TW201134820A - Arylsulfonamide CCR3 antagonists - Google Patents
Arylsulfonamide CCR3 antagonists Download PDFInfo
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- TW201134820A TW201134820A TW100109234A TW100109234A TW201134820A TW 201134820 A TW201134820 A TW 201134820A TW 100109234 A TW100109234 A TW 100109234A TW 100109234 A TW100109234 A TW 100109234A TW 201134820 A TW201134820 A TW 201134820A
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Classifications
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- A61K31/445—Non condensed piperidines, e.g. piperocaine
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- A61K31/445—Non condensed piperidines, e.g. piperocaine
- A61K31/4523—Non condensed piperidines, e.g. piperocaine containing further heterocyclic ring systems
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201134820 六、發明說明: 【發明所屬之技術領域】 本發明提供可用於調節CCR3活性之芳基罐醯胺、及其 醫藥組合物。本文亦提供使用其來治療、預防或改善 - CCR3介導之病症、疾病或病狀之一或多種症狀的方法。 t 本文主張對於201〇年3月17日提出申請之標題為 「Arylsulfonamide CCR3 Antagonists」之美國臨時申請案 第6 1/314,971號的優先權。上文所提及申請案之全部内容 以引用方式併入本文中。 【先前技術】 CC趨化因子受體3 (CCR3)係七跨膜G蛋白偶聯受體,其 與多種C-C趨化因子結合,包括嗜酸性球趨化因子 (eotaxin)(CCLll)、嗜酸性球趨化因子-3 (CCL26)、MCP-3 (CCL7)、MCP-4 (CCL13)、及 RANTES (CCL5)。已知 CCR3係在過敏性炎性細胞上表現之主要趨化因子受體, 包括嗜酸性球、嗜鹼性球、肥大細胞及T輔助細胞2型 CD4+細胞(Combadiere 等人,J. Biol. Chem. 1995,270, 1649卜 16494 ; Post 等人,J. Immunol. 1995, 155, 5299-_ 5305)。嗜酸性球與許多炎性疾病之發病機制有關,例如 . 枝氣管哮喘(Durham及 Kay,Clin· Allergy 1985,15,411- 418 ; Kroegel等人,J. Allergy Clin. Immunol. 1994,93, 725-734)、炎性鼻炎(Durham, Clin. Exp. Allergy 1998, 28,增刊 2,11-16.)、異位性皮炎(Leung,J. Allergy Clin. Immunol. 1999,104,S99-108)、及嗜酸性球性胃腸炎 154881.doc 201134820 (Bischoff等人,Am. J.Gastro. 1999, 94, 3521-3529)。已證 實,活性嗜酸性球釋放主要鹼性蛋白(MBP),其阻斷神經 上之抑制性M2毒蕈鹼受體(M2R),使乙醯膽鹼釋放增加, 並加強迷走神經介導之枝氣管收縮(Evans等人,J. Clin. Invest. 1997, 100, 2254-2262)。 許多報導顯示CCR3在過敏性病狀中發揮重要作用。舉 例而言,已報導,在異位性及非異位性哮喘患者中, CCR3及其配體、嗜伊紅趨化因子、嗜伊紅趨化因子-2、 RANTES及MCP-4之mRNA及蛋白質含量均有所增加(Ying 等人,J. Immunol. 1999,99,6321-6329)。亦已證實, CCR3基因缺失會削弱急性實驗哮喘模型中之嗜酸性球募 集(Humbles 等人,Proc. Natl. Acad. Sci. USA 2002,99, 1479-1484 ; Ma等人,J· Clin. Invest. 2002, 109, 621-628 ; Pope等人,J· Immunol. 2005,175,5341-5350 ; Fulkerson 等人,Proc· Natl. Acad. Sci. USA 2006,103,16418-16423)。另外,研究顯示,CCR3拮抗劑(例如抗-CCR3單 株抗體)可阻斷CCR3配體與CCR3轉染子或嗜酸性球之結 合,由此阻斷C-C趨化因子(例如嗜伊紅趨化因子、 RANTES或MCP-3)誘導之嗜酸性球的趨化作用(Heath等 人,J. Clin. Invest. 1997,99,178-184 ; Grimaldi等人,J. Leukocyte Biol. 1999,65,846-853 ; Justice等人,Am. J. Physiol. 2003,284,L168-L178)。因此,CCR3拮抗劑可用 於治療炎性疾病,例如過敏性鼻炎及過敏性哮喘。此外, CCR3拮抗劑亦可用於阻止CCR3表現細胞被一些微生物(例 154881.doc 201134820 如HIV)感染,此乃因已知CCR3係一些微生物之進入共同 受體。 【發明内容】 本文提供式I及π之芳基續酿胺化合物:
⑴ (II) 或其對映異構體、對映異構體之混合物、兩種或更多種非 對映異構體之混合物、互變異構體或兩種或更多種互變異 構體之混合物;或其醫藥上可接受之鹽、溶劑合物、水合 物或前藥; 其中: R1、R2、R3、R4、R5及R6各自獨立地為⑷氫、齒基、氰 基、硝基或胍;(b) Cw烷基、C2_6烯基、c2.6炔基、C3-7環 烷基、C6_M芳基、C7.1S芳烷基、雜芳基或雜環基;(c)氘; 或⑷-C(0)Rla、-C(0)0Rla、-C(0)NRlbRlc、-C(NRla)NRlbRlc、 -ORla、-0C(0)R丨a、-0C(0)0Rla、-〇c(〇)NRlbRlc、 -OC(=NRla)NRlbRlc、-〇S(0)Rla、-〇S(0)2Rla、-〇s(〇)NRlbRlc、 0S(0)2NRlbRle、-NRlbRlc、-NRlaC(0)Rld、-NRlaC(0)0Rld、 -NR,aC(0)NRlbR,c > -NRlaC(=NRld)NRlbRlc > -NRlaS(0)Rld 、-NRlaS(0)2Rld、_NRlaS(0)NRlbRlc、_NRlaS(0)2NRlbRlc 154881.doc 201134820 、-SRla、-S(0)Rla、-S(0)2Rla、-3(0如1111}1^或-8(0)办1111^1(:; R7為(a)氫、鹵基、氰基、硝基、側氧基、或胍;(b) Ck 烷基、C2.6烯基、C2.6炔基、C3-7環烷基、C6.14芳基、C7_15 芳烷基、雜芳基或雜環基;或(c) -C(0)Rla、-C(0)0Rla、 -C(0)NRlbRlc、-C(NRla)NRlbRlc、-〇Rla、-0C(0)Rla、 -0C(0)0Rla、-0C(0)NRlbRlc、-OC(=NRla)NRlbRlc、-〇S(0)Rla、 -OS(0)2Rla、-0S(0)NRlbRlc、-0S(0)2NRlbRlc、-NRlbRlc、 -NRlaC(0)Rld、-NRlaC(0)0Rld、-NRlaC(0)NRlbRlc、 -NRlaC(=NRld)NRlbR丨c、-NRlaS(0)Rld、-NRlaS(〇)2Rld、 -NRlaS(0)NRlbRlc、-NR丨aS(0)2NRlbRlc、-SRU、-S(〇)Rla、 -S(0)2Rla、-8(0輝1|5111<:或-8(0)2抓11)111<:; X係O或S ; Y係-C(0)Rla、-C(S)Rla、-C(0)NRlbRlc、-C(s)NRlbRlc、 -C(0)0Rle、-3(0)1113或-8(0)21113 ; R8係氫、Cw烷基或C3_7環烷基;或 Y及R8與其所連接之N原子一起形成雜芳基或雜環基; Z係-C(0)Rla、-C(S)Rla、-C(0)NRlbRlc、_c(s)NRlb^c、 -C(0)0Rle、-3(0)1113或_8(0)21^ ; m係0至3之整數; R9係氫、CN6烷基或C3_7環烷基; m係0至3之整數; η係1至3之整數; ρ係1至4之整數;且 各Rh、Rib、Ru、Rld及Rle獨立地係氣、q —烧基 154881.doc • 6 - 201134820 烯基、C2·6炔基、C3-7環烷基、C6_M芳基、雜芳基或雜環 基;或每對11115與111(:與其所連接之N原子一起獨立形成雜 芳基或雜環基,前提係RleF為第三丁基或苄基; 其中各烷基、烯基、炔基、環烷基、芳基、芳烷基、雜 環基及雜芳基視需要經一或多個基團取代,其各自獨立地 ' 選自⑷氰基、鹵基及硝基;(b) Cw烷基、C2.6烯基、c26 炔基、C3·7環烷基、CVh芳基、C7·!5芳烧基、雜芳基及雜 %基’其各自視需要進一步經一或多個、在一實施例中1 個、2個、3個或4個取代基Q取代;及⑷_C(〇)Ra、_c(〇)〇Ra、 -C(0)NRbRc、-C(NRa)NRbRc、-〇Ra、-0C(0)Ra、_〇c(〇)〇Ra、 -〇C(0)NRbRe、-〇C(=NRa)NRbRe、_0S(0)Ra、_〇s(〇)2Ra、 -0S(0)NRbRc、-〇S(0)2NRbRC、_NRbRC、_NRac(〇)Rd、 NR C(0)0Rd、_NRaC(0)NRbRc、_NRaC(=NRd)NRbRc、 -NR S(0)Rd、-NRaS(0)2Rd、-NRaS(0)NRbRc、-NRaS(0)2NRbRc、 -SR、-S(0)Ra、_s(〇)2Ra、-S(〇)NRbRc&-S(〇)2NRbRc,其 中Ra、Rb、Rc&Rd各自獨立地為:⑴氫;(ii) 烷基、 c2-6稀基、c2.6块基、C3_7環烷基、C6i4芳基、c7i5芳烷 基、雜芳基或雜環基,其各自視需要經一或多個、在一實 她例中1個、2個、3個或4個取代基q取代;或(iii) Rb及Rc • 與其所連接之N原子一起形成雜環基,其視需要經一或多 個在實施例中1個、2個、3個或4個取代基Q取代; 其中各Q獨立地選自由以下組成之群:(a)氘;(b)氰基、 鹵基、及硝基;(c) Ci-6烷基、C2-6烯基、c2_6炔基、C3-7環 烷基、C6·14芳基、C7.1S芳烷基、雜芳基、及雜環基;及(d) 154881.doc 201134820 -C(0)Re、-C(0)0Re、-C(0)NRfRg、-C(NRe)NRfRg、-ORe、 -0C(0)Re、-OC(0)ORe、-0C(0)NRfRg、-OC(=NRe)NRfRg、 -0S(0)Re、-0S(0)2Re、-0S(0)NRfRg、-0S(0)2NRfRg、 -NRfRg、-NReC(0)Rh、-NReC(0)0Rh、-NReC(0)NRfRg、 -NReC(=NRh)NRfRg、-NReS(0)Rh、-NReS(0)2Rh、-NReS(0)NRfRg、 -NReS(0)2NRfRg、-SRe、-S(0)Re、-S(0)2Re、-S(0)NRfRg、 及-S(0)2NRfRg ; 其中各Re、Rf、Rg、及Rh獨立地係(i)氫;(ii)(:丨_6烷基、 C2-6稀基、C2-6块基、C3_7環烧基、C6-14芳基、C7-15芳烧 基、雜芳基、或雜環基;或(iii) Rf&Rg與其所連接之N原 子一起形成雜環基8 在一實施例中,化合物具有式I,前提係若Y及R8與其所 連接之N原子一起形成雜芳基,則該雜芳基包含至少一個 額外Ο、S、或N原子。 