TWI436995B - 作為5-ht6受體拮抗劑之經取代之6-(1-六氫吡基)-嗒類 - Google Patents
作為5-ht6受體拮抗劑之經取代之6-(1-六氫吡基)-嗒類 Download PDFInfo
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- TWI436995B TWI436995B TW098122349A TW98122349A TWI436995B TW I436995 B TWI436995 B TW I436995B TW 098122349 A TW098122349 A TW 098122349A TW 98122349 A TW98122349 A TW 98122349A TW I436995 B TWI436995 B TW I436995B
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Description
本發明關於具有5-HT6
-拮抗性質的新穎經取代之6-(1-六氫吡基)-嗒類。本發明進一步關於製備此等新穎化合物之方法,包含該新穎化合物作為活性成分之醫藥組成物,以及該化合物作為藥劑之用途。
WO-2003/066604尤其關於具有組織胺H3受體活性之3-芳基-6-六氫吡-1-基嗒類,其可用於治療嗜睡病。
5-羥基色胺受體6((5-HT6
)受體)屬於G-蛋白偶合受體家族且與刺激腺苷酸環化酶活性的G蛋白之Gs-家族,包括5-HT4
及5-HT7
受體偶合。5-HT6
受體亦顯現出調節麩胺能及膽鹼能神經元活性。5-HT6
受體選擇性地發現於涉及認知過程的腦部區域中。羥色胺5-HT6
的阻斷可能有利於較高的認知過程,諸如記憶及認為與精神分裂症有關聯的負面病徵時。事實上,許多臨床前數據顯示5-HT6
受體拮抗作用在囓齒類中具有正面認知過程效應(Mitchell and Neumaier(2005)5-HT6
receptors:a novel target for cognitive enhancement. Pharmacology & Therapeutics 108:320-333)。5-HT6
受體具有些微或不表現在末梢組織中,其可造成靶定藥物之選擇性,具有較少的副作用。
具有5-HT6
受體親和性之化合物通常更可進一步有用於治療各種中樞神經系統病症、焦慮症、抑鬱症、注意力不足過動障礙症、阿滋海默氏症(Alzheimer’s disease)、癲癇症及精神分裂症。
另外,5-HT6
拮抗作用亦與食慾及食物攝取抑制有關係。攝食症的盛行(像是例如肥胖症)使其成為所有年齡族群的公共健康問題。攝食症易感染各種嚴重的疾病,諸如糖尿病、胃腸道病症、心血管疾病、睡眠呼吸中止症及骨關節炎。5-HT6
受體引起作為發展新一代安全且更有效的減肥藥之分子標靶的極大興趣。
本發明的目的係提供為選擇性5-HT6
受體拮抗劑的新穎化合物,其具有與其他受體可忽略的交互作用,造成較少的副作用。本發明進一步關於此化合物之製備方法及包含此化合物之醫藥組成物。本發明亦關於這些衍生物用於製造供治療或預防認知障礙及食物相關病症之藥劑的用途。
本發明關於根據式(I)之新穎化合物:
及其立體異構物形式,其中R1
為氯基、三氟甲基或氰基;R2
為苯基或以鹵基取代之苯基;R3
為氫、C1-4
-烷基或吡啶基甲基;X為-O-、-NH-、-CH2
-、-CH(OH)-、-SO2
-、-CO-、-NH-CH2
-、-O-CH2
-、1,2-乙烯二基或乙炔二基;及其醫藥上可接受之加成鹽類與溶劑合物。
現將進一步敘述本發明。在下列的段落中更詳細定義本發明不同的觀點。如此定義的每一觀點可與任何其他觀點或觀點等組合,除非有對立的明確指示。特別地,任何指示為較佳或有利的特色可與任何指示為較佳或有利的其他特色組合。
例如,本發明關於式(I)化合物及其立體異構物形式,其中R1
為三氟甲基;R2
為苯基或以鹵基取代之苯基;R2
較佳為以鹵基取代之苯基;R3
為氫、C1-4
-烷基或吡啶基甲基;R3
較佳為氫、甲基或吡啶基甲基;X為-O-、-NH-、-CH2
-、-CH(OH)-、-SO2
-、-CO-、-NH-CH2
-、-O-CH2
-、1,2-乙烯二基或乙炔二基;及其醫藥上可接受之加成鹽類與溶劑合物。
本發明特別關於式(I)化合物及其立體異構物形式,其中R1
為三氟甲基;R2
為苯基或以氟基取代之苯基;R3
為氫、甲基或吡啶基甲基;X為-O-、-NH-、-CH2
-、-CH(OH)-、-SO2
-、-CO-、-NH-CH2
-、-O-CH2
-、1,2-乙烯二基或乙炔二基;及其醫藥上可接受之加成鹽類與溶劑合物。
在進一步的具體例中,本發明關於根據任何其他具體例的化合物,其中R2
為苯基或以一或多個選自由鹵基所組成之群組的取代基取代之苯基。
在進一步的具體例中,本發明關於根據任何其他具體例的化合物,其中R2
為苯基或以1、2或3個選自由鹵基所組成之群組的取代基取代之苯基。
在進一步的具體例中,本發明關於根據任何其他具體例的化合物,其中R2
為苯基或以一個鹵基取代之苯基。
在進一步的具體例中,本發明關於根據任何其他具體例的化合物,其中鹵基為氟基。
在式(I)化合物及其立體異構物形式之中,最有興趣者為例如:4-(4-氟苯氧基)-6-(1-六氫吡基)-3-(三氟甲基)-嗒,N
-(4-氟苯基)-6-(1-六氫吡基)-3-(三氟甲基)-4-嗒胺,4-(苯基甲基)-6-(1-六氫吡基)-3-(三氟甲基)-嗒,苯基[6-(1-六氫吡基)-3-(三氟甲基)-4-嗒基]-甲酮,α-苯基-6-(1-六氫吡基)-3-(三氟甲基)-4-嗒甲醇,4-(苯基磺醯基)-6-(1-六氫吡基)-3-(三氟甲基)-嗒,4-[(Z)-2-(4-氟苯基)乙烯基]-6-(1-六氫吡基)-3-(三氟甲基)-嗒,4-[(E)-2-(4-氟苯基)乙烯基]-6-(1-六氫吡基)-3-(三氟甲基)-嗒,4-[(4-氟苯基)乙炔基]-6-(1-六氫吡基)-3-(三氟甲基)-嗒,6-(4-甲基-1-六氫吡基)-4-[(E)-2-苯基乙烯基]-3-(三氟甲基)-嗒,[6-(4-甲基-1-六氫吡基)-3-(三氟甲基)-4-嗒基]苯基-甲酮,N
-[(4-氟苯基)甲基]-6-(1-六氫吡基)-3-(三氟甲基)-4-嗒胺,4-[(4-氟苯基)甲氧基]-6-(1-六氫吡基)-3-(三氟甲基)-嗒,4-[(E)-2-苯基乙烯基]-6-(1-六氫吡基)-3-(三氟甲基)-嗒,N
-(4-氟苯基)-6-(1-六氫吡基)-3-(三氟甲基)-4-嗒胺‧2.5HCl‧0.5H2
O,4-[(E)-2-苯基乙烯基]-6-[4-(4-吡啶基甲基)-1-六氫吡基]-3-(三氟甲基)-嗒,4-[(E)-2-苯基乙烯基]-6-[4-(2-吡啶基甲基)-1-六氫吡基]-3-(三氟甲基)-嗒,及其醫藥上可接受之加成鹽類與溶劑合物。
本發明化合物的化學名稱係根據Chemical Abstracts Service(CAS)承認的命名規則而產生。在互變異構物形式的例子,以所描述之結構的互變異構物形式產生名稱。然而,應明白其他未描述之互變異構物形式亦包括於本發明的範圍內。
