CN1020452C - 10-二氢-10-脱氧-11-氮杂红霉内酯a衍生物的制备方法 - Google Patents
10-二氢-10-脱氧-11-氮杂红霉内酯a衍生物的制备方法 Download PDFInfo
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Abstract
制备10-二氢-10-脱氧-11-氮杂红霉内酯A衍生物(式Ⅰ)及其有选择可药用的与酸形成的盐的方法。式Ⅰ中R1代表氢原子、低级烷基、或低级烷酰基,R2、R3和R4有相同或不同的意义,各自代表氢原子或低级烷酰基。
化合物(Ⅰ)具有抗炎作用,可以用作药物。
Description
本发明涉及制备具有生物活性的10-二氢-10-脱氧-11-氮杂红霉内酯A衍生物及其可药用的与酸形成的盐的方法。
众所周知,许多抗菌素除具有基本的抗菌作用外,还具有抗炎作用。但是,抗菌素的这种特性很少被用来治疗不是由病原微生物所引起的炎症。原因是要避免微生物过快地产生抗性和人体对它们可能产生的过敏。所以,有抗炎作用却无抗菌作用的物质一直是很需要的。这些物质的化学结构通常不同于抗菌素,或者在例外情况下,这些物质可用化学转化的方法从抗菌素获得。我们知道D-青霉胺就是由青霉素衍生而来的(见Abraham等,Nature,151,107(1943)和Ruiz-Torres,Arzneimittel-Forsch,24,914(1974))。
按照已知和确定的先有技术,先进行红霉素A肟的贝克曼(Beckmann)重排,然后将得到的红霉素A亚氨基酸还原,合成了10-二氢-10-脱氧-11-氮杂红霉素A(美国专利,4328334,5/1982,Djokic等J.chem,Sco.Perkin Trans.1,1986,1881)。按照改良的埃谢韦勒-克莱克(Eschweiler-clark)方法,将所得胺用甲醛在甲酸存在下还原甲基化,制得N-甲基-11-氮杂-10-脱氧-10-二氢红霉素A(英国专利,2094293,Kobrehel和Djokic),这是一种
新的15员氮杂环内酯的半合成大环内酯抗菌素;这种抗菌素已以迭氮斯罗霉素(azithromycin)的属名进行了临床试验。美国专利4464527(1984)叙述了获得10-二氢-10-脱氧杂红霉素A的N-乙基和N-正丙基衍生物的方法。这些衍生物是有效的抗菌剂。
申请者对先有技术的检索表明,目前还无人报道过10-二氢-11-氮杂红霉内酯A类化合物,尤其是它们的N-烷基衍生物、它们的盐和/或O-和/或N,O-取代的烷酰基衍生物。
本发明旨在提出制备化合物10-二氢-10-脱氧-11-氮杂红霉内酯A(式Ⅰ)及可选择制备的其可药用的与酸形成的盐的方法。结构式(Ⅰ)中,R1代表氢原子、低级烷基或低级烷酰基;R2、R3和R4可以相同也可不同,各自代表氢原子或低级烷酰基。
这一方法包括:
A)使10-二氢-10-脱氧-11-烷基-11-氮杂红霉素A(式Ⅱ)经一步或二步水解,在
式Ⅱ中,R1意义同上,R′ 2代表德糖胺基,R′ 3代表克拉定糖基,R′ 4代表氢原子;
或B)使10-二氢-10-脱氧-11-氮杂红霉内酯A(式Ⅲ),在甲酸的存在下,或者在氢及贵金属催化剂的存在下,与式Ⅳ的脂肪醛反应,在式Ⅳ中,R5代表氢或低级烷基(最好是C1-C3烷基);
和C)如果需要,可将按A)或B)获得的产物用低级脂肪酸酐,最好是C1-3脂肪酸酐进行酰化,并且如果需要,可将按A)、B)或C)得到的产物转化成可作药用的与酸形成的盐。
本发明方法步骤A的水解可以一步完成,也可以二步完成。一步水解具体可以先用高浓度无机酸在惰性溶剂(如氯仿)存在下,加热回流16至60小时,然后在pH值为8至9的条件下,用同一溶剂萃取将产物分离出来。二步水解包括:ⅰ)在室温下,用稀的无机酸将式(Ⅱ)化合物水解10至20小时,然后用有机溶剂(如二氯甲烷、氯仿或乙醚)在pH值为9至11条件下萃取中间产物6-0-德糖胺基-10-二氢-10-脱氧-11-烷基-11-氮杂红霉素A(式Ⅴ),式中R1、R2′意义同上。
ⅱ)接着按上述“一步”方法水解已分离的中间产物(Ⅴ)。
将化合物Ⅲ还原烷基化的本发明方法B)可按下面两种方式之一进行:B1)使化合物Ⅲ在惰性溶剂中,于甲酸存在条件下,与甲醛反应;B2)使化合物Ⅲ在惰性溶剂中,于氢和贵金属催化剂存在下,与式Ⅳ的醛反应。
按照本发明的B1)方法,在反应混合物的回流温度下,于惰性溶剂(如丙酮、卤代烷(最好是氯仿))中,在至少等量的甲酸存在下,使化合物Ⅲ与过量1-3摩尔的甲醛反应2-8小时,得到化合物Ⅰ(其中R1为甲基,R2、R3和R4各自代表氢原子)。
B2)方法是在惰性溶剂〔如甲醇或乙醇(96%m/m)等低级醇〕中,于贵金属存在下,用式Ⅳ的醛和氢将化合物Ⅲ还原烷基化。具体反应条件是醛过量1-2倍摩尔,贵金属催化剂(最好是钯-炭(5%m/m))为0.5至等摩尔量。还原烷基化反应是在温和的
温度下(如18至25℃)和在初始氢压为10至30巴的条件下进行2至10小时。反应完成后,滤去催化剂,然后用常规方法分离产物,最好是在减压条件下蒸发乙醇,再用惰性有机溶剂(如二氯甲烷、氯仿或四氯化碳)萃取水悬浮液,从而使式(Ⅰ)产物分离,式(Ⅰ)中,R1代表低级烷基,R2、R3和R4均为氢原子。
酰化步骤则可按通用的酰化方法(如Jones等,J.Med.Chem.,15,631(1972)进行。
具体的一组式(Ⅰ)化合物是式ⅠA的新10-二氢-10-脱氧-11-氮杂红霉内酯A化合物及其可作药用的与酸形成的盐,
