR溶液后,CAR峰电流降低,氧化峰电流的降低值△Ipa,1与BSA的浓度在2.92×10-7～1.09×10-5mol/L范围内呈良好线性关系,BSA的检出限为4.1×10-8mol/L.电化学结果表明,CAR与BSA之间形成1∶1的结合物,结合常数为3.14×106L/mol.紫外光谱表明CAR的加入使BSA的吸收峰发生红移且有增色效应.红外光谱表明CAR与BSA分子中氨基酸残基的硫及氮原子形成键合作用.     

Fluorescence Labeling and Determination of Pepsin with CdSe Quantum Dots

Based on the solid phase/liquid deposition CdSe quantum dots (QD) were synthesized using selenium and cadmium‐salt as precursor at room temperature. The average diameter of CdSe QD estimated from the high resolution transmission electron microscopy (HRTEM) graph and absorption spectra was ca. 3–3.5 nm. The mercaptoacetic‐acid stabilized CdSe QD exhibited ultraviolet absorption at 350 and 380 nm and strong fluorescence emission at 481.6 nm, respectively. When conjugated with pepsin, the fluorescence peak intensity of CdSe QD decreased considerably and the fluorescence peak shifted to 467.2 nm. Under optimal conditions, a concentration in 5–50 mg· L^?1 of pepsin could be determined on the basis of fluorescence decrease ratio of CdSe QD, with a detection limit 3δ of 0.36 mg·L^?1 (n=10). The proposed method was applied to detection of the concentration of pepsin in human gastric juice.     

Synthesis and self-association, absorption, and fluorescence properties of differentially functionalized hexakis(p-substituted-phenylethynyl)benzenes

The dual Sonogashira coupling reactions of 1,3,5-tribromo-2,4,6-triiodobenzene with p-X-phenylacetylene followed by another p-Y-phenylacetylene (X, Y = OSiMe(2)Bu-t or CO(2)Et) produced a series of differentially functionalized hexakis(p-substituted-phenylethynyl)benzenes with D(3)(h)() symmetry (3h: 1,3,5-X-2,4,6-Y) and C(2)(v)() symmetry (3g,i: 1,2,3,5-X-4,6-Y; 3f,j: 1-X-2,3,4,5,6-Y). In a similar manner, 1,3,5-tris(p-X-phenylethynyl)-2,4,6-tris(p-Y-phenylethynyl)benzenes and 1,2,3,5-tetrakis(p-X-phenylethynyl)-4,6-bis(p-Y-phenylethynyl)benzenes (3l: X = OSiMe(2)Bu-t, Y = NO(2); 3m,n: X = N(n-octyl)(2), Y = NO(2); 3o,p: X = N(n-octyl)(2), Y = CH(OCH(2)CH(2)O); 3q,r: X = N(n-octyl)(2), Y = CHO; 3s,t: X = N(n-octyl)(2), Y = CH=C(CN)(2)) were prepared. Compounds 3 with electron-withdrawing groups self-aggregated by a pi-pi stacking interaction and solvophobic effect. In the absorption and fluorescence spectra of 3, lambda(max)(abs) and lambda(max)(em) showed red shifts as the donor-acceptor dipole at the end functional groups of the para position was increased. In the absorption spectra, lambda(max)(abs) showed red shifts upon increasing the number of combination of electron-donating and -withdrawing groups on the diagonal line in a molecule, whereas lambda(max)(em) in the fluorescence spectra exhibited red shifts upon decreasing the molecular symmetry.     

Quantification of nimesulide in human plasma by high-performance liquid chromatography with ultraviolet detector (HPLC-UV): application to pharmacokinetic studies in 28 healthy Korean subjects

Nimesulide is a selective COX-2 inhibitor that is as effective as the classical non-acidic nonsteroidal anti-inflammatory drugs in the relief of various pain and inflammatory conditions, but is better tolerated with lower incidences of adverse effects than other drugs. After oral dose of 100 mg nimesulide to western subjects, a mean maximal concentration (C(max)) of 2.86 ～ 6.5 μg/mL was reached at 1.22 ～ 2.75 h and mean t(1/2β) of 1.8 ～ 4.74 h. This study developed a robust method for quantification of nimesulide for the pharmacokinetics and suitability of its dosage in Korea and compared its suitability with other racial populations. Nimesulide and internal standard were extracted from acidified samples with methyl tert-butyl ether and analyzed by high-performance liquid chromatography with ultraviolet detection (HPLC-UV). The 28 healthy volunteers took 2 tablets of 100 mg nimesulide and blood concentrations were analyzed during the 24 h post dose. Several pharmacokinetic parameters were represented: AUC(0-infinity) = 113.0 mg-h/mL, C(max) = 12.06 mg/mL, time for maximal concentrations (T(max)) = 3.19 h and t(1/2β) = 4.51 h. These were different from those of western populations as follows: AUC was 14.5% and C(max) was 28% that of of Korean subjects and T(max) and t(1/2β) were also different. The validated HPLC-UV method was successfully applied for the pharmacokinetic studies of nimesulide in Korean subjects. Because the pharmacokinetics of nimesulide were different from western populations, its dosage regimen needs to be adjusted for Koreans.