在本發明的任何時候所使用之術語〝經取代〞意謂著表示在使用〝經取代〞之詞句中所指示之原子上的一或多個氫,較佳為從1至3個氫,更佳為1個氫以選自指示之基團置換,其先決條件係不超過指示之原子的正常價數,且取代作用得到化學上穩定的化合物,亦即足以完全從反應混合物分離而倖存為有用的純度且調配成治療劑的化合物。例如,當苯基以鹵基取代時,此意謂該苯基以一或多個選自鹵基之取代基取代。
在整個此申請案之中,術語〝C1-4
烷基〞定義具有1至4個碳原子之直鏈或支鏈不飽和烴基,諸如甲基、乙基、丙基、1-甲基乙基、丁基、1,1-二甲基乙基。作為基團或基團一部的術語鹵基一般為氟基、氯基、溴基及碘基,除非有來自上下文的另外指示或澄清。
當任何變體在任何成分中出現一次以上時,每一定義各自獨立。
醫藥上可接受之鹽類係經定義成包含以根據式(I)之化合物能夠形成在治療上有活性的無毒性酸加成鹽類形式。該鹽類可藉由以適當的酸類,例如無機酸類,例如氫鹵酸(特別為氫氯酸、氫溴酸)、硫酸、硝酸及磷酸;有機酸類,例如乙酸、羥基乙酸、丙酸、乳酸、特戊酸、草酸、丙二酸、丁二酸、順丁烯二酸、苦杏仁酸、反丁烯二酸、蘋果酸、酒石酸、檸檬酸、甲烷磺酸、乙烷磺酸、苯磺酸、對-甲苯磺酸、環己基胺基磺酸、柳酸、對-胺基柳酸、雙羥萘酸及苦杏仁酸處理根據式(I)之化合物的鹼形式而獲得。相反地,該鹽類形式可藉由以適當的鹼處理而轉換成游離形式。含有酸性質子的式(I)化合物亦可藉由以適當的有機及無機鹼處理而轉換成其無毒性金屬或胺加成鹽形式。適當的鹼鹽形式包含例如銨鹽類;鹼與鹼土金屬鹽類(例如,鋰、鈉、鉀、鎂、鈣鹽類及類似物);與有機鹼,例如一級、二級及三級脂族及芳族胺,諸如甲胺、乙胺、丙胺、異丙胺、四種丁胺異構物、二甲胺、二乙胺、二乙醇胺、二丙胺、二異丙胺、二-正丁胺、吡咯啶、六氫吡啶、嗎啉、三甲胺、三乙胺、三丙胺、奎寧環、吡啶、喹啉及異喹啉之鹽類;芐星(benzathine)、N-甲基-D-葡萄糖胺、哈胺(hydrabamine)鹽類;及與胺基酸,諸如精胺酸、離胺酸及類似物之鹽類。相反地,鹽形式可藉由以酸處理而轉換成游離酸形式。
術語溶劑合物包含以式(I)化合物能夠形成的水合物及溶劑加成形式,以及其鹽類。此形式之實例為例如水合物、醇化物及類似物。
應理解一些式(I)化合物及其醫藥上可接受之加成鹽類與立體異構物形式可含有一或多個對掌性中心且以立體異構物形式存在。
如上述所使用之術語〝立體異構物形式〞係定義式(I)化合物可具有的所有可能的異構物形式。除非有其他另外的說明或指示,化合物的化學名稱代表所有可能的立體異構物形式之混合物,該混合物含有基本分子結構的所有非鏡像異構物及鏡像異構物。更特別地,立體異構中心可具有R-或S-組態;在二價環狀(部分)飽和基上的取代基可具有順-或反-組態。包含雙鍵的化合物可具有在該雙鍵上的E或Z-立體化學性。式(I)化合物的立體異構物形式係包含在本發明的範圍內。
當指示特殊的立體異構物形式時,此意謂著該形式實質上為游離形式,亦即與少於50%,較佳為少於20%,更佳為少於10%,甚至更佳為少於5%,還更佳為少於2%,而最佳為少於1%之其他異構物聯結。
用於治療的式(I)化合物之鹽類為那些其中抗衡離子為醫藥上可接受之鹽類。然而,不為醫藥上可接受之酸及鹼之鹽類亦可於例如醫藥上可接受之化合物的製備或純化中發現其用途。所有不論是醫藥上可接受或不可接受之鹽類皆包括在本發明的範圍內。
如下述方法中所製備之式(I)化合物可合成為鏡像異構物的外消旋性混合物形式,其可以依照本技藝已知的分解程序互相分離。式(I)之外消旋性化合物可藉由與適合的對掌性酸反應而轉換成對應之非鏡像異構性鹽形式。該非鏡像異構性鹽形式接著藉由例如選擇或分段結晶而分離,且鏡像異構物係藉由鹼而從混合物釋出。分離式(I)化合物的鏡像異構物形式的替換方式包含使用對掌性靜相的液態層析術。該純立體異構物形式亦可從適當的起始材料之對應的純立體異構物形式衍生而來,其先決條件係反應以立體特異性方式發生。如果希望有特殊的立體異構物,則較佳地該化合物可以立體特異性製備方法合成。這些方法最好使用純鏡像異構性起始材料。
在本申請案的架構中,根據本發明的化合物本性意欲包含其化學元素的所有同位素組合。在本申請案的架構中,化學元素,特別在述及關於根據式(I)之化合物時,包含此元素的所有同位素及同位素混合物。特別在述及氫時,則應瞭解係指1
H、2
H、3
H及其混合物。
根據本發明的化合物因此本性包含具有一或多個元素的一或多種同位素及其混合物的化合物,包括放射性化合物,亦稱為放射標記化合物,其中一或多個非放射性原子被其放射性同位素中之一置換。以術語〝放射標記化合物〞意謂含有至少一種放射性原子的任何根據式(I)之化合物,或其醫藥上可接受之鹽。例如,化合物可以正子或以γ發射放射性同位素標記。以3
H-原子或125
I-原子為放射配體結合技術欲置換之選擇原子。最常用於成像之正子發射(PET)的放射性同位素為11
C、18
F、15
O及13
N,所有皆由加速器產生且分別具有20、100、2及10分鐘(min)之半衰期。因為這些放射性同位素的半衰期如此短,所以只適合在有加速器於生產場合的機構使用這些放射性同位素,因此限制其使用。最廣泛使用的放射性同位素為18
F、99m
Tc、201
Tl及123
I。這些放射性同位素的處置、產生、分離及併入分子中為熟習本技藝者所知。
放射性原子特別選自氫、碳、氮、硫、氧及鹵素之群組。放射性同位素特別選自3
H、11
C、18
F、122
I、123
I、125
I、131
I、75
Br、76
Br、77
Br及82
Br之群組。
如申請書及所附之申請專利範圍中所使用之單數形式〝a〞、〝an〞及〝the〞亦包括複數個指示目標,除非上下文有另外明確的規定。例如,〝化合物(a compound)〞意謂一種化合物或超過一種以上的化合物。
上述術語及在說明書中所使用的其他術語為那些熟習本技藝者所熟知。
為了尋得具有治療認知障礙及食物相關病症之活性的化合物,吾等篩選與羥色胺5-HT6
受體選擇性交互作用的化合物。在本發明範圍內的化合物經發現具有勻稱的分布,對測試的受體具有低的親和性,除了羥色胺5-HT6
受體以外。
可進一步預期本發明化合物在‘在大鼠中逆轉以亞慢性PCP誘發之注意力定勢轉移(Reversal of subchronic PCP-induced attentinoal set shifting in rats)’試驗中具有活性(J.S. Rodefer等人之Neurospychopharmacology(2007),1-10)。
有鑑於式(I)化合物的上述藥理,其因而適合用作為藥劑。
