聚对氨基苯磺酸/氧化石墨烯修饰电极同时测定多巴胺和抗坏血酸

用循环伏安法制备了聚对氨基苯磺酸/氧化石墨烯修饰玻碳电极(PABSA/GO/GCE),研究了多巴胺(DA)和抗坏血酸(AA)在该修饰电极上的电化学行为,并建立了同时测定多巴胺和抗坏血酸电化学分析新方法,相对于裸玻碳电极,该电极测定DA和AA的峰电流明显增加。实验结果表明:在实验条件下,DA测定的线性范围为0.50～300μmol/L;检出限为5.0μmol/L。AA测定的线性范围是0.10～2.4 mmol/L,检出限为0.50μmol/L。     

基于氧化石墨烯修饰玻碳电极的多巴胺和尿酸的电化学检测

将超声分散的氧化石墨烯(GO)悬浮液滴涂于玻碳电极(GCE)表面,制备成GO/GCE,并用扫描电子显微镜(SEM)和电化学阻抗谱(EIS)对GO/GCE进行表征,利用差分脉冲伏安法(DPV)、循环伏安法(CV)对多巴胺(DA)和尿酸(UA)进行了电化学测定。研究了pH对DA和UA电化学行为的影响并计算相关的动力学参数。结果表明:该修饰电极对DA和UA的氧化还原反应具有良好的电化学催化作用,在1.0~98.0μmol/L和0.5~90.0μmol/L范围内峰电流与DA和UA浓度呈良好的线性关系,检出限分别为0.50μmol/L和0.25μmol/L。而且可以在抗坏血酸(AA)共存下同时测定DA和UA。该传感器具有良好的选择性与稳定性,有望应用于DA和UA的同时测定。     

聚三聚氰胺-石墨烯复合膜修饰电极对多巴胺与尿酸的同时测定

采用循环伏安法制备了聚三聚氰胺-石墨烯复合膜修饰电极(poly-(MA)-ERGO/GCE)。研究了抗坏血酸(AA)、尿酸(UA)和多巴胺(DA)在该修饰电极上的电化学行为。结果表明,该修饰电极对AA、UA和DA均有良好的电化学响应,且三者的氧化峰在该修饰电极上可完全分离。据此建立了在大量AA存在下同时测定UA和DA的新方法。在优化条件下,微分脉冲伏安法(DPV)测定UA和DA的线性范围均为1.0×10~(-8)~5.0×10-6mol·L~(-1),检出限(3sb)均为5.0×10~(-9)mol·L~(-1)。     

TiO2-石墨烯-Nafion复合膜修饰玻碳电极同时测定多巴胺和尿酸

利用在玻碳电极上修饰了TiO2-石墨烯-Nafion复合膜制得的修饰电极进行多巴胺(DA)和尿酸(UA)的同时测定。用循环伏安法(CV)和差分脉冲伏安法(DPV)研究了该修饰电极的电化学行为。在pH为7.0的磷酸盐缓冲液(PBS)中,修饰电极对于DA和UA的电化学氧化具有良好的电催化性能。DA和UA的氧化峰电流分别在2～120和60～300μmol/L浓度范围内呈良好的线性关系,检出限分别为0.066和0.102μmol/L。实验结果表明,TiO2-石墨烯-Nafion复合膜修饰电极显著提高了检测的灵敏度,并表现出良好的选择性和重现性。     

用于多巴胺选择性电化学检测的多孔Fe-N-C纳米颗粒簇

多巴胺(DA)是人类神经系统的神经递质之一,也是诊断多种神经疾病的重要生物标志物,因此,快速准确地检测DA浓度受到广泛关注。本文以普鲁士蓝(PB)为前体制备了一种多孔Fe-N-C纳米颗粒簇,将其修饰在玻碳电极(GCE)表面,发现该修饰电极在使用线性扫描伏安法(LSV)和差分脉冲伏安法(DPV)时能够有效地降低尿酸(UA)和抗坏血酸(AA)的电化学氧化响应,而不影响DA的电化学氧化反应,并能够将三者的氧化峰有效分开,从而可以实现对DA的选择性电化学分析。研究结果表明,在含有高浓度的UA(100μmol/L)和AA(100μmol/L)的DA混合溶液中使用LSV检测DA,分段线性范围可以达到5~100μmol/L和100~700μmol/L,灵敏度分别为8.32×10~(-2)和3.44×10~(-2)A·(mol/L)~(-1),检测下限为5μmol/L。     

