CN1696128A - 一种合成盐酸雷莫司琼的新方法 - Google Patents
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Abstract
本发明公开了一种合成盐酸雷莫司琼的新方法。本法以四氢苯并咪唑为起始原料,采用咪唑环酰基保护,制备得到酰化的四氢苯并咪唑衍生物,随后经芳香碳酰化,制得化合物(I),再经酸水解,制备混旋雷莫司琼,总收率为76%左右,高于现有文献所报道的合成收率(70%左右),从而以一种新的合成方法,完成了该发明。本发明和现有技术相比,制备方法简单,反应条件温和,革除了部分限制使用的溶媒,简化了操作方法,同时节约了原料,降低了生产成本。适于工业化生产。
Description
技术领域
本发明涉及一种酰化的四氢苯并咪唑衍生物的制备方法,更具体的说是一种合成盐酸雷莫司琼的新方法。
背景技术
盐酸雷莫司琼(Ramosetron hydrochloride)化学名称为(-)-5-(R)-[(3-(1-甲基吲哚基))羰基]-4,5,6,7-四氢苯并咪唑盐酸盐,是一种新型高选择性5-HT3受体拮抗剂,它是通过阻断存在于消化道粘膜内传入迷走神经末梢的5-HT3受体,抑制化疗药物、手术等引起的恶心、呕吐等胃肠道副作用。临床上主要用于预防或治疗化疗药物引起的恶心、呕吐等消化道症状。
中国专利ZL90100544.4授权了四氢苯并咪唑衍生物的制备方法,它是以5-羧酸苯并咪唑硫酸甲酯为起始原料,通过氢化、水解、酰胺化、芳香环碳酰化、拆分、成盐共六步反应制备盐酸雷莫司琼。该专利制备方法中,部分中间体如N-(4,5,6,7-四氢苯并咪唑-5-基)羰基吡咯及其盐酸盐,均易溶于水,实验操作中难于通过常用的萃取、重结晶等技术达到分离、纯化的目的,且收率较低(约30%左右)。此外,芳香环碳酰化反应中,采用1、2二氯乙烷作为反应溶剂,该试剂属于国家一类控制试剂,毒性较强,不利于工业化生产,应避免使用。
发明内容
为解决以上技术难点,本发明人经多次实验研究,首次采用咪唑环酰基保护的方法,制备得到酰化的四氢苯并咪唑衍生物,随后以乙腈为反应溶剂,经芳香碳酰化,制备得到化合物(I)。该中间体为固体,可以通过重结晶的方法进行纯化。将(I)酸水解脱保护基制备混旋雷莫司琼,总收率为76%。高于原专利的合成收率,从而以一种新的合成方法,完成了该发明。经检索,本发明的合成方法目前未见任何文献报道。
本发明的目的在于,提供一种适合工业化生产的合成盐酸雷莫司琼的新方法,具体步骤如下:
(1).将化合物(I)与1-12N(优选3-6N)盐酸,混合加热回溜,冷却,将混合物滴加到5-50%(优选5-25%)的氢氧化钠水溶液中,制得5-[(1-甲基吲哚-3-基)羰基]-4,5,6,7-四氢苯并咪唑(化合物IV)。
其中,R为C1~C4的直链或支链的烷烃;如甲基、乙基、丙基、异丙基等优选甲基、乙基。
(2).化合物(IV)经手性拆分剂,制得盐酸雷莫司琼(V)。所述的手性拆分剂包括酒石酸、二苯甲酰酒石酸,优选二苯甲酰酒石酸,按已知方法拆分,制得(-)-(R)-5-[(1-甲基吲哚-3-基)羰基]-4,5,6,7-四氢苯并咪唑盐酸盐(V)即盐酸雷莫司琼。
上述的化合物(I)可采用如下方法制备:
(A).在碱性条件下化合物(II)与烷酰氯反应制备化合物(III)。
所述的碱性条件为已知的无机碱、有机碱例如NaOH、Na2CO3、甲胺、二乙胺或三乙胺等。化合物(II)与烷酰氯的克分子比为1∶0.5-5,优选1∶1-3。
所述的反应时间为2-10小时;反应温度为20-160℃,优选2-4小时,温度为50-130℃。
(B).化合物(III)在乙腈或氯仿中与四氢吡咯、N-甲基吲哚反应制得1-烷酰基-5-[(1-甲基吲哚-3-基)羰基]-4,5,6,7-四氢苯并咪唑化合物(I)。
所述化合物III:四氢吡咯:N-甲基吲哚的克分子比为1∶0.1-3∶1-5,优选1∶0.5-3∶1-3。反应时间为1-10小时;反应温度为0-160℃,优选温度为2-140℃。