更尤其為治療或預防其中認知有障礙之症狀、阿滋海默氏症、帕金森氏(Parkinson’s)症、精神分裂症、亨丁頓氏(Huntingdon’s)症、路易氏體(Lewy body)失智症、由於HIV疾病所致的失智症、由於庫茲德-賈克氏(Creutzfeldt-Jakob)症所致的失智症、失憶症、溫和型認知障礙及與年齡有關的認知衰退;用於治療及/或預防進食病症及疾病、用於調節食慾、用於維持、增加或減輕體重、厭食症、貪食症、肥胖症、惡病質、II型糖尿病(非胰島素依賴型糖尿病)、由肥胖症所引起的II型糖尿病;用於治療及/或預防中風、偏頭痛、頭部創傷、癲癇症、大腸急躁症候群、刺激性腸症候群;用於治療中樞神經系統之病症、類精神分裂症、情感型精神分裂症、妄想症、暫時性精神病、共有型精神病、由於一般醫學症狀的精神病、由物質誘發之精神病、非特異性精神病、與失智症有關的精神病、重鬱症、輕鬱症、經前不悅症、非特異性抑鬱症、第一型躁鬱症、第二型躁鬱症,循環性情感症、非特異性躁鬱症、由於一般醫學症狀的情感性病症、由物質誘發之情感性病症、非特異性情感性病症、廣泛性焦慮症、強迫症、恐慌症、急性壓力障礙、創傷後壓力障礙、智能不足、廣泛性發展障礙、注意力不足症、注意力不足/過動障礙症、擾亂性行為障礙、妄想型人格障礙、類精神型分裂人格障礙、精神分裂型人格障礙、抽動症、妥瑞氏(Tourette’s)症候群、拔毛症、痙攣、癲癇發作、物質依賴、物質濫用、物質戒斷;用於治療及/或預防藥物成癮及/或戒斷;用於治療及/或預防尼古丁成癮及/或戒斷;用於治療及/或預防酒精成癮及/或戒斷之藥劑。
式(I)化合物可與其他精神治療性化合物一起投予,使遭受上述段落中所述之病症的病患達到最適化治療。
本發明亦提供一種治療遭受此病症的溫血性動物之方法,該方法包含以全身性投予有效治療上述病症的治療量之式(I)化合物。
本發明亦關於如上述定義之式(I)化合物用於製造藥劑之用途,更尤其為治療或預防其中認知有障礙之症狀、阿滋海默氏症、帕金森氏症、精神分裂症、亨丁頓氏症、路易氏體失智症、由於HIV疾病所致的失智症、由於庫茲德-賈克氏症所致的失智症、失憶症、溫和型認知障礙及與年齡有關的認知衰退;用於治療及/或預防進食病症及疾病、用於調節食慾、用於維持、增加或減輕體重、厭食症、貪食症、肥胖症、惡病質、II型糖尿病(非胰島素依賴型糖尿病)、由肥胖症所引起的II型糖尿病;用於治療及/或預防中風、偏頭痛、頭部創傷、癲癇症、大腸急躁症候群、刺激性腸症候群;用於治療中樞神經系統之病症、類精神分裂症、情感型精神分裂症、妄想症、暫時性精神病、共有型精神病、由於一般醫學症狀之精神病、由物質誘發之精神病、非特異性精神病、與失智症有關的精神病、重鬱症、輕鬱症、經前不悅症、非特異性抑鬱症、第一型躁鬱症、第二型躁鬱症,循環性情感症、非特異性躁鬱症、由於一般醫學症狀之情感性病症、由物質誘發之情感性病症、非特異性情感性病症、廣泛性焦慮症、強迫症、恐慌症、急性壓力障礙、創傷後壓力障礙、智能不足、廣泛性發展障礙、注意力不足症、注意力不足/過動障礙症、擾亂性行為障礙、妄想型人格障礙、類精神型分裂人格障礙、精神分裂型人格障礙、抽動症、妥瑞氏症候群、拔毛症、痙攣、癲癇發作、物質依賴、物質濫用、物質戒斷;用於治療及/或預防藥物成癮及/或戒斷;用於治療及/或預防尼古丁成癮及/或戒斷;用於治療及/或預防酒精成癮及/或戒斷之藥劑。
在具體例中,該症狀係選自治療及/或預防之藥物成癮及/或戒斷、治療及/或預防之尼古丁成癮及/或戒斷、治療及/或預防之酒精成癮及/或戒斷。
在具體例中,該疾病或症狀係選自其中認知有障礙之症狀、中樞神經系統之病症、焦慮症、抑鬱症、注意力不足過動障礙症、阿滋海默氏症、癲癇症、精神分裂症、進食症及疾病。
在具體例中,該疾病或症狀係選自其中認知有障礙之症狀、中樞神經系統之病症、焦慮症、抑鬱症、注意力不足過動障礙症、阿滋海默氏症、癲癇症及精神分裂症。
在具體例中,該疾病或症狀係選自其中認知有障礙之症狀、焦慮症、阿滋海默氏症及精神分裂症。
在具體例中,該疾病或症狀係選自焦慮症、阿滋海默氏症及精神分裂症。
在具體例中,該疾病為精神分裂症。
在具體例中,該疾病為阿滋海默氏症。
在具體例中,該症狀為其中認知有障礙之症狀。
本發明亦關於如上述定義之式(I)化合物用於製造藥劑之用途,更尤其用在治療該等疾病或症狀之藥劑。
本發明亦關於用在治療或預防上述疾病或症狀之式(I)化合物。
本發明亦關於用在治療上述疾病或症狀之式(I)化合物。
本發明亦關於用於治療或預防上述疾病或症狀之式(I)化合物。
本發明亦關於用於治療上述疾病或症狀之式(I)化合物。
那些熟習此等疾病治療者可從以下呈現之試驗結果決定有效的治療日劑量。有效的治療日劑可從約0.01毫克/每公斤體重至約10毫克/每公斤體重,更佳從約0.05毫克/每公斤體重至約1毫克/每公斤體重。
本發明亦關於一種包含醫藥上可接受之載劑及作為活性成分的治療有效量之根據式(I)之化合物的醫藥組成物。
為了容易投予,本發明化合物可調配成各種以投予為目的的醫藥形式。根據本發明的化合物,特別為根據式(I)之化合物、其醫藥上可接受之酸或鹼加成鹽、其立體異構物形式或其任何亞群組或組合可調配成各種以投予為目的的醫藥形式。可引述經常用於全身性投予藥物的所有組成物作為適當的組成物。可將作為活性成份的有效量之特殊化合物(視需要以加成鹽形式)與醫藥上可接受之載劑組合成密切的摻合物,以製備本發明的醫藥組成物,此載劑可取決於所欲投予之製劑形式而採用各種廣泛的形式。這些醫藥組成物希望具有特別適合於經口服、直腸、皮膚投予,以非經腸注射或吸入投予的單一劑型。例如,可使用任何常見的醫藥介質製備具有口服劑型之組成物,諸如在口服液體製劑,諸如懸浮液、糖漿、酏劑、乳液及溶液之例子中的水、二醇類、油、醇及類似物;或在藥粉、藥丸、膠囊及藥片之例子中的固體載劑,諸如澱粉、糖、高嶺土、稀釋劑、潤滑劑、結合劑、崩散劑及類似物。藥片及膠囊代表最有利的口服單位劑型,因為其容易投予,在該例子中顯然使用固體醫藥載劑。用於非經腸組成物之載劑經常包含無菌水,至少大部分為無菌水,雖然可包括例如輔助溶解度的其他成分。可製備例如可注射溶液,其中載劑包含食鹽水溶液、葡萄糖溶液或食鹽水與葡萄糖溶液之混合物。含有式(I)化合物的可注射溶液可調配於油中,以延長作用。適合於此目的的油為例如花生油、芝麻油、棉籽油、玉米油、大豆油、長鏈脂肪酸的合成甘油酯及這些油與其他油的混合物。亦可製備可注射懸浮液,在該例子中可使用適當的液體載劑、懸浮劑及類似物。亦包括意欲在臨用前轉換成液體形式製劑的固體形式製劑。在適合於經皮膚投予之組成物中,載劑視需要包含穿透增強劑及/或適合的濕潤劑,其視需要與少量任何本性之適合的添加劑組合,該添加劑不會在皮膚上引入顯著的有害效果。該添加劑可加速投予皮膚及/或可助於製備所欲之組成物。這些組成物可以各種方式投予,例如成為穿透皮膚貼片、成為點滴劑、成為軟膏。由於式(I)化合物的酸或鹼加成鹽類的水溶解度高於對應之鹼或酸形式,故其更適合於製備水性組成物。
尤其有利的是將上述醫藥組合物調配成容易投予且劑量均一的單位劑型。如本文所使用之單位劑型係指適合呈單位劑量之物理性分離單位,每一單位含有經計算與所需之醫藥載劑聯結以產生所欲之治療效果的預定量活性成份。此等單位劑型的實例為藥片(包括有刻槽或包膜之藥片)、膠囊、藥丸、散劑包、粉片、栓劑、可注射溶液或懸浮液及類似物,及其分開之多重組合。
因為根據本發明的化合物為有效經口服投予之化合物,所以包含用於口服投予之該化合物的醫藥組成物尤其有利。
為了增強醫藥組成物中的式(I)化合物之溶解度及/或穩定度,故可能有利的是使用α-、β-或γ-環糊精或其衍生物,特別為經羥烷基取代之環糊精,例如2-羥丙基-β-環糊精。共溶劑,諸如醇亦可改進根據本發明的化合物在醫藥組成物中的溶解度及/或穩定度。
取決於投予模式而定,醫藥組成物較佳地包含從0.05至99重量%,更佳從0.1至70重量%,甚至更佳從0.1至50重量%之式(I)化合物,及從1至99.95重量%,更佳從30至99.9重量%,甚至更佳從50至99.9重量%之醫藥上可接受之載劑,所有的重量百分比係以組成物總重量為基準計。
