以OT为底物固体电极伏安法测定辣根过氧化物酶及其标记物的研究

以玻碳电极为工作电极研究了邻联甲苯胺(OT)为底物微分脉冲伏安法测定辣根过氧化物酶(HRP)及其标记物的方法。HRP能够催化H2O2氧化OT,其反应产物在玻碳电极上-0.58V(vs.Ag/AgCl)左右被还原产生一个灵敏的还原峰,还原峰电流随着酶浓度的增大而增大,借助此还原电流可以测定HRP,并进而可用于以HRP为标记物的酶免疫分析。对酶催化反应条件和酶催化反应产物的测定条件进行了详细的研究,在最佳实验条件下测定游离HRP的线性范围是2.0×10-9～4.0×10-8g/mL,检出限为1.6×10-9g/mL;测定游离的酶标记物(IgG HRP),稀释范围为1∶2000～1∶400000,最大稀释比为1∶400000。     

OAP-H2O2-HRP酶促产物的固体电极法研究及应用

采用电化学方法和紫外-可见光谱法对邻氨基酚(OAP)-H2O2-辣根过氧化物酶(HRP)酶联免疫分析体系的反应产物进行了较为详细地研究.紫外-可见光谱实验表明HRP的加入极大地催化了H2O2氧化OAP的反应.循环伏安实验结果表明,其酶促产物在玻碳电极上发生可逆的氧化还原反应,峰电流与扫描速率的平方根成线性关系;微分脉冲伏安曲线表明酶促产物在-0.336 V左右(一8.0 B-R缓冲溶液中)产生了1个峰形良好的还原峰,峰电流随HRP浓度的增大而增大,借助此还原电流可用于测定HRP.用微分脉冲伏安法对酶促产物的测定条件进行了优化.在最佳条件下测定游离HRP的线性范围为8.0×10-11～4.0×10-9-g/mL.检出限为6.9×10-11g/mL.     

血红蛋白模拟过氧化物酶催化H2O2氧化邻氨基酚的固体电极伏安法研究

探讨了用血红蛋白作为辣根过氧化物酶的替代物,用于催化H2O2氧化邻氨基酚的反应体系.其催化反应生成一种具有电化学活性的产物,该产物在玻碳电极上于-0.370 V(vs.Ag/AgCl)产生一个峰形良好的还原峰.还原峰电流随着血红蛋白浓度的增大而增大.同时用微分脉冲伏安法对血红蛋白的催化反应条件进行了优化,选择了催化反应产物的伏安测定的最佳条件.在该条件下,该体系可用于血红蛋白的测定,线性范围为4.0×10-8～8.0×10-7mol/L,检出限为3.4 × 10-8 mol/L.用循环伏安法研究了该产物在不同pH B-R缓冲溶液中于玻碳电极上的电化学性质.     

ODA-H_2O_2-HRP伏安酶联免疫分析新体系的研究

提出邻联茴香胺-H_2O_2-HRP伏安酶联免疫分析新体系,并用于测定HRP和HRP标记物.该方法是将HRP催化H_2O_2氧化邻联茴香胺的酶催化反应与邻联茴香胺的氧化产物的电极还原反应相偶合,在BR缓冲溶液中,在-0.56V(SCE)左右产生灵敏的极谱波.应用此极谱波测定HRP的检测限为3.7×10~(-12)g/mL,线性范围为1.O×1O~(-11)～2.0×10~(-9)g/mL.对邻联茴香胺-H_2O_2-HRP伏安酶联免疫分析新体系的偶合反应机理及电极还原过程进行了较详细的探讨.     

基于固体酶催化反应电化学测定酶含量

提出了以固体辣根过氧化物酶(HRP)对过氧化氢氧化邻苯二胺的催化作用为基础的测定HRP及其标记物的电化学方法.测定中以Au-Pt/PAN/GCE为工作电极,并详细叙述其制备过程.将一定浓度的HRP按规定方法固定在上述修饰电极上制得HRP/Au-Pt/PAN/GCE修饰电极,将此电极浸入含5.0×10-3mol·L-1邻苯二胺及2.5×10-3mol·L-1过氧化氢的磷酸盐缓冲溶液(pH 5.0)中,反应10 min后将电极取出,记录溶液中酶催化反应产物的方波伏安峰及峰电流.结果表明:酶催化反应前,底物在工作电极上于-0.488 V(vs.SCE)处有明显的还原峰,在酶催化反应后,在-0.584 V处出现一个更大的还原峰,电位负移160 mV,且峰电流明显增大.峰电流值(Ip)与修饰在Au-Pt/PAN/GCE电极上的HRP的含量在1.0×10-2～2.0×102μg·L-1之间呈线性关系,方法的检出限(3S/N)为3.0 ng·L-1.     