其中R′ 1表示除氢原子以外的R1,R3和R4意义同上。
式(Ⅴ)中间体也是新的化合物。
应该指出,当R1为氢原子时,化合物(Ⅰ)本身属于先有技术(见前述S.Djoki
等,J.Chem.Soc.,Perkin
Trans,1,1986,1881);但本申请人已经发现了它们的新的、明显改进的制备方法(根据上述方法A)和医药用途,这些目前仍是未知的。10-二氢-10-脱氧-11-氮杂红霉丙酯A(式Ⅰ)的可作药用的与酸形成的盐也包括在本发明范围内,其制备方法是:使至少等摩尔量合适的酸(如盐酸、氢溴酸、硫酸、磷酸、醋酸、丙酸、柠檬酸、琥珀酸和苯甲酸等)与10-二氢-10-脱氧-11-氮杂红霉内酯A类化合物(式Ⅰ)反应,此反应可选择在于此反应的条件下为惰性的溶剂中进行。与酸形成的盐的分离方法有:若它们不溶于所用的惰性溶剂,就采用过滤法;加入不溶解相应盐的溶剂使该盐沉淀出来;或者蒸发溶剂,最常用的是冷冻干燥法。
根据体外和体内研究发现,上述式(Ⅰ)化合物具有十分显著的抗炎作用。用人体多形核白细胞的溶酶体酶细胞外释放的模型(Weissman等,J.Exp.Med.,134,149(1971);Carevi
,Agents and Actions,16,407(1985),通过与已知的抗炎药物双氯芬酸(DICL)和D-青霉胺(D-PEN)进行比较,测定了它们的体外抗炎作用,结果见附图1和2。
图1明显表明,将迭氮斯罗霉素(azithromycin)水解并制备相应6-0-德糖胺基衍生物(DESAZ)得到了具有良好抗炎活性的产物。DESAZ在10-5浓度条件下与浓度为10-7的D-PEN具有大约相等的活性。通过消除双糖基并合成10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A(AZER),得到了能显著抑制溶酶体酶从多形核白细胞的细胞外释放的化合物,其活性与D-PEN相近,在浓度为10-7,则活性更强。
表1
本发明新的氮杂红霉内酯A的抗炎活性
角叉菜酸引起的大白鼠爪水肿
化合物 n
剂量(mg/kg)RO 抑制%
DE 4 50 29
AZER 6 50 29
AE 4 50 32
APR 5 50 25
ALA-3 5 50 34
AZER.HCl 5 50 38
D-PEN 4 50 28
乙酰水扬酸 22 50 40
n=组的数目(每组五只鼠)
DE-10-二氢-10-脱氧-11-氮杂红霉内酯A
AEER-10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A
AE-10-二氢-10-脱氧-11-乙基-11-氮杂红霉内酯A
APR-10-二氢-10-脱氧-11-正丙基-11-氮杂红霉内酯A
ALA-3-4,6,13-三乙酰基-10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A
AZER,HCl-10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A盐酸盐
实例1.10-二氢-10-脱氧-11-氮杂红霉内酯A
加热回流10-二氢-10-脱氧-11-氮杂红霉素A(100g,136.06mmole)、6M HCl(750ml)和CHCl3(380ml)的混合物16小时。冷却至室温后使液体分层,水层用CHCl3(2×100ml)萃取。加入钠碱液调节水溶液PH至5.0,再用CHCl3(3×100ml)萃取。在PH为8.5时重复同一操作(3×250ml)。PH8.5的氯仿萃取液用K2CO3干燥,然后减压蒸发,得到53.77g(94.2%)10-二氢-10-脱氧-11-氮杂红霉内酯A粗品。用乙醚(300ml)进行结晶后,得到34.45g纯的产物(TLC(薄层层析),C6H6∶CHCl3∶CH3OH=40∶55∶5,NH3Rf0.233),其物理化学常数见J.Chem.Soc.,Perkin Trans.,1,1986,1881。
实例2.10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A
将迭氮斯罗霉素(azithromycin)(Ⅱ)(10g,13.35mmole)、6M HCl(75ml)和氯仿(38ml)的混合物加热回流48小时。冷却至室温后使液体分层,水层用氯仿萃取。用钠碱液调节水溶液PH至5.0,再用氯仿萃取。在PH为8.5时重复相同步骤。将所得PH为8.5的氯仿萃取液真空浓缩至约10ml,静置析出结晶。过滤并干燥后得到4.7g(81.2%)产物,如需要可用氯仿进行重结晶。熔点:208-210℃。
C H N
C22H43NO7计算值:60.94 10.00 3.23
测得值:60.72 9.63 2.96
实例3.6-0-德糖胺基-10-二氢-10-脱氧-11-甲基-11-氮杂红霉素A
将迭氮斯罗霉素(azithromycin)(10g,13.35mmole)在0.25M HCl(500ml)中的溶液在室温下静置15小时。用氯仿(3×75ml)萃取,然后萃取液用1M HCl和水洗涤。加钠碱液使所得水层PH为10,再用氯仿重新萃取。氯仿萃取液用K2CO3干燥,然后减压蒸发至干。粗产物用乙醚洗涤后得到产物6.9g(87.8%)。熔点:203-205℃。
C H N
C30H58N2O9计算值:60.99 9.90 2.96
