CN102482266A - 环状叠氮基钠通道阻断剂 - Google Patents
环状叠氮基钠通道阻断剂 Download PDFInfo
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- CN102482266A CN102482266A CN2010800308012A CN201080030801A CN102482266A CN 102482266 A CN102482266 A CN 102482266A CN 2010800308012 A CN2010800308012 A CN 2010800308012A CN 201080030801 A CN201080030801 A CN 201080030801A CN 102482266 A CN102482266 A CN 102482266A
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Landscapes
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- Plural Heterocyclic Compounds (AREA)
Abstract
本发明涉及具有钠通道阻断性的三嗪化合物,和涉及所述化合物用于制备治疗相关疾病的药物的用途。所述三嗪化合物为式(I)的化合物或其盐,其中:R1为氢或取代基;R2为氨基或取代基;当R1为氢时N*为氨基或者或当R1为取代基时N*为=NH;R3和R4均为碳环、杂环或烷基,且可以相同或不同;和R5为氢、烷基或环芳基,条件是:当R3和R4均为烷基时,它们连接形成环烷基,以及R5为环状芳族基团;和当R3和R4均为碳环或杂环基时,R5为氢或烷基。
Description
技术领域
本发明涉及具有钠通道阻断性的三嗪化合物,以及涉及所述化合物用于制备治疗相关疾病的药物的用途。
背景技术
美国专利4,649,139公开了式(A)的化合物:
其中R1为C1-10烷基、C2-10烯基、C2-10炔基或C3-10环烷基,任何这些可以任选取代,和R2至R6独立地选自氢、卤素、C1-6烷基、烯基、炔基或烷氧基(全部任选由一个或多个卤素、羟基和芳基取代)、氨基、单-或二-取代氨基、烯氧基、酰基、酰氧基、氰基、硝基、芳基和硫代烷基,或者连接R2至R6任何邻接的两个从而形成(-CH=CH-CH=CH-)基团。公开了这些化合物在治疗心脏疾病方面是积极的,以及在治疗心律失常方面是特别有用的。
我们的在先专利申请WO2008/007149公开了式(B)的化合物的用途:
其中R1为氢(和=NH为NH2),或羧酰氨基、C1-10烷基、C2-10烯基、C1-3烷基-芳基、C1-3烷基-杂环基或C3-10环烷基,任何这些可以任选由羟基、卤素、羧酰氨基、卤代C1-6烷基、C1-6烷基或C1-6烷氧基取代;和R2至R6独立地选自氢、卤素、C1-6烷基、烯基、炔基或烷氧基(全部任选由一个或多个卤素、羟基和芳基取代)、氨基、单-或二-取代氨基、烯氧基、酰基、酰氧基、氰基、硝基、芳基和硫代烷基;
(a)作为电压依赖性钠通道阻断剂(voltage-dependent sodiumchannel blocker),用于治疗哺乳动物尤其是人类的疾病,特别地癫痫症、多发性硬化症、青光眼和葡萄膜炎(uevitis)、脑外伤和脑缺血、中风、头颅损伤、脊髓损伤、手术创伤、神经退行性疾病、运动神经元病、阿兹海默症、帕金森病、慢性炎症性疼痛、神经性疼痛、偏头疼、躁郁症、情绪病、焦虑症和认知障碍、精神分裂症和三叉自主神经性头痛;
(b)作为抗叶酸剂(antifolates),用于治疗哺乳动物尤其是人类的疾病,特别地用于治疗哺乳动物癌症,和作为针对间日疟原虫和恶性疟原虫疟疾的抗疟药。
发明内容
本发明提供一种式(I)的化合物,
其中:
R1为氢或取代基;
R2为氨基或取代基;
当R1为氢时N*为氨基或者或当R1为取代基时N*为=NH;
R3和R4均为碳环、杂环或烷基;和
R5为氢、烷基或环芳基,条件是:当R3和R4均为烷基时,它们连接形成环烷基,以及R5为芳族基团或脂环族基团;和当R3和R4均为碳环或杂环基时,R5为氢、烷基或芳族基团。
优选地,R3和R4为芳族碳环或芳族杂环,以及R5为氢。
适合地,R3和R4均为烷基,并连接形成环丙基、环丁基、环戊基或环己基。
适合地,R3、R4或R5选自任选例如由卤素或烷氧基取代的甲基、乙基、丙基和丁基。
