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LU Bin 1, WU De zhu 2, CHEN Shi zhi 3, XU Jian xing 1(1 Institute of Biophysics, Chinese Academy Sciences, Beijing 100101, China;2 China Institute of Atomic Energy, P.O.Box 275 39, Beijing 102413, China; 3 Institute of Materia Medica, Chinese Academy of Medical Science, Beijing 100050, C. Synthesis of ~3H-3-azidosalicyl-N-(n-decyl)amide[J]. Atomic Energy Science and Technology, 2000, 34(2): 132-132. DOI: 10.7538/yzk.2000.34.02.0132
Citation: LU Bin 1, WU De zhu 2, CHEN Shi zhi 3, XU Jian xing 1(1 Institute of Biophysics, Chinese Academy Sciences, Beijing 100101, China;2 China Institute of Atomic Energy, P.O.Box 275 39, Beijing 102413, China; 3 Institute of Materia Medica, Chinese Academy of Medical Science, Beijing 100050, C. Synthesis of ~3H-3-azidosalicyl-N-(n-decyl)amide[J]. Atomic Energy Science and Technology, 2000, 34(2): 132-132. DOI: 10.7538/yzk.2000.34.02.0132
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    • Abstract
  • A novel method for the synthesis of molecular probe of ubiquinone binding protein is described. With 3 nitrosalicylic acid and decylamine as initial compounds and under the existence of DCC, the 3 nitrosalicyl N (n decyl)amide is synthesized at room temperature. Then, 3 nitrosalicyl N (n decyl)amide is reduced by hydrogen with 5 % Pd/C as catalist to form 3 aminosalicyl N (n decyl)amide which is exchanged with tritium to be 3H 3 aminosalicyl N (n decyl)amide. At the temperature below 5 ℃, 3H 3 aminosalicyl N (n decyl)amide reacts with NaNO 2 and HCl, and the 3 diazosalicyl N (n decyl)amide is formed in an ice salt bath. As soon as the reaction is completed, NaN 3 is added to the mixture and stirred for 3 h at the temperature between 0~5 ℃ and in the dark, the molecular probe of studying ubiquinone binding protein, i. e., 3H 3 azidosalicyl N (n decyl)amide is produced.
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