测定值:60.63 9.58 4.36
实例4.按实例1所述方法,从10g实例3产物得到6.56g(89.4%)实例2产物。
实例5.10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A
向10-二氢-10-脱氧-11-氮杂红霉内酯A(1g,2.38mmole)的CHCl3(20ml)溶液中加入0.184ml(2.38mmole)甲醛(36%)和0.183ml(4.77mmole)甲酸(98-100%),反应混合物搅拌回流8小时。然后冷却至室温,静置24小时,滤出析出的结晶体,用CHCl3洗涤并干燥,得1.0g(96.5%)10-二氢-
10-脱氧-11-甲基-11-氮杂红霉内酯A粗品。如需要可将产物从氯仿中结晶(TLC,Rf0.306)。
熔点:208-210℃。
1H NMR(CD3OD):2.351ppm(N-CH3)。
实例6.10-二氢-10-脱氧-11-乙基-11-氮杂红霉内酯A
向10-二氢-10-脱氧-11-氮杂红霉内酯A(5g,11.92mmole)的乙醇(96%)(50ml)溶液中加入乙醛(7ml,120.5mmole)和钯-炭(5%)(2.5g),在20巴压力和搅拌下将反应混合物氢化10小时。滤出催化剂,用乙醇(20ml)洗涤,通过减压蒸发将合并的液相浓缩至约30ml。向反应混合物中加水(100ml)和CHCl3(50ml),再加2M HCl调节PH至4.5,分层后水相用氯仿(2×50ml)萃取。用钠碱水溶液(3×50ml)调PH至8.5后重复用氯仿萃取步骤。用K2CO3使氯仿萃取液干燥,再减压蒸发,得到4.65g(87.2%)10-二氢-10-脱氧-11-乙基-11-氮杂红霉内酯A粗品。把所得产物悬浮在乙醚(10ml)中,室温下搅拌1小时,过滤后用乙醚洗涤沉淀,然后干燥,得到3.2g色谱纯的产物(TLC,Rf0.390),熔点204-206℃。
实例7.10-二氢-10-脱氧-11-正丙基-11-氮杂红霉内酯A
向10-二氢-10-脱氧-11-氮杂红霉内酯A(6g,14.30mmole)的乙醇(96%)(60ml)溶液中加入
丙醛(11.4ml,157.31mmole)和钯-炭(5%)(3.0g),在22巴压力和搅拌下将反应混合物氢化10小时。滤除催化剂,将滤液减压蒸发至粘稠浆状,通过PH梯度萃取分离产物。再向反应混合物中加水(100ml)和二氯甲烷(50ml),然后用2M HCl调节PH至4.5。液体分层后用二氯甲烷(2×50ml)萃取水层。用钠碱水溶液碱化使PH至8.5,再重复二氯甲烷的萃取步骤(1×150ml,2×50ml)。将PH为8.5的合并的有机萃取物过滤,滤液经减压蒸发浓缩成粘稠悬浮液,过滤析出的结晶,用二氯甲烷洗涤并干燥,得到4.3g(65.2%)色谱纯的标题化合物(TLC,Rf0.415)。
熔点:212-216℃。
实例8.4-0-乙酰基-10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A
向10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A(5g,11.53mmole)的吡啶(30ml)溶液中加入乙酐(30ml)。反应混合物于室温下静置2小时。加入冰块,酰化反应停止进行,在PH9.0条件下用CHCl3(3×50ml)萃取使产物分离。用K2CO3干燥合并的有机萃取液,再经蒸发,得3.4g粗产物。把粗产物悬浮在乙醚(10ml)中,于室温下搅拌1小时,然后过滤,得到1.75g(53.2%)标题化合物,熔点187-189℃(TLC,Rf 0.564)。
IR(KBr):1725(C=0内酯和酯)和1235cm-1(OAC)
1H NMR(CD3OD):2.343(s,3H,N-CH3),
2.052(s,3H,4-OAC)和5.227ppm(d,1H,4-H)。
在上述方法中,仅把乙酐换成丙酸酐而其它不变,可制得相应的4-0-丙基衍生物。
实例9.4,6,13-0-三乙酰基-10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A
向10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A(5g,11.53mmole)的吡啶(50ml)溶液中加入乙酐(50ml),室温下将反应混合物静置7天。加冰终止反应,按实例8的方法用氯仿萃取分离产物。合并的有机萃取液用K2CO3干燥后蒸发至干,再在硅胶柱上进行层析,用CH2Cl2/CH3OH/NH4OH(90∶9∶1.5)溶剂系统为洗脱剂。将后流出的部分合并,蒸发除去溶剂并将所得非晶形产物干燥,得到4,6,13,-0-三乙酰基衍生物,熔点:180-182℃(Rf0.337)。
IR(KBr):1740(C=0,酯),1715(C=0,内酯)和1240cm-1(OAC)
13C NMR(CDCl3):43.1(q,N-CH3),173.5(s,C=0内酯)和170.2,170.1和169.1ppm(s,C=0乙酸酯)。
实例10.11-N,4,6-0-三乙酰基-10-二氢-10-脱氧-11-氮杂红霉内酯A