任选地,R1为羧酰氨基、C1-10烷基、C2-10烯基、C1-3烷基-芳基、C1-3烷基-杂环基或C3-10环烷基,任何这些任选由羟基、卤素、羧酰氨基、卤代C1-6烷基、C1-6烷基或C1-6烷氧基取代的。
适合地,R1为未取代C1-6烷基,典型地甲基、乙基、异丙基、正丙基、异丁基或正丁基,其任选由羟基或卤素如氯、溴或氟取代。
可选择地,R1为任选由1个或多个卤素如氯、溴或氟取代的C1-10卤代烷基,优选甲基、乙基、异丙基、正丙基、异丁基或正丁基。优选的取代基为二卤代或三卤代(尤其是氯代和/或氟代)。
可选择地,R1为未取代的C2-6烯基,如烯丙基;C3-10环烷基,如环己基;C1-3烷基芳基,如苄基;其任选由1个或多个卤素、卤代烷基或烷氧基如氯、氟、三氟甲基、三氟甲氧基、甲氧基或乙氧基取代。
可选择地,R1为C1-3烷基杂环基,如任选N-取代的哌啶基-甲基,或噻吩基-甲基或呋喃基-甲基。
典型地,1个或多个R3、R4和R5为碳环环系统,如苯基。可以存在R3、R4和R5的任选取代基,如卤素(氯、氟、溴)和烷氧基,如甲氧基。
在式(1)的化合物组中,R3、R4和R5中至少之一为杂环环系统,如具有1个或多个氧或硫或氮原子的单环或双环杂环,尤其是芳族杂环环系统。在优选的实施方案中,R3=R4。
适合地,杂环基团为:i)选自噻吩基和苯并噻吩基的含硫杂环基;ii)选自呋喃基、苯基呋喃基和苯并吡喃基的含氧杂环基;或选自吡啶基、吲哚基、喹啉基、异喹啉基的含氮杂环基。有利地,关于上述结构,关于碳环A环,例如由卤素、烷基或烷氧基,尤其是由1、2或3个氯或溴原子取代。含氮杂环任选由烷基如甲基N-取代,或者由苯氧基或硫代苯基取代,其中苯基任选由卤素如氯取代。
本发明还提供任何上述化合物的盐。优选的盐为药学上可接受的酸加成盐(addition salt)。适合的药学上可接受的酸加成盐包括用有机酸和无机酸二者形成的那些,所述有机酸和无机酸例如由盐酸、硫酸、柠檬酸、酒石酸、磷酸、乳酸、丙酮酸(pyruvic)、乙酸、丙二酸、琥珀酸、草酸、富马酸、马来酸、草酰乙酸、甲磺酸、对甲苯磺酸、苯磺酸、谷氨酸、萘甲酸和羟乙基磺酸。乙磺酸盐、苹果酸盐、扁桃体酸盐、安息香酸盐和水杨酸盐也是适合的。
本发明还提供任何式(I)的化合物或其盐的溶剂化物。所述化合物或其盐可以作为反应溶剂或结晶溶剂或其组分的溶剂化物以所述化合物制剂而得到。适合的药学上可接受的溶剂化物包括水合物。
式(I)的化合物可具有手性中心且可以作为外消旋酸盐、外消旋混合物和作为个别对映体或非对映异构体出现。所有此类同质异构形式包括在本发明的范围中。本发明的范围内还包括无论是作为个别异构体或其混合物的所有式(I)的化合物的几何异构体。因而,反式-和顺式-构造中的式(I)的化合物涵盖在本发明中;互变异构形式及其混合物,和多形态的结晶形式也涵盖在本发明中。
特定式(I)的化合物可以通过上述美国专利4,649,139中公开的工艺制备,在此将其全部公开内容引入以作参考且应进一步参考。特定式(I)的化合物也可以通过EP0021121A中公开的方法制备,在此将其全部公开内容引入以作参考且应进一步参考。
上述具体化合物的制备在本说明书中稍后示出。本发明的范围内的相关化合物可以通过公开工艺的显而易见或常规变化使用适当的原料从而引入式(I)范围内的化合物的期望的取代基和部分来制备。
式(I)的化合物的盐可以通过在制备工艺中残余酸的存在而获得。可选择的盐可以通过在适合的溶剂中将式(I)的化合物作为游离碱与药学上可接受的酸混合并除去溶剂从而回收盐或者从溶剂中使盐结晶而制备。
在另一个方面中,本发明提供一种药物组合物,其包括与药学上可接受载体混合的式(I)的化合物或其药学上可接受的盐或溶剂化物。所述化合物适合用于治疗疾病如癫痫症、多发性硬化症、青光眼和葡萄膜炎、脑外伤和脑缺血、中风、头颅损伤、脊髓损伤、手术创伤、神经退行性疾病、运动神经元病、阿兹海默症、帕金森病、慢性炎症性疼痛、神经性疼痛、偏头疼、躁郁症、情绪病、焦虑症和认知障碍、精神分裂症和三叉自主神经性头痛;用于治疗哺乳动物癌症;和用于治疗疟疾。
式(I)的化合物以有效单位剂量的形式即以足以有效针对活体内疾病的量存在于本发明的组合物中。
本发明的组合物中存在的药学上可接受的载体可以是常规用于将药物给药目的的材料。这些可以是液体或固体材料,另外是惰性或医学上可接受的以及与活性成分相容的。
这些药物组合物可以经口或不经肠胃例如作为栓剂、药膏、乳霜、粉剂或皮肤贴剂给药。然而,优选口服给药和静脉注射该组合物。
