期刊文献+
任意字段
题名或关键词
题名
关键词
文摘
作者
第一作者
机构
刊名
分类号
参考文献
作者简介
基金资助
栏目信息

3-取代吲哚-2-酮类化合物的设计、合成及抗肿瘤活性研究

Design,synthesis and anti-tumor activities in vitro of novel 3-substituted indolin-2-one compounds
下载PDF
导出
摘要 目的设计合成对微管蛋白和血管内皮细胞生长因子受体2(VEGFR-2)激酶具有双重抑制作用的3-取代吲哚-2-酮类化合物,考察其体外抑瘤活性。方法以取代的苯胺为起始原料,经缩合、环合、还原、取代等反应制得系列目标化合物,并考察该系列化合物对微管蛋白和肿瘤细胞的抑制活性。结果共合成了11个新的目标化合物。实验结果显示,化合物j9对微管蛋白和VEGFR-2激酶具有双重抑制活性。所有目标化合物对3种肿瘤细胞株均有中等强度的抑制活性。结论该类化合物是一类具有多靶点作用的抗肿瘤化合物。 Objective To compose and evaluate anti‐tumor activities of 3‐substituted indole‐2‐one compounds which may have dual inhibitory activities against both tubulin protein and VEGFR‐2 tyrosine kinase .Methods Target compounds were prepared starting from substituted aniline viacondensation ,cyclization and reduction .Results 11 target compounds were syn‐thesized and all the compounds displayed moderate anti‐proliferative activities against three tumor cell lines .Compound j9 showed a certain inhibitory activity against both VEGFR‐2 kinase and tubulin protein in vitro .Conclusion This series of indo‐lin‐2‐one derivatives were found to be a novel kind of multi‐target inhibitor .
作者 周浩 周峰 周有骏
机构地区 第二军医大学药学院药物化学教研室
出处 《药学实践杂志》 CAS 2015年第2期131-133,142,共4页 Journal of Pharmaceutical Practice
基金 国家自然科学基金(21172260)
关键词 血管靶向药物 3-取代吲哚-2-酮类化合物 微管蛋白抑制活性 激酶抑制活性 vascular targeting drug 3-substituted indolin-2-one compounds tubulin inhibitory activities kinase inhibi-tory activities
分类号 R916.1 [医药卫生—药学]
  • 相关文献

参考文献9

  • 1Folkman J. Tumor angiogenesis: therapeutic implications[J]. N Engl J Med,1971,285(21):l182-1186. 被引量:1
  • 2Bergers G, Benjamin IrE. Tumorigenesis and the angiogenic switch[J]. Nat Rev Cancer,2003,3(6):401-410. 被引量:1
  • 3Brem S,Brem H,Folkman J,et al. Prolonged tumor dormancy by prevention of neovascularization in the vitreous[J]. Cancer Res, 1976,36(8) : 2807-2812. 被引量:1
  • 4FongTA,Shawver LK,Sun L,etal. Su5416 is a potent and selective inhibitor o{ the vascular tyrosine kinase catalysis, tumor vaseularization, and growth endothelial growth factor re- ceptor (FIk-1/KDR) that inhibits of multiple tumor types~J3. Cancer Res, 1999,59 ( 1 ) ~ 99-106. 被引量:1
  • 5吕金玲,赵临襄.苹果酸舒尼替尼(sunitinib malate)[J].中国药物化学杂志,2007,17(3):194-194. 被引量:5
  • 6Belleri M,Rihatti D, Nicoli S,et al. Antiangiogenic and vascu lar-targeting activity of the microtubule-destabilizing trans-res- veratrol derivative 3,5,4'-trimethoxystilbeneEJ3. Mol Pharma- co1,2005,67(5) :145]-1459. 被引量:1
  • 7Gieni RS, Li Y, Hayglass KT. Comparison of E:~ HI thymidine incorporation with MTT- and MTS-based bioassays for hu- manand murine IL-2 and IL-4 analysis, tetrazolium assays pro- vide markedly enhanced sensitivity I-J1. J Immunol Methods, 1995,187(1)~85-93. 被引量:1
  • 8张帆,王晓欢,马俊杰,王晓,李博志,顾玉诚,宫平.4,6-双苯基-2-氨基-3-氰基吡啶类化合物的合成及其抗肿瘤活性研究[J].中国药物化学杂志,2011,21(5):352-357. 被引量:2
  • 9Hamel E. Evaluation of antimitotic agents by quantitative comparisons of their effects on the polymerization of purified tubulin[J]. Cell Biochem Biophys, 2003,38 (1) : 1-22. 被引量:1