本文亦提供醫藥組合物,其包含本文所揭示之化合物 (例如,式I或II化合物,包括其對映異構體、對映異構體 之混合物、兩種或更多種非對映異構體之混合物、互變異 構體或兩種或更多種互變異構體之混合物;或其醫藥上可 接受之鹽、溶劑合物、水合物或前藥);與一或多種醫藥 上可接受之載劑。 本文進一步提供調節CCR3活性之方法,其包含使CCR3 與本文所揭示之治療有效量之化合物(例如,式I或II化合 物’包括其對映異構體、對映異構體之混合物、兩種或更 多種非對映異構體之混合物、互變異構體或兩種或更多種 154881.doc 201134820 互變異構體之混合物;或其醫藥上可接受之鹽、溶劑合 物、水合物或前藥)接觸。 預防或改善個體之CCR3介導之病 本文另外提供治療 其包含向該個體 如,式I或II化合 症、疾病或病狀的一或多種症狀的方法, 投與治療有效量之本文所揭示化合物(例 物、或其對映異構體、對映異構體之混合物、兩種或更多 種非對映異構體之混合物、互變異構體或兩種或更多種互 變異構體之混合物;或其醫藥上可接受之鹽、溶劑合物、 水合物或前藥)。 【實施方式】 下文將定義諸多術語以有助於理解本文所述之揭示内 容。 通常,本文所用之命名及本文所述有機化學、醫藥化學 及藥理學中之實驗室程序已為業内所熟知且普遍採用。除 非另有定義,否則本文所用之所有技術及科學術語皆具有 與A習此項技術者通常所瞭解含義相同之含義。除非另有 說明,否則在對於本文所用術語存在複數種定義時,以此 部分中之定義為準。 術語「個體」係指動物,包括但不限於靈長類動物(例 如,人類)、牛、豬、綿羊、山羊、馬、狗、貓、兔、大 鼠或小鼠。術語「個體」與「患者」在本文中可互換使 用’其係指(例如)哺乳動物個體,例如人類個體,在一實 施例中係人類。 術s吾「治療(treat、treating及treatment)」意欲包括減輕 154881.doc 201134820 或消除病症、疾病或病狀、或與該病症、疾病或病狀有關 之或多種症狀,或減輕或根除該病症、疾病或病狀本身 之病因。 術語「預防(prevent、preventing及 preventi〇n)」意欲包 括延遲及/或阻止病症、疾病或病狀及/或其伴隨症狀之發 作;使個體並不獲得病症、疾病或病狀;或降低個體獲得 病症、疾病或病狀之風險的方法。 術語「治療有效量」意欲包括當投與時足以防止所治療 病症、疾病或病狀之一或多種症狀發生或使其減輕至一定 程度之化合物的量。術語「治療有效量」亦係指足以引發 研究人員、獸醫、醫生或臨床醫師所尋求之生物分子(例 如’蛋白質、酶、RNA或DNA)、細胞、組織、系統、動 物或人類之生物或醫學反應之化合物的量。 術語「醫藥上可接受之載劑」、「醫藥上可接受之賦形 劑」、「生理上可接受之載劑」或「生理上可接受之賦形 劑」係醫樂上可接受之材料、組合物或媒劑,例如液體 或固體填充劑、稀釋劑、溶劑或囊封材料。在一實施例 中’各組份在以下意義上係「醫藥上可接受的」:與醫藥 調配物之其他成份相容’且適用於與人類及動物之組織或 器官接觸而不會產生過度毒性、刺激、過敏反應、免疫原 性或其他問題或併發症’與合理之效益/風險比相稱。參 見 ’ Remington: The Science and Practice of Pharmacy,第 21 版,Lippincott Williams & Wilkins: Philadelphia, PA, 2005 ; Handbook of Pharmaceutical Excipients,第 5版, 154881.doc 201134820
Rowe 等人編輯,The Pharmaceutical Press and the American Pharmaceutical Association: 2005 ;及 Handbook of Pharmaceutical Additives,第 3 版,Ash 及 Ash 編輯, Gower Publishing公司:2007 ; Pharmaceutical Preformulation and Formulation,第 2版,Gibson編輯,CRC Press LLC: Boca Raton,FL,2009 o 術語「約」或「大約」意指熟習此項技術者所測定之特 定值的可接受誤差,其部分地取決於該值之量測或測定方 式。在某些實施例中,術語「約」或「大約」意指在1、 2、3或4個標準偏差内。在某些實施例中,術語「約」或 「大約」意指在給定值或範圍之50%、20%、1 5%、10%、 9%、8%、7%、6%、5%、40/〇、3〇/〇、20/〇、1%、〇.5〇/0 或 0.05%以内。 術語「活性成份」及「活性物質」係指單獨或與一或多 種醫藥上可接受之賦形劑組合投與至個體以治療、預防或 改善病狀、病症或疾病之一或多種症狀的化合物❶本文所 用之「活性成份」及「活性物質」可為本文所述化合物之 光學活性異構體。 術語「藥物」、「治療劑」&「化學治療劑」係指投與至 個體以治療、肋或改善餘、病症或疾病之—或多種症 狀的化合物或其醫藥組合物。 ’ 術語「隸」係指錢或具支鍵鮮單價料團,其中 炫基可視需要如本文所述經取代。在某些實施例中,烧某 係具有 U20個(Cl.2。)、HO個% 154881.doc 201134820 至6個(Ci·6)碳原子之直鍵飽和單價烴基團、或具有3至2〇 個(C3-2。)、3 至 15個(C3_15)、3 至 10個(C3.i〇)或 3 至 6個(C3.6) 碳原子之具支鏈飽和單價烴基團。本文所用之直鏈Ci 6及 具支鏈C3-6燒基亦稱為「低碳烧基」。烧基之實例包括但不 限於曱基、乙基、丙基(包括所有異構體形式)、正丙基、 異丙基、丁基(包括所有異構體形式)' 正丁基、異丁基、 第二丁基、第三丁基 '戊基(包括所有異構體形式)及己基 (包括所有異構體形式)。舉例而言,Ci·6烷基係指具有丄至 6個碳原子之直鏈飽和單價烴基團或具有3至6個碳原子之 具支鍵飽和單價烴基團。 術語「烯基」係指含有一或多個(在一實施例中〗至5 個,在另一實施例中〗個)碳碳雙鍵之直鏈或具支鏈單價烴 基團。烯基可視需要如本文所述經取代。如彼等熟習此項 技術者所瞭解’術語「稀基」亦涵蓋具有「順式」及「反 式」構型或另一選擇為「2」及「E」構型之基團。除非另 有說明,否則本文所用之術語「烯基」涵蓋直鏈及具支鍵 烯基二者。例如,CM烯基係指具有2至6個碳原子之直鏈 不飽和單價«團或具有3至6個碳原子之具支鍵不飽和單 價煙基團。在某些實施例中,烯基係具有2至2G個(C2.2〇)、 至15個(C2-〗5)、2至1〇個((:2 μ或2至6個(C2 ο碳原子之直 鍵單價烴基團、或具有3錢個 ^個(c3_,。)她6個(C36)碳原子之具支鍵單價煙基團。 稀基之實例包括但不艰7 @ _不限於乙烯基、丙烯-1-基、丙烯_2· 土烯丙基、丁烯基及4_甲基丁烯基。 J54881.doc • J2- 201134820 術語「炔基」係指含有一或多個(在一實施例中丨至5 個、在另一實施例中1個)碳碳三鍵之直鏈或具支鏈單價炉 基團。炔基可視需要如本文所述經取代。除非另有說明, 否則術語「炔基」亦涵蓋直鏈及具支鏈炔基二者。在某此 實施例中,炔基係具有2至20個(C2.20)、2至15個(C2_15)、2 至10個(Cno)或2至6個(C2·6)碳原子之直鏈單價烴基團、戍 具有 3 至 20 個(C3.20)、3至 15 個(C3.15)、3至 10 個(C3-10)或 3至 6個(C3·6)碳原子之具支鍵單價烴基團。块基之實例包括但 不限於乙炔基(《Η)及炔丙基(-CP^CsCH:^舉例而言, Che炔基係指具有2至6個碳原子之直鏈不飽和單價煙基團 或具有3至6個碳原子之具支鏈不飽和單價烴基團。 術語「環烷基」係指環狀單價烴基團,其可視需要如本 文所述經取代。在一實施例中,環烷基可為飽和、及/或 橋接、及/或非橋接、及/或稠合雙環基團。在某些實施例 中,環烷基具有3至20個(C3.20)、3至15個(C3-15)、3至1〇個 (C3.1Q)或3至7個(C3.7)碳原子。環烷基之實例包括但不限於 環丙基、環丁基、環戊基、環己基、環庚基、雙環[2 ι ι] 己基、雙環[2.2.1]庚基、萘烷基及金鋼烷基。 術s吾「芳基」係指含有至少一個芳族碳環之單價單環芳 私基團及/或單價多環芳族基團。在某些實施例中,芳基 具有6至20個(C6_2。)、6至15個((:6.15)或6至1〇個(C6_〗Q)環原 子。芳基之實例包括但不限於苯基、萘基、苐基、甘菊藍 基、蒽基、菲基、芘基、聯苯及三聯苯。芳基亦係指雙環 或三環碳環中該等環中之—者係芳族環且其他環可為 154881.doc -13- 201134820 :和之'部分不飽和之或芳族環’例如,二氫萘基節 基或四氫萘基(四氫化萘基在某些實施例 肀,方基可視需要如本文所述經取代。 術語「芳院基”戈「芳基·烧基」係指經芳基取代之單 價貌基。在某些實施例中,烧基及芳基部分視需要如本文 所述經取代。 術語「烧氧基」係指基團「视」,其中R係燒基或環烧 基。舉例而言,烧氧基包括甲氧基、乙氧基、正丙氧基、 異丙氧基、正丁氧基、第三丁氧基、第二丁氧基、正戊氧 基、正己氧基、及12-二甲基丁氧基。 術語「雜芳基」係指含有至少一個芳族環之單價單環芳 族基團及/或多環芳族基團,其中至少一個芳族環在環中 含有一或多個獨立地選自〇、8及1^之雜原子。雜芳基經由 芳族環結合至分子之其餘部分。雜芳基之每一環可含有一 個或兩個Ο原子、一個或兩個s原子、及/或〖至4個^^原子, 前提係每一環中之雜原子的總數係4或更小且每一環含有 至少一個碳原子。在某些實施例中,雜芳基具有5至2〇 個、5至15個或5至10個環原子。單環雜芳基之實例包括但 不限於呋喃基、咪唑基、異噻唑基、異噁唑基、噁二唑 基、°惡二°坐基、°惡°坐基、°比°秦基、批°坐基、塔嗪基、η比咬 基、嘧啶基、吡咯基、噻二唑基、噻唑基、噻吩基、四唑 基、三嗪基及三唑基。雙環雜芳基之實例包括但不限於苯 并呋喃基、笨并咪唑基、苯并異噁唑基、苯并比喃基、苯 并噻二唑基、笨并噻唑基、苯并噻吩基、笨并三唑基、苯 154881.doc •14· 201134820 并噁唑基、呋喃并吡啶基、咪唑并吡啶基、咪唑并噻唑 基、吲嗪基、吲哚基、吲唑基、異苯并呋喃基、異苯并噻 吩基、異吲哚基、異喹啉基、異噻唑基、萘啶基、噁唑并 比定基太°秦基、喋咬基、嘌吟基、〇比咬并η比。定基、吧〇各 並吡啶基、喹啉基、喹喔啉基、喹唑啉基、噻二唑并嘧啶 基及噻吩并吡啶基。三環雜芳基之實例包括但不限於吖啶 基、苯并叫卜朵基、味唾基、二苯并吱喊基、蔡嵌間二氣雜 本基、菲咯啉基、菲啶基、吩吡嗪基、吩嗪基、吩噻嗪 基、吩-惡嗓基及,山基。在某些實施例中,雜芳基亦可視需 要如本文所述經取代。 術語「雜環基」或「雜環」係指含有至少一個非芳族環 之單價單環非芳族環系統及/或多環系統,其中非芳族環 原子中之一或多者係獨立地選自〇、3或1^之雜原子;且其 餘環原子係碳原子。在某些實施例中,雜環基或雜環基圏 具有3至20個、3至15個、3至1〇個、⑴個、㈤個、或$ 至6個環原子。雜環基經由非芳族環結合至分子之其餘部 分。在某些實施例中,雜環基係、單環、雙環、三環或四環 系統,其Τ包括稠合或橋接環系统,且其中氮或硫原子可 視需要經氧化,氮原子可視需要經四㈣化,且-些環可 部分或全部係飽和、或芳族環。雜環基可在任-雜原子或 故原子處連接至主結構,此可產生穩定化合物。此等雜環 基團之實例包括但不限於氮呼基、苯并二㈣基、笨并間 二氧環戊稀基一__1州、苯并以酮基、苯并。比嗓 酮、本并吨味基、苯并四氫吱嚼基、笨并四氮嗟吩基、笨 154881.doc -15- 201134820 并噻喃基、苯并噁嗪基、j3_„弄啉基、苯并二氫^比喃基、色 酮基、4啉基、香豆素基、十氫異喹啉基、二氫苯并異噻 嗪基、二氫苯并異噁嗪基、二氫呋喃基、二氫異吲哚基、 一氫吡喃基、二氫吡唑基、二氫吡嗪基、二氫吡啶基、二 氫嘧啶基、二氫吡咯基、二氧戊環基、丨,4-二噻烷基、呋 喃酮基、咪唑啶基、咪唑啉基、二氫吲哚基、異苯并四氫 呋喃基、異苯并四氫噻吩基、異苯并二氫η比喃基、異香豆 素基、異二氫吲哚基、異噻唑啶基、異噁唑啶基、嗎啉 基、八氫’嗓基、八氫異吲哚基、噁唑啶酮基、噁唑啶 基、環氧乙烷基、六氫吡嗪基、六氫吡啶基、4_六氫吡啶 酮基、吡唑啶基、吡唑啉基、吡咯啶基、吡咯啉基、奎寧 環基、四氫呋喃基、四氫異喹啉基、四氫吡喃基、四氫噻 吩基、硫嗎啉基、噻唑啶基、四氫喹啉基及^彡三噻烷 基。