对于口服给药,细粉或粒剂包含稀释剂、分散剂和/或表面活性剂,并且可以存在于药水(draught)中、水或糖浆中,以干状态或以其中包括悬浮剂的非水性悬浮液或者以在水或糖浆中的悬浮液形式存在胶囊或小袋(sachets)中。如果期望或需要可以包括调味剂、防腐剂(preserving agent)、悬浮剂或增稠剂。可以压缩干粉末或粒剂从而形成片剂或被容纳在胶囊中。
对于注射,所述化合物可以存在于可包含抗氧化剂或缓冲剂的消毒水注射液中。
游离碱或者其盐或溶剂化物也可以以其不与其它添加剂结合的纯净形式给药,在该情况下,胶囊或小袋是优选的载体。
可选择地,活性化合物以有效单位剂量的纯形式例如被压缩为片剂等存在。
可包括的其它化合物例如为,药物惰性的成分,如固体和液体稀释剂例如用于片剂或胶囊的乳糖、淀粉或磷酸钙;用于软胶囊的橄榄油或油酸乙酯;和用于悬浮液或乳液的水或植物油;润滑剂如滑石或硬脂酸镁;胶凝剂如胶质粘土;增稠剂如黄蓍胶或海藻酸钠;和其它治疗上可接受的助剂如湿润剂、防腐剂、缓冲剂和抗氧化剂,在此类配方中这些可用作载体。
以单独单元提供的片剂或其它存在形式可以方便地包含在此剂量下有效的量的或作为该剂量的多倍有效的量的式I化合物,例如所述单元包含5mg-500mg、通常在约10mg-250mg。
本发明的药物组合物可以通过式(I)的化合物与药学上可接受载体的混合而制备。如有必要可以混合常规的药学赋形剂。适合的配方的实例在上述美国专利4,649,139中给出。
本发明提供通过将无毒有效量的式(I)的化合物或者其药学上可接受的盐或溶剂化物,或者如上文中定义的组合物给药的治疗方法。所述方法特别适合于治疗易受到钠通道阻断剂和抗叶酸剂影响的哺乳动物的疾病,特别是疾病如癫痫症、多发性硬化症、青光眼和葡萄膜炎、脑外伤和脑缺血、中风、头颅损伤、脊髓损伤、手术创伤、神经退行性疾病、运动神经元病、阿兹海默症、帕金森病、慢性炎症性疼痛、神经性疼痛、偏头疼、躁郁症、情绪病、焦虑症和认知障碍、精神分裂症和三叉自主神经性头痛;适合于治疗哺乳动物癌症;和适合于治疗疟疾。
本发明还提供式(I)的化合物或者其药学上可接受的盐或溶剂化物,或者如上文中定义的组合物,其用于药物的制备。所述药物特别适合于治疗易受到钠通道阻断剂和抗叶酸剂影响的哺乳动物的疾病,特别是疾病如癫痫症、多发性硬化症、青光眼和葡萄膜炎、脑外伤和脑缺血、中风、头颅损伤、脊髓损伤、手术创伤、神经退行性疾病、运动神经元病、阿兹海默症、帕金森病、慢性炎症性疼痛、神经性疼痛、偏头疼、躁郁症、情绪病、焦虑症和认知障碍、精神分裂症和三叉自主神经性头痛;用于治疗哺乳动物癌症;和用于治疗疟疾。
如上所示,式(I)的化合物通常通过口服或静脉注射用于治疗此类疾病。
式(I)的化合物通常以每日0.01mg/kg-20mg/kg、优选每日0.1-5.0mg/kg的剂量给药。
鉴于结构上类似的化合物如拉莫三嗪和在式(I)范围内的其它已知化合物在人类中的已知应用,在式(I)的化合物的应用中预期没有大的毒性问题。然而,在临床应用前应进行合适的试验工序。
具体实施方式
本发明的上述和其它方面现在将参考所附实施例进一步详细地解释。
以下报道式(I)的示例性化合物和用于试验的其它化合物的制备的方法学。这可以适合于制备具有此处提及的另外或可替换的取代基或部分的类似化合物。
在以下工艺中,所有熔点的单位为℃。
一般工艺
6-烷基/芳烷基-3,5-二氨基-1,2,4-三嗪化合物
氯化三苯乙烷[3;R1=R2=R3=Ph]
将三苯基乙酸(21.7g;0.075mol)和干燥二甲基甲酰胺(2滴)在干燥二氯甲烷(100cm3)中的搅拌混合物经~25分钟用以大约四等分添加的草酰氯(14g;0.11mol)处理。将混合物在35°下搅拌直至氯化氢的散发终止(~4小时)。将所得无色溶液在真空中在40°下蒸发至恒重从而得到作为无色结晶固体的标题化合物。产量=23.24g(100.0%)。将该产物直接用于下一阶段。
类似的制备如下:
氰化三苯乙烷[4;R1=R2=R3=Ph]
将氰化三苯乙烷(23.24g;0.075mol)、干燥甲苯(40cm3)、干燥乙腈(10cm3)、氰化铜I(9.20g;0.103mol)、C盐(3.5g)和微细粉碎的碘化钾(2g)良好搅拌的混合物[桨式搅拌器]在回流下加热直至没有残留酸式氯化物(~18小时)。将暗色反应混合物冷却至~75°并用甲苯(150cm3)稀释。搅拌额外的~30分钟之后,将所得浆料通过层析硅胶(~2.5cm)床过滤,和无色滤出液在真空下蒸发至恒重从而得到作为无色固体的标题化合物。产量=21.97g(98.7%),Mpt=67-69°。将该产物直接用于下一阶段。
希夫碱,氰基腙,[4;R1=R2=R3=Ph]