反应中所述的烷酰氯主要包括乙酰氯、丙酰氯或丁酰氯、异丁酰氯等优选乙酰氯或丙酰氯。
下面是本发明盐酸雷莫司琼新的合成路线。
本发明以4,5,6,7-四氢苯并咪唑-5-羧酸硫酸盐为起始原料,通过芳香环碳酰化、水解、拆分,成盐共4步反应制备目标化合物。新方法中制得的中间体1-烷基酰-5-羧酸-4,5,6,7-苯并咪唑(III)、1-烷酰基-5-[(1-甲基吲哚-3-基)羰基]-4,5,6,7-四氢苯并咪唑(I)等均为新化合物,制备过程中通过酰化、水解、拆分等反应制备盐酸雷莫司琼(V)。
本发明和现有技术相比,制备方法简单,反应条件温和,革除了毒性较强的1,2二氯乙烷,中间体可采用重结晶的方法纯化,操作简便,总收率高于专利的制备方法,并且降低了生产成本。本工艺路线经小试探索、中试放大研究证实,制得的盐酸雷莫司琼,各步中间体控制方法简单、准确,产品收率较高,合成工艺稳定,质量可控,适于工业化生产。
具体实施方式
下面结合实施例对本发明作进一步的说明,但下列给出的具体实施例操作并不局限本发明要求保护的范围。
本发明原料5-羧酸甲酯苯并咪唑硫酸盐的制备,参考精细有机化工手册(P482-496)中苯并咪唑类衍生物合成制备方法制得。
4,5,6,7-四氢苯并咪唑-5-羧酸硫酸盐(II)的制备是采用中国专利ZL90100544.4的方法获得(具体见参考实施例1-2)。
参考实施例1
5-羧酸甲酯苯并咪唑硫酸盐的制备
在5L的反应瓶中加入3200ml甲醇,304g的5-羧酸苯并咪唑硫酸盐,搅拌下滴加352ml的浓硫酸,加热回流7小时,冷却,加入20g的活性碳,加热回流0.5小时,热过滤,滤液浓缩,冷却,得白色结晶,过滤、干燥得240g,熔点:169-171℃,收率74%。
参考实施例2
4,5,6,7-四氢苯并咪唑-5-羧酸硫酸盐的制备(II)
在2L的高压釜中加入1200ml的乙酸、80g的5-羧酸苯并咪唑甲酯硫酸盐,40g的10%Pd/C(干重),80℃、60kg/cm2的压力条件下氢化反应约16小时(至压力不再变化为止),冷却,出料,过滤催化剂,减压浓缩,得浅黄色油状物,加入300ml的6N盐酸,加热回流4小时,减压浓缩至干,加入30ml的丙酮,过滤,干燥、得53.6g的白色结晶,熔点145-148℃,收率70%。
实施例1
1-乙酰基-5-羧酸-4,5,6,7-苯并咪唑的制备(III)
将66g的4,5,6,7-四氢苯并咪唑-5-羧酸硫酸盐,62.0g的三乙胺,300ml的乙腈加入反应瓶中,滴加36.2g乙酰氯,加热回流搅拌4小时,将乙腈层减压浓缩至干,冷却,滴加300ml的水,用乙酸乙酯提取,干燥,过滤,滤液减压浓缩至干,得棕色油状物70g,可直接投入下一步进行反应。
实施例2
1-乙酰基-5-[(1-甲基吲哚-3-基)羰基]-4,5,6,7-四氢苯并咪唑的制备(I)
将乙酰四氢苯并咪唑70g,200ml的乙腈,40ml的氯化亚砜加入反应瓶中,加热至回流,搅拌2小时,减压蒸馏出部分溶剂带出过量的氯化亚砜。冷却,在2℃的条件下缓慢滴加53g的四氢吡咯与100ml的乙腈溶液,滴毕,升温至室温,搅拌2小时,40℃搅拌1小时,减压浓缩,得棕色油状物132g。
将132g的棕色油状物,100g的N-甲基吲哚加入300ml的乙腈中,加入132g的磷酰氯,在加热、剧烈回流下搅拌7小时,冷至室温。冷却条件下,缓慢滴加660ml的水,500ml的乙酸乙酯搅拌,分层,有机层用水洗涤2次后,用无水硫酸镁干燥,过滤,减压浓缩至干得浅棕色固体87.7g,熔点:176-178℃,收率81.2%,HPLC检测含量大于98%。
通过核磁进行结构确证,具体的测试结果见下:
1H NMR(400MHz,CDCl3)δ:2.03-2.04(1H,d),2.21(1H,s),2.66(3H,s),2.79-3.23(4H,m),3.47(1H,s),3.855(3H,s),7.258-7.34(3H,m),7.79(1H,s),8.36-8.51(2H,q).