以2-磷酸抗坏血酸酯为底物检测碱性磷酸酯酶的微分脉冲伏安法

提出以2_磷酸抗坏血酸酯为碱性磷酸酯酶(ALP)底物微分脉冲伏安法测定ALP的方法 ;2_磷酸抗坏血酸酯在ALP的催化作用下发生水解反应生成抗坏血酸 ,抗坏血酸在玻碳电极上 +0.40V(vsAg/AgCl)被氧化而产生一个灵敏的氧化峰 ,氧化峰电流随着酶浓度的增大而增大 ,借助此氧化峰电流可以测定ALP ,进而可用于以ALP为标记酶的酶免疫分析 ;用微分脉冲伏安法对酶催化反应条件和酶催化反应产物的测定条件进行了详细的研究 ,建立了以2_磷酸抗坏血酸酯为底物的伏安酶联免疫分析新体系 ,测定游离ALP的线性范围是0.4～2.0×103 U/L,检测限为0.3U/L,对游离的IgG_ALP的测定最大稀释比为1∶200000。     

聚L-白氨酸修饰电极伏安法测定痕量多巴胺的研究

用循环伏安法制备了聚L-白氨酸修饰玻碳电极,研究了多巴胺在聚L-白氨酸修饰玻碳电极上的电化学行为,建立了循环伏安法测定痕量多巴胺的新方法。实验结果表明,在pH 6.0的磷酸盐缓冲溶液中,多巴胺在聚L-白氨酸修饰玻碳电极上产生一对灵敏的氧化还原峰,峰电位分别为Epa=0.281V,Epc=0.170 V(相对Ag/AgCl电极)。峰电流与多巴胺的浓度在5.0×10-8~5.0×10-4mol/L的范围内有线性关系,检出限为5.0×10-9mol/L。对1.0×10-5mol/L多巴胺溶液平行测定9次,其相对标准偏差为4.0%。已用于针剂中多巴胺的测定。     

甲基红-H2O2-HRP伏安酶联免疫分析法测定HRP及其标记物

提出了一种新的辣根过氧化物酶的底物-甲基红,它本身具有电化学活性,能够在静汞电极上发生还原反应,产生灵敏的伏安电流信号.以H2O2为氧化剂,HRP能催化氧化还原反应的发生,使甲基红被氧化分解,其平衡浓度降低,对应的还原峰电流降低,峰电流的降低值与HRP的质量浓度在5.0×10-8～5.0×10-7g/mL之间呈线性关系,对2.0×10-7g/mL HRP进行11次测定的相对标准偏差为4.6%,方法的检出限为1.8×10-8g/mL.应用于IgG-HRP和Avidin-HRP的测定.     

OT-H2O2-HRP伏安酶联免疫分析新体系

本文首次提出了邻联甲苯胺(OT)-H2O2-辣根过氧化物酶(HRP)伏安酶联免疫分析新体系。本方法以线性扫描二阶导数伏安法检测HRP催化H2O2氧化OT的产物, 用于游离HRP和各种HRP标记物测定, 灵敏度比经典的ELISA光度法分别高两个至四个数量级。测定游离HRP的检测限达到1.8×10^-^1^2 g/mL, 线性范围为5.0×10^-^1^2-1.0×10^-^8 g/mL。对此伏安酶联免疫分析新体系的偶合反应机理及电极还原过程也进行了详细的研究。     

以3,3′,5,5′-四甲基联苯胺为底物的伏安酶联免疫分析体系研究

对 3 ,3′,5 ,5′ 四甲基联苯胺 (TMB) H2 O2 辣根过氧化物酶 (HRP)伏安酶联免疫分析体系进行了研究。HRP催化H2 O2 氧化TMB ,其氧化产物在汞电极上可以发生还原反应 ,在B R缓冲溶液中 ,-0 .76V(vs.SCE)处产生较为灵敏的伏安波。将此伏安波应用于测定HRP和HRP的标记物。测定HRP的线性范围为 6.0×1 0 - 1 1 ～ 5 .0× 1 0 - 9g mL ,检测限为 5 .0× 1 0 - 1 1 g mL。对该体系酶催化反应机理及产物的电极还原过程进行了探讨     

二氧化碳和丙烯直接合成甲基丙烯酸的NiPMo/TiO2催化剂的研究

用溶胶-凝胶法以磷钼酸(MPA)的镍盐溶液水解钛酸四丁酯制备了NiPMo/TiO2催化剂.使用ICP、 XRD、 TG-DTA、 IR、 TPD-MS和微反应技术研究了催化剂的化学组成、热稳定性、化学吸附性质和催化反应性能.杂多钼酸盐与TiO2通过O2-在TiO2表面发生了键合.在623 K下,杂多阴离子仍保持原有的Keggin结构.CO2在Lewis酸位Ni(Ⅱ)和Lewis碱位Ni-O-Mo的桥氧协同作用下生成CO2卧式吸附态Ni(Ⅱ)←O-(CO)←(O--Ni).丙烯有多种吸附态在催化剂上吸附.在563 K、 1 MPa和空速1500 h-1的反应条件下,丙烯的摩尔转化率为3.2%,产物MAA选择性为95%.     