向氨基胍二甲磺酸盐(15.00g;0.0564mol)在99.5%甲磺酸(22.5g)中在65-70°下的搅拌溶液中经~25分钟逐滴添加氰化三苯乙烷(8.91g;0.030mol)在乙腈(25cm3)中的溶液。然后将混合物在68°下搅拌直至样品得到在水中的清澈溶液(~28小时),然后灌入粉碎的冰/水(150g)得到半固体无色沉淀物。将混合物用48%氢氧化钠(17.5cm3)中和(pH8-9)得到作为乳状颗粒固体的标题化合物。将产物过滤,用水洗涤和在真空下在45°下干燥。产量=8.47g(80.0%),Mpt=112-114°,TLC[SiO2板,10%在氯仿中的甲醇],Rf=0.68。将该产物直接用于下一阶段。
三嗪化合物
生物试验
式(VII)的化合物如下测试各种活性:
筛查策略
设计筛查策略从而以适当的钠通道阻断活性和低副作用倾向性来选择化合物。为此,所有化合物通过一次钠通道分析(藜芦碱诱发的摄取[14C]胍至大鼠前脑突触体)和由产生的浓度-效应曲线计算的IC50值处理。为了补充该数据,还测量用于选择的化合物以抑制[3H]BTX-B的结合(binding of[3H]BTX-B)的IC50。
先前的研究已经显示取代的三嗪为潜在的二氢叶酸还原酶(DiHydroFolate Reductase)(DHFR)活性的抑制剂(McCullough和Bertino 1971;Cashmore等,1975;Booth等,1987和Sapse等,1994)。DHFR的抑制剂(如甲氨喋呤)已经用于治疗各种癌症(Suster等,1978和Niculescu-Duvaz等,1982),因为该酶的抑制干扰细胞生长,但由于该效果(在细胞生长方面)DHFR的抑制剂也会致畸(Skalko和Gold,1974;Feldcamp和Carey,1993和Buckley等,1997)。应发现作为潜在的DHFR的抑制剂的化合物,然后此类化合物它们自身可以具有作为抗癌试剂的潜力。几种方法可用于测量DHFR活性的抑制,为了该研究,我们已经调查了化合物抑制[3H]甲氨蝶呤的结合的效果(Myers等,1975和Rothenberg等,1977)。
另外的共同副作用标记为由于通过长期QT综合症的发展引起的心脏衰竭会致命的人类Ether-a-go-go相关基因(humanEther-a-go-go Related Gene)钾(hERG)钾通道(内向整流性,IKr)活性的抑制。评价影响该通道潜力的可用初步筛查通过测量[3H]阿司咪唑(astemizole)对表现hERG的细胞膜的结合的抑制来评价。选择的化合物通过测量在10μM下的抑制而测试该活性。如果抑制值位于10%和90%之间,可以计算各化合物的外推IC50。
上述筛查级联鉴定具有低的(较低的)前述副作用倾向性倾向的具有适当钠通道阻断活性的化合物。为了进一步开发这些化合物,需要它们药效动力学性质的一些知识。
钠通道阻断剂如西帕曲近(Sipatrigine)(在大鼠中大脑中动脉阻塞后既降低神经功能缺损又减少梗死体积)(Smith等,1997)和苯妥英(phenytoin)(保护青光眼的实验模型中视网膜神经节细胞死亡)(Hains和Waxman,2005)在神经退化的模型范围中显示神经保护功效。由于氧供给的失败使糖酵解和氧化磷酸化妥协,因此缺血性损伤最终导致电气失败(神经信号)和泵浦失败(细胞膜电位的还原)。这些失败(电气和离子泵浦活性的)与ATP降低的局部浓度相关(Astrup等1981)。因而,使用所述化合物在严重代谢刺激之后维持在大鼠海马0.4mm切片中的ATP浓度的效果。
实验工序
大鼠前脑突触体和匀浆的制备
实验使用重175-250g的雄性维斯塔(Wistar)大鼠的前脑(全脑,较少小脑/髓质)进行。进行所有努力以减少使用动物的数量,和所有实验根据1986年英国动物(科学程序法)法案和欧洲共同体理事会1986年11月24日指示(86/609/EEC)进行。使动物昏倒后杀死和斩首,将前脑(全脑,较少小脑/髓质)快速切开并转移至含冰冷却的0.25M蔗糖的称重管。
突触体(重和轻的包含突触体的线粒体部分)通过以下制备:通过转移前脑(已知的湿重量)至已添加9体积冰冷却的0.25M蔗糖的玻璃波特(Potter)容器,并通过设定至900rpm的布朗波特(Braun Potter)S马达驱动的匀浆器的8次′上下击打′使用特氟隆杵来匀浆化。将所得匀浆在4°下在1036×g时离心10分钟并收集上清液。如上所述,将残余颗粒在新鲜冰冷却的0.25M蔗糖中再悬浮并重复离心步骤。将上清液部分汇集并在4°下在40,000×g(平均)时离心15分钟,并将所得颗粒在以每ml适当分析缓冲液为20-25mg湿重的浓度的适当分析缓冲液中再悬浮。