在某些實施例中,雜環基團亦可視需要如本文所述經 取代。 術語「齒素」、「函化物」或r _基」係指氣、氣、漠及/ 術語「視需要經取代」意指基團(例如烷基、烯基、炔 基、環烷基、芳基、芳烷基、雜芳基、或雜環基)可經一 或多個獨立地選自以下之取代基取代:例如,(a) Ci 6烷 基、C2.6烯基、c2.6快基、〇3 7環烧基、c6丨4芳基、丨5芳 烧基、雜芳基及雜環基’其各自視需要經—或多個、在一 實施例中1個、2個、3個或4個取代基Q取代;及(b)函基、 氰基(-CN)、硝基(_N〇2)、-C(0)Ra、-C(0)0Ra、、 154881.doc -16- 201134820 -C(NRa)NRbRc、-ORa、-0C(0)Ra、-0C(0)0Ra、-0C(0)NRbRc、 -OC(=NRa)NRbRc、-0S(0)Ra、-0S(0)2Ra、-0S(0)NRbRc、 -0S(0)2NRbRc、-NRbRc、-NRaC(0)Rd、-NRaC(0)ORd、 -NRaC(0)NRbRc、-NRaC(=NRd)NRbRc ' -NRaS(0)Rd、 -NRaS(0)2Rd、-NRaS(0)NRbRc、-NRaS(0)2NRbRc、-SRa、 -S(0)Ra、-S(0)2Ra、-S(0)NRbRc及-S(0)2NRbRc,其中 Ra、 Rb、{^及!^各自獨立地為:(i)氫;(ii) Cw烷基、C2.6烯 基、C2_6炔基、C3_7環烷基、C6_14芳基、C7-15芳烷基、雜芳 基或雜環基,其各自視需要經一或多個、在一實施例中1 個、2個、3個或4個取代基Q取代;或(iii) Rb及Rl其所連 接之N原子一起形成雜芳基或雜環基,其視需要經一或多 個、在一實施例中1個、2個、3個或4個取代基Q取代。除 非另有說明,否則本文所用之所有可經取代之基團皆「視 需要經取代」。本文所用之術語「視需要經取代」亦意欲 包括使用氘原子取代氫。 在一實施例中,Q各自獨立地選自由以下組成之群:(a) 氘;(b)氰基、鹵基及硝基;及(c) CN6烷基、C2.6烯基、C2.6 快基、C3-7環烧基、C6-14芳基、C7-I5芳炫基、雜芳基及雜 環基;及(d) -C(0)Re、-C(0)0Re、-C(0)NRfRg、-C(NRe)NRfRg、 -ORe、-0C(0)Re、-0C(0)0Re、-0C(0)NRfRg、-OC(=NRe)NRfRg、 _0S(0)Re、-0S(0)2Re、-0S(0)NRfRg、-0S(0)2NRfRg、 -NRfRg、-NReC(0)Rh、-NReC(0)0Rh、-NReC(0)NRfRg、 -NReC(=NRh)NRfRg、-NReS(0)Rh、-NReS(0)2Rh、-NReS(0)NRfRg、 NReS(0)2NRfRg、-SRe、-S(0)Re、-S(0)2Re、-S(0)NRfRg 154881.doc •17· 201134820 及-S(〇)2NRfRg;其中Re、Rf、Rg及Rh各自獨立地為:⑴ 氫;(ii) C丨·6烷基、C2.6烯基、c2 6炔基、c3 7環烷基、C6 14 芳基、C^5芳烷基、雜芳基或雜環基;或…〇 Rf&Rg與其 所連接之N原子一起形成雜芳基或雜環基。 在某些實施例中,「光學活性」及「對映異構體活性」 係指分子集合,其具有不小於約5〇%、不小於約㈣、不 小於約80%、不小於約90%、不小於約91%、不小於約 92%、不小於約㈣、不小於約94%、不小於約㈣、不小 於約96。/。、不小於約97%、不小於約嫩、不小於約99%、 不小於約99.5%或不小於約99.8%之對映異構體過量。在某 些實施例中,基於所討論外消旋物之總重量,化合物包含 約95。/。或更多一種對映異構體及約5%或更少另一對映異構 體。 在闡述光學活性化合物時,使用字首尺及8來表示分子之 對掌性中心絕對組態。使用(+)及㈠來表示化合物之旋光 性,亦即,由光學活性化合物旋轉偏振光平面之方向。㈠ 字首表示化合物係左旋的,亦即,化合物向左或以逆時針 方向旋轉偏振光平面。(+)字首表示化合物係右旋的,亦 即,化合物向右或以順時針方向旋轉偏振光平面。然而, 旋光性之符號(+)及㈠與分子之絕對組態尺及8無關。 術语「溶劑合物」係指進一步包括藉由非共價分子間力 結合之化學計量量或非化學計量量之溶劑的本文所提供化 合物或其鹽。當溶劑為水時,溶劑合物係水合物。 當用於生物材料(例如核酸分子、多肽、宿主細胞及諸 154881.doc • 18· 201134820 如此類)時,術語「天然存在」或「天然」係指自然界中 發現而非由人類製備之材料。類似地,「非天然存在」或 「非天然」係指未在自然界中發現或經人類進行結構修飾 或合成之材料。 術語「CCR3」係指CC趨化因子受體3或其變體,其能夠 調介多種趨化因子之細胞反應,該等趨化因子包括但不限 於嗜伊紅趨化因子(CCL11)、嗜伊紅趨化因子-3 (CCL26)、MCP-3 (CCL7)、MCP-4 (CCL13)及 RANTES (CCL5)。CCR3變體包括與天然CCR3實質上同源之蛋白 質,亦即,與天然CCR3之胺基酸序列相比具有一或多個 天然或非天然存在之胺基酸缺失、插入或取代之蛋白質 (例如,CCR3衍生物、同源物及片段)。CCR3變體之胺基 酸序列與天然CCR3至少約80%—致、至少約90%—致、或 至少約95%—致。 術語「CCR3拮抗劑」係指(例如)部分或完全阻斷、降 低、阻止、抑制或下調CCR3活性之化合物。術語「CCR3 结抗劑」亦係指結合CCR3受體、延遲其激活、使其失活 或降低其敏感性之化合物。CCR3拮抗劑可藉由干擾CCR3 受體與其趨化因子配體之相互作用來發揮作用,該配體包 括但不限於嗜酸性球趨化因子(CCL11)、嗜酸性球趨化因 子-3 (CCL26) > MCP-3 (CCL7)、MCP-4 (CCL13)及 / 或 RANTES (CCL5)。 術語「CCR3介導之病症或疾病」及「CCR3介導之病 狀、病症或疾病」係指特徵在於CCR3活性不適當(例如, 154881.doc -19- 201134820 低於正常或高於正常)之病狀、病症或疾病。不適當之 CCR3功能活性可能由以下情況引起:正常情況下不表現 CCR3之細胞中之CCR3表現,CCR3表現增加或細胞内激活 程度增加,導致(例如)炎性及免疫相關病症或疾病;或 CCR3表現降低。CCR3介導之病狀、病症或疾病可能完全 或部分地由不適當之CCR3活性介導。具體而言,CCR3介 導之病狀、病症或疾病係調節CCR3受體對潛在之病狀或 病症具有一定效應者’例如,CCR3抬抗劑或激動劑使至 少一些所治療患者發生一定改善。 化合物 本文提供用於調節CCR3活性之芳基磺醯胺。本文亦提 供包含該等化合物之醫藥組合物及使用該等化合物及組合 物治療CCR3介導之病症、疾病或病狀的方法。 在一實施例中, 本文提供式I及II之芳基磺醯胺化合物:
物或前藥; I54881.doc -20· 201134820 其中:
Rl、R2、R3、R4、R5及R6各自獨立地為⑷氫、氘、鹵 基、氰基、硝基或胍;(b) CN6烷基、C2_6烯基、c26块 基、C3·7環烧基、Cbi4芳基、Cn5芳烧基、雜芳基或雜環 基;或(c) -C(0)Rla、-C(0)0Rla、-C(0)NRlbRlc、-C(NRu)NRlbRic 、-ORla、_OC(0)Rla、-OC(0)ORla、-0C(0)NRlbRlc、 -OC(=NRla)NRlbR,c ' -OS(0)Rla > -0S(0)2R,a > -0S(0)NRlbRlc 、-OS(0)2NRlbRle、-NRlbRlc、-NRlaC(0)Rld、-NRlaC(0)0Rld、 _NRlaC(0)NRlbRlc、-NRlaC(=NRld)NRlbRlc、-NRlaS(0)Rld、 -NRlaS(0)2Rld、-NRlaS(0)NRlbRlc、-NRlaS(0)2NRlbRlc、 -SRla、-S(0)Rla、-S(0)2Rla、-S(0)NRlbRlc^-S(0)2NRlbRlc ; R7為(a)氫、鹵基、氰基、硝基、側氧基、或胍;(b) Cw 烷基、C2_6烯基、C2.6炔基、C3.7環烷基、C6.14芳基、C7.15 芳烷基、雜芳基或雜環基;或(c) -C(0)Rla、-C(0)0Rla、 -C(0)NRlbRlc、-C(NRla)NRlbRlc、-ORla、-0C(0)Rla、 _0C(0)0Rla、-0C(0)NRlbRlc、-OC( = NRla)NRlbRlc、 -0S(0)Rla、-0S(0)2Rla、-〇S(0)NR丨bRlc、-0S(0)2NRlbRlc、 -NRlbRlc、-NRlaC(0)R丨d、-NRlaC(0)0Rld、-NRlaC(0)NRlbRlc、 -NRlaC(=NRld)NRlbRlc、-NRlaS(0)Rld、-NRlaS(0)2Rld、 -NRlaS(0)NRlbRlc、-NRlaS(0)2NRlbRlc、-SRla、-S(0)Rla、 -S(0)2Rla、-S(0)NRlbRlc或-S(0)2NRlbRlc ; X係O或S ; Y係-C(0)Rla、-C(S)Rla、-C(0)NRlbRlc、-C(S)NRlbRlc、 -C(0)0Rle、-S(0)Rla4-S(0)2Rla ; 15488i.doc •21· 201134820 R8係氫、C!·6烷基或Gy環烷基;或 Υ及R*與其所連接之Ν原子—起形成”基或 Z#.-C(0)Rla > -C(S)R*a . .C(〇)NRibRlc ^ .C(S)nrI"; -C(0)0Rle、-S(0)Rla4_S(〇)2Rla ; m係0至3之整數; R9係氫、Cw烷基或c3_7環烷基; m係0至3之整數; η係1至3之整數; ρ係1至4之整數;且 各…、^、^…及^蜀立地係氫…说基^ 稀基、C2.6炔基、c3.7環烷基、C6.丨4芳基、雜芳基或雜: 基;或每對及Rie與其所連接之N原子一起獨立形成雜 芳基或雜環基’前提係15^不為第三丁基或节基; 其中各烷基、烯基、炔基、環烷基、芳基、芳烷基、雜 環基及雜芳基視需要經一或多個基團取代,其各自獨立地 選自⑷氰基、鹵基及硝基;(b) Cw烷基、C2-6烯基、c2 6 炔基、C3·7環烧基、ον μ芳基、C7·!5芳院基、雜芳基及雜 環基,其各自視需要進一步經一或多個、在一實施例中1 個、2個、3個或4個取代基Q取代;及(c) _c(0)Ra、-C(0)0Ra、 -C(0)NRbRc、-C(NRa)NRbRc、-〇Ra、-〇C(0)Ra、-0C(0)0Ra、 -OC(0)NRbRc、-〇C(=NRa)NRbRc、-〇S(0)Ra、-0S(0)2Ra、 -OS(0)NRbRc、-0S(0)2NRbRc、-NRbRc、-NRaC(0)Rd、 -NRaC(0)0Rd、-NRaC(0)NRbRc、-NRaC(=NRd)NRbRc、 -NRaS(0)Rd、-NRaS(0)2Rd、-NRaS(0)NRbRc、-NRaS(0)2NRbRc 154881.doc -22- 201134820 、-SR、-S(0)R、-S(〇)2Ra、_s(〇)NRbRC& _s(〇)2NRbRC, 其中Ra、Rb、Rc及Rd各自獨立地為:⑴氮;(H) ^ 6烧基、 c2-6烯基、c2.6炔基、C3_7環烷基、C6u芳基、C7i5芳烷 基、雜芳基或雜環基,其各自視需要經一或多個、在一實 施例中1個、2個、3個或4個取代基Q取代;或(iH) Rb&RC 與其所連接之N原子一起形成雜環基,其視需要經一或多 個、在一實施例中1個、2個、3個或4個取代基Q取代; 其中各Q獨立地選自由以下組成之群:(a)氘;(b)氰基、 鹵基、及硝基;(c) Cw烷基' C26烯基、C26炔基、C37環 烷基、C6.M芳基、c'丨5芳烷基、雜芳基、及雜環基;及(d) -C(0)R、-C(0)0Re、-C(〇)NRfRg、-C(NRe)NRfRg、-〇Re、 -0C(0)R ' -OC(0)〇Re s -0C(0)NRfR8 ' -OC(=NRe)NRfRg ' -0S(0)R、-〇S(〇)2Re、_〇s(〇)NRfRg、-〇S(〇)2NRfRg、 -NR Rg、-NReC(〇)Rh、,NReC(0)0Rh、-NReC(0)NRfRg、 -NR C(-NR )NRfRg、-NReS(0)Rh、-NReS(0)2Rh、-NReS(0)NRfRg 、-NReS(0)2NRfRg、-SRe、-S(〇)Re、-S(〇)2Re、-S(0)NRfRg 、及-S(0)2NRfRg ; 其中各Re、Rf、Rg、及Rh獨立地係⑴氫;⑴)烷基、 c2-6烯基、c2.6炔基、(:3·7環烷基、c6丨4芳基、c7丨5芳烷 基、雜芳基、或雜環基;或(iii) Rf&Rg與其所連接之N原 子一起形成雜環基。 在另一實施例中,本文提供式la及IIa之芳基磺醯胺化合 物: 154881.doc -23- 201134820