式(I-a)化合物,
其中R1
為氯基、三氟甲基或氰基,R3a
為C1-4
烷基或吡啶基甲基,且其中R2
及X係如上述所定義,可藉由式(I-b)化合物
其中R1
、X及R2
係如上述所定義,與C1-4
-醛(諸如甲醛或乙醛)或吡啶甲醛在鹼(諸如Et3
N)、還原劑(諸如NaBH(OAc)3
)、Pt/C(不適合於R1a
=Cl)或雷尼(Raney)鎳(不適合於R1a
=CN)及適合的反應溶劑(諸如二氯甲烷(DCM)、甲醇或乙醇)存在下反應而製備。
式(I-b)化合物
其中取代基係如上述所定義,可藉由式(II)中間物中的保護基,
其中L代表適合的保護基,諸如第三丁氧基羰基,且R1
、R2
及X係如上述所定義,在適合的條件下,諸如在DCM中的三氟乙酸(TFA),或在甲醇(MeOH)中的磺酸化聚苯乙烯類型之酸陽離子交換樹脂(例如,AMBERLITETM
酸),或在溶劑(如二烷)中的HCl存在下去保護而製備。
式(II’)中間物
其中L代表適合的保護基,諸如第三丁氧基羰基,且R2
及X係如上述所定義,可藉由氯基衍生物(II”)與Zn(CN)2
在鈀觸媒,諸如在適合的溶劑(諸如DMF)中的肆(三苯膦)鈀存在下反應而製備。
式(II-a)中間物
其中R1a
為氯基或三氟甲基及其他的取代基係如上述所定義,通常係在式(III)中間物
其中R1a
及L係如上述所定義,與市售可取得的Rx
-酚,其中Rx
為氫或鹵基之間以N,N-二甲基甘胺酸促進之Ullmann偶合反應而製備。該類型反應典型地可在銅或鎳催化之條件下(例如,使用銅或鎳鹽,諸如Cu2
O、CuI或Ni(OAc)2
)及在鹼條件下(如Cs2
CO3
、K3
PO4
或K2
CO3
)於上升溫度下(70-100℃)及在適當的惰性溶劑中(諸如二烷或甲苯)執行。
式(II-b)中間物
其中R1a
、R2
及L係如上述所定義,通常係藉由式(III)中間物與市售可取得的Rx
-苯胺,其中Rx
為氫或鹵基,反應而製備,典型地在配體(諸如(1S)-[1,1'-雙萘]-2,2'-二基雙[二苯膦]((S)-BINAP))及鹼(如Cs2
CO3
、K3
PO4
、K2
CO3
或第三丁醇鈉(第三-BuONa))存在下於上升的溫度下(70-100℃)及在適當的惰性溶劑中(諸如二烷或甲苯)。
式(II-c)中間物
其中R1a
、R2
及L係如上述所定義,通常係藉由式(III)中間物與Rx
-苯亞磺酸鈉鹽,其中Rx
為氫或鹵基,在鹼(如Cs2
CO3
、K3
PO4
或K2
CO3
)存在下於上升的溫度下(70-100℃)及在適當的溶劑中(諸如二甲亞(DMSO))以CuI/L-脯胺酸催化之偶合反應而製備。
式(II-d)中間物
其中R1a
、R2
及L係如上述所定義且其中X’為1,2-乙烯二基或乙炔二基,通常係藉由式(III)中間物與[(Rx
-苯基)乙烯基]-硼酸或(Rx
-苯基)乙炔基,其中Rx
為氫或鹵基,在催化劑(如肆(三苯膦)鈀(Pd(PPh3
)4
))、鹼(如Cs2
CO3
、K3
PO4
或K2
CO3
)及視需要在銅或鎳鹽(諸如Cu2
O、CuI或Ni(OAc)2
)存在下,視需要在適合的溶劑(諸如二烷或N,N-二甲基甲醯胺(DMF))存在下,在適合的反應條件下,諸如在合宜的溫度下(以慣例的加熱或在微波照射下)經確保反應完成的時間期偶合而製備。
式(II-e)中間物
其中R1a
、R2
及L係如上述所定義且其中X”為-NH-CH2
-或-O-CH2
-,通常係藉由式(III)中間物與Rx
-苯甲胺或Rx
-苯甲醇,其中Rx
為氫或鹵基,在鹼(如NaH)及適合的溶劑(如THF或DMF)存在下,在適合的反應條件下,諸如在合宜的溫度下經確保反應完成的時間期偶合而製備。
式(II-f)中間物
其中R1a
及L係如上述所定義,可藉由式(II-g)中間物
其中R1a
及L係如上述所定義,以Pd/C觸媒在H2
氣下於適當的溶劑中(諸如EtOH或MeOH)及室溫下還原而製備。
式(II-h)中間物
其中R1a
及L係如上述所定義,可藉由式(II-g)中間物以氧化劑(諸如MnO2
或1,1,1-參(乙醯氧基)-3H-1,2-苯并碘氧五圜-3-酮(Dess Martin試劑))在適合的溶劑中(諸如DCM或乙酸乙酯(EtOAc))及低溫下(典型地在0℃)氧化而製備。
式(II-g)中間物可藉由式(IV)化合物
其中R1a
及L係如上述所定義,與苯甲醛在適合的鹼(諸如丁基鋰與2,2,6,6-四甲基六氫吡啶之混合物)存在下於適合的惰性溶劑中(諸如四氫呋喃(THF))及低溫下(典型地在從-78℃至0℃為範圍)反應而製備。
式(III)中間物可藉由式(IV)中間物與碘在適合的鹼(諸如丁基鋰與2,2,6,6-四甲基六氫吡啶之混合物)存在下於適合的惰性溶劑中(諸如THF)及低溫下(典型地在從-78℃至0℃為範圍)反應而製備。
式(IV’)中間物
可藉由6-氯-3-三氟甲基嗒(藉由依照Goodman,A.J.,Stanforth,S.P.,Tarbit B.在Tetrahedron 1999,55,15067-15070中所述之程序而製備)與1-六氫吡羧酸第三丁酯在適合的鹼(諸如二異丙基乙胺(DIPEA))存在下於適合的溶劑中(諸如CH3
CN)及合宜的溫度下(藉由慣例的加熱或微波照射下)經確保反應完成的時間期反應而製備。
下列的實例例證本發明。
在下文中,術語〝DCM〞意謂二氯甲烷,〝MeOH〞意謂甲醇,〝THF〞意謂四氫呋喃,〝LCMS〞意謂液相層析術/質譜法,〝q.s.〞意謂適量,〝HPLC〞意謂高性能液相層析術,〝r.t.〞意謂室溫,〝Pd(OAc)2
〞意謂乙酸鈀,〝DIPEA〞意謂二異丙基乙胺,〝min〞意謂分鐘,〝h〞意謂小時,〝(S)-BINAP〞意謂(1S)-[1,1'-雙萘]-2,2'-二基雙[二苯膦],〝EtOAc〞意謂乙酸乙酯,〝Et3
N〞意謂三乙胺,〝EtOH〞意謂乙醇,〝r.m.〞意謂反應混合物,〝DMSO〞意謂二甲亞,〝TFA〞意謂三氟乙酸,〝Pd(PPh3
)4
〞意謂肆(三苯膦)鈀,及〝NaBH(OAc)3
〞意謂三乙醯氧基硼氫化鈉。
以微波協助之反應係在單模式反應器中:EmrysTM
Optimizer微波反應器(Personal Chemistry A.B.,目前為Biotage)執行。
1
H NMR光譜係記錄在具有標準脈衝順序,分別在400MHz及500MHz下操作,使用CDCl3
及DMSO-d 6
作為溶劑的Bruker DPX-400上或Bruker AV-500光譜計上。化學位移(δ)係從用作為內標準物的四甲基矽烷(TMS)之低磁場以每百萬計(ppm)之份量記述。
將在CH3
CN(10毫升)中的6-氯基-3-三氟甲基嗒(0.666公克,5.09毫莫耳)(藉由依照Goodman,A.J.,Stanforth,S.P.,Tarbit B.在Tetrahedron 1999,55,15067-15070中所述之程序而製備)、1-六氫吡羧酸第三丁酯(1.138公克,6.11毫莫耳)與DIPEA(1.95毫升,1.12毫莫耳)之混合物在微波照射下以180℃攪拌30分鐘。將溶劑在真空中蒸發且將殘餘物以管柱層析術(矽膠;己烷/EtOAc)純化,得到成為淺黃色固體的中間物1(1.67公克,99%)。C14
