CN1239101A - 克拉霉素抗生素药物合成 - Google Patents
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Abstract
已知制备化学式(Ⅰ)表示的克拉霉素。所述方法包括:在催化剂和溶剂存在条件下,红霉素A9肟与醚化剂反应,保护9位肟羟基,醚化保护产物不经分离与硅烷化试剂反应,得化学式(Ⅱ)。化学式(Ⅰ),式(Ⅱ)为:R1可以是:CH3-,CH3CH2-,CH3CH2CH2-,CH3O-R2可以是:C1-3烷基R3可以是:CH3-,CH3CH2-,CH3CH2CH2-R5,R6,R7均为:(CH3)3Si-本发明提高了6位羟基甲基化选择性,保护与去保护很容易实现,收率高,适合工业化大规模生产要求。
Description
本发明涉及克拉霉素抗生素药物合成。所述的克拉霉素对酸和酶稳定,半衰期为红霉素A的2倍,并具有良好的药代动力学性质,口服效果更好。因此克拉霉素是一种广谱,优秀的抗感染药物。
已知下列化学式(1)表示的克拉霉素。
目前国内外生产克拉霉素的主要方法为:
1)美国专利NO,4,311,803公开了一种在红霉素A上进行2′位羟基,3′位二甲胺基保护,6位羟基甲基化,去保护,3′位二甲胺基甲基化,得克拉霉素。由于红霉素A有多个羟基,因此在6位羟基甲基化反应时,会得到多种其他位羟基甲基化产物,这会造成产品分离困难,收率低,成本高。
2)欧洲专利158,467公开了一种在红霉素A上进行9位肟羟基,2′位羟基和/3′位二甲胺基保护,6位羟基甲基化,去保护,3′位胺基甲基化,得克拉霉素。按照欧洲专利158,467公开技术能进行6位羟基甲基化选择反应,但甲基化后,去保护催化还原过程复杂。
3)美国专利0,272,110公开了一种在红霉素A上进行9位肟羟基保护,2′位羟基和4″位羟基保护,6位羟基甲基化,去保护,得克拉霉素。公开文献没有对3′位二甲胺基保护。我们对此公开路线反复实验,的确能对6位羟基进行甲基化造反反应,但同样存在工艺路线复杂,去保护后,大量副产物蒙蔽于产品上,造成不易分离,收率很低。
本发明已很好地解决了现有技术收率低,工艺复杂,分离困难等问题,提高了6位羟基甲基化选择性,保护和去保护很容易实现,因此能够满足工业化大规模生产要求。
本发明提供制备化学式(I)的新方法,所述方法包括:
a)在催化剂和溶剂存在条件下,红霉素A9肟与醚化剂反应,保护9
位肟羟基。
b)醚化保护产物不经分离与硅烷化试剂反应,得化学式(II),式
(II)为:
R1可以是:CH3-,CH3CH2-,CH3CH2CH2-,CH3O-
R2可以是:C1-3烷基
R3可以是:CH3-,CH3CH2-,CH3CH2CH2-
R5,R6,R7均为:(CH3)3Si-
醚硅化保护选用的醚化剂为:乙烯基乙醚,2-甲氧基丙烯,2-乙氧基丙烯,2-甲氧基-1-丁烯,2,2-二乙氧基丙烷。优选:2,2-二乙氧基丙烷,2-甲氧基丙烯。特别优选:2-甲氧基丙烯。
醚化剂用量为红霉素A9肟的2~5.3倍当量。
硅烷化试剂选用:三甲基氯硅烷,三甲硅基咪唑,六甲基二硅胺烷。优选含三甲基氯硅烷的混合硅烷化试剂。例如:三甲基氯硅烷与六甲基二硅胺烷混合试剂,其摩尔比为1∶1~10。
硅烷化试剂用量为红霉素A9肟的1~5倍当量。
醚硅化保护所选用的有机溶剂为不影响反应的惰性溶剂,例如:甲醇,乙醇,二氯甲烷,三氯甲烷,丙酮,N,N-二甲基甲酰胺,苯。
溶剂用量为:每克红霉素A9肟为10ml~50ml。
催化剂选用:吡啶盐酸盐,三乙胺盐酸盐。优选:吡啶盐酸盐。催化剂用量为红霉素A9肟的1~2倍当量。