二级参考文献15

  • 1HERON M. Leading causes for 2004[J].Natl Vital Stat Rep,2007,56(5) :1 -96. 被引量:1
  • 2KEMNITZER W, DREWE J, JIANG S C, et al. Discovery of 4-aryl-4H-chromenes as a new series of apoptosis inducers using a cell- and caspase-based high-throughput screening assay. 1. Structure-activity relationships of the 4-aryl group [ J ]. J Med Chem, 2004,47 (25) :6299 - 6310. 被引量:1
  • 3KEMNITZER W, KASIBHATLA S, JIANG S C, et al. Discovery of 4-aryl-4H-chromenes as a new series of apoptosis inducers using a cell- and caspase-based high-throughput screening assay. 2. Structure-activity relationships of the 7- and 5-, 6-, 8-position [J]. B ioorg Med Chem Lett,2005,15 (21) :4745 -4751. 被引量:1
  • 4KEMNITZER W, DREWE J, JIANG S C, et al. Discovery of 4-aryl-4H-chromenes as a new series of apoptosis inducers using a cell- and caspase-based high-throughput screening assay. 3. Structure-activity relationships of fused rings at the 7,8-position[ J ]. J Med Chem,2007,50 ( 12 ) : 2858 - 2864. 被引量:1
  • 5KEMNITZER W, DREWE J, JIANG S C, et al. Discovery of 4-aryl-4H-chromenes as a new series of apoptosis inducers using a cell- and caspase-based high-throughput screening assay. 4. Structure-activity relationships of N-alkyl substituted pyrrole fused at the 7,8-positions [J].J Med Chem, 2008,51 ( 3 ) : 417 -423. 被引量:1
  • 6KEMNITZER W, JIANG S C, WANG Y, et al. Discovery of 4-aryl-4H-chromenes as a new series of apoptosis inducers using a cell- and caspase-based HTS assay. Part 5. Modifications of the 2- and 3-positions [J].Bioorg IVied Chem Lett, 2008,18 ( 2 ) : 603 - 607. 被引量:1
  • 7KASIBHATLA S, GOURDEAU H, MEEROVITCH K, et al. Discovery and mechanism of action of a novel series of apoptosis inducers with potential vascu- lar targeting activity [J ]. Mol Cancer Ther, 2004,3 ( 11 ) : 1365 - 1374. 被引量:1
  • 8GOURDEAU H, LEBLOND L, HAMELIN B, et al. Antivascular and antitumor evaluation of 2-amino-4-(3- bromo-4,5-dimethoxy-phenyl ) -3 -cyano-4H-chromenes, a novel series of anticancer agents [ J ]. Mol Cancer Ther,2004,3 ( 11 ) :1375 - 1384. 被引量:1
  • 9CAI S X, DREWE J, KEMNITZER W, et al. Discovery of 4-aryl-4H-chromenes as potent apoptosis inducers using a cell- and caspase-based anti-cancer screening apoptosis program (ASAP) : SAR studies and the identification of novel vascular disrupting agents [ J ]. Anticancer Agents Med Chem, 2009,9 (4) :437 -456. 被引量:1
  • 10HERON M. Leading causes for 2006 [J ]. Natl Vital Stat Rep,2010,58(14) :1 - 100. 被引量:1

共引文献5

药学实践杂志
2015年 第2期

相关作者

内容加载中请稍等...

相关机构

内容加载中请稍等...

相关主题

内容加载中请稍等...

浏览历史

内容加载中请稍等...
;
使用帮助 返回顶部