按照例8所述方法,从10-二氢-10-脱氧-11-氮杂红霉内酯A(5.0g,11.9mmole)和乙酐(50ml)的吡啶(50ml)溶液通过酰化反应,得到11-N,4,6-0-三乙酰基-10-二氢-10-脱氧-11-氮杂红霉内酯A的粗品。24小时后使酰化反应终止,产物用常规的CHCl3萃取的方法分离,粗产物纯化的方法是:将所得粗产物悬浮在乙醚(50ml)中并在室温下搅拌悬浮液1小时,最后滤出不溶的标题化合物,产量:4.08g(68.3%)。熔点220-223℃。Rf0.417。
IR(KBr):1715(C=0,内酯和酯),1605(NAC)和1240cm-1(OAC)。
1H NMR(CD3OD):2.115(s,3H,N-Ac),2.053(s,3H,4-OAc)和2.040ppm(s,3H,6-OAc)。
实例11.10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A盐酸盐
将10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A(4.34g,10mmole)悬浮在25ml水中,在1小时内于搅拌下滴加0.25N HCl,把PH调至5.8。将清澈的反应混合物于室温下继续搅拌1小时,然后过滤并冷冻干燥,得4.48g(95.5%)10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A盐酸盐。
1H NMR(CD3OD):3.03ppm(s,3H,N-CH3)
元素分析:Cl
计算值 7.54%
测定值 6.97%
按同样方式,可以用氢溴酸、醋酸、硫酸、磷酸、柠檬酸和苯甲酸等酸代替盐酸,可制得10-二氢-10-脱氧-11-烷基-11-氮杂红霉内酯A和它们的N-和/或N,O-取代衍生物的相应的盐。
实例12.10-二氢-10-脱氧-11-甲基-11-氮杂红霉内酯A(方法B)
按照实例5的方法,以10-二氢-10-脱氧-11-氮杂红霉内酯A(1g,2.38mmole)、甲醛(36%)(0.184ml,2.38mmole)和甲酸(98-100%)(0.183ml,4.77mmole)为起始原料,在丙酮(20ml)中进行反应,得到0.93g(89.8%)标题化合物。
实例13.10-二氢-10-脱氧-11-乙基-11-氮杂红霉内酯A(方法B)
按照实例1所述方法,以10-二氢-10-脱氧-11-乙基-11-氮杂红霉素A(5g,6.55mmole)为起始原料,可分离得到2.45g(83.57%)标题化合物,其物化常数与实例6所述相同。
实例14.10-二氢-10-脱氧-11-正丙基-11-氮杂红霉内酯A(方法B)
按实例1所述方法,以10-二氢-10-脱氧-11-正丙基-11-氮杂红霉素A(5g,6.44mmole)为起始原料,可分离得到2.4g(80.7%)标题化合物,其物理化学常数与
实例7所述相同。
实例15.6-0-德糖胺基-10-二氢-10-脱氧-11-乙基-11-氮杂红霉内酯A
将10-二氢-10-脱氧-11-乙基-11-氮杂红霉素A(1g,1.31mmole)溶于0.25MHCl(50ml),于室温下静置16小时,然后用CHCl3(3×10ml)萃取反应混合物,合并的有机萃取液用1MHCl和水洗涤,合并的水层用钠碱水溶液碱化至PH为10,再用CHCl3(3×20ml)重新萃取。CHCl3萃取液用K2CO3干燥处理后再蒸发至干。用乙醚洗涤粗产物之后,得到0.7g(88.4%)标题化合物。
1H NMR(CDCl3):2.24ppm(s,6H,N(CH3)2)。
用同样的方法,将6-0-德糖胺基-10-二氢-10-脱氧-11-正丙基-11-氮杂红霉素A水解可以得到相应的N-正丙基衍生物。
Claims (5)
1、制备式Ⅰ的10-二氢-10-脱氧-11-氮杂红霉内酯A化合物及可选择制备的其可药用的与酸形成的盐的方法,
式中R1代表氢原子、含1-3个碳原子的烷基或含1-3个碳原子的低级烷酰基,R2,R3和R4相同或不相同,各自代表氢原子或含1-3个碳原子的低级烷酰基,该方法包括:
A)使10-二氢-10-脱氧-11-烷基-11-氮杂红霉素A(式Ⅱ)在高浓度无机酸中,在惰性溶剂存在下,在回流温度下,水解16-60小时
其中R1为氢原子,C1-3烷基,R′ 2表示德糖胺基,R′ 3表示克拉定糖基,R′ 4表示氢原子,从而生成R1如上定义,R2,R3和R4分别为氢原子的式(Ⅰ)10-二氢-10-脱氧-11-氮杂红霉内酯A或将式(Ⅱ)红霉素A衍生物(式中各基团定义同上)先于室温下,用稀无机酸水解,生成式(V)红霉素衍生物
(式中各基团定义同上),然后再将式(V)红霉素A衍生物于高浓度无机酸中,如上所述水解,从而生成R1如上所定义,R2,R3和R4分别为氢原子的式(Ⅰ)10-二氢-10-脱氧-11-氮杂红霉内酯
A;
或B)使10-二氢-10-脱氧-11-氮杂红霉内酯A(式Ⅲ)在98-100%甲酸存在下,于回流温度下,在惰性溶剂中,与1-3摩尔甲醛反应2-8小时,生成R1为甲基,R2,R3和R4分别为氢原子的10-二氢-10-脱氧-11-氮杂红霉内酯A,
或者在氢和贵金属催化剂存在下,于室温,在氢压10-30巴下,与式(Ⅳ)的1-2摩尔脂肪醛反应2-10小时,
其中R5为氢原子或含1-3个碳原子的低级烷基,从而生成R1为含1-3个碳原子的低级烷基,R2,R3和R4分别为氢原子的式Ⅰ化合物,
和C)若需要,将R1为氢原子或含1-3个碳原子的低级烷基的式(Ⅰ)10-二氢-10-脱氧-11-氮杂红霉内酯A用低级脂肪酸酐酰化,生成R1为含1-3个碳原子的低级烷基或含1-3个碳
