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Synthesis of fluorescent molecules for the detection of nerve agents and synthesis of novel pyrazolo and isoxazolo quinoline derivatives as potential drugs.

机译:合成用于检测神经毒剂的荧光分子,以及合成潜在的新型吡唑和异恶唑喹啉衍生物。

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摘要

The main focus of chapters I and II of this dissertation is the synthesis and characterization of novel materials that will have high specificity and sensitivity for the detection of highly toxic organophosphate and organophosphonate nerve agents. The study was divided into two main sections, synthesis of quinolinone and 4-aminonaphthalimide derivatives, and binding studies of synthesized target molecules with nerve agent mimics, DCP and DFP. Nine quinolinone target molecules (TR-1, TR-2, TR-3, TR-4, TR-5, 8, 32, 9, and 10) were synthesized, and binding studies of these molecules with nerve agent mimic were also carried out. All the molecules containing the Schiff base moiety (e.g. TR-1, TR-2, TR-3 and TR4) undergo protonation upon attempted reaction with DCP. On the other hand, 7-dimethylamino-4-methyl-2-oxo-1,2-dihydroquinoline-3-carbaldehyde oxime (8) react with nerve agent mimic DCP during reaction studies. Three molecules containing functionalized tethers (TR-4S, TR-5S, and TR-1C) were synthesized so that they can bind to anodic aluminum oxide (AAO) with the help of covalent bonds in order to fabricate sensors for nerve agents. Two 4-aminonaphthalimide dyes, the lithium salt of lucifer yellow (38) and the potassium salt of lucifer yellow 43, were also synthesized successfully. Reactions of nerve agent mimic DCP with AAO which had been impregnated with 38 were studied by fluorescence spectroscopy. Twenty-seven other novel compounds, beside target molecules, were generated in the process of synthesizing quinolinone and 4-aminonaphthalimide target molecules. Chapter III of this dissertation deals with the synthesis of novel pyrazolo and isoxazolo quinoline derivatives as potential medicinal agents. Four pyrazolo and isoxazolo quinoline derivatives (51, 53, 54 and 55) were synthesized and are yet to be tested for the antiviral activity. Nine novel compounds were generated in the synthetic routes described in this chapter.
机译:本论文第一章和第二章的重点是新型材料的合成和表征,该新型材料对高毒性有机磷酸酯和有机膦酸酯类神经毒剂的检测具有很高的特异性和敏感性。该研究分为两个主要部分,喹啉酮和4-氨基萘二甲酰亚胺衍生物的合成,以及合成靶分子与神经毒剂模拟物DCP和DFP的结合研究。合成了九种喹啉酮靶分子(TR-1,TR-2,TR-3,TR-4,TR-5、8、32、9和10),并且还进行了这些分子与神经毒剂模拟物的结合研究出来。尝试与DCP反应后,所有包含席夫碱部分的分子(例如TR-1,TR-2,TR-3和TR4)都会发生质子化。另一方面,在反应研究过程中,7-二甲基氨基-4-甲基-2-氧代-1,2-二氢喹啉-3-甲醛甲醛肟(8)与神经毒物模仿DCP反应。合成了三个包含官能化系链的分子(TR-4S,TR-5S和TR-1C),以便它们可以借助共价键与阳极氧化铝(AAO)结合,从而制造出神经毒剂传感器。还成功合成了两种4-氨基萘酰亚胺染料,荧光素黄的锂盐(38)和荧光素黄43的钾盐。用荧光光谱法研究了神经药模拟物DCP与AAO的反应,该反应物已被38A浸渍。在合成喹啉酮和4-氨基萘二甲酰亚胺靶分子的过程中,除靶分子外还产生了二十七种其他新型化合物。本文的第三章讨论了新型吡唑和异恶唑喹啉衍生物的合成。合成了四种吡唑并异恶唑喹啉衍生物(51、53、54和55),尚待测试其抗病毒活性。通过本章中描述的合成途径生成了九种新化合物。

著录项

  • 作者

    Sit, Rakesh Kumar.;

  • 作者单位

    University of Nevada, Reno.;

  • 授予单位 University of Nevada, Reno.;
  • 学科 Chemistry General.;Chemistry Organic.
  • 学位 Ph.D.
  • 年度 2009
  • 页码 169 p.
  • 总页数 169
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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