IMECH-IR  > 力学所知识产出(1956-2008)
抗癌药长春新碱及其与微管蛋白相互作用的电化学研究
Alternative TitleStudy on the electrochemical behaviors of vincristine and the interaction of vincristine with tubulin
于泳; 胡劲波; 尚军; 李启隆
Source Publication化学学报
2004
Volume62Issue:2Pages:137-141
ISSN0567-7351
Abstract在0.05 mol/L Tris,0.15 mol/L NaCl溶液中,用吸附伏安法研究长春新碱(VCR),其峰电位在-1.68 V(vs. Ag/AgCl),峰电流与1.0*10^{-8}~2.0*10^{-7}mol/L VCR浓度成正比,检测限为7.0*l0^{-9} mol/L,用常规脉冲极谱法、线性扫描和循环伏安法等研究该体系的电化学行为,实验表明,电极还原过程为具有吸附特征的不可逆过程。VCR的吸附符合Frumkin吸附等温式。也研究了VCR与微管蛋白的相互作用。实验表明,VCR与微管蛋白形成一电活性的结合物,这一结合物具有吸附性,且还原过程也为不可逆过程。
Other AbstractA sensitive reduction peak of vincristine (VCR) is obtained by adsorptive stripping voltammetry in 0.05 mol/L Tris and 0.15 mol/L NaCl buffer solution. The peak potential is - 1.68 V (vs. Ag/AgCl). The peak current is directly proportional to the concentration of VCR (1.0xl0~(-8)~2.0 * 10~(-7)mol/L) , with a detection limit of 7.0 x 10~(-9) mol/L. The electrochemical behavior of this system was studied by the methods of normal pulse polarography, linear-sweep and cyclic voltammetry. The reduction process is irreversible with adsorptive characteristics. The adsoiption of VCR obeys the Frumkin isotherm. The electrochemical behavior of the binding of VCR to tubulin was studied by cyclic voltammetry. The results showed that the reaction of tubulin dimer with VCR formed an electrochemically active complex, and the reduction process of the complex is irreversible.
Keyword长春新碱 伏安法 吸附 微管蛋白 Vincristine (Vcr) Voltammetry Adsorption Tubulin
Subject Area力学
Indexed BySCI ; CSCD
Language中文
WOS IDWOS:000188418600006
CSCD IDCSCD:1511795
Citation statistics
Cited Times:5[WOS]   [WOS Record]     [Related Records in WOS]
Cited Times:4[CSCD]   [CSCD Record]
Document Type期刊论文
Identifierhttp://dspace.imech.ac.cn/handle/311007/16462
Collection力学所知识产出(1956-2008)
Recommended Citation
GB/T 7714
于泳,胡劲波,尚军,等. 抗癌药长春新碱及其与微管蛋白相互作用的电化学研究[J]. 化学学报,2004,62,2,:137-141.
APA 于泳,胡劲波,尚军,&李启隆.(2004).抗癌药长春新碱及其与微管蛋白相互作用的电化学研究.化学学报,62(2),137-141.
MLA 于泳,et al."抗癌药长春新碱及其与微管蛋白相互作用的电化学研究".化学学报 62.2(2004):137-141.
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