原子的低级烷酰基,R2,R3和R4为氢原子或如上定义的烷酰基的式(Ⅰ)10-二氢-10-脱氧-11-氮杂红霉内酯A,或如需要,通过与至少等摩尔量的无机或有机酸反应将A),B)或C)和产物转变为其药用酸加成盐。
2、权利要求1的方法,其中所述高浓度无机酸为6MHCl。
3、权利要求1的方法,其中所述稀无机酸为0.25MHCl。
4、权利要求1的方法,其中所述惰性溶剂为氯仿或丙酮。
5、权利要求1的方法,其中所述贵金属催化剂为5%Pd/c。
Applications Claiming Priority (4)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| YUP1631/87 | 1987-09-03 | ||
| YU163187A YU44641B (en) | 1987-09-03 | 1987-09-03 | Process for preparing derivatives of 10-dihydro-10-deoxo-11-azaeritronolides |
| YU85/88A YU45054B (en) | 1988-01-18 | 1988-01-18 | Process for preparing derivative of 10-dihydro-10-deoxo-11-azaerithronolide a |
| YUP85/88 | 1988-01-18 |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| CN1031703A CN1031703A (zh) | 1989-03-15 |
| CN1020452C true CN1020452C (zh) | 1993-05-05 |
Family
ID=27130708
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CN88103197A Expired - Fee Related CN1020452C (zh) | 1987-09-03 | 1988-05-20 | 10-二氢-10-脱氧-11-氮杂红霉内酯a衍生物的制备方法 |
Country Status (12)
| Country | Link |
|---|---|
| US (1) | US4886792A (zh) |
| EP (1) | EP0283055B1 (zh) |
| JP (1) | JPH01287076A (zh) |
| CN (1) | CN1020452C (zh) |
| BG (1) | BG49825A3 (zh) |
| CA (1) | CA1296000C (zh) |
| CS (1) | CS274462B2 (zh) |
| DE (1) | DE3860503D1 (zh) |
| HU (1) | HU198913B (zh) |
| PL (1) | PL155159B1 (zh) |
| RO (1) | RO105811B1 (zh) |
| RU (1) | RU2007398C1 (zh) |
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| US5049557A (en) * | 1986-05-13 | 1991-09-17 | Chai-Tech Corporation | Metallo-organic salt compounds and pharmaceutical uses thereof |
| US5254682A (en) * | 1989-12-08 | 1993-10-19 | Merck & Co., Inc. | Cyclic renin inhibitors containing 3(S)-amino-4-cyclohexyl-2(R)-hydroxy-butanoic acid or 4-cyclo-hexyl-(2R, 3S)-dihydroxybutanoic acid or related analogs |
| EP0432975A1 (en) * | 1989-12-08 | 1991-06-19 | Merck & Co. Inc. | Cyclic renin inhibitors |
| US5194605A (en) * | 1989-12-08 | 1993-03-16 | Merck & Co., Inc. | Cyclic renin inhibitors containing 2-substituted (3S,4S)-4-amino-5-cyclohexyl-3-hydroxy pentanoic acid, 2-substituted (3S,4S)-5-cyclohexyl-3,4-di-hydroxy pentanoic acid or 2-substituted (4S,5S)-5-amino-6-cyclohexyl-4-hydroxyhexanoic acid or its analogs |
| YU45590A (sh) * | 1990-03-07 | 1992-07-20 | PLIVA FARMACEVTSKA, KEMIJSKA, PREHRAMBENA I KOZMETIČKA INDUSTRIJA s.p.o. | Novi kompleksi odnosno helati antibiotika s dvovalentnim i/ili trovalentnim metalima i postupci za njihovo dobijanje |