或其對映異構體、對映異構體之混合物、兩種或更多種非 對映異構體之混合物、互變異構體或兩種或更多種互變異 構體之混合物,或其醫藥上可接受之鹽、溶劑合物、水合 物或前藥; R'
R 其中 Rl、R2、R3、r4 X、Y、Z、m、n、及p如本文所
Rlb、R】c、Rld、R丨6 義;
Rd係氘;且 q係〇至3之整數。 式 I、II、la及 Ila 中之基團 Rl、r2、r3、r4、r5、R< R7、R8、R9、R丨、、Ru、Rld、R,e、χ、γ z、订 n p及q進—步疋義於本文所述之實施例中。該等基團 本文所提供實施例之所有組合皆屬於本發明範圍内。 在某些實施例中,R1係氫ϋ基、氰基、石肖基、 胍。在某些實施例中,D 1 β, 卜 R係氳。在某些實施例中,R1 *在某二實施例中’ R1係鹵基。在某些實施例中, 說或氣。在某些實施例中,R1係視需要如本文所述經取 Mm某些實施例中’ Rl係視需要經請、_ 個齒基取代之Cl.成基。在某些實施例中,Ri係甲基、 154881.doc •24- 201134820 基、丙基(例如,正丙基及異丙基)、丁基(例如,正丁基、 2-丁基、異丁基或第三丁基)、戊基(例如,正戊基、2戊 基、3-戊基、2_甲基丁基、3·甲基丁基、u二甲基丙 基、1,2-二甲基丙基或2,2_二曱基丙基)。在某些實施例 中,R1係甲基。在某些實施例中,Ri係視需要如本文所述 經取代之(^·6烷氧基。在某些實施例中,Rl係視需要經i 個、2個或3個鹵基取代之C w炫氧基。在某些實施例中, R1係視需要如本文所述經取代之C,_6烷硫基。在某些實施 例中,R1係視需要經1個、2個或3個鹵基取代之c16烷硫 基。在某些實施例中’ R1係CM烯基、C2.6炔基、c3_7環烷 基、C6」4芳基、C7·!5芳烧基、雜芳基、或雜環基,其各自 視需要如本文所述經取代。在某些實施例中,Rl 係-C(0)Rla、-C(0)ORla、-C(0)NRlbRlc、-C(NRla)NRlbRlc、 -ORla、-0C(0)Rla、-0C(0)0Rla、-〇C(0)NRlbRlc、-〇C(=NRla)NRlbRlc 、-〇S(0)Rla、-〇S(0)2Rla、-0S(0)NRlbRlc、-〇S(0)2NRlbRlc、 -NRlbRu、-NRlaC(0)Rld、-NRlaC(0)0Rld、-NRlaC(0)NRlbRlc 、-NRlaC(=NRld)NRlbRlc、-NRlaS(0)Rld、-NRlaS(0)2Rld ' -NR,aS(0)NRlbRlc ' -NRlaS(0)2NRlbRlc ' -SRla ' -S(0)R,a ' S(0)2Rla、-S(0)NRlbRlc 或-S(0)2NRlbRlc ;其中 Rla、
Rlb、Rle&Rld各自如本文所定義。 在某些實施例中,R2係氫、氘、鹵基、氰基、硝基、或 胍。在某些實施例中,R2係氫。在某些實施例中,R2係鹵 基。在某些實施例中,R2係氟或氣。在某些實施例中,r2 係視需要如本文所述經取代之Cw烷基。在某些實施例 154S81.doc •25· 201134820 中’ R2係視需要經1個、2個或3個鹵基取代之Cw烧基。在 某些實施例中,R2係甲基、乙基、丙基(例如,正丙基及 異丙基)、丁基(例如,正丁基、2-丁基、異丁基或第三丁 基)、戊基(例如,正戊基、2-戊基、3-戊基、2-甲基丁 基、3-曱基丁基、ι,ι_二甲基丙基、12_二曱基丙基或2 2_ 二甲基丙基)。在某些實施例中,R2係甲基。在某些實施 例中’ R2係視需要如本文所述經取代之C16烷氧基。在某 些實施例中,R2係視需要經1個、2個或3個鹵基取代之Cw 院氧基。在某些實施例中,R2係視需要如本文所述經取代 之烧硫基。在某些實施例中,R2係視需要經1個、2個 或3個鹵基取代之Cl_6烷硫基。在某些實施例中,尺2係€2 6 稀基、C2.6炔基、(:3_7環烷基、C6·丨4芳基、C7·丨5芳烷基、雜 芳基、或雜環基’其各自視需要如本文所述經取代。在某 些實施例中,R2係 _C(0)Rla、-C(0)〇Rla、_C(〇)NRlbRlc、 -C(NRU)NRlbRlc、-OR丨a、-〇C(〇)Rla、_〇C(〇)〇Rla、 -〇C(0)NR,bRlc , -〇C(=NRla)NRlbRlc . -〇S(0)R,a ^ -0S(0)2R,a ' -〇S(0)NRlbRlc , -〇S(0)2NR,bR,c > -NR,bRlc > -NR,aC(0)R,d ' -NRlaC(〇)〇Rld . -NRlaC(0)NRlbR,c . -NRlaC(=NRld)NRlbR,c ' -NRlaS(〇)R^ , .NR^S(0)2R,d ^ -NR,aS(0)NR,bRlc ^ -NRlaS(〇)2NRibRu、_SRu、_s(〇)Ru、s(〇)2Rla、_s(〇)NRlbRlc 或_S(〇)2NR〗bRic ;其中、Rib、Rlc及Rld各自如本文所 定義。 在某些實施例中,R3係氫、氘、鹵基、氰基、硝基、或 脈在某些實施例中,R3係氣。在某些實施例中,R3係鹵 15488I.doc -26· 201134820 基。在某些實施例中,R3係氟或氯》在某些實施例中,R3 係視需要如本文所述經取代之Cw烷基。在某些實施例 中’ R3係視需要經1個、2個或3個鹵基取代之Cl6烧基。在 某些實施例中,R3係甲基、乙基、丙基(例如,正丙基及 異丙基)、丁基(例如,正丁基、2 -丁基、異丁基咬第=丁 基)、戊基(例如,正戊基、2-戊基、3-戊基、2_甲基丁 基、3-甲基丁基、ι,ΐ-二曱基丙基、丨,2_二曱基丙基或22_ 二甲基丙基)。在某些實施例中,R3係甲基。在某些實施 例中,R3係視需要如本文所述經取代之Cl·6烷氧基。在某 些實施例中,R3係視需要經1個、2個或3個卤基取代之Ci 6 烧氧基。在某些實施例中,R3係視需要如本文所述經取代 之(^_6烷硫基。在某些實施例中,R3係視需要經1個、2個 或3個鹵基取代之C ! _6烧硫基。在某些實施例中,R3係6 烯基、C2·6炔基、C:3·7環统基、C:6·!4芳基、C7_丨5芳院基、雜 芳基、或雜環基,其各自視需要如本文所述經取代。在某 些實施例中,R3係-C(〇)Rla、-C(0)〇Rla、_c(0)NRlbRlc、 -C(NRla)NRlbR,c . -〇Rla> -0C(0)Rla. -OC(0)OR,a. -0C(0)NRlbRlc > -OC(=NR,a)NRlbRlc > -0S(0)Rla ^ -0S(0)2Rla . _0S(0)NRlbRlc、_〇s(〇)2NR丨bRlc、-NRlbRlc、-NRlaC(0)Rld、 -NRlaC(0)〇Rld , -NRlaC(0)NRlbRlc ^ -NRlaC(=NRld)NR,bRIc > -NRlaS(0)Rld . -NRlaS(0)2Rld ^ -NRlaS(0)NRlbRlc .
NRlaS(0)2NRlbRle、_SRla、-S(0)Rla、-S(0)2Rla、-S^NR1 bRU 或-S(0)2NRlbR,c ;其中Ria、Rib、Rlc及Rld各自如本文所 定義。 154881.doc ·27· 201134820 在某些實施例中,R4係氫、氘、鹵基、氰基、硝基、或 胍。在某些實施例中,R4係氫。在某些實施例中,R4係鹵 基。在某些實施例中,R4係氟或氯。在某些實施例中,R4 係視需要如本文所述經取代之C 1 -(5烧基。在某些實施例 中,R4係視需要經1個、2個或3個鹵基取代之Cw烷基。在 某些實施例中,R4係甲基、乙基、丙基(例如,正丙基及 異丙基)、丁基(例如,正丁基、2-丁基、異丁基或第三丁 基)、戊基(例如,正戊基、2-戊基、3 -戊基、2-曱基丁 基、3 -甲基丁基、ι,ι_二甲基丙基、ι,2-二甲基丙基或2,2-二曱基丙基)。在某些實施例中,R4係甲基。在某些實施 例中,R4係視需要如本文所述經取代之C〗_6烷氧基。在某 些實施例中’ R4係視需要經1個、2個或3個鹵基取代之Cw 烷氧基。在某些實施例中,R4係視需要如本文所述經取代 之C!·6烧硫基。在某些實施例中,R4係視需要經1個、2個 或3個鹵基取代之Cw烷硫基。在某些實施例中,R4係c2.6 烯基、C2·6炔基、(:3.7環烷基、CV丨4芳基、C7·丨5芳烷基、雜 芳基、或雜環基,其各自視需要如本文所述經取代。在某 些實施例中,R4係-C(0)Rla、-C(0)0Rla、-C(0)NRlbRlc、 -C(NRla)NRlbRlc、-〇Rla、-0C(0)Rla、-0C(0)0Rla、 -0C(0)NRlbRlc、-〇C(=NRla)NRlbRle、-0S(0)Rla、-〇S(0)2Rla、 -0S(0)NRlbRle、-〇S(0)2NRlbRle、-NRlbRle、-NRlaC(0)Rld、 -NRlaC(0)0Rld、-NRlaC(0)NRlbRlc、-NRlaC(=NRld)NRlbRlc、 -NRlaS(0)Rld、-NRlaS(0)2Rld、-NRlaS(0)NRlbRlc、 -NRlaS(0)2NR,bRlc ^ -SRla ' -S(0)RIa > -S(0)2Rla > -S(0)NR,bR,c 154881.doc • 28- 201134820 各自如本文所 或-S(0)2NRlbRlc ;其巾 Ru、Rib、Ric及 Rld 定義。 在某些實施例中,R5係氫、氘、函基、氰基、硝基、或 胍。在某些實施財,r5係氫。在某些實施例中,r5係齒 基。在某些實施例中,R5係氟或氣。在某些實施例中,R5 係視需5要如本文所述經取代之匕·6烷基。在某些實施例 中,R5係視需要經丨個、2個或3個鹵基取代之烷基。在 某些實施例中,R5係甲基、乙基、丙基(例如,正丙基及 異丙基)、丁基(例如,正丁基、2_丁基、異丁基或第三丁 基)、戊基(例如,正戊基、2-戊基、3-戊基、2_曱基丁 基、3-甲基丁基、丨卜二曱基丙基、12_二甲基丙基或2,2_ 二曱基丙基)。在某些實施例中,R5係甲基。在某些實施 例中’ R5係視需要如本文所述經取代之Cl_6烷氧基。在某 些實施例中’ R5係視需要經i個、2個或3個鹵基取代之Cl_6 烧氧基。在某些實施例中’ R5係視需要如本文所述經取代 之烧硫基。在某些實施例中,R5係視需要經1個、2個 或3個鹵基取代之Cl_6烷硫基。在某些實施例中,R5係c2 6 烯基、C2-6炔基、C3-7環烧基、C6-14芳基、C7-15芳烧基、雜 芳基、或雜環基’其各自視需要如本文所述經取代。在某 些實施例中,R5係-C(0)Rla、-C(0)0Rla、-C(0)NRlbRlc、 -C(NRla)NRlbRlc、_〇Rla、_〇C(0)Rla、_0C(0)0Rla、 0C(0)NRlbRlc、-〇C(=NRla)NRlbRlc、-0S(0)Rla、-OS(0)2Rla、 -OS(0)NRlbRlc、-〇S(0)2NRlbRlc、-NRlbRlc、-NRlaC(0)Rld、 -NRlaC(0)0Rld、-NRlaC(0)NRlbRlc、-NRlaC(=NRld)NRlbRlc、 154881.doc •29· 201134820 -NR丨aS_ld、-NR,aS(0)2Rld、-NR,aS(〇)NRlbR丨c、撕>)2 NRlbRk、-SRla、-S(0)Rla、-S(0)2R“、_s(〇)NRlbR】, 或-S(0)2NR丨bR〗c ;其中R丨a、R丨b、R丨c及Rid各自如本文所 定義。 在某些實施例中,R1、R2、R3、R4、及以中之兩者係鹵 基或視需要如本文所述經取代之Cw烷基。在某些實施例 中,R〗、R2、R3、R4、及R5中之兩者係鹵基或視需要如本 文所述經取代之C〗.6烷基,且其餘三者係氫。在某些實施 例中,R1、R2、R3、R4及R5中之二者係氯或甲基。在某些 實施例中,R丨、R2、R3、R、及之二者係氣或甲基, 且其餘三者係氫。在某些實施例中,Rl、R3、及R5係氫, 且R2及R4係鹵基或視需要如本文所述經取代之Cw烷基。 