匀浆通过转移已知重量的前脑至包含9体积冰冷却的50mM pH7.4HEPES缓冲液的冷却的管中制备。将混合物在4°下通过设定至最大速度的Ultra-TurraxTM匀浆器的3×5sec爆破(bursts)匀浆化。将所得匀浆在4°下在40,000×g(平均)时离心15分钟并弃用上清液。将所得颗粒在9体积新鲜冰冷却的pH7.4缓冲液中再悬浮(同上),重复离心步骤,并将所得颗粒在以每ml分析缓冲液为20-25mg湿重的浓度在[3H]BTX-B结合缓冲液中再悬浮。
[14C]胍通量和[3H]BTX-B的结合
两种分析均使用添加在试验中浓度范围内的化合物的14ml聚丙烯试管进行。将试验化合物溶解于DMSO中并添加至分析液以致DMSO的最大浓度不超过2%v/v。
[14C]胍通量:
除了在30°下进行2 1/2分钟以外,[14C]胍通量分析使用Pauwels PJ等(1986)的方法测量。
参考:
Pauwels PJ,Leysen JE,Laduron PM.[3H]Batrachotoxinin A20-alpha-benzoate binding to sodium channels in rat brain:characterization and pharmacological significance.Eur JPharmacol.1986年5月27日;124(3):291-8。
[3H]BTX-B的结合
除了两种牛血清白蛋白和TTX从温育介质中略去以外,[3H]BTX-B结合使用由Catterall等(1981)描述的方法进行。将试验化合物溶解于DMSO中并添加至分析液以致DMSO的最大浓度不超过2%v/v。
参考:
Catterall WA,Morrow CS,Daly JW,Brown GB.Binding ofbatrachotoxinin A 20-alpha-benzoate to a receptor site associatedwith sodium channels in synaptic nerve ending particles.J Bio.Chem.1981年9月10日;256(17):8922-7。
[3H]甲氨蝶呤的结合
所有步骤在4°下(或冰上)进行。将新切开的大鼠肝脏切开至0.25M冰冷却的蔗糖中,随后在含15mM二硫苏糖醇的50mMpH6.0磷酸缓冲液(10ml/g组织)中匀浆化(U-turrax)。将所得匀浆在47,500×g下离心20分钟并将上清液(通过脱脂棉过滤从而去除脂肪块)在使用前贮存在-80°下(Rothenberg等)。
[3H]甲氨蝶呤对大鼠肝脏匀浆上清液部分的结合的抑制大致如Arons等,1975描述的进行。计算结果作为由浓度-效应曲线衍生的IC50值(见下文)或作为通过对照和冷的甲氨蝶呤(10μM最终浓度)结合值的比较确定的抑制百分率值。
参考:
Elliot Arons,Sheldon P.Rothenberg,Maria da Costa,CraigFischer and M.Perwaiz Iqbal;Cancer 30Research 35,1975年8月1日,2033-2038。
IC50值的计算
IC50值通过绘制log10浓度与结合的配体/摄取的胍由放射性配体取代或胍通量抑制曲线根据以下等式获得:-
y=Rmin+Rsp/{1+exp[-n(x-C)]}
其中y=结合量(bound)(dpm)
x=log10化合物浓度
Rmin=下渐近线(即,100%抑制)
Rsp=上渐近线-Rmin(即,特定结合)
n=斜率(loge)
和C=IC50(即,抑制50%特定结合所需的浓度)。
海马切片分析
除了使用碘乙酸盐(400μM)2作为代谢刺激以外,神经保护功效在大鼠海马0.4mm切片中使用由Fowler和Li(1998)1描述的方法测量。化合物(通常30μM)总是直接与河豚毒素(1μM)3比较它们在抑制糖酵解之后维持ATP的切片浓度的能力。
参考:
1.Fowler J C,Li Y.Contributions of Na flux and the anoxicdepolarization to adenosine 5′-triphosphate levels inhypoxic/hypoglycemic rat hippocampal slices.Neuroscience 1998,83,717-722。