本发明醚硅化保护反应温度在0℃至回流状态下进行,优选15℃至30℃之间进行醚硅化保护反应。
C)化学式(II)6位羟基甲基化。甲基化试剂选用:CH3I,CH3Br,其用量为化学式(II)的1~2.5倍摩尔量。反应适宜的溶剂可以选用:四氢呋喃,二甲基亚砜,N,N-二甲基甲酰胺。无机碱选用:NaOH,KOH,碱用量为化学式(II)的1~2倍当量。6位羟基甲基化反应适宜的温度在18℃~28℃之间进行。
d)本发明方法中,涉及粗品精制。粗品精制是以C1-3醇中加入脱色剂,回流状态下得纯品,C1-3醇中优选乙醇,脱色剂选用:活性碳。
本发明方法中,6位羟基甲基化选择性很好。
本发明方法中,异构化程度明显降低,产品精制提纯容易实现。
以下通过实施例具体地解释本发明,但本发明不受这些实施例的限定。
实施例1:(1)于1000ml反应缸将20g红霉素A9肟溶于300ml乙醇/二氯甲烷(1∶5)溶剂中,搅拌,加入4.6g盐酸吡啶,加入2-甲氧基丙烯9ml,室温下反应30分钟,加入三甲硅基咪唑5ml,三甲基氯硅烷2ml,继续反应30分钟,终止反应,向反应液中加入正巳烷100ml,过滤,滤液中加入300ml饱和NaHCO3溶液,搅拌,分液,有机相用150ml×2饱和NaCl溶液洗涤二次,分出有机相,有机相用无水Na2SO4干燥,减蒸得24.5g醚硅化红霉素A9肟中间体。
(2)将上步产物24.5g用四氢呋喃/二甲基亚砜(1∶1)500ml溶解,倾入1000ml反应缸,加入1.8mlCH3I,加入KOH粉末0.8g,室温下搅拌反应1hr,加入33%的二甲胺水溶液5ml,继续搅拌30分钟,向反应液中加入300ml水,乙酸乙酯150ml×3萃取3次,分出有机相,有机相用150ml×2饱和NaCl溶液洗涤二次,无水Na2SO4脱水,减蒸得26.7g6位羟基甲基化2′位4″位硅烷化红霉素A9肟中间体。
(3)将上步产物26.7g溶于270ml乙醇/水(1∶1)溶剂中,倾入反应缸,2ml甲酸溶于50ml水,加入反应缸,加入30.7gNaHSO3,升温至回流,搅拌反应1hr,终止反应。冷却反应液,加入300ml水,用2NHaOH溶液调PH至9~10,有大量结晶物析出,反应结晶物抽滤得克拉霉素粗品25.2g。
(4)将25.2g粗品用95%乙醇150ml溶解,升温至回流,加入少量活性碳,回流30分钟,反应液抽滤,浓缩结晶得克拉霉素精品6.2g。
实施例II:
(1)于1000ml反应缸将20g红霉素A9肟溶于300mlCH2CI2溶剂中,搅拌,加入2-甲氧基丙烯9ml,加入4.6g盐酸吡啶,室温反应30分钟,加入六甲基二硅胺烷3.2ml,三甲基氯硅烷0.36ml,继续反应2小时,终止反应,向反应液中加入300ml饱和NaHCO3溶液,搅拌,分液,有机相用150ml×2饱和NaCl溶液洗涤二次,分出有机相,有机相用无水Na2SO4干燥,减蒸得25.0g醚硅化红霉素A9肟中间体。
余下步骤按实施例I(2),(3),(4)得克拉霉素精品6.2g。
实施例III:
(1)于1000ml反应红缸将20g红霉素A9肟溶于450mlCH2CI2溶剂中,搅拌,加入2-甲氧基丙烯9.8ml,加入4.6g盐酸吡啶,室温反应20分钟,加入六甲基二硅胺烷3.6ml,继续反应3小时,终止反应,向反应液中加入300ml饱和NaHCO3溶液,搅拌,分液,有机相用150ml×2饱和NaCI溶液洗涤二次,分出有机相,有机相用无水Na2SO4干燥,减蒸除溶剂,残渣用丙酮-乙醚重结晶得25.0g醚硅化红霉素A9肟中间体。
余下步骤按实施例I(2),(3)得克拉霉素精品25.0g。