聚钙羧酸修饰玻碳电极差分脉冲伏安法同时测定多巴胺和尿酸

采用电化学方法将钙羧酸(CCA)聚合修饰在玻碳电极(GCE)表面制备了聚钙羧酸指示剂修饰玻碳电极(PCCA/GCE),并用循环伏安法和交流阻抗法研究了电极的电化学性能。结果表明:在pH 6.0的磷酸盐缓冲溶液中,多巴胺(DA)和尿酸(UA)在聚钙羧酸修饰电极上的氧化峰得以分开,峰电位差为0.14V,据此提出了聚钙羧酸修饰电极差分脉冲伏安法同时测定多巴胺和尿酸的方法。DA和UA的浓度分别在5.0～43.8μmol.L-1和5.0～50.0μmol.L-1范围内与其氧化峰电流呈线性关系,检出限(3S/N)分别为0.2μmol.L-1和0.5μmol.L-1。方法可用于多巴胺注射液样品中DA和UA的测定,测定值的相对标准偏差(n=5)依次为2.43%和2.35%。     

基于MnO_2纳米线-还原石墨烯复合修饰电极的多巴胺电化学检测

通过电化学还原法制备MnO_2纳米线/还原石墨烯复合修饰电极(MnO_2-RGO/GCE),用于多巴胺(DA)的检测。采用扫描电镜和X-射线粉末衍射对不同的修饰电极微观形貌进行了表征,优化了电化学还原条件和测定DA实验条件。此外,还研究DA在裸电极及RGO或MnO_2-RGO修饰电极上的循环伏安响应。MnO_2-RGO/GCE复合修饰电极实现AA、DA和UA氧化峰的有效分离,AA-DA和DA-UA的氧化峰电位差分别为268和128 m V。检测DA的线性范围为0.06~1.0μmol/L和1.0~80μmol/L,检出限为1.0 nmol/L(S/N=3)。制备的MnO_2-RGO/GCE成功用于人血清样品的多巴胺含量分析。     

多巴胺在聚亚甲基蓝/石墨烯修饰电极上的电化学行为研究

利用电聚合方法在石墨烯修饰的玻碳电极表面制备了聚亚甲基蓝/石墨烯修饰电极(PMB/GH/GCE)。采用循环伏安法(CV)和差分脉冲伏安法(DPV)研究了多巴胺(DA)和抗坏血酸(AA)在该修饰电极上的电化学行为。在pH 6.9的磷酸盐缓冲溶液中,DA和AA分别在0.208 V和-0.108 V处产生灵敏的氧化峰,与其在聚亚甲基蓝和石墨烯单层修饰电极上的电化学行为相比,两者的峰电流明显增加,峰电位差达316 mV。研究表明,电聚合方法使亚甲基蓝牢固地非共价修饰到石墨烯上,并产生协同增效作用,较好地提高了电极的灵敏度和分子识别性能,有利于在大量AA存在下实现对DA的选择性测定。在1.00×10-3mol/L AA的存在下,DA的差分脉冲伏安法峰电流与其浓度在1.00×10-7～5.00×10-3mol/L范围内呈良好的线性关系,检出限达1.00×10-8mol/L。将该方法用于盐酸多巴胺注射液的测定,结果满意。     

柠檬酸修饰电极对抗坏血酸、多巴胺和尿酸的同时检测

研究柠檬酸(CA)修饰玻碳电极(CA/GC)在抗坏血酸(AA)、多巴胺(DA)和尿酸(UA)混合体系中的循环伏安(CV)行为.结果表明,AA、DA和UA在CA/GC电极上氧化峰电流增大,且三者氧化峰电位明显分离(ΔEp(DA,AA)=170 mV,ΔEp(DA,UA)=130 mV,ΔEp(AA,UA)=300 mV).据此,可同时检测AA、DA和UA.在优化的实验条件下,AA、DA和UA的氧化峰电流与其浓度分别在2.0×10-6～1.5×10-3mol.L-1,6.0×10-7～1.0×10-3mol.L-1和6.0×10-7～1.0×10-3mol.L-1范围内呈线性关系.该电极重现性好,可用于盐酸多巴胺针剂DA、VC片剂AA及人体尿液UA的测定.     

Electrochemical Behavior of Dopamine at Poly( Methylene Blue)/Graphene Modified Glassy Carbon Electrode

利用电聚合方法在石墨烯修饰的玻碳电极表面制备了聚亚甲基蓝/石墨烯修饰电极( PMB/GH/GCE).采用循环伏安法(CV)和差分脉冲伏安法(DPV)研究了多巴胺(DA)和抗坏血酸(AA)在该修饰电极上的电化学行为.在pH 6.9的磷酸盐缓冲溶液中,DA和AA分别在0.208 V和-0.108 V处产生灵敏的氧化峰,与其在聚亚甲基蓝和石墨烯单层修饰电极上的电化学行为相比,两者的峰电流明显增加,峰电位差达316 mV.研究表明,电聚合方法使亚甲基蓝牢固地非共价修饰到石墨烯上,并产生协同增效作用,较好地提高了电极的灵敏度和分子识别性能,有利于在大量AA存在下实现对DA的选择性测定.在1.00×10-3 mol/L AA的存在下,DA的差分脉冲伏安法峰电流与其浓度在1.00×10--7～5.00×10-3 mol/L范围内呈良好的线性关系,检出限达1.00 × 10-6mol/L.将该方法用于盐酸多巴胺注射液的测定,结果满意.     

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.