2.Reiner PB,Laycock AG,Doll CJ.A pharmacologicalmodel of ischemia in the hippocampal slice.Neurosci Lett 1990;119:175-8。
3.Boening JA,Kass IS,Cottrell JE,Chambers G.The effectof blocking sodium influx on anoxic damage in the rathippocampal slice.Neuroscience.1989.卷33(2),263-268。
ATP和蛋白质的测量
个别切片通过超声处理分裂,将所得匀浆在4°下在10,000×g时离心5分钟。将上清液导入新鲜管中并将任何残余上清液通过真空吸引术去除。将颗粒通过超声处理在0.5ml 0.1MKOH中再悬浮,并将所得悬浮液在温和振荡时在37°下加温30分钟。
ATP的浓度通过与荧光素酶试剂(Perkin Elmer的ATPLite)混合和测量在96-孔板计数器中随后的发光在6μl上清液中来测量。
蛋白质浓度使用BCATM蛋白质分析(Pierce)与牛血清白蛋白作为参考标准测量。
ATP浓度表示为nmol/mg蛋白质和通过与1μM TTX的效果直接比较计算的神经保护指标(%保护)。
hERG:
将化合物送至MDS Pharma以测量它们在10μM浓度下抑制[3H]阿司咪唑对表现人类重组(recombinant)hERG的HEK-293细胞的结合。假设结合斜率为1.0,对于表示由5%和95%之间的结合抑制的化合物,可计算IC50值(见上文)。
L-型钙通道
将化合物送至MDS Pharma以测量它们在10μM浓度下抑制[3H]尼群地平(nitrendipine)对大鼠脑皮质膜的结合。假设结合斜率为1.0,可计算IC50值(见上文)用于表示由5%和95%之间的结合抑制的化合物。
大鼠微粒体稳定性
将化合物送至BioFocus以测量它们在1μM浓度下在与大鼠肝脏微粒体在37°下温育40分钟之后的稳定性。
关于本发明代表性化合物获得的筛查数据指出通式(I)的化合物用于以下的适宜性:治疗易受到钠通道阻断剂和抗叶酸剂影响的哺乳动物的疾病,特别是疾病如癫痫症、多发性硬化症、青光眼和葡萄膜炎、脑外伤和脑缺血、中风、头颅损伤、脊髓损伤、手术创伤、神经退行性疾病、运动神经元病、阿兹海默症、帕金森病、慢性炎症性疼痛、神经性疼痛、偏头疼、躁郁症、情绪病、焦虑症和认知障碍、精神分裂症和三叉自主神经性头痛;治疗哺乳动物癌症;和治疗疟疾。
由各种工序得到的数据示于下表:
(CEN-001)使用相同酶制剂在125μM下的拉莫三嗪结果给出26%抑制。
Claims (22)
1.一种式(I)的化合物或其盐,
其中:
R1为氢或取代基;
R2为氨基或取代基;
当R1为氢时N*为氨基或者或当R1为取代基时N*为=NH;
R3和R4均为碳环、杂环或烷基,且可以相同或不同;和
R5为氢、烷基或环芳基,条件是:当R3和R4均为烷基时,它们连接形成环烷基,以及R5为芳族基团或脂环族基团;和当R3和R4均为碳环或杂环基时,R5为氢、烷基或芳族基团。
2.根据权利要求1所述的化合物,其中R3和R4为芳族碳环或芳族杂环,以及R5为氢。
3.根据权利要求1所述的化合物,其中R3和R4均为烷基,并连接形成环丙基、环丁基、环戊基或环己基。
4.根据权利要求1所述的化合物,其中R3、R4或R5的烷基选自任选例如由卤素或烷氧基取代的甲基、乙基、丙基和丁基。
5.根据权利要求1所述的化合物,其中R3、R4和R5中至少之一为任选例如由一个或多个卤素和/或烷氧基取代的碳环环系统,如苯基。
6.根据权利要求1所述的化合物,其中R3、R4和R5中至少之一为杂环环系统,如具有1个或多个氧或硫或氮原子的单环或双环杂环,优选芳族杂环环系统。
7.根据权利要求6所述的化合物,其中R3=R4。
8.根据权利要求6或7所述的化合物,其中所述杂环环系统选自:
i)任选例如由卤素、烷基或烷氧基取代的噻吩基和苯并噻吩基;
ii)任选例如由卤素、烷基或烷氧基取代的呋喃基、苯基呋喃基和苯并吡喃基;和/或
iii)任选例如由卤素、烷基或烷氧基取代的吡啶基、吲哚基、喹啉基、异喹啉基,特别地如氯吡啶基和二氯吡啶基,任选由烷基如甲基N-取代的吡啶基、吲哚基、喹啉基、异喹啉基,或由苯氧基或硫代苯基取代的吡啶基、吲哚基、喹啉基、异喹啉基,其中苯基任选由卤素取代。