H19
F3
N4
O2
必需為332;實測為333(MH+
)。
將2,2,6,6-四甲基六氫吡啶(3.808毫升,22.56毫莫耳)在0℃下加入THF(125毫升)中的丁基鋰混合物(在己烷中的2.5M)(6.31毫升,15.79毫莫耳)中。將反應混合物在室溫下攪拌1小時。將混合物冷卻至-78℃且接著加入在THF(20毫升)中的中間物1(2.5公克,7.52毫莫耳)之溶液。將混合物在-78℃下攪拌1小時,然後加入在THF(10毫升)中的碘(2.29公克,9.024毫莫耳)之溶液。將混合物在-78℃下攪拌1小時且接著以在THF中的10%乙酸溶液稀釋。接著允許混合物達到室溫且將溶劑在真空中蒸發。將殘餘物以DCM稀釋且以水萃取。將有機層分離,乾燥(MgSO4
),過濾且將溶劑在真空中蒸發。將殘餘物從二乙醚沉澱,得到成為淺黃色固體的中間物2(2.81公克,82%)。C14
H18
F3
IN4
O2
必需為458;實測為459(MH+
)。
其係根據類似於中間物2之方案而製備,但是使用苯甲醛代替碘。產量:84%。
將在二烷(5毫升)中的中間物2(0.490公克,1.069毫莫耳)、4-氟酚(0.215公克,1.92毫莫耳)、N,N-二甲基甘胺酸(0.107毫莫耳)、CuI(0.0061公克,0.032毫莫耳)與Cs2
CO3
(0.697公克,2.14毫莫耳)之混合物以N2
沖洗且在100℃下加熱16小時。接著將混合物冷卻,並加入DCM、H2
O及濃縮NH4
OH溶液。將混合物萃取且將分離的有機層經棉過濾。將溶劑蒸發且將殘餘物以經過矽膠的快速管柱層析術(溶析劑:DCM/EtOAc 0-1-2-5%)純化。收集所欲部分且將溶劑蒸發,得到成為白色固體的0.435公克(92%)中間物3。
將在甲苯(2毫升)中的中間物2(0.15公克,0.327毫莫耳)、4-氟苯胺(0.034毫升,0.3毫莫耳)、(S)-BINAP(0.0061公克,0.009毫莫耳)、Pd(OAc)2
(0.002公克,0.009毫莫耳)、Cs2
CO3
(0.533公克,1.63毫莫耳)與Et3
N(0.002毫升,0.02毫莫耳)之混合物攪拌且在100℃下加熱24小時。接著將混合物冷卻,經由矽藻土(CELITETM
)過濾且將有機層蒸發。將殘餘物以經過矽膠的快速管柱層析術(溶析劑:DCM/EtOAc 100/0-97/3-95/5)純化。收集所欲部分且將溶劑蒸發,得到成為黃色固體的0.117公克(81%)中間物4。
將在DMSO(1.5毫升;無水)中的中間物2(0.200公克,0.0004莫耳)之溶液以N2
沖洗數分鐘。接著將苯亞磺酸鈉鹽(0.143公克,0.0009莫耳)、L-脯胺酸(0.020公克,0.0002莫耳)、CuI(0.08公克)與K3
PO4
(0.093公克,0.0004莫耳)之混合物加入溶液中且將反應混合物在85℃下攪拌18小時。接著將混合物以DCM稀釋且將所得混合物以氨水溶液清洗。將有機層分離,乾燥(MgSO4
),過濾且將濾液蒸發。將殘餘物以快層析術(溶析劑:DCM/(在MeOH中的NH3
7N溶液),先以100/0,接著以90/10)純化。收集所欲部分且將溶劑蒸發。產量:成為淡黃色固體的0.148公克中間物7(72%)
將中間物2(0.2公克,0.00043莫耳)、[2-(4-氟苯基)乙烯基]硼酸(0.092公克,0.00055莫耳)、Pd(PPh3
)4
(0.015公克,0.0000086莫耳)、K2
CO3
(0.118公克,0.000129莫耳)、二烷(2毫升)與DMF(0.5毫升)之混合物在微波照射下以160℃照射1小時。接著將溶劑蒸發且將殘餘物以經過矽膠的快速管柱層析術(溶析劑:DCM/(在MeOH中的NH3
7N溶液)97/3)純化。收集所欲部分且將溶劑蒸發。產量:成為黃色油的0.179公克中間物8(92%;E/Z之混合物)。
其係根據類似於用以合成中間物8之方案而製備,但是使用(E)-(2-苯基乙烯基)硼酸代替[2-(4-氟苯基)乙烯基]硼酸作為起始材料。
將中間物2(0.2公克,0.43毫莫耳)、1-乙炔基-4-氟苯(0.067公克,0.55毫莫耳)、Pd(PPh3
)4
(0.010公克,0.0086毫莫耳)、CuI(0.002公克,0.129毫莫耳)與Et3
N(2毫升)之混合物在55℃下攪拌3小時。接著將混合物冷卻,經由矽藻土(CELITETM
)過濾且將濾液蒸發。將殘餘物以經過矽膠的快速管柱層析術(溶析劑:DCM/(在MeOH中的NH3
7N溶液)97/3)純化。收集所欲部分且將溶劑蒸發。產量:0.132公克中間物9(68%)。
將中間物2(0.400公克,0.873毫莫耳)與4-氟苯甲胺(1.2毫升,10.5毫莫耳)之混合物在150℃下攪拌1小時。接著加入水、NH4
Cl飽和溶液及DCM。將有機分離且經由棉過濾。將濾液蒸發且將殘餘物以經過矽膠的快速管柱層析術(溶析劑:DCM/EtOAc 100/0-95/5)純化。收集所欲部分且將溶劑蒸發。產量:0.340公克中間物12(86%)。
將4-氟苯甲醇(0.19毫升,1.74毫莫耳)加入NaH(0.062公克,1.55毫莫耳;在油中的60%溶液)與DMF(4毫升;無水)之混合物中。將此混合物攪拌10分鐘且接著加入在DMF(2毫升;無水)中的中間物2(0.400公克,0.873毫莫耳)。將反應混合物在室溫下攪拌1小時。接著加入NH4
Cl飽和溶液、水及DCM。將有機層分離且經由棉過濾。將濾液蒸發且將殘餘物以快速管柱層析術(溶析劑:DCM/EtOAc 100/0-98/2-96/4)純化。收集所欲部分且將溶劑蒸發。產量:0.295公克中間物13(74%)。
將中間物5(0.06公克,0.0001莫耳)溶解在EtOH(5毫升)中且將Pd/C(0.005公克)加入此溶液中。將反應混合物在室溫及H2
氣下的大氣壓力下攪拌2天。接著將混合物經由矽藻土(CELITETM
)墊過濾且將濾液蒸發。將殘餘物以管柱層析術(溶析劑:DCM)純化。收集所欲部分且將溶劑蒸發。產量:0.050公克中間物6(86%)。
將中間物5(0.08公克,0.00018莫耳)溶解在DCM(2毫升)中且將溶液冷卻至0℃。將1,1,1-參(乙烯氧基)-3H-1,2-苯并碘氧五圜-3-酮(Dess Martin試劑)(0.12公克,0.00027莫耳)加入此溶液中且將反應混合物在0℃下攪拌1小時。接著加入水且將層分離。將有機層乾燥(Na2
SO4
),過濾且將溶劑蒸發。產量:中間物11(粗產物,以如此用於下一反應步驟中)。
將MnO2
(5公克,0.058莫耳)加入在EtOAc(60毫升)中的中間物5(3公克,0.007莫耳)中。將反應混合物在室溫下攪拌隔夜。接著將混合物過濾且將溶劑蒸發,得到2.5公克中間物11(83%;粗產物,以如此用於下一反應步驟中)。B.化合物之製備
將在TFA(2毫升)及DCM(18毫升)中的中間物3(0.435公克,0.983毫莫耳)之混合物在室溫下攪拌3小時。接著加入DCM、Na2
CO3
飽和溶液及H2