实施例3
5-[(1-甲基吲哚-3-基)羰基]-4,5,6,7-四氢苯并咪唑的制备(IV)
将20g 1-乙酰基-5-[(1-甲基吲哚-3-基)羰基]-4,5,6,7-四氢苯并咪唑加入100ml,6N的盐酸水溶液中,加热搅拌,回流4小时,冷却,滴加到25%的氢氧化钠水溶液中,析出浅黄色固体,过滤干燥得淡黄色固体16.5g,熔点118-120℃,收率95%。
核磁测定数据:
1H NMR(400MHz,DMSO)δ:1.81-1.91(1H,m),2.14-2.17(1H,d),2.67-2.90(4H,m),3.62-3.69(1H,t),3.86(3H,s),7.21-7.30(2H,m),7.53-7.55(1H,d),8.19-8.21(1H,d),8.54(1H,s),8.91(1H,s)。
实施例4
(-)-(R)-5-[(1-甲基吲哚-3-基)羰基]-4,5,6,7-四氢苯并咪唑盐酸盐的制备(V)
将22.5g的5-[(1-甲基吲哚-3-基)羰基]-4,5,6,7-四氢苯并咪唑和30.7g的(+)DIBTA单水物加入200ml的DMF中,搅拌至全溶,缓慢滴加100ml的水,室温搅拌2小时,过滤,干燥,得浅黄色固体22g。将该固体用DMF/水(2∶1)重结晶三次,得18g的(-)-(R)-[(1-甲基吲哚-3-基)羰基]-4,5,6,7-四氢苯并咪唑.(+)DIBTA盐,熔点169-170℃,收率35%。
将18g的上述盐加入100ml的水中,加入100ml的氯仿,搅拌下滴加20ml的氨水,分层,水层提取2次,合并有机层,减压蒸馏,得浅黄色固体,加入80ml的异丙醇,搅拌溶解,加入4ml的浓盐酸,搅拌,逐渐析出白色固体,过滤,干燥,得7.5g的产品。
将7.5g的产品加入75ml异丙醇与水(10∶1)溶液中,加入1g的活性炭,加热回流15分钟,热过滤,冷却析出白色结晶,过滤,干燥,得6g,熔点240-245℃,重结晶收率80%。
旋光度:-42.9(c1.12,甲醇)
HPLC:C8柱,含量大于99.5%(归一法)
核磁数据:YMCA-K03(4.6mm×25cm)柱,(R)的含量大于99%。
1H NMR(400MHz,DMSO)δ:1.81-1.91(1H,m),2.14-2.17(1H,d),2.67-2.90(4H,m),3.62-3.69(1H,t),3.86(3H,s),7.21-7.30(2H,m),7.53-7.55(1H,d),8.19-8.21(1H,d),8.54(1H,s),8.91(1H,s)。
Claims (7)
1、一种合成盐酸雷莫司琼的新方法,它包括如下步骤:
(1).将化合物(I)与1-12N盐酸混合加热回溜,冷却,将混合物滴加到5-50%的氢氧化钠水溶液中,制得化合物(IV);
其中,R为C1~C4的直链或支链的烷烃;
(2).化合物(IV)经手性拆分剂拆分,制得盐酸雷莫司琼(V)。
2、如权利要求1所述的新方法,其特征在于,所述的化合物(I)可采用如下方法制备:
(1).在碱性条件下化合物(II)与烷酰氯反应制备化合物(III);
(2).化合物(III)与四氢吡咯、N-甲基吲哚反应制得化合物(I)。
3、如权利要求2所述的新方法,其特征在于,所述的碱为甲胺、二乙胺或三乙胺。
4、如权利要求2所述的新方法,其特征在于,化合物(II)与烷酰氯的克分子比为:1∶0.5-5。
5、如权利要求2所述的新方法,其特征在于,化合物(III):四氢吡咯:N-甲基吲哚的克分子比为1∶0.1-3∶1-5。
6、如权利要求2所述的新方法,其特征在于,所述的烷酰氯为乙酰氯、丙酰氯或丁酰氯。
7、如权利要求2所述的新方法,其特征在于,反应时间为2-10小时;反应温度为0-160℃。
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Cited By (9)
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| US7652052B2 (en) | 2005-04-11 | 2010-01-26 | Astellas Pharma Inc. | Process for producing ramosetron or its salt |
| CN102212059A (zh) * | 2011-04-15 | 2011-10-12 | 南京新港医药有限公司 | 一种消旋化循环制备盐酸雷莫司琼的方法 |
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| CN101585831B (zh) * | 2008-05-23 | 2012-11-07 | 北京成宇化工有限公司 | 雷莫司琼的合成方法 |
| CN105646456A (zh) * | 2016-03-01 | 2016-06-08 | 苏州艾缇克药物化学有限公司 | 一种高收率的雷莫司琼的生产方法 |
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| CN100390165C (zh) * | 2005-06-24 | 2008-05-28 | 天津康鸿医药科技发展有限公司 | 一种含烷酰基雷莫司琼的药物组合物及其应用 |
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| DE69028934T2 (de) * | 1989-02-02 | 1997-03-20 | Yamanouchi Pharma Co Ltd | Tetrahydrobenzimidazol-Derivate |
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