9.根据权利要求1-8任一项所述的化合物,其中R1为任选由羟基、卤素、羧酰氨基、卤代C1-6烷基、C1-6烷基或C1-6烷氧基取代的羧酰氨基、C1-10烷基、C2-10烯基、C1-3烷基-芳基、C1-3烷基-杂环基或C3-10环烷基。
10.根据权利要求9所述的化合物,其中R1为任选由羟基或卤素取代的C1-6烷基,如甲基、乙基、异丙基、正丙基、异丁基或正丁基。
11.根据权利要求9所述的化合物,其中R1为C1-10卤代烷基。
12.根据权利要求11所述的化合物,其中R1典型地为由1个或多个卤素取代的甲基、乙基、异丙基、正丙基、异丁基或正丁基。
13.根据权利要求11或12所述的化合物,其中R1为二卤代或三卤代取代的。
14.根据权利要求9所述的化合物,其中R1为未取代的C2-6烯基,如烯丙基。
15.根据权利要求9所述的化合物,其中R1为任选由1个或多个卤素、卤代烷基或烷氧基如氯、氟、三氟甲基、甲氧基或乙氧基取代的环己基。
16.根据权利要求9所述的化合物,其中R1为苄基,其中所述苯基任选由1个或多个卤素、卤代烷基或烷氧基如氯、氟、三氟甲基、三氟甲氧基、甲氧基或乙氧基取代。
17.根据权利要求9所述的化合物,其中R1为任选N-取代的哌啶基-甲基,或噻吩基-甲基或呋喃基-甲基。
18.根据权利要求1所述的化合物,其中所述化合物选自:
19.一种药物组合物,其包括与药学上可接受载体混合的根据权利要求1-18任一项所述的化合物或者其药学上可接受的盐或溶剂化物。
20.根据权利要求19所述的药物组合物,其用于治疗易受到钠通道阻断剂和抗叶酸剂影响的哺乳动物的疾病,包括癫痫症、多发性硬化症、青光眼和葡萄膜炎、脑外伤和脑缺血、中风、头颅损伤、脊髓损伤、手术创伤、神经退行性疾病、运动神经元病、阿兹海默症、帕金森病、慢性炎症性疼痛、神经性疼痛、偏头疼、躁郁症、情绪病、焦虑症和认知障碍、精神分裂症和三叉自主神经性头痛;用于治疗哺乳动物癌症;或用于治疗疟疾。
21.根据权利要求1-18任一项所述的化合物或其药学上可接受的盐或溶剂化物,或者根据权利要求19或20所述的组合物,其用于治疗以下疾病,或其用于制备治疗以下疾病的药物,所述疾病为易受到钠通道阻断剂和抗叶酸剂影响的哺乳动物的疾病,特别是疾病如癫痫症、多发性硬化症、青光眼和葡萄膜炎、脑外伤和脑缺血、中风、头颅损伤、脊髓损伤、手术创伤、神经退行性疾病、运动神经元病、阿兹海默症、帕金森病、慢性炎症性疼痛、神经性疼痛、偏头疼、躁郁症、情绪病、焦虑症和认知障碍、精神分裂症和三叉自主神经性头痛;哺乳动物癌症;或疟疾。
22.根据权利要求1-18任一项所述的化合物或其药学上可接受的盐或溶剂化物,或者根据权利要求19或20所述的组合物用于治疗以下疾病或用于制备治疗以下疾病的药物的用途,所述疾病为易受到钠通道阻断剂和抗叶酸剂影响的哺乳动物的疾病,特别是疾病如癫痫症、多发性硬化症、青光眼和葡萄膜炎、脑外伤和脑缺血、中风、头颅损伤、脊髓损伤、手术创伤、神经退行性疾病、运动神经元病、阿兹海默症、帕金森病、慢性炎症性疼痛、神经性疼痛、偏头疼、躁郁症、情绪病、焦虑症和认知障碍、精神分裂症和三叉自主神经性头痛;哺乳动物癌症;或疟疾。
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2009
- 2009-07-08 GB GB0911993A patent/GB2471713A/en not_active Withdrawn
-
2010
- 2010-07-08 ES ES10732408.9T patent/ES2550052T3/es active Active
- 2010-07-08 WO PCT/GB2010/051127 patent/WO2011004196A1/en active Application Filing
- 2010-07-08 EP EP10732408.9A patent/EP2451807B1/en not_active Not-in-force
- 2010-07-08 IN IN871DEN2012 patent/IN2012DN00871A/en unknown
- 2010-07-08 CN CN201080030801.2A patent/CN102482266B/zh not_active Expired - Fee Related
- 2010-07-08 JP JP2012519066A patent/JP5847079B2/ja active Active
- 2010-07-08 AU AU2010269982A patent/AU2010269982B2/en not_active Ceased