Toward new camptothecins. Part 6: Synthesis of crucial ketones and their use in Friedländer reaction

In the context of the preparation of camptothecin and luotonin A analogs, the synthesis of some key keto-precursors and their use in Friedländer condensation are described. This paper also focuses on the stability of these keto intermediates and emphasizes the major differences between indolizinones and pyrroloquinazolinones series. Noteworthy is also the report of some original structures isolated as by-products of some experiments.     

CoFe2O4自形成磁性液体场致结构化对磁化的影响

The Langevin paramagnetic theory can’t describe the relation between magnetization of ferrofluids and applied magnetic field. The structuralization of ferrofluids, which is considered the main influence factor of the magnetization, is regarded. The part of magnetization works is deposited when the structure is forming. This action influences the magnetization of ferrofluids directly or indirectly. On the base of the “compressing” model, the Langevin function that usually describes the magnetization of ferrofluid is modified, and a well-fitted curve is obtained. An equation of the relation between the equivalent volume fraction after being “compressed” and the intensity of magnetic field is discovered, which approximately describes the process of magnetization. The relation between the approximate initial susceptibility and the volume fraction can be obtained from modified formula.     

Highly regioselective Buchwald–Hartwig amination at C-2 of 2,4-dichloropyridine enabling a novel approach to 2,4-bisanilinopyridine (BAPyd) libraries

The highly regioselective Buchwald–Hartwig amination at C-2 of the cheap and readily accessible reagent, 2,4-dichloropyridine with a range of anilines and heterocyclic amines is described. This new methodology is robust and provides a facile access to 4-chloro-N-phenylpyridin-2-amines on 0.25 mol scale. These intermediates undergo a further Buchwald–Hartwig amination at higher temperature to enable rapid exploration of the chemical space at C-4 and to provide a library of 2,4-bisaminopyridines.     

KMnO4-mediated oxidative CN bond cleavage of tertiary amines: Synthesis of amides and sulfonamides

KMnO₄-mediated oxidative CN bond cleavage of tertiary amines producing secondary amine was introduced, which was trapped by electrophiles (acyl chloride and sulfonyl chloride) to form amides and sulfonamides. The reaction could take place at mild condition, tolerating a wide range of function groups and affording products in moderate to excellent yields.     

Chemistry of heterocyclic compounds at the A. E. Favorsky Irkutsk Institute of Chemistry, Siberian Branch of the Russian Academy of Sciences, over 50 years (Review)

The review contains a concise historical account and information on the most significant researches undertaken by the staff at the A. E. Favorsky Irkutsk Institute of Chemistry, Siberian Branch of the Russian Academy of Sciences on the Chemistry of Heterocyclic Compounds. Dedicated to Academician of the Russian Academy of Sciences B. A. Trofimov on his 70th jubilee. Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 10, pp. 1443–1502, October, 2008.     

Sulfur-directed metal-free and regiospecific methyl C(sp3)–H imidation of thioanisoles

Regiospecific and direct imidation of the methyl C(sp³)–H bond of thioanisoles is realized under mild and metal-free conditions with N-fluorobis(benzenesulfonyl)imide as an oxidant and nitrogen source. Proposed mechanism suggests that thionium ion intermediates and a Pummerer-type reaction are involved. The imidation has advantages such as high step-economy, excellent functionality tolerance, and regiospecificity, giving structurally diverse imidation products.     

Selective syntheses of 2H-1,3-oxazines and 1H-pyrrol-3(2H)-ones via temperature-dependent Rh(II)-carbenoid-mediated 2H-azirine-ring expansion

The Rh(II)-catalyzed reaction of 2-carbonyl-substituted 2H-azirines with ethyl 2-cyano-2-diazoacetate or 2-diazo-3,3,3-trifluoropropionate provides an easy access to 2H-1,3-oxazines and 1H-pyrrol-3(2H)-ones. These compounds can be selectively prepared from the same starting material using temperature as the only varied parameter. The 2-azabuta-1,3-diene intermediate, a common precursor for both heterocyclic products, isomerizes into 2H-1,3-oxazine under kinetic control, while 1H-pyrrol-3(2H)-one is the sole product of the reaction at elevated temperatures. According to DFT-calculations a one-atom oxazine ring contraction involving ring-opening to a 2-azabuta-1,3-diene intermediate, followed by a 1,5- and 1,2-prototropic shift leads to the consecutive formation of imidoylketene and azomethine ylide, which then further undergo cyclization to the pyrrole derivative.     

Synthesis of 1-benzyloxypyrazin-2(1H)-one derivatives

Different approaches for the synthesis of 1-benzyloxypyrazin-2(1H)-one derivatives from simple amino acids have been investigated. A library of 33 precursors for the preparation of N-hydroxy pyrazinones was obtained in moderate to good yields.