在某些實施例中,R〗、R3、及r5係氫或氘,且尺2及尺4係函 基或視需要如本文所述經取代之Gw烷基。在某些實施例 中,R1、R3及R5係氫,且R2&R4係氯或甲基。在某些實施 例中,R1、R3及R5係氫,且尺2及R4係氯。在某些實施例 中,R1、R3及R5係氫,且R2&R4係曱基。在某些實施例 中R尺、及尺係氫,且R1及R4係鹵基或視需要如本文 所述、·至取代之C丨—烧基。在某些實施例中,R2、R3及r5係 氮’且Rl&R4係'氣或甲基。在某些實施例中,R2、R3及R5 係風,且Rl&R4係氣。在某些實施例中,R2、R3及r5係 氫,且R1及R4係甲基。 在某些實施例中,R6係氫、齒基、氰基、硝基、或胍。 在某些實施例中,r6係氫。在某些實施例巾,尺6係齒基。 154881.doc 201134820 在某些實施例中,R6係氟或氣。在某些實施例中,R6係氰 ^在某些實施例中,R6係硝基。在某些實施例中,R6係 視6需要如本文所述經取代之Ci·6烷基。在某些實施例中, R係視需要經1個、2個或3個鹵基取代之烷基。在某些 實施例中,R6係甲基、乙基、丙基(例如,正丙基及異丙 基)' 丁基(例如,正丁基、2_ 丁基、異丁基或第三丁基)、 戊基(例如,正戊基、2-戊基、3-戊基、2-曱基丁基、3_甲 基丁基、1,1-二甲基丙基、二甲基丙基或2,2_二甲基丙 基)。在某些實施例中,R6係曱基。在某些實施例中,R6 係視需要如本文所述經取代之Cl_6烷氧基。在某些實施例 中’ R6係視需要經1個、2個或3個鹵基取代之Cl_6烷氧基。 在某些實施例中’ R6係視需要如本文所述經取代之Ci 6烷 硫基。在某些實施例中,R6係視需要經1個、2個或3個画 基取代之(^·6烷硫基。在某些實施例中,以係^“烯基' C2·6快基、C3_7環炫基、C6.!4芳基、C7_丨5芳院基、雜芳基、 或雜環基’其各自視需要如本文所述經取代。在某些實施 例中,R6係 _C(0)Rla、-C(0)0Rla、-C(0)NRlbRlc、-C(NRla) NRlbRlc、-〇Rla、-〇C(0)Rla、-0C(0)0Rla、-〇C(〇)NRlbRlc、 -OC(=NRla)NRlbRlc、-0S(0)Rla、-0S(0)2Rla、-〇S(〇)NRlbRlc、 -〇S(0)2NRlbRlc、-NRlbRlc、-NRlaC(0)Rld、-NRlaC(0)0Rld、 -NRlaC(0)NRlbRlc、-NRlaC(=NRld)NRlbRlc、-NRlaS(0)Rld、 -NRlaS(0)2Rld、-NRlaS(0)NRlbRlc、-NRlaS(0)2NRlbRlc、 SRla、-S(0)Rla、-S(0)2Rla、-S(0)NRlbRlc^-S(0)2NRlbRlc ; 其中Rla、Rlb、Rle及Rld各自如本文所定義。 154881.doc •31- 201134820 在某些實施例中,R7係氫、鹵基、氰基、硝基、側氧基 或胍。在某些實施例中,R7係氫。在某些實施例中,&7係 鹵基。在某些實施例中,R7係氟或氣。在某些實施例中, R係氰基。在某些實施例中,R7係硝基。在某些實施例 中,R係側氧基。在某些實施例中,R7係視需要如本文所 述經取代之C w烷基》在某些實施例中,R7係視需要經i 個、2個或3個鹵基取代之Ci 6烷基。在某些實施例中,R7 係曱基、乙基、丙基(例如,正丙基及異丙基)、丁基(例 如,正丁基、2-丁基、異丁基或第三丁基)、戊基(例如, 正戊基、2-戊基、3-戊基、2-曱基丁基、3-甲基丁基、1,^ 二甲基丙基、1,2-二甲基丙基或2,2-二甲基丙基)。在某些 貫施例中’ R7係曱基。在某些實施例中,R7係視需要如本 文所述經取代之C1 烷氧基。在某些實施例中,R7係視需 要經1個、2個或3個鹵基取代之Cl-6烷氧基。在某些實施例 中’ R係視需要如本文所述經取代之Cl_6烷硫基。在某些 實施例中,R7係視需要經1個、2個或3個鹵基取代之C16烷 硫基。在某些實施例中,R7係c2 6烯基、c2-6炔基、c3.7環 烧基、(:6-Μ芳基、C7_15芳烷基、雜芳基、或雜環基,其各 自視需要如本文所述經取代。在某些實施例中,R7 係-C(0)Rla、-C(0)〇Rla、_c(〇)NRlbRlc、-C(NRla)NRlbRlc、 -ORla、-0C(0)Rla、-〇c(〇)〇Rla、-〇c(〇)NRlbRlc、-OC(=NRla) NRlbR,c - -0S(0)R,a x -〇S(〇)2R,a > -〇S(0)NRlbRlc ' -0S(0)2 NR,bRlc ' -NRlbR,c . -NRlaC(0)R,d ' -NRlaC(0)0Rld ' -NR,aC(0) NR,bR,c ' -NRlaC(=NRld)NRlbRlc ' -NR,aS(0)R,d ' -NRlaS(0)2Rld ]34881.doc -32- 201134820 、-NRlaS(〇)NR丨bRle、-NR“s(〇)2NRlbRle、_SRla、s(〇)Rla S(0)2R、-S(〇)NRlbR1{^_s(〇)2NRibRic ;其中 Rla、
Rlb、Rle及Rld各自如本文所定義。 在某些貫施例中,R8係氫。在某些實施例中,R8係視需 要如本文所述經取代之Cw烷基。在某些實施例中,R8係 視需要經1個、2個或3個_基取代之cw烷基。在某些實施 例中’ R8係曱基、乙基、丙基(例如,正丙基及異丙基)、 丁基(例如,正丁基、2_ 丁基、異丁基或第三丁基)、戊基 (例如,正戊基、2-戊基' 3-戊基、2-甲基丁基、3-曱基丁 基、1,1-二甲基丙基、1,2-二甲基丙基或2,2_二甲基丙 基)。在某些實施例中,R8係曱基。在某些實施例中,r8 係C3-7環烷基》 在某些實施例中在某些實施例中,r9係視需 要如本文所述經取代之Cl_6烷基。在某些實施例中,Μ係 視需要經1個、2個或3個齒基取代之Cm烷基。在某些實施 例中,R係曱基、乙基、丙基(例如,正丙基及異丙基)、 丁基(例如,正丁基、2_ 丁基、異丁基或第三丁基)、戊基 (例如’正戊基、2-戊基、3-戊基、2·甲基丁基、3甲基丁 I’1 一甲基丙基、1,2-二甲基丙基或2,2·二甲基丙 基)。在某些實施例中,R9係甲I。在某些實施例中,r9 係〇3·7環烷基》 在某些實施例中,X係0。在某些實施例中,乂係8。 在某些實施例中,Υ係-C(0)Rla,其中Rla如本文所定 義。在某些實施财,Y係·(:(0)々‘基。在某些實施例 15488l.doc -33- 201134820 中’ Y係-C(0)-C2.6烯基。在某些實施例中,¥係_匸(〇)-(:3-7 環烷基。在某些實施例中,Y係-C(0)-C6-14芳基。在某些 實施例中,γ係-c(o)-C7·】5芳院基。在某些實施例中,γ 係-C(S)R〗a ’其中Rla如本文所定義。在某些實施例中,γ 係-(^(ShCu烷基。在某些實施例中,6烯基。 在某些實施例中,丫係_C(S)-C3-7環烷基》在某些實施例 中’ Y係-C(S)-C6-丨4芳基。在某些實施例中,γ係_C(S)-C7-15 芳烷基。在某些實施例中,Y係-C(0)NRlbRlc,其中Rlb及 Rlc各自如本文所定義。在某些實施例中,YS—C^C^NH-Cw 烷基。在某些實施例中,Y係-C^C^NH-Cw烷基,其中Cw 烷基經1個、2個或3個自基取代。在某些實施例中,Y 係-(^(CONH-Cm烧基,其中Ci-6院基經雜環基取代。在一 實施例中,Y係-C^CONH-Cw烷基,其中Ck烷基經雜環基 取代’且其中若Cu烷基係乙基,則雜環基不為嗎啉基》 在某些實施例中,Y係-C(0)NH-C2-6烯基。在某些實施例 中’ Y係-c(o)nh-c3.7環烷基。在某些實施例中,Y 係-c(o)nh-c6.14芳基。在某些實施例中,Y係_C(0)NH-C7-15
芳烷基。在某些實施例中,γ係-C(S)NRlbRlc,其中Rlb及 Rlc各自如本文所定義。在某些實施例中,γ係-C^SWH-Cw 烷基。在某些實施例中,γ係_C(S)NH-C2-6烯基。在某些 實施例中’ γ係_C(S)NH-C3.7環烷基。在某些實施例中,Y 係-c(s)nh-c6.14芳基。在某些實施例中,Y係-C(S)NH-C7-15 芳烧基。在某些實施例中,Y係_S(0)Rla,其中Rla如本文 所定義。在某些實施例中,γ係4(0)-(^.6烷基《在某些實 154881.doc •34- 201134820 施例中,Y係-S(0)-C2.6烯基。在某些實施例中,Υ 係-S(〇)-C3_7環烷基。在某些實施例中,Υ係-s(〇)-c614# 基。在某些實施例中,Y係-S(0)-C7-u芳烷基◦在某些實 施例中’ Y係-S(0)2Rla,其中Rla如本文所定義。在某些實 施例中’ Y係-S(0)2_C〗_6烷基。在某些實施例中,γ 係-S(〇)2-C2_6烯基。在某些實施例中,γ係·3(〇)2_(:3_7環院 基。在某些實施例中,Υ係-S(0)2-C6.u芳基。在某些實施 例中’ γ係_S(〇)2_c7_15芳烧基。 在某些實施例中,Y及R8與其所連接之N原子一起形成 雜芳基或雜環基。在一實施例中,丫及R8與其所連接之N 原子一起形成雜芳基。在一實施例中,γ及R8與其所連接 之N原子一起形成雜芳基,其中雜芳基包含至少一個額外 〇、S、或N原子。在一實施例中,丫及尺8與其所連接之N 原子一起形成視需要如本文所述經取代之三唑基。在一實 施例中,Y及R8與其所連接之N原子一起形成雜環基。 在某些實施例中,Z係-C(〇)Ria,其中R“如本文所定 義。在某些實施例中,乙係-匸⑴)-^-6烷基。在某些實施例 中’ Z係-C(0)-C2_6烯基。在某些實施例中,乙係/⑼-心 環烷基。在某些實施例中,芳基。在某些 實施例中,Z係-C(0)-C7·!5芳烷基。在某些實施例中,z 係-C(S)R,其中R a如本文所定義。在某些實施例中,Z 係-C⑻-Cw院基。在某些實施例中,z係·c(s)_Cw稀基。 在某些實施例中’ Z係-C⑻·C3_7環烷基。在某些實施例 中’ Z係-c(s)-c6.14芳基。在某些實施例巾, 154881.doc -35- 201134820 芳烷基。在某些實施例中,Z係-C(〇)NRlbRlc,其中Rb及 R各自如本文所定義。在某些實施例中,乙係6 烷基。在某些實施例中,Z係-C(〇)NH-C2_6烯基。在某些 實施例中’ Z係-C(0)NH-C3·7環烷基。在某些實施例中,z 係-C(0)NH-C6·丨4芳基。在某些實施例中,z係_c(0)NH_C7 15 芳烷基。在某些實施例中,Z係-C(S)NRlbRlc,其中R〗b及 Rle各自如本文所定義。在某些實施例中,Z係{(SWH-Ck 院基。在某些實施例中’ Z係-C(S)NH-C2_6烯基。在某些實 施例中,Z係-C(S)NH-C3-7環烷基。在某些實施例中,z 係-C(S)NH-C6.m芳基。在某些實施例中,z係-C(S)NH-C7.15 芳烷基。在某些實施例中,z係-S(0)R〗a,其中Rla如本文所 定義。在某些實施例中’ Z係4(0)-(:,-6烷基。在某些實施 例中,Z係-S(0)-C2.6烯基。在某些實施例中,Z係-S(0)-C3.7 環烷基。在某些實施例中,z係-S(0)_C6-I4芳基。在某些 實施例中’ Z係-S(0)-C7-15芳烷基。在某些實施例中,z 係-S(0)2Rla,其中Ru如本文所定義。在某些實施例中,z 係4(0)2-(:,-6烷基。在某些實施例中,Z係-S(0)2-C2-6稀 基。在某些實施例中’乙係_S(0)2-C3-7環烷基。在某些實 施例中,Z係-S(0)2_C6_M芳基。在某些實施例中,z 係-S(〇)2-C7-丨5芳烷基。 在某些實施例中’ m為〇。在某些實施例中,m為1。在 某些實施例中’ m為2。在某些實施例中,m為3 » 在某些實施例中’ η為1。在某些實施例中’ η為2。在某 些實施例中,η為3。 154881.doc • 36 · 201134820 在某些實施例中’ m為1且n4l。在某些實施例中,— 1且η為2。 在某些貫施例中,ρ為1。在某些實施例中,ρ為2。在某 些實施例中,Ρ為3。在某些實施例中,卩為々。 在某些實施例中,q為〇。在某些實施例中,4為丨。在某 些實施例中,q為2。在某些實施例中,9為3。 在某些實施例中,Rla係氫。在某些實施例中,Rla係視 需要如本文所述經取代之Cw烷基。