- 2010-07-08 US US13/382,741 patent/US8748600B2/en active Active
- 2010-07-08 KR KR1020127002940A patent/KR20120048593A/ko not_active Application Discontinuation
- 2010-07-08 CA CA2767298A patent/CA2767298A1/en not_active Abandoned
-
2012
- 2012-01-02 IL IL217330A patent/IL217330B/en not_active IP Right Cessation
Patent Citations (5)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US3637688A (en) * | 1970-01-09 | 1972-01-25 | American Home Prod | 6-(fluoro and trifluoromethyl phenyl)-3 5-diamino - 1 2 4 - triazines and substituted - 6 - phenylalkyl-3,5-diamino-1 2 4-triazines |
| EP0021121B1 (en) * | 1979-06-01 | 1983-05-11 | The Wellcome Foundation Limited | 1,2,4-triazine derivatives, process for preparing such compounds and pharmaceutical compositions containing them |
| WO2003008393A1 (de) * | 2001-07-17 | 2003-01-30 | Helm Ag | Verfahren zur herstellung von lamotrigin aus alpha-oxo-2,3-dichlorphenylacetamidino-aminoguanidino-hydrazon durch ringschlussreaktion |
| WO2009090431A1 (en) * | 2008-01-16 | 2009-07-23 | University Of Greenwich | Cyclic triazo and diazo sodium channel blockers |
| CN101918378A (zh) * | 2008-01-16 | 2010-12-15 | 格林威治大学 | 环状叠氮和重氮钠通道阻滞剂 |
Also Published As
| Publication number | Publication date |
|---|---|
| AU2010269982B2 (en) | 2015-05-14 |
| CA2767298A1 (en) | 2011-01-13 |
| AU2010269982A1 (en) | 2012-02-16 |
| JP2012532858A (ja) | 2012-12-20 |
| EP2451807B1 (en) | 2015-09-02 |
| JP5847079B2 (ja) | 2016-01-20 |
| US8748600B2 (en) | 2014-06-10 |
| US20120135993A1 (en) | 2012-05-31 |
| IN2012DN00871A (zh) | 2015-07-10 |
| GB0911993D0 (en) | 2009-08-19 |
| ES2550052T3 (es) | 2015-11-04 |
| WO2011004196A1 (en) | 2011-01-13 |
| CN102482266B (zh) | 2015-07-08 |
| KR20120048593A (ko) | 2012-05-15 |
| GB2471713A (en) | 2011-01-12 |
| IL217330B (en) | 2018-12-31 |
| IL217330A0 (en) | 2012-02-29 |
| EP2451807A1 (en) | 2012-05-16 |
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