O且萃取混合物。將分離的有機層經由棉過濾,將溶劑蒸發且將殘餘物以經過矽膠的快速管柱層析術(DCM/(在MeOH中的NH3
7N溶液)100/0-98/2)純化。收集所欲部分且將溶劑蒸發,得到0.316公克(94%)化合物1。
1
H NMR(400MHz,CDCl3
)ppm:2.86-3.06(m,4H)3.57-3.64(m,4H)5.96(s,1H)7.08-7.25(m,4H)。
將在MeOH(8毫升)中的中間物4(0.117公克,0.33毫莫耳)與磺酸化聚苯乙烯類型之酸陽離子交換樹脂(AMBERLITETM
酸)(適量)之混合物搖動24小時。將樹脂濾出且將有機層棄置。接著將樹脂以MeOH清洗且在MeOH中的NH3
7N溶液中攪拌30分鐘。將樹脂濾出且將所獲得的有機層在真空中濃縮。將殘餘物以經過矽膠的快速管柱層析術(DCM/MeOH 70/30)純化。收集所欲部分且將溶劑蒸發,得到黃色固體。將此固體以HPLC再純化,得到0.048公克(53%)白色固體。將非晶形固體從乙醚結晶,得到成為結晶狀白色固體的0.015公克化合物2(游離鹼)。
1
H NMR(400 MHz,DMSO-d6
)ppm 2.81-2.93(m,4H)3.47-3.53(m,4H)6.15(s,1H)7.26(t,J=8.81Hz,2H)7.30-7.39(m,2H)8.13(s,1H)。
將中間物4(0.425公克,0.963毫莫耳)、DCM(18毫升)與TFA(2毫升)之混合物在室溫下攪拌3小時。接著加入DCM、飽和Na2
CO3
及H2
O且萃取混合物。將分離的有機層經由棉過濾且將溶劑蒸發。將殘餘物以經過矽膠的快速層析術(溶析劑:DCM/(在MeOH中的NH3
7N溶液),從100/0直到97/3)純化。收集所欲部分且將溶劑蒸發。將殘餘物溶解在EtOAc/DIPE中且加入在2-丙醇中的HCl溶液(5-6N)。接著將大部分溶劑蒸發。將額外的EtOAc加入濃縮液中且以超聲波浴中的超聲波施加於混合物。將沉澱物濾出且乾燥。產量:0.388公克化合物16(97%;‧2.5HCl‧0.5H2
O)。
1
H NMR(400MHz,DMSO-d6
)δppm:3.14(br.s.,4H)3.71-3.79(m,4H)6.28(s,1H)7.28(t,J=8.79Hz,2H)7.32-7.42(m,2H)8.47(s,1H)9.43(br.s.,2H)。
化合物7(Z-異構物)及化合物8(E-異構物)係根據類似於用以合成化合物2之方案而製備,但是使用中間物8(E/Z之混合物)代替中間物4作為起始材料。在HPLC純化之後獲得兩種純異構物。
1
H NMR(400MHz,DMSO-d6
)δppm:2.59-2.82(m,4H)3.45-3.57(m,4H)6.59(br.d,J=12.4Hz,1H)6.91(s,1H)6.96(d,J=12.4Hz,1H)7.04-7.25(m,4H)。
1
H NMR(400MHz,DMSO-d6
)δppm:2.75-2.88(m,4H)3.65-3.77(m,4H)7.05(dd,J=16.17,1.87Hz,1H)7.24-7.34(m,2H)7.53(s,0H)7.64-7.76(m,3H)。
化合物9係根據類似於用以合成化合物2之方案而製備,但是使用中間物9代替中間物4作為起始材料。產量:成為黃色固體的化合物9(80%)。
1
H NMR(400MHz,DMSO-d6
)δppm:2.72-2.86(m,4H)3.63-3.75(m,4H)7.31-7.41(m,2H)7.60(s,1H)7.62-7.69(m,2H)。
將中間物6(0.05公克,0.0001莫耳)溶解在二烷中的HCl 4M(1毫升)中。將溶液在室溫下攪拌1小時。將溶劑蒸發且將殘餘物溶解在DCM中。將此溶液以NaHCO3
飽和溶液清洗,乾燥(Na2
SO4
)且過濾。將化合物以正相管柱層析術(溶析劑:DCM/(在MeOH中的NH3
7N溶液))純化。收集所欲部分且將溶劑蒸發,得到0.035公克化合物3(90%)。
1
H NMR(500MHz,CDCl3
)δppm:2.82-2.89(m,4H)3.42-3.61(m,4H)3.98(s,2H)6.32(s,1H)7.09(d,J=7.51Hz,2H)7.20-7.26(m,1H)7.29(t,J=7.37Hz,2H)。
將中間物5(0.054公克,0.109毫莫耳)及在二烷中的4M HCl溶液之溶液在室溫下攪拌16小時。將溶劑蒸發且將殘餘物以乙醚處理,得到淺黃色沉澱物,將其濾出。產量:0.0426公克化合物5(92%;HCl-鹽)。
1
H NMR(400MHz,DMSO-d6
)δppm:3.18-3.32(m,4H)3.82-4.20(m,4H)5.87(s,1H)7.14-7.43(m,5H)7.65(s,1H)9.07(br.s.,2H)。
將中間物11(粗產物;在實例A3.a中獲得的殘餘物)溶解在二烷中的4M HCl溶液(2毫升)中且將混合物在室溫下攪拌1小時。將溶劑蒸發且將殘餘物以NaHCO3
飽和溶液處理,以DCM萃取且以管柱層析術(溶析劑:DCM/EtOAc 7/3)處理。收集所欲部分且將溶劑蒸發。產量:0.030公克化合物4(50%)。
化合物4,化合物12的HCl-鹽係藉由將中間物11(0.5公克,0.001145莫耳)溶解在MeOH中的HCl溶液(15毫升)中而獲得。將反應混合物在室溫下攪拌4小時。接著將溶劑蒸發,得到0.350公克化合物12(81.9%;HCl-鹽形式)。
將在DCM(5毫升)中的化合物12(0.080公克,0.215毫莫耳)、甲醛(0.050公克,0.47毫莫耳)、NaBH(OAc)3
(0.100公克,0.47毫莫耳)與Et3
N(0.1公克,1毫莫耳)之混合物在室溫下攪拌隔夜。接著將混合物以NaHCO3
飽和溶液清洗。將分離的有機層乾燥(Na2
SO4
),過濾且將溶劑在真空中蒸發。將殘餘物以製備性TLC(溶析劑:DCM/MeOH 20/1)純化。產量:化合物13(42%)。
將TFA(1毫升)加入在DCM(4毫升)中的中間物7(0.145公克,0.0003莫耳)之溶液中且將反應混合物在室溫下攪拌2小時。接著將溶劑蒸發且將殘餘物溶解在DCM中。將此有機溶液以Na2
CO3
飽和溶液清洗。將有機層分離,乾燥(MgSO4
),過濾且將濾液蒸發。將產物以快速管柱層析術(溶析劑:DCM/(在MeOH中的NH3
7N溶液),先以100/0,接著以95/5)純化。收集所欲部分且將溶劑蒸發,得到0.103公克淡黃色固體。將此固體以HPLC進一步純化,得到成為淡黃色固體的0.0513公克化合物6(45%)。
1
H NMR(400MHz,CDCl3
)δppm:2.96-3.08(m,4H)3.80-3.89(m,4H)7.45-7.54(m,2H)7.58-7.64(m,1H)7.66(s,1H)7.79(d,J=7.88Hz,2H)。
將中間物12(0.340公克,0.7465毫莫耳)、TFA(1毫升)與DCM(9毫升)之混合物在室溫下攪拌3小時。接著加入Na2
CO3
飽和溶液、水及DCM。將有機層分離且經由棉過濾。將溶劑蒸發且將殘餘物以經過矽膠的快速管柱層析術(溶析劑:DCM/(在MeOH中的NH3
