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阿哌沙班的合成工艺研究
引用本文:陶海燕,米斌,郭国贤,宫平. 阿哌沙班的合成工艺研究[J]. 中国药物化学杂志, 2013, 0(5): 385-389
作者姓名:陶海燕  米斌  郭国贤  宫平
作者单位:沈阳药科大学制药工程学院,辽宁沈阳110016
摘    要:目的研究阿哌沙班的合成工艺。方法以环戊酮肟为原料,经重排、双氯取代、缩合、亲核取代3步反应得到关键中间体3-吗啉-4-基-1-(4-硝基苯基)-5,6-二氢-1H-吡啶-2-酮(5);再以对甲氧基苯胺为起始原料,经Japp-Klingmann反应得到中间体2-氯-2-[2-(4-甲氧基苯基)腙]乙酸乙酯(6);中间体5与中间体6经过1,3-偶极环加成、脱吗啉基、还原、酰胺化、环合、胺解6步反应得到目标化合物。结果与结论目标化合物的结构经1H-NMR、MS谱确证。总收率达32.5%(以环戊酮肟计)。与文献报道的工艺相比,该路线原料易得、操作简便、条件温和、收率较高,有利于工业化生产。

关 键 词:阿哌沙班  抗血栓  Ⅹa因子直接抑制剂  合成工艺

Study on the synthesis of apixaban
TAO Hai-yan,MI Bin,GUO Guo-xian,GONG Ping. Study on the synthesis of apixaban[J]. Chinese Journal of Medicinal Chemistry, 2013, 0(5): 385-389
Authors:TAO Hai-yan  MI Bin  GUO Guo-xian  GONG Ping
Affiliation:( School of Pharmaceutical Engineering, Shenyang Pharmaceutical University, Shenyang 110016, China)
Abstract:Apixaban, a novel efficient oral factor X a direct inhibitor,is developed by the cooperation of Bristol-Myers Squibb and Pfizer. In this paper, a new synthetic route has been established based on the literatures. Using cyclopentanone oxime and 4-methoxybenzenamine as the starting materials, apixaban is synthesized through ten steps, including Beckmann rearrangement, a-active hydrogen dichlorination, condensation with morpholine, nucleophilic substitution, 1,3-dipolar cycloaddition, olefination, reduction, acylation by 5- chlorovalerylchloride, cyclization and aminolysis. The total yield of the procedure is 32. 5 % (according to the quantity of the cyclopentanone oxime) and the HPLC purity of the final product is 99.7 %. The structures of the finial compound and some important intermediates have been identified by 1H-NMR and MS. The improved process has several advantages over these reported procedures, such as mild conditions, short reaction time and simple operations. Anyway it's more suitable for industrial production.
Keywords:apixaban  anticoagulation  factor X a direct inhibitor  synthesis process
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