| US5912331A (en) * | 1991-03-15 | 1999-06-15 | Merck & Co., Inc. | Process for the preparation of 9-deoxo-9(Z)-hydroxyiminoerythromycin A |
| US5985844A (en) * | 1992-03-26 | 1999-11-16 | Merck & Co., Inc. | Homoerythromycin A derivatives modified at the 4"-and 8A-positions |
| US5189159A (en) * | 1992-04-02 | 1993-02-23 | Merck & Co., Inc. | 8a-AZA-8a-homoerythromycin cyclic iminoethers |
| US5215980A (en) * | 1992-01-17 | 1993-06-01 | Merck & Co., Inc. | 10-AZA-9-deoxo-11-deoxy-erythromycin A and derivatives thereof |
| FR2691464B1 (fr) * | 1992-05-21 | 1995-06-02 | Roussel Uclaf | Nouveaux dérivés de la 1-oxa 6-azacyclopentadécane 13,15-dione, leur procédé de préparation et leur application comme médicaments. |
| US5185365A (en) * | 1992-06-24 | 1993-02-09 | Cornell Research Foundation, Inc. | Insect deterrent azamcrolides |
| US5210235A (en) * | 1992-08-26 | 1993-05-11 | Merck & Co., Inc. | Methods of elaborating erythromycin fragments into amine-containing fragments of azalide antibiotics |
| US5332807A (en) * | 1993-04-14 | 1994-07-26 | Merck & Co., Inc. | Process of producing 8A- and 9A-azalide antibiotics |
| AU7961498A (en) * | 1997-06-26 | 1999-01-19 | Merck & Co., Inc. | 9a-azalides, compositions containing such compounds and methods of treatment |
| AU7986098A (en) * | 1997-06-27 | 1999-01-19 | Merck & Co., Inc. | 9a-aza-3-ketolides, compositions containing such compounds and methods of treatment |
| DE69824201T2 (de) * | 1997-10-16 | 2005-09-22 | Pliva - Istrazivacki Institut D.O.O. | Neue 9a-azalide |
| AP9801420A0 (en) * | 1998-01-02 | 1998-12-31 | Pfizer Prod Inc | Novel macrolides. |
| AP1060A (en) * | 1998-01-02 | 2002-04-23 | Pfizer Prod Inc | Novel erythromycin derivatives. |
| JP2003500414A (ja) * | 1999-05-24 | 2003-01-07 | ファイザー・プロダクツ・インク | 13−メチルエリスロマイシン誘導体 |
| HRP20010018A2 (en) | 2001-01-09 | 2002-12-31 | Pliva D D | Novel anti-inflammatory compounds |
| US20030207819A1 (en) * | 2002-05-02 | 2003-11-06 | Moskowitz Roland W. | Compositions and methods for treating inflammatory connective tissue diseases |
| AU2003264917A1 (en) | 2002-07-08 | 2004-01-23 | Pliva - Istrazivacki Institut D.O.O. | Hybrid molecules of macrolides with steroid/non-steroid anti-inflammatory, antineoplastic and antiviral active molecules |
