• Title/Summary/Keyword: Benzoylation

Search Result 8, Processing Time 0.017 seconds

Synthesis of Tiaprofenic Acid (Tiaprofenic Acid의 합성)

  • Choi, Hong-Dae
    • YAKHAK HOEJI
    • /
    • v.33 no.4
    • /
    • pp.237-240
    • /
    • 1989
  • A new synthetic method for tiaprofenic acid, which is a potent anti-inflammatory agent, was described. Friedel-Crafts reaction of thiophene with ethyl ${\alpha}-chloro-{\alpha}-(methylthio)$ acetate (1) gave ethyl ${\alpha}-methylthio-2-thiopheneacetate$ (3). Ethyl ${\alpha}-methyl-2-thiopheneacetate$ (5) was prepared by treatment of (3) with NaH and MeI, followed by desulfurization with zinc dust-acetic acid of the resultant ethyl ${\alpha}-methyl-{\alpha}-methylthio-2-thiopheneacetate$ (4). Tiaprofenic acid (7) could be easily synthesized by benzoylation of (5) and hydrolysis of the resultant ethyl $5-benzoyl-{\alpha}-methyl-2-thiopheneacetate$ (6).

  • PDF

A Study on the Syntheses of Simple Analogs of Tetracycline and Flavonoid (Tetracycline과 Flavonoid의 간단한 유도체 합성에 관한 연구)

  • Kim, Hakwon
    • Journal of the Korean Chemical Society
    • /
    • v.40 no.8
    • /
    • pp.549-556
    • /
    • 1996
  • This work describes studies aimed at the synthesis of simple analogs of antibiotic tetracycline(TC) and flavonoid. The synthesis of proposed analogs of tetracycline and flavonide has been accomplished from readily available compounds 9 and 15. The 1,3-cyclohexanedione derivative 9 was transformed to the benzoate derivative 12 followed by base-mediated intramolecular benzoylation to give the bicyclic TC-analog 13. The bicyclic TC-analog 25 and the flavonoid-analogs 26 and 27 have been prepared from the quinol derivative 15.

  • PDF

항바이러스 작용이 기대되는 6-azauridine의 acyclic 및 cyclic phosphate 유도체의 합성

  • 천문우
    • Proceedings of the Korean Society of Applied Pharmacology
    • /
    • 1993.04a
    • /
    • pp.113-113
    • /
    • 1993
  • 항바이러스 작용을 기대하여 6-azauridine의 2',3'-seco 유도체와 이들의 cyclic phosphate 유도체를 합성하였다. 6-azauridine으로부터 periodate oxidation에 의해 2',3'위치를 개열, 환원하여 얻은 triol의 3',5'위치를 acetonide 형으로 보호한 후 2'위치를 tosylation, azidation 하고 deprotection하여 2'-azido-2',3'-seco 유도체 (1)를 얻었다. 2',3'-diazido-2',3'-seco 유도체(2)는 6-azauridine의 2',3'-위치를 먼저 보호한후 5'위치를 benzoylation, 2',3'-deprotection, periodate oxidation 개열로 얻은 diol을 tosyl화 azido화 하고 deprotection하여 얻었다. 5'-azido-2',3'-seco 유도체(3)는 화합물 (2)의 합성시와 동일하게 먼저 2',3'-acetonide로 한후 5'-위치를 tosyl화, azido화 하고 deprotection, 2',3'-perodate 산화 개열등으로 얻었다. cyclic phosphate 유도체 (4)는 상기화합물 (2)를 4-NPPDC로 처리하여 3',5'-p-nitrophenylphosphoryltrioxy 유도체 (5)를 얻고 이것으로부터 3',5'-phosphoryltrioxy 유도체의 ammonium salt(4)를 얻었다. 이들 화합물의 DNA 및 RNA virus에 대한 antiviral activity는 현재 수행중이다.

  • PDF