(4)将25.0g粗品用无水乙醇150ml溶解,升温至回流,加入少量活性碳,回流30分钟,反应液抽滤,浓缩结晶得克拉霉素精品6.2g。
Claims (8)
1)一种制备化学式(I)表示的克拉霉素。所述方法包括:
a)在催化剂和溶剂存在条件下,红霉素A9肟与醚化剂反应,保护9位肟羟基。
b)醚化保护产物不经分离与硅烷化试剂反应,得化学式(II)。化学式(I),式(II)为:
R1可以是:CH3-,CH3CH2-,CH3CH2CH2-,CH3O-
R2可以是:C1-3烷基
R3可以是:CH3-,CH3CH2-,CH3CH2CH2-
R5,R6,R7均为:(CH3)3Si-,
c)本发明方法中,涉及粗品精制。
2)根据权利要求1的方法,其特征在于醚硅化保护连续完成。
3)根据权利要求1的方法,其特征在于醚化剂优选2-甲氧基丙烯。
4)根据权利要求1的方法,其特征在于硅烷化试剂选用:三甲基氯硅烷,三甲硅基咪唑,六甲基二硅胺烷。
5)根据权利要求4)的方法,硅烷化试剂优选含三甲基氯硅烷的混合硅烷化试剂。
6)根据权利要求5)的方法,硅烷化试剂特别优选三甲基氯硅烷与六甲基二硅胺烷的混合试剂。
7)根据权利要求6)的方法,三甲基氯硅烷与六甲基二硅胺烷的摩尔比为1∶1~10。
8)根据权利要求1)的方法,其特征在于醚硅化保护所选用的有机溶剂是:CH2CI2,丙酮,甲醇,N,N-二甲基甲酰胺,CHCI3,苯。
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Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN102250180A (zh) * | 2010-05-18 | 2011-11-23 | 上海医药工业研究院 | 2’,4”-o-二(三甲基硅基)-红霉素a衍生物和克拉霉素制备方法 |
| CN108117573A (zh) * | 2017-12-26 | 2018-06-05 | 宁夏启元药业有限公司 | 4"-o-(三甲基硅)红霉素a 9-o-(1-乙氧基-1-甲基乙基)肟的合成方法 |
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| KR960000434B1 (ko) * | 1986-12-17 | 1996-01-06 | 다이쇼 세이야꾸 가부시끼가이샤 | 에리스로마이신 a유도체 및 그의 제조 방법 |
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Cited By (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN102250180A (zh) * | 2010-05-18 | 2011-11-23 | 上海医药工业研究院 | 2’,4”-o-二(三甲基硅基)-红霉素a衍生物和克拉霉素制备方法 |
| CN102250180B (zh) * | 2010-05-18 | 2015-07-22 | 上海医药工业研究院 | 2’,4”-o-二(三甲基硅基)-红霉素a衍生物和克拉霉素制备方法 |
| CN108117573A (zh) * | 2017-12-26 | 2018-06-05 | 宁夏启元药业有限公司 | 4"-o-(三甲基硅)红霉素a 9-o-(1-乙氧基-1-甲基乙基)肟的合成方法 |
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