| CA2489398A1 (en) * | 2002-07-08 | 2004-01-15 | Pliva-Istrazivacki Institut D.O.O. | Novel nonsteroidal anti-inflammatory substances, compositions and methods for their use |
| RS20050008A (en) * | 2002-07-08 | 2007-06-04 | Pliva-Istraživački Institut D.O.O., | New compounds,compositions and methods for treatment of inflammatory diseases and conditions |
| ITMI20022292A1 (it) * | 2002-10-29 | 2004-04-30 | Zambon Spa | 9a-azalidi ad attivita' antiinfiammatoria. |
| HRP20030324A2 (en) | 2003-04-24 | 2005-02-28 | Pliva-Istra�iva�ki institut d.o.o. | Compounds of antiinflammatory effect |
| WO2005030227A1 (en) | 2003-09-23 | 2005-04-07 | Enanta Pharmaceuticals, Inc. | 9a, 11-3C-BICYCLIC 9a-AZALIDE DERIVATIVES |
| US7402568B2 (en) | 2004-09-29 | 2008-07-22 | Enanta Pharmaceuticals, Inc. | Bicyclic 9a-azalide derivatives |
| CA2585711A1 (en) | 2004-10-27 | 2006-05-04 | Glaxosmithkline Istrazivacki Centar Zagreb D.O.O. | Conjugates with anti-inflammatory activity |
| US7271155B2 (en) | 2005-01-07 | 2007-09-18 | Enanta Pharmaceuticals, Inc. | 9A, 11-2C-bicyclic 9a-azalide derivatives |
| US20080200403A1 (en) * | 2005-01-14 | 2008-08-21 | Glaxosmithkline | 9A-Carbamoyl and Thiocarbamoyl Azalides with Anti-Inflammatory Activity |
| WO2009055557A1 (en) | 2007-10-25 | 2009-04-30 | Cempra Pharmaceuticals, Inc. | Process for the preparation of macrolide antibacterial agents |
| US20100031410A1 (en) * | 2008-08-08 | 2010-02-11 | Linda Clark | Multi-Positionable Face Shield |
| US8796232B2 (en) | 2008-10-24 | 2014-08-05 | Cempra Pharmaceuticals, Inc. | Methods for treating resistant diseases using triazole containing macrolides |
| US9937194B1 (en) * | 2009-06-12 | 2018-04-10 | Cempra Pharmaceuticals, Inc. | Compounds and methods for treating inflammatory diseases |
| CN101619085B (zh) * | 2009-08-11 | 2015-04-22 | 沈阳药科大学 | 红霉素衍生物及其作为肿瘤细胞增殖抑制剂的用途 |
| JP5914335B2 (ja) | 2009-09-10 | 2016-05-11 | センプラ ファーマシューティカルズ,インコーポレイテッド | マラリア、結核、及びmac病の治療方法 |
| KR20180110181A (ko) | 2010-09-10 | 2018-10-08 | 셈프라 파마슈티컬스, 인크. | 질환을 치료하기 위한 수소결합 형성 플루오로 케토라이드 |
| CA2868262A1 (en) | 2012-03-27 | 2013-10-03 | Cempra Pharmaceuticals, Inc. | Parenteral formulations for administering macrolide antibiotics |
| CN105163785A (zh) | 2013-03-14 | 2015-12-16 | 森普拉制药公司 | 用于治疗呼吸道疾病的方法及其制剂 |