7N溶液),先以100/0,接著以99/1,接著以98/2)純化。收集所欲部分且將溶劑蒸發。將黏性產物以在2-丙醇中的5-6N HCl(0.5毫升)處理。將溶劑蒸發且將EtOAc加入殘餘物中。以超聲波浴中的超聲波施加於混合物,並接著將化合物濾出且乾燥。產量:0.275公克化合物14(86%;‧2.5HCl‧0.5H2
O)。
1
H NMR(400MHz,DMSO-d6
)δppm:3.17(br.s.,4H)3.80-3.92(m,4H)4.59(d,J=6.01Hz,2H)6.36(s,1H)7.18(t,J=8.79Hz,2H)7.44(dd,J=8.67,5.66Hz,2H)7.85(br.s.,1H)9.51(br.s.,2H)。
化合物15係根據類似於用以合成化合物6之方案而製備,但是使用中間物13代替中間物7作為起始材料。產量:化合物15(88%)。
1
H NMR(400MHz,CDCl3
)δppm:2.93-3.04(m,4H)3.62-3.76(m,4H)5.15(s,2H)6.23(s,1H)7.10(t,J=8.67Hz,2H)7.38(dd,J=8.55,5.32Hz,2H)。
將中間物10(5.5公克,0.0127莫耳)及在MeOH中的HCl溶液(110毫升)之混合物在室溫下攪拌4小時。接著將溶劑蒸發,得到4.5公克化合物10(95%;HCl-鹽)。
將在DCM(5毫升)化合物10(0.080公克,0.22毫莫耳)、甲醛(0.25毫莫耳)、NaBH(OAc)3
(適量)與Et3
N(0.101公克,1毫莫耳)之混合物在室溫下攪拌隔夜。接著將溶劑蒸發且將殘餘物以製備性TLC(溶析劑:DCM/MeOH 20/1)純化,得到化合物11。
如表1中所述之下列式(I)化合物係以類似於上述實例(實例編號)而製備。一些化合物係以鹽形式獲得。假使有測定真實的化學計量,則將結果顯示於‘鹽形式’的欄位中,例如參見欄位編號14及16。假使未測定真實的化學計量,則僅顯示化合物的鹽形式類型,例如參見欄位編號5。
HPLC測量係使用包含幫浦、光二極體陣列偵測器(PDA)(所使用之波長為220nm)、管柱烘箱及如下述個別方法中指明之管柱的Shimadzu 2010 LCMS-系統執行。來自管柱的流動分出至Shimadzu 2010 MSD偵測器。MS偵測器係由API-ES(大氣壓力電噴灑離子化)所建構。質譜係從100掃描至1000而獲得。正離化模式的界面電壓為4500V。噴霧氣體流速為1.5公升/分鐘。CDL(具有加熱之毛細管的曲線型去溶劑線(Curved Desolvation Line))溫度為250℃及CDL電壓為30V。加熱塊溫度為200℃。偵測器電壓為1500V。
LC測量係使用包含二元幫浦、樣品排列器、管柱加熱器(設定在55℃)、二極體陣列偵測器(DAD)及如下述個別方法中指明之管柱的Acquity超性能液相層析術(UPLC)(Waters)系統執行。來自管柱的流動分出至Shimadzu 2010 MSD偵測器。MS偵測器係由電噴灑離子化源極所建構。質譜係使用0.02秒之停留時間以0.18秒從100掃描至1000而獲得。毛細管針壓力為3.5kV及源極溫度維持在140℃。使用氮作為噴霧氣體。數據擷取係以Waters-Micromass MassLynx-Openlynx數據系統執行。
除了通用程序A以外,逆相HPLC係在具有1.0毫升/分鐘之流速的YMC-Pack ODS-AQ,50x2.0毫米,5微米管柱上進行。使用兩種移動相(移動相A:具有0.1%TFA之水;移動相B:具有0.5%TFA之CH3
CN)於0.01分鐘內以從99%A及1%B至90%A及10%B之梯度運行。接著施予2.2分鐘的20%A及80%B之梯度且以其維持0.28分鐘。使用1微米的典型注射體積。烘箱溫度為50℃。(MS極性:正)。
除了通用程序B以外,逆相UPLC係在具有0.8毫升/分鐘之流速的橋連型乙基矽氧烷/二氧化矽雜混物(BEH)C18管柱(1.7微米,2.1 x 50毫米;Waters Acquity)上進行。使用兩種移動相(移動相A:在H2
O/MeOH 95/5中的0.1%甲酸;移動相B:MeOH)於1.3分鐘內以從95%A及5%B至5%A及95%B之梯度條件運行且維持0.2分鐘。使用0.5微米之注射體積。正離子化模式之錐體壓力為10V及負離子化模式之錐體壓力為20V。
許多化合物的熔點係在Mettler FP62裝置上的開放式毛細管中測定。熔點係以3至10℃/分鐘之溫度梯度測量。最大溫度為300℃。熔點係從數位式顯示器讀取。
人類5-HT6
受體之試管內結合親和性
將以人類羥色胺5-HT6
受體-轉染之HEK細胞的冷凍細胞膜解凍,旋即使用Ultra-Turrax T25均化器均化且在含有10mM MgCl2
、1mM EDTA及10μM巴吉林(Pargyline)之50mM Tris-HCl檢定緩衝液(以HCl調整至pH 7.4)中稀釋成最適化於特異性及非特異性結合之適當的蛋白質濃度。放射配體[3
H]麥角酸二乙基醯胺(Perkin Elmer,特異活性~80Ci/毫莫耳)係在檢定緩衝液中稀釋為20nM之濃度。接著將放射配體(20微升)與40微升10%DMSO控制物,梅噻平(Methiothepine)(10-5
M之最終濃度,用於測量非特異性結合)或有興趣的化合物一起與70微升經製備之細胞膜溶液及70微升以WGA(小麥胚芽凝集素)塗佈之PVT(聚乙烯基甲苯胺(polyvinyltoluidene))珠(0.25毫克/每槽孔最終濃度)培育。每槽孔之放射配體的最終濃度為2nM。在室溫下搖動24小時之後,將平盤在TopcountTM
閃爍計數器中計數。特異性結合百分比及競爭結合曲線係使用S-Plus軟體(Insightful)計算。
化合物與穩定地表現在SK-N-MC細胞中的克隆人類H3
受體的結合係如先前所述方式執行(Lovenberg TW,Pyati J,Chang H,Wilson SJ,Erlander MG.之Cloning of rat histamine H3
receptor reveals distinct species pharmacological profiles. J Pharmacol Expt Ther 2000,293,771-778)。簡言之,將來自表現人類H3
受體之SK-N-MC細胞的沉澱細胞在50mM Tris-HCl/5mM EDTA中均化且在30000g下離心30分鐘。將沉澱細胞在50mM Tris/5mM EDTA(pH 7.4)中再均化。將細胞膜與以50mM Tris-HCl/5mM EDTA中的冷碘普西芬(iodoproxifan)稀釋之125
I-碘普西芬在25℃下培育1小時。在反應中的最終總碘普西芬濃度為1nM。其包括0.975nM之冷碘普西芬最終濃度及0.025nM之125
I-碘普西芬最終濃度。反應係藉由經過在細胞採集器上的GF/B平盤(以0.3%聚乙烯亞胺預處理)過濾而終止。將平盤以緩衝液清洗5次。非特異性結合係限定在100μM組織胺的存在下。抑制濃度(對應於50%之最大效應的抑制作用,IC50
)值係以單位置曲線(single site curve)-擬合程式(GraphPad,San Diego,CA)測定且以1nM之125