在某些實施例中,Rla 係視需要經-或多個鹵基、Cl_6烷氧基、Ci 6烷硫基、雜環 基或雜芳基取代之C】·6烷基。在某些實施例中,Rla係曱 基、乙基、丙基(例如,正丙基或異丙基)、丁基(例如,正 丁基、2-丁基、異丁基或第三丁基)、或戊基(例如,正戊 基、2-戊基、3-戊基、2-曱基丁基、3_甲基丁基、u二甲 基丙基、1,2-二甲基丙基或2,2·二甲基丙基)。在某些實施 例中’ R a係曱基、乙基、異丙基、異丁基第三丁基、 1,1 一甲基丙基或2,2-二甲基丙基,在某些實施例中,Rla 係視需要如本文所述經取代之c:26烯基。在某些實施例 中,Rla係視需要如本文所述經取代之C2·6炔基。在某些實 施例中,Rla係視需要如本文所述經取代之A.7環烷基。在 某些實施例t ’ 111&係視需要經-或兩個Ci 6絲取代之Cy 環烷基。在某些實施例中’ Rla係視需要經兩個曱基取代 之C:3·7環烷基。在某些實施例中,尺4係環丁基、環戊基、 環己基或二甲基雙環-[2.23]庚基(例如,7,7_二甲基雙環 [2.2_1]-庚基)。在某些實施例中,1113係環丁基、環戊某、 154881.doc •37· 201134820 環己基或(18,28,411)-7,7-二甲基雙環[2.2.1]-庚基。在某些 實施例中,RU係視需要如本文所述經取代之(:6.14芳基。 在某些實施例中,Rla係視需要經一或多個齒基或Cl-6烷基 取代之C6·14芳基,其中該烷基視需要經1個、2個或3個鹵 基取代。在某些實施例中,Ria係視需要經氟、氣、甲 基、二氟曱基或乙基取代之C6 M芳基。在某些實施例中, RU係苯基、氟苯基(例如,2-氟苯基、3-氟苯基或4_氟笨 基)、氣苯基(例如,2-氣苯基、3-氣苯基或4-氣笨基)、甲 基苯基(例如’ 2-甲基苯基、3_甲基苯基或4_甲基笨基)、 二氟曱基苯基(例如,2_三氟f基苯基、3-三氟曱基苯基或 4-二氟曱基苯基)或乙基苯基(例如,2_乙基苯基、3_乙基 苯基或4-乙基苯基)。在某些實施例中,Ria係苯基、ί 苯基、3-曱基苯基、4-氣苯基、4-甲基笨基、4-三氟甲基 苯基或4-乙基苯基。在某些實施例中,Ria係視需要如本文 所述經取代之雜芳基。在某些實施例中,RU係雜環基。 在某些實施例_,R〗b係氫。在某些實施例中,Rlb係視 需要如本文所述經取代之Cw烷基。在某些實施例中,Rib 係視需要經一或多個鹵基、Cw烷氧基、Cw烷硫基、雜環 基或雜芳基取代之C!·6烷基。在某些實施例中,Rib係視需 要如本文所述經取代之C2_6烯基β在某些實施例中,Rib係 視需要如本文所述經取代之C2_6炔基。在某些實施例中, Rlb係視需要如本文所述經取代之C3_7環烷基《在某些實施 例中’ 11115係視需要如本文所述經取代之C6_M芳基。在某 些實施例中,R1 b係視需要如本文所述經取代之雜芳基。 154881.doc • 38- 201134820 在某些實施例令 基0 R係視需要如本文所述經取代之雜環 在某些實施例中,# 需要如本立淋+ R係風。在某些實施例中,係視
W 取代之C“烷基。在某些實施例中,RIC 係視需要經—或容 τ 基或雜关其一、 土、C丨-6烷氧基、C丨-6烷硫基、雜環 土〆土取代之C丨-6烷基。在某些實施例中,Rlc係甲 土丙基(例如,正丙基或異丙基)、丁基(例如’正 丁基' 2_丁基、異τ基或第三丁基)、或戊基(例如,正戊 基、2-戊基、3_戊基、2_甲基丁基、3_甲基丁基叫山二子 基丙基、1,2·二甲基丙基或2,2_二甲基丙基在某些實施 例中,R,c係甲基、乙基、異丙基、異丁基、第三丁基、 1,1-二曱基丙基或2,2-二甲基丙基。在某些實施例中,r1c 係視需要如本文所述經取代之CM烯基。在某些實施例 中,RlcS視需要如本文所述經取代之C2·6炔基。在某些實 施例中,尺卜係視需要如本文所述經取代之c3 7環烷基。在 某些實施例中,Rle係視需要經一或兩個Ci.6烷基取代之C37 環烷基。在某些實施例中,Rlc係視需要經兩個甲基取代 之(:3·7環烷基。在某些實施例中,厌1£:係環丁基、環戊基、 環己基或二甲基雙環- [2.2.1]庚基(例如,7,7-二曱基雙環 [2.2.1]-庚基)。在某些實施例中’汉1(:係環丁基、環戊基、 環己基或(lS,2S,4R)-7,7-二曱基雙環[2.2_1]-庚基。在某些 實施例中,Rle係視需要如本文所述經取代之C6_14芳基。 在某些實施例中,Rlc係視需要經一或多個鹵基或Cw烷基 取代之C6-14芳基’其中該院基視需要經1個、2個或3個鹵 154881.doc -39· 201134820 基取代《在某些實施例中,Rlc係視需要經氟、氣、甲 基、三氟曱基或乙基取代之C6_M芳基。在某些實施例中, R係苯基、氟苯基(例如,2_氟苯基、3_氟笨基或4_氟苯 基)、氣苯基(例如,氣苯基、3_氯苯基或4_氣苯基)、曱 基苯基(例如,2-曱基苯基、3_曱基苯基或4_曱基苯基)、 三氟甲基苯基(例如’ 2-三I曱基苯基、3-三敗甲基苯基或 4-二氟曱基苯基)或乙基苯基(例如,2_乙基苯基、3•乙基 苯基或4-乙基苯基)。在某些實施例中,Rlc係笨基、%氟 苯基、3-曱基苯基、4_氣苯基、4_甲基苯基、4_三氟曱基 苯基或4-乙基苯基。在某些實施例中,Rlc係視需要如本文 所述經取代之雜芳基。在某些實施例中,Rlc係雜環基。 在某些實施例中,Rib及RU與其所連接之N原子一起獨 立地形成視需要如本文所述經取代之雜芳基。在某些實施 例中,R及Rlc與其所連接之N原子一起獨立地形成視需 要如本文所述經取代之雜環基。 在某些實施例中,Rld係氫。在某些實施例中,Rid係視 需要如本文所述經取代之Ci0烷基。在某些實施例中,Rld 係視需要如本文所述經取代之C2·6烯基。在某些實施例 中,尺1£|係視需要如本文所述經取代之C2·6炔基。在某些實 施例中,R係視需要如本文所述經取代之CM環烷基。在 某些實施例中,RW係視需要如本文所述經取代之芳 基在某些貫施例中,R1 d係視需要如本文所述經取代之 雜方基。在某些實施例中,Rld係視需要如本文所述經取 代之雜環基。 15488 丨.d〇c 201134820 在某二貫施例中,Rle係氫。在某些實施例中,R卜係視 需要如本文所述經取代之c!6烷基,前提係Rle不為第三= 基。在某些實施例中,Rle係視需要經一或多個鹵基、Cl 烷氧基、Cm烷硫基、雜環基或雜芳基取代之Ci 6烷基。在6 某些實施例中,Rle係甲基、乙基、丙基(例如,正丙基或 異丙基)、正丁基、2-丁基、異丁基、或戊基(例如,正戊 基、2-戊基、3-戊基、2-甲基丁基、基丁基、•二甲 基丙基、1,2-二甲基丙基或22_二曱基丙基)。在某些實施 例中,以係甲基、乙基 '異丙基、異丁基、1山二甲基丙 基或2,2-二甲基丙基。在某些實施例中,Rle係視需要如本 文所述經取代之CM烯基。在某些實施例中,尺^係視需要 如本文所述經取代之Gw炔基。在某些實施例中,Rle係視 需要如本文所述經取代之C3·7環烷基。在某些實施例中, Rle係視需要經一或兩個Cl_6烷基取代之C37環烷基。在某 些實施例中,Rle係視需要經兩個甲基取代之C37環烷基。 在某些實施例中,RU係環丁基、環戊基、環己基或二甲 基雙環-[2.2.1]庚基(例如’ 7,7_二曱基雙環[2 2 庚基)。 在某些實施例中,Rle係環丁基、環戊基、環己基或 (18’28,411)-7,7-二甲基雙環[2.2.1]_庚基。在某些實施例 中,Rle係視需要如本文所述經取代之C6 i4芳基。在某些 貫施例中,R係視需要經一或多個鹵基或C烷基取代之 C6-M芳基’其中該烷基視需要經1個、2個或3個卤基取 代。在某些實施例中,Rle係視需要經氟、氣、甲基、三 氟曱基或乙基取代之C6.!4芳基。在某些實施例中,尺“係 154B81.doc •41- 201134820 本^氣本基(例如,2_敗笨基、3•氣苯基或4_氣苯基)、 氣苯基(例:it〇,2-氣苯基、3_氣苯基或4·氣苯基)、甲基笨 基(例如,”基笨基、3_甲基苯基或"基苯基)、三敦 甲基苯基(例如’ 2~三氟甲基苯基、3·三I甲基苯基或4_三 氟曱基苯基)或乙基苯基(例如,2_乙基苯基、3乙基苯基 或4-乙基苯基)。在某些實施例巾,rU係苯基、3氟苯 基、3-甲基苯基、4_氣苯基、4_曱基苯基、4·三氟曱基苯 基或4·乙基笨基。在某些實施例中,Rle係視需要如本文所 述經取代之雜芳基。在某些實施例中,Rle係雜環基。 在一實施例中,在式I中, R、R、R 、R4及R5各自獨立地為氫、鹵基或C丨6烷 基; R6係氰基或硝基; R7係氫或CN6烷基; R8係氫或Ck烷基; X係0或S ; m為0、1或2 ; η為1或2 ; ρ為1、2、3、或4;且 Υ係-C(0)Rla、-C(S)Rla、_c(〇)NRlbRlc、-C(S)NRlbRlc、 -C(0)0Rle、-5(0)1113或-8(〇)21^ ;其令
Rla、R1(^Rle各自獨立地係:(a) C〗_6烷基,其視需要經 一或多個鹵基、C!·6烷氧基、(:!.6烷硫基、雜環基或雜芳基 取代;(b) C2·6烯基,其視需要經一或多個鹵基取代;(c) 154881.doc •42- 201134820 C3-7環院基,其視需要經一或多個鹵基、或一或兩個C!-6炫 基取代;(d) Cli4芳基,其視需要經一或多個鹵基、C!.6烧 基取代,其中該烧基進一步視需要經1個、2個或3個鹵基 或Cw烷氧基取代,其中該烷氧基進一步視需要經1個、2 個或3個鹵基取代;(e)雜芳基,其視需要經一或兩個Cw 烷基取代;或(f) C7_15芳烷基,其視需要經一或多個鹵 基、C w烧基取代’其中該烧基進一步視需要經1個、2個 或3個鹵基、或C!·6烧氧基取代,其中該烧氧基進一步視需 要經1個、2個或3個函基取代;且 Rlb係氫或甲基;或
Rlb&Rle與其所連接之;^原子一起形成雜環基; 前提係尺16不為第三丁基或节基。 在一實施例中,在式I中, R1、R2、R3、R4及R5各自猶t 目獨立地為虱、鹵基或C丨-6烷 基; R6係氰基或確基; R7係氫; R8係氫或Ck烷基; X係Ο或S ; m為1 ; η為1 ; ρ為1、2、3、或4 ;且 Υ係-C(0)Rla、_c(S)Rla、 -3(0)尺13或-8(0)21113 ;其中 -C(0)NRlbRlc -C(S)NRlbRlc、 154881.doc -43- 201134820
Rla&RlC各自獨立地係:(a) CN6烷基,其視需要經一或 多個齒基、C!.6烷氧基、c16烷硫基、雜環基或雜芳基取 代;(b) C:2·6烯基,其視需要經一或多個鹵基取代; 環烧基’其視需要經一或多個鹵基、或一或兩個Ci6烷基 取代;(d) C6-M芳基,其視需要經一或多個鹵基、烷基 取代’其中該烧基進一步視需要經丨個、2個或3個鹵基或 C!.6烧氧基取代’其中該烷氧基進一步視需要經丨個、2個 或3個卤基取代;(e)雜芳基,其視需要經一或兩個6烷 基取代;或(f) ον,5芳烷基,其視需要經一或多個函基、 C,·6烧基取代,其中該烷基進一步視需要經1個、2個或3個 鹵基、或烷氧基取代’其中該烷氧基進一步視需要經1 個、2個或3個齒基取代;且
Rlb係氫或甲基;或
Rlb及Rle與其所連接之N原子一起形成雜環基。 在一實施例中,在式I中, R1、R2、R3、R4及R5各自獨立地為氫、齒基或C丨.6烷 基; R6係氰基或硝基; R7係氫; R8係氫或甲基; X係Ο或S ; m為1 ; η為1 : ρ為1、2、3、或4;且 154881.doc -44- 201134820 Y係-C(0)Rlaa-C(S)Rla ;其中 1113係(&) C〗·6烷基,其視需要經一或多個鹵基取代;(b) Cm烯基;(c) C3·7環烷基;或(d) C6 i4芳基,其視需要經一 或多個鹵基、C!·6烷基或C!·6烷氧基取代。 在一實施例中,在式I中, R1、R2、R3、R4及R5各自獨立地為氩、_基或C16烷 基; R6係氰基或硝基; R7係氮; R8係氫或甲基; X係Ο或S ; m為1 ; η為1 ; ρ為1、2、3、或4 ;且 Υ係其中 Rlb係氫;且
RlU) C,·6烧基,其視需要經一或多個齒基、或心炫 氧基、Cw烷硫基、雜環基、或雜芳基取代;⑻k烯 基,(c) C3-7環烧基;或(d) C/: it ^ . ^』k·丨4方基,其視需要經一或多 個鹵基、C!·6烷基或Ck烷氧基取代;且 Rlb係氫或曱基;或