| CA2907085A1 (en) | 2013-03-15 | 2014-09-18 | Cempra Pharmaceuticals, Inc. | Convergent processes for preparing macrolide antibacterial agents |
| WO2014166503A1 (en) | 2013-04-10 | 2014-10-16 | Probiotic Pharmaceuticals Aps | Azithromycin antimicrobial derivatives with non-antibiotic pharmaceutical effect |
| GB201608236D0 (en) * | 2016-05-11 | 2016-06-22 | Fidelta D O O | Seco macrolide compounds |
| CN106478542A (zh) * | 2016-10-17 | 2017-03-08 | 南开大学 | 一种大环内脂类衍生物盐、其制备方法及用途 |
Family Cites Families (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| YU43116B (en) * | 1979-04-02 | 1989-04-30 | Pliva Pharm & Chem Works | Process for preparing 11-aza-4-o-cladinosyl-6-o-desosaminyl-15-ethyl-7,13,14-trihydroxy-3,5,7,9,12,14-hexamethyl-oxacyclopentadecane-2-one(11-aza-10-deox |
-
1988
- 1988-04-08 EP EP88105626A patent/EP0283055B1/en not_active Expired - Lifetime
- 1988-04-08 DE DE8888105626T patent/DE3860503D1/de not_active Expired - Lifetime
- 1988-04-08 HU HU881778A patent/HU198913B/hu not_active IP Right Cessation
- 1988-04-12 US US07/180,491 patent/US4886792A/en not_active Expired - Fee Related
- 1988-04-13 CS CS253388A patent/CS274462B2/cs unknown
- 1988-04-13 CA CA000564025A patent/CA1296000C/en not_active Expired - Lifetime
- 1988-04-14 RO RO144712A patent/RO105811B1/ro unknown
- 1988-04-22 PL PL1988272025A patent/PL155159B1/pl unknown
- 1988-04-26 BG BG83878A patent/BG49825A3/xx unknown
- 1988-05-16 RU SU884355672A patent/RU2007398C1/ru active
- 1988-05-20 CN CN88103197A patent/CN1020452C/zh not_active Expired - Fee Related
- 1988-07-21 JP JP63180450A patent/JPH01287076A/ja active Pending
Also Published As
| Publication number | Publication date |
|---|---|
| HUT47552A (en) | 1989-03-28 |
| JPH01287076A (ja) | 1989-11-17 |
| PL155159B1 (en) | 1991-10-31 |
| CA1296000C (en) | 1992-02-18 |
| CN1031703A (zh) | 1989-03-15 |
| HU198913B (en) | 1989-12-28 |
| DE3860503D1 (de) | 1990-10-04 |
| RO105811B1 (ro) | 1992-12-30 |
| US4886792A (en) | 1989-12-12 |
| PL272025A1 (en) | 1989-03-06 |
| BG49825A3 (en) | 1992-02-14 |
| CS274462B2 (en) | 1991-04-11 |
| EP0283055A3 (en) | 1989-03-15 |
| EP0283055B1 (en) | 1990-08-29 |
| EP0283055A2 (en) | 1988-09-21 |
| RU2007398C1 (ru) | 1994-02-15 |
| CS253388A2 (en) | 1990-09-12 |
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