I-碘普西芬解離常數(Kd
)為基準轉換成Ki
值。
如整個這些實例之中所使用的〝活性成分〞(A.I.)係關於式(I)化合物、其醫藥上可接受之酸或鹼加成鹽類及其立體異構物形式。
將500公克A.I.在60~80℃下溶解在0.5公升2-羥基丙酸及1.5公升聚乙二醇中。在冷卻至30~40℃之後,加入35公升聚乙二醇且將混合物徹底攪拌。接著加入在2.5公升純水中的1750公克糖精鈉之溶液中,且在攪拌的同時加入2.5公升可可香料及適量聚乙二醇至50公升體積,以提供包含10毫克/毫升之A.I.的口服滴劑溶液。將所得溶液填充至適合的容器中。
將9公克4-羥基苯甲酸甲酯及1公克4-羥基苯甲酸丙酯溶解在4公升沸騰純水中。先將10公克2,3-二羥基丁烷二酸加入3公升此溶液中且接著加入20公克A.I.。將後者溶液加入前者溶液的剩餘部分中,並將12公升1,2,3-丙三醇及3公升70%之山梨醇溶液加入其中。將40公克糖精鈉溶解在0.5公升水中,並加入2毫升覆盆子及2毫升醋栗香精。將後者溶液與前者溶液合併,加入適量水至20公升體積,以提供每一茶匙(5毫升)包含5毫克活性成份的口服溶液。將所得溶液填充至適合的容器中。
將100公克A.I.、570公克乳糖與200公克澱粉之混合物徹底混合且接著以在約200毫升水中的5公克十二烷基硫酸鈉及10公克聚乙烯基吡咯烷酮之溶液濕潤。將濕的粉末混合物過篩,乾燥且再過篩。接著加入100公克微結晶狀纖維素及15公克氫化植物油。將全部徹底混合且壓縮成藥片,得到10,000個藥片,各含有10毫克活性成分。
將在150毫升二氯甲烷中的5公克乙基纖維素之溶液加入在75毫升變性乙醇中的10公克甲基纖維素之溶液中。接著加入75毫升二氯甲烷及2.5毫升1,2,3-丙三醇。將10公克聚乙二醇熔融且溶解在75毫升二氯甲烷中。將後者溶液加入前者溶液中,並接著加入2.5公克十八酸鎂、5公克聚乙烯基吡咯烷酮及30毫升濃縮色彩懸浮液且將全部均化。將藥片核心以因此獲得的混合物在包膜裝置中包膜。
將1.8公克4-羥基苯甲酸甲酯及0.2公克4-羥基苯甲酸丙酯溶解在用於注射的約0.5公升沸騰水中。在冷卻至約50℃之後,在攪拌的同時加入4公克乳酸、0.05公克丙二醇及4公克A.I.。將溶液冷卻至室溫且以用於注射的水適量補充至1公升,得到包含4毫克/毫升之A.I.的溶液。將溶液以過濾消毒且填充至無菌容器中。
Claims (8)
- 一種式(I)化合物
- 根據申請專利範圍第1項之化合物,其中R1 為三氟甲基;R2 為苯基或以氟基取代之苯基;R3 為氫、甲基或吡啶基甲基;X為-O-、-NH-、-CH2 -、-CH(OH)-、-SO2 -、-CO-、-NH-CH2 -、-O-CH2 -、1,2-乙烯二基或乙炔二基;或其醫藥上可接受之加成鹽或溶劑合物。
- 根據申請專利範圍第1項之化合物,其中R2 為苯基或以一個氟基取代之苯基。
- 根據申請專利範圍第1項之化合物,其中該化合物為N-(4-氟苯基)-6-(1-六氫吡基)-3-(三氟甲基)-4-嗒胺。
- 根據申請專利範圍第1項之化合物,其中該化合物為N-(4-氟苯基)-6-(1-六氫吡基)-3-(三氟甲基)-4-嗒胺.2.5HCl.0.5H2 O。
- 一種根據申請專利範圍第1-5項中任一項之化合物用於製造供治療與5-HT6 受體相關的疾病的藥劑之用途。
- 根據申請專利範圍第6項之用途,其係用作在治療或預防其中認知有障礙之症狀、阿滋海默氏症、帕金森氏(Parkinson’s)症、精神分裂症、亨丁頓氏(Huntingdon’s)症、路易氏體(Lewy body)失智症、由於HIV疾病所致的失智症、由於庫茲德-賈克氏(Creutzfeldt-Jakob)症所致的失智症、失憶症、溫和型認知障礙及與年齡有關的認知衰退;用於治療及/或預防進食病症及疾病、用於調節食慾、用於維持、減輕體重、貪食症、肥胖症、II型糖尿病(非胰島素依賴型糖尿病)、由肥胖症所引起的II型糖尿病;用於治療及/或預防中風、偏頭痛、頭部創傷、癲癇症、大腸急躁症候群、刺激性腸症候群;用於治療中樞神經系統之病症、類精神分裂症、情感型精神分裂症、妄想症、暫時性精神病、共有型精神病、由於一般醫學症狀所致的精神病、由物質誘發之精神病、非特異性精神病、與失智症有關的精神病、重鬱症、輕鬱症、經前不悅症、非特異性抑鬱症、第一型躁鬱症、第二 型躁鬱症,循環性情感症、非特異性躁鬱症、由於一般醫學症狀所致的情感性病症、由物質誘發之情感性病症、非特異性情感性病症、廣泛性焦慮症、強迫症、恐慌症、急性壓力障礙、創傷後壓力障礙、智能不足、廣泛性發展障礙、注意力不足症、注意力不足/過動障礙症、擾亂性行為障礙、妄想型人格障礙、類精神型分裂人格障礙、精神分裂型人格障礙、抽動症、妥瑞氏(Tourette’s)症候群、拔毛症、痙攣、癲癇發作、物質依賴、物質濫用、物質戒斷;用於治療及/或預防藥物成癮及/或戒斷;用於治療及/或預防尼古丁成癮及/或戒斷;用於治療及/或預防酒精成癮及/或戒斷之藥劑。
- 一種醫藥組成物,其包含醫藥上可接受之載劑及作為活性成分的治療有效量之如申請專利範圍第1-5項中任一項所定義之化合物。
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| Publication number | Publication date |
|---|---|
| RU2502734C2 (ru) | 2013-12-27 |
| TW201016684A (en) | 2010-05-01 |
| CA2729313A1 (en) | 2010-01-07 |
| CN102159554B (zh) | 2014-09-24 |
| CN102159554A (zh) | 2011-08-17 |
| AU2009266001B2 (en) | 2014-03-27 |
| EP2310374A1 (en) | 2011-04-20 |
| RU2011103759A (ru) | 2012-08-10 |
| BRPI0915834A2 (pt) | 2015-11-03 |
| US8530474B2 (en) | 2013-09-10 |
| HK1158640A1 (zh) | 2012-07-20 |
| AU2009266001A1 (en) | 2010-01-07 |
| CA2729313C (en) | 2016-08-30 |
| AR072547A1 (es) | 2010-09-08 |
| US20110112107A1 (en) | 2011-05-12 |
| JP5417439B2 (ja) | 2014-02-12 |
| JP2011526269A (ja) | 2011-10-06 |
| WO2010000456A1 (en) | 2010-01-07 |
| MX2011000043A (es) | 2011-02-22 |
| EP2310374B1 (en) | 2012-10-31 |
| ES2398625T3 (es) | 2013-03-20 |
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