Rlb及^與其所連接之⑽子-起形成雜環基。 在一實施例中,在式I中, R1、R2、R3、R4及R5各自獨立 烷
Ώ馬氧、鹵基或C 154881.doc •45· 201134820 基; R6係氰基或硝基; R7係氫; R8係氫或曱基; X係Ο或S ; m為1 ; η為1 ; ρ為1 ;且 Υ係-C(0)NRlbRu或-C(S)NRlbRle;其中 Rlb係氫;且 尺卜係匚^烷基,其視需要經(a)—或多個鹵基、或(b)雜 環基取代;且 Rlb係氩或曱基。 在一實施例中,在式I中, R1係氫; R2係氣; R3係氩; R4係氣; R5係氫; R6係氰基; R7係氫; X係Ο或S ; m為1 ; η為1 ; 154881.doc -46· 201134820 p為 1、2、3、或 4 ; Y係-(:(0州11115111<:或-(:(8州11115111<:;其中 Rlb係氫; 或(b)雜 尺卜係匚^6烷基,其視需要經(a)一或多個鹵基、 環基取代;且 Rlb係氫或甲基。 在一實施例中,在式I中, 或Ci-6炫· R、R、R、R及R5各自獨立地為氫、鹵基 基; R6係氰基或硝基; R7係氫; R8係氫或甲基; X係Ο或S ; m為1 ; η為1 ; ρ為1、2、3、或4;且 Υ係-S(0)2Rla ;其中 -或多個 '其視需 或CN6烷 尺13係(&) Ci-6烧基’(b) C6-i4芳基,其視需要經. 鹵基、Cl·6统基或Cl.6院氧基取代;或(c)雜芳基 要經一或兩個Ck烷基取代。 在一實施例中,在式I中, R1、R2、R3、R4及R5各自獨立地為氫、鹵基 基; R6係氰基或硝基; 154881.doc -47- 201134820 R7係氫; X係o或s; m為1 ; n為1 ; ρ為1、2、3、或4;且 w席子一起形成雜 芳基包含至少一個額外〇、s、或Ν原子, 、 兩個Cw烷基取代》 ' 在一實施例中,在式I中, R1 基; R2 ' R3 R4及R5各自獨立地為氫、 函基或Cw烷 R6係氰基或硝基; R7係氫; X係Ο或S ; m為1 ; η為1 ; ρ為1、2、3、或4;且 Υ及R8與其所連接之Ν原子—起形成5員雜芳基,其中 雜芳基包含至少-個額外〇、s、或Ν原子,其視需要經 或兩個Cw烷基取代。 在一實施例中,在式I中, R ' R、R、R4及R5各自獨立地為氫、齒基或c】-6烧 R6係氰基或硝基; 154881.doc -48- 201134820 R7係氫; X係o或s ; m為1 ; n為1 ; ρ為1、2、3、或4 ;且 Υ及R8與其所連接之Ν原子一起形成三唑基,其視需要 經一或兩個甲基取代。 在另一實施例中,在式I中, R1係氫; R2係氣或曱基; R3係氫; R4係氣或甲基; R5係氫; R6係氰基; R7係氫; X係Ο或S ; m為1 ; η為1 ; ρ為1、2、3、或4 ;且 Υ及R8如本文中其他處所定義。 在一實施例中,在式la中, R1、R2、R3、R4及R5各自獨立地為氫、氘、鹵基&Ci-6 烧基; R6係氰基或硝基; 154881.doc -49- 201134820 R8係氫; …係氘; X係Ο或S ; m為0、1或2 ; η為1或2 ; ρ為 1、2、3、或 4 ; q為3 ;且 Y係-C(0)Rla、-C(S)Rla、-C(0)NRlbRlc、-C(S)NRlbRlc、 -C(0)0Rle、-S(0)Rla4_s(〇)2Rla ;其中 R 、R及R各自獨立地係:(a) CV6烷基,其視需要經 一或多個鹵基、Cw烷氧基、Cl 6烷硫基、雜環基或雜芳基 取代;(b) C2·6烯基,其視需要經一或多個鹵基取代;(c) C3·7環烷基,其視需要經一或多個鹵基、或一或兩個烷 基取代,(d) C6.M芳基,其視需要經一或多個鹵基、烷 基取代,其中該烷基進一步視需要經1個、2個或3個鹵基 或C,·6烷氧基取代,其中該烷氧基進一步視需要經丨個、2 個或3個函基取代;(e)雜芳基,其視需要經一或兩個 烷基取代;或(f) C7.15芳烷基,其視需要經一或多個鹵 ' 烧基取代,其中該烧基進一步視需要經1個、2個 或3個_基或氧基取代,其中該烧氧基進__步視需 要經1個、2個或3個齒基取代;且
Rlb係氫或曱基;或 R及R與其所連接之_子—起形成雜環基。 在另一實施例中,在式Ia中, 154881.doc 201134820 R1 烷基 R2、R3 R4及R5各自獨 立地為氫、氘、鹵基或Cu R6係氰基; R8係氫; …係氘; X係Ο或S ; m為1 ; η為1 ; ρ為4 ; q為3 ;且 Y係-C(0)Rla、-C(S)Rla、_c(〇)NRlbRlc、-C(S)NRlbRlc、 -C(0)ORle、-S(0)Rla或 _S(〇)2Ru ;其中
Rla、Rlc及Rle各自獨立地係:(a) Cl 6烷基,其視需要經 一或多個函基、C!.6烷氧基、Cw烷硫基、雜環基或雜芳基 取代;(b) C2_6烯基’其視需要經一或多個鹵基取代; c:3.7環烧基’其視需要經一或多個鹵基、或一或兩個Cl6烧 基取代;(d) C6·〗4芳基’其視需要經一或多個鹵基、Cl.6烷 基取代,其中該院基進一步視需要經1個、2個或3個鹵基 或Cw烷氧基取代,其中該烷氧基進一步視需要經1個、2 個或3個鹵基取代;(e)雜芳基,其視需要經一或兩個(^.6 烷基取代;或(f) C7.15芳烷基,其視需要經一或多個鹵 基、Cw烷基取代,其中該烷基進一步視需要經1個、2個 或3個鹵基、或Cw烷氧基取代,其中該烷氧基進一步視需 要經1個、2個或3個自基取代;且 154881.doc •51- 201134820
Rlb係氫或曱基;或 及R】e與其所連接之N原子—起形成雜環基。 在另一實施例中,在式la中,
Ri、R2、R3、R4 及 R5 各自 — 分目獨立地為虱、氘、鹵基或Ci 6 烷基; R6係氰基; R8係氫;
Rd係氘; X係Ο或S ; m為1 ; η為1 ; ρ為4 ; q為3 ;且 Y係 _C(0)NRlbRlc ;其中
Rlc係:(a) C,·6烷基’其視需要經一或多個鹵基、烷 氧基' C,·6烷硫基、雜環基或雜芳基取代;(b) c2.6稀基, 其視需要經一或多個鹵基取代;(c) C3-7環烷基,其視需要 經一或多個鹵基、或一或兩個cN6烷基取代;(d) (:6_14芳 基’其視需要經一或多個鹵基' Cl_6烷基取代,其中該烷 基進一步視需要經1個、2個或3個鹵基或(:1-6烷氧基取代, 其中該烷氧基進一步視需要經1個、2個或3個鹵基取代; (e)雜芳基,其視需要經一或兩個Cl.6烷基取代;或(f) C7-15 芳烷基,其視需要經一或多個鹵基、Cw烷基取代,其中 該烷基進一步視需要經1個、2個或3個鹵基、或CN6烧氧基 15488I.doc • 52· 201134820 取代,其中該烷氧基進-步視需要經i個、2個或3個鹵基 取代;且
Rlb係氫。 在另一實施例中,在式中, R、R、R、R4及R5各自獨立地為氫、鹵基或C"烷 基, R6係氰基; R8係氫;
Rd係氘; X係Ο或S ; m為1 ; η為1 ; ρ為4 ; q為3 ;且 Y係-C(0)NRlbRlc ;其中
RlcS(a)經雜環基取代之c16烷基;或(b) Cw烯基;且 Rlb係氫。 在一實施例中,在式II中, R1、R2、R3、R4及R5各自獨立地為氫、自基或Cl.6烷 基; R6係氰基或硝基; R7係氫或CK6烧基; R9係氫或Cw烷基; X係〇或S ; 154881.doc -53· 201134820 m為0、1或2 ; η為1或2 ; ρ為1、2、3、或4;且 Ζ係-C(0)Rla、-C(S)Rla、-C(0)NRlbRlc、-C(S)NRlbRlc、 -C(0)0Rle、-S(0)Rla4-S(0)2Rla ;其中
Rla、Rlc及Rle各自獨立地係:(a) C丨-6烷基,其視需要經 一或多個鹵基、Cw烷氧基、Cw烷硫基、雜環基或雜芳基 取代;(b) C2·6烯基’其視需要經一或多個鹵基取代;(c) C3·7環烷基,其視需要經一或多個鹵基、或一或兩個cl6烷 基取代;(d) C6-M芳基,其視需要經一或多個鹵基、6烷 基取代,其中該烷基進一步視需要經1個、2個或3個鹵基 或Ci.6烧氧基取代,其中該烧氧基進一步視需要經1個、2 個或3個齒基取代;(e)雜芳基,其視需要經一或兩個Ci6 烷基取代,或(f) C:7」5芳烷基,其視需要經一或多個鹵 基、Cw烷基取代,其中該烷基進一步視需要經i個、2個 或3個鹵基、或C!·6烷氧基取代,其中該烷氧基進一步視需 要經1個、2個或3個函基取代;且
Rlb係氫或甲基;或
Rlb及Rl£:與其所連接之N原子一起形成雜環基; 前提係Rle不為第三丁基或苄基。 在一實施例中,在式II中, R R及R各自獨立地為氩、鹵基或c!-6院 基; R6係氰基或硝基; 154881.doc -54- 201134820 R7係氫; R9係氫或甲基; X係0或s; m為1 ; η為1 ; Ρ為1、2、3、或4 ;且 Ζ係-(:(0)1113或-(:(8)1113 ;其中 R〗a係(a) Ck烷基,其視需要經一或多個鹵基取代;(b) C2·6烯基;(c) Cm環烷基;或(d) C6 i4芳基,其視需要經一 或多個鹵基、C!·6烷基或C!·6提氧基取代。 在一實施例中,在式II中, …、^尺^及“各自獨立地為氫’齒基或^^院 基; R6係氰基或硝基; R7係氫; R9係氫或曱基; X係Ο或S ; m為1 ; η為1 ; ρ為1、2、3、或4;且 2係-(:(0州1111)111(:或-(:(8州111151^.甘士 *具1Ρ
Rlb係氫;且 1- 6烷 2- 6歸
Rlc係(a) Cm烧基’其視需要經一或多個齒基、或〔 氧基、c丨-6烧硫基、雜環基、或雜芳基取代;(b) c 154881.doc -55- 201134820 一或多 基,(c) C3·7環烧基’或(d) C6·丨4芳基,其視需要經 個鹵基、C〗-6烧基或Ci-6烧氧基取代;且 Rlb係氫或曱基;或 R〗b及Rle與其所連接之N原子一起形成雜環基。 在一實施例中,在式Π中,
Ci-6 烧 尺1、112、113、114及115各自獨立地為氫、_基或 基; R6係氰基或硝基; R7係氫; R9係氫或甲基; X係Ο或S ; m為1 ; η為1 ; Ρ為1、2、3、或4 ;且 Ζ係-S(0)2Rla ;其中 或多個 其視需 R】、(a) Ci·6烧基;(b) C6·丨4芳基,其視需要經一 鹵基、C!·6烧基或C!·6烧氧基取代;或(c)雜芳基 要經一或兩個C 1.6烧基取代。 在另一實施例中,在式II中, R1係氫; R2係氣或甲基; R3係氫; R4係氣或甲基; R5係氫; 154881.doc -56- 201134820 R6係氰基; R7係氫; X係ο或s; m為1 ; η為1 ; ρ為1、2、3、或4 ;且 Ζ及R如本文中其他處所定義。 在一實施例中,在式Ha中, R R、R、R4及R5各自獨立地為氫、氘、 烷基; K6 R6係氰基或硝基; R7係氫或CN6烷基; R9係氫或Cw烷基;
Rd係氘; X係0或S ; m為0、1或2 ; η為1或2 ; ρ為1、2、3、或4 ;且 q為3 ;且 Z係-C(0)Rla、_c(S)Rla、-C(0)NRlbRlc、-C(S)NRlbRic、 -C(0)0Rle、-S(0)Rla4-S(0)2Rla ;其中
Rla、Rle及Rle各自獨立地係··(a) Cl_6烷基,其視需要經 一或多個鹵基、CN6烷氧基、Cw烷硫基、雜環基或雜芳基 取代;(b) C2-6烯基,其視需要經一或多個鹵基取代;(C) 134881.doc • 57· 201134820 c:3·7環烷基,其視需要經一或多個鹵基、或一或兩個ci 6烷 基取代;(d) C6.〗4芳基,其視需要經一或多個鹵基、c16烷 基取代’其中該烷基進—步視需要經1個、2個或3個鹵基 或C!·6炫氧基取代,其中該烷氧基進一步視需要經1個、2 個或3個鹵基取代;(e)雜芳基,其視需要經一或兩個ci 6 烧基取代,或(f) C7·,5芳烷基’其視需要經一或多個鹵 基、C〗·6烧基取代’其中該烧基進一步視需要經丨個、2個 或3個鹵基、或Ci.β烧氧基取代’其中該燒氧基進一步視需 要經1個、2個或3個鹵基取代;且 Rlb係氫或甲基;或 R〗b&Rle與其所連接之N原子一起形成雜環其。 在一實施例中’本發明提供選自由下列組成之群之化合 物:
154881.doc • 58 _ 201134820
15488I.doc -59 201134820
15
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31
33 32
34 154881.doc -61 - 201134820
43 44 154881.doc -62- 201134820
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及其對映異構體、對映異構體之混合物、兩種或更多種非 154881.doc •63- 201134820 對映異構體之混合物 異構體之混合物.及装互變異構體、及兩種或更多種互變 合物、及前藥及其醫藥上可接受之鹽、溶劑合物、水 意學’否則本發明所提供之化合物 有稀基或伸異^體。當本文所提供化合物含 Z/E)異構體或其混人 戍饤順式/反式(或 換,則化合二:广式存在。倘若結構異構體可互 ……單—互變異構體或互變異構體之混合物 ,子。纟含有(例如)亞胺基 此可採取質子互鐵里槐 X肟基之化合物中 中可採取所1 構形式;或在含有芳族部分之化合物 "P 了採取所谓的價互變 規X μ # 構式。因此,單個化合物可表 現不止一種類型之異構現象。
構提供化合物可為純對映異構體,例如單-對映異 =早體一二:映異構體’或立體異構體混合物,例如對 物體混。物’例如,兩種對映異構體之外消旋混合 物,或兩種或更多種非對映異構體之混合物。因此,熟習 此項技術者可瞭解,對於在活體内發生差向異構之化合物 而吕,以其W形式投與該化合物等效於以其⑻形式投與 該化合物。製備/分離㈣對映異構體之W 適宜光學純前體之合成、自非對掌性起始材料之不對稱1 成、或對映異構體混合物之拆分,例如,對掌性層析、重 結晶、拆分、非對映異構體鹽形成、或衍生化成非對映異 構體加合物隨後實施分離。 、 當本文所提供化合物含有酸性或鹼性部分時,其亦可以 154881.doc •64· 201134820 醫藥上可接受之鹽形式提供(參見,Berge等人,J. Pharm. Sci. 1977,66, 1-19 ;及「Handbook of Pharmaceutical Salts,Properties,and Use」,Stahl及 Wermuth編輯;Wiley-VCH及 VHCA,Zurich,2002) o 適用於製備醫藥上可接受之鹽的酸包括但不限於乙酸、 2,2-二氣乙酸、醯化胺基酸、己二酸、海藻酸、抗壞血 酸、L-天冬胺酸、苯磺酸、苯甲酸、4-乙醯胺基苯曱酸、 硼酸、(+)-樟腦酸、樟腦磺酸、(+)-(lS)-樟腦-10-磺酸、癸 酸、己酸、辛酸、肉桂酸、檸檬酸、環拉酸、環己烷胺基 磺酸、十二烷基硫酸、乙烷_1,2_二磺酸、乙磺酸、2-羥 基-乙續酸、曱酸、富馬酸、半乳糖二酸、龍膽酸、葡庚 糖酸、D-葡糖酸、D-葡糖搭酸、L-糙胺酸、α-酮戊二酸、 羥基乙酸、馬尿酸、氫溴酸、鹽酸、氫碘酸、(+)_L-乳 酸、(±)-DL-乳酸、乳糖酸、月桂酸、馬來酸、蘋果 酸、丙二酸、(士)-DL-扁桃酸、曱磺酸、萘_2·磺酸、萘· 1,5-二續酸、1 -經基-2-萘甲酸、終酸、确酸、油酸、乳清 酸、草酸、棕櫚酸、巴莫酸、高氣酸、磷酸、L_焦麩胺 酸、糖酸、水楊酸、4 -胺基-水揚酸、癸二酸、硬脂酸、號 珀酸、硫酸、鞣酸、(+)-L-酒石酸、硫氰酸、對甲苯續 酸、Η—稀酸及戊酸。 在一實施例中,本文所提供化合物係鹽酸鹽。 適用於製備醫藥上可接受之鹽的鹼包括但不限於無機 驗’例如氳氧化鎂、氫氧化躬、氫氧化卸、氫氧化鋅或氫 氧化納;及有機驗,例如一級、二級、三級及四級脂肪族 154881.doc -65· 201134820 及芳族胺’包括L-精胺酸、苯乙节胺、n,n,_二节基乙 胺、膽鹼、二甲基乙醇胺、二乙醇胺、二乙胺、二甲, 二丙胺、二異丙胺、2_(二乙基胺基)·乙醇、乙醇胺、乙 胺、乙二胺、異丙胺、N•曱基_葡萄糖胺、哈胺 (hydrabamine)、1H-咪唑、L·離胺酸、嗎啉、4_(24 基)-嗎啉、甲胺、六氫吡啶 '六氫吡β秦、丙胺吡咯啶、 M2-羥乙基)-吡咯啶、吡啶、奎寧環、喹啉、異喹啉、i 級胺、三乙醇胺、三甲胺、=匕脸 ·^ 一乙胺N_甲基-D-葡萄糠 胺、2-胺基-2-(羥甲基)-1,3_丙二醇及胺基丁三醇。 本文所提供化合物亦可以前藥形式提供,其為(例如)式^ 或II化合物之功能衍生物,且可容易地在活體内轉化成母 體化合物。經常使用前藥’此乃因在一些情況下其可能較 母體化合物更容易投與。舉例而言,前藥可藉由經口投與 供生物利用,而母體化合物則不行。前藥在醫藥組合物中 亦可具有優於母體化合物之增強之溶解性。前藥可藉由多 種機制轉化成母體藥物,包括酶促過程及代謝水解。參 見,Harper,Progress in Drug Research 1962, 4, 221-294 ; Morozowich等人,「Design of Biopharmaceutical Properties through Prodrugs and Analogs」,Roche編輯,APHA Acad. Pharm· Sci. 1977 ;「Bioreversible Carriers in Drug in Drug Design, Theory and Application」,Roche 編輯,APHA Acad. Pharm. Sci· 1987 ;「Design of Prodrugs」, Bundgaard,Elsevier,1985 ; Wang 等人,Curr. Pharm· Design 1999,5,265-287 ; Pauletti 等人,Adv. Drug- 154881.d〇c -66 - 201134820
Delivery Rev. 1997, 27,235-256 ; Mizen fA,Pharm. Biotech. 1998,11,345-365 ; Gaignault等人,Pract. Med. Chem. 1996,671-696 ; Asgharnejad,「Transport Processes in Pharmaceutical Systems」,Amidon等人編輯,Marcell Dekker,185-218,2000 ; Balant等人,Eur. J. Drug Metab. Pharmacokinet. 1990,15,143-53 ; Balimane及 Sinko,Adv. Drug Delivery Rev. 1999, 39, 183-209 ; Browne, Clin. Neuropharmacol. 1997,20, 1-12 ; Bundgaard, Arch. Pharm. Chem. 1979, 86, 1-39 ; Bundgaard, Controlled Drug
Delivery 1987, 17, 179-96 ; Bundgaard, Adv. Drug Delivery Rev. 1992,8,1-38 ; Fleisher 等人,Adv. Drug Delivery Rev. 1996, 19, 1.1 5-130 ; Fleisher等人,Methods Enzymol. 1985,112,360-381 ; Farquhar等人,J. Pharm. Sci. 1983, 72, 324-325 ; Freeman 等人,J. Chem· Soc.,Chem.
Commun. 1991,875-877 ; Friis 及81111(1§汪31(1,丑111···!'· Pharm. Sci. 1996, 4,49-59 ; Gangwar等人,Des. Biopharm. Prop. Prodrugs Analogs, 1977,409-421 ; Nathwani 及 Wood,Drugs 1993, 45, 866-94 ; Sinhababu 及 Thakker, Adv· Drug Delivery Rev. 1996,19, 241-273 ; Stella等人, Drugs 1985,29,455-73 ; Tan等人,Adv. Drug Delivery Rev. 1999, 39, 117-151 i Taylor, Adv. Drug Delivery Rev. 1996,19, 131-148 ; Valentino及 Borchardt,Drug Discovery Today 1997,2,148-155 ; Wiebe 及 Knaus,Adv. Drug Delivery Rev, 1999,39,63-80 ;及 Waller等人,Br. J. Clin. 154881.doc -67- 201134820
Pharmac. 1989, 28, 497-507 〇 合成方法 可藉由熟習此項技術者已知之任一方法來製備、分離、 或獲得本文所提供化合物。舉例而言,式I化合物可如反 應圖1中所示製得,其中y係氫或胺基保護基團,例如, Boc、Cbz、或Fmoc ;且RL係離去基團,例如,氣、漠、 碘、咪唑、或羧酸根。 經由親核性芳族取代反應使化合物A與化合物b反應以 形成化合物C並釋放鹽酸。使用還原試劑(例如,連二亞硫 酸鈉或氣化錫(II))將化合物C之硝基還原為胺基以形成苯 胺D ’其隨後經由Sandmeyer反應轉化為續醯氣E。然後使 化合物E與胺F偶合,其中胺基保護基團P1在一些實施例中 係可選的。自化合物G去除保護基團P1以形成化合物η, 使化合物Η與Y-RL反應以形成式I化合物。 產生式I化合物之替代途徑示於反應圖2中。 在與上文所述且示於反應圖1中之方法相似的方法中, 式II化合物可如反應圖3中所示製得,其中P1係氫或胺基保 護基團’例如,Boc、Cbz、或Fmoc ;且rl係離去基團, 例如,氣、溴、碘、咪唑、或羧酸根。 154881.doc -68 - 201134820 反應圖1
Η (I) 154881.doc -69- 201134820 反應圖2
154881.doc •70 201134820 反應圖3
z-rl -hrl
(Π) 醫藥組合物 本文提供醫藥組合物,其包含本文所提供化合物(例 如,式I或II化合物,包括其對映異構體、對映異構體之混 合物、兩種或更多種非對映異構體之混合物、互變異構體 或兩種或更多種互變異構體之混合物;或其醫藥上可接受 之鹽、溶劑合物、水合物或前藥)作為活性成份;以及醫 藥上可接受之媒劑、載劑、稀釋劑、或賦形劑或其混合 物。 154881.doc •71 · 201134820 本文所提供化合物可單獨或與一或多種本文所提供之其 他化合物組合投與《包含本文所提供化合物(例如,式I或 II化合物)之醫藥組合物可以各種劑型調配用於經口、非經 腸及局部投與。亦可將醫藥組合物調配為改良釋放劑型, 包括延遲-、延續-、延長_、持續·、間斷_、受控_、加速_ 、快速-、靶向-、程式化釋放劑型及胃滞留劑型。該等劑 型可根據彼等熟習此項技術者所習知之習用方法及技術來 製備(參見 Remington: The Science and Practice of
Pharmacy,如上所述;Modified_Release Drug Technology,第 2版,Rathbone等人編輯 ’ Marcel Dekker^ 司:New York,NY,2008)。 在一實施例中,醫藥組合物係以供經口投與之劑型提 供,該等醫藥組合物包含本文所提供化合物(例如,式以匕 合物,包括其對映異構體、對映異構體之混合物、兩種或 更多種非對映異構體之混合物、互變異構體或兩種或更多 種互變異構體之混合物;或其醫藥上可接受之鹽、溶劑合 物、水合物或前藥);及一或多種醫藥上可接受之賦形劑 或載劑。 在另一實施例中,醫藥組合物係以供非經腸投與之劑型 提供’該等醫藥組合物包含本文所提供化合物(例如,式j 或II化合物’包括其對映異構體、對映異構體之混合物、 兩種或更多種非對映異構體之混合物、互變異構體或兩種 或更多種互變異構體之混合物;或其醫藥上可接受之鹽、 溶劑合物、水合物或前藥);及一或多種醫藥上可接受之 154881.doc -72· 201134820 賦形劑或載劑。 在另-實施例中’醫藥組合物係以供局部投與之劑型提 供’該等醫藥組合物包含本文所提供化合物(例如,式工或 II化合物’包括其對映異構體、對映異構體之混合物、兩 種或更多種非對映異構體之混合物、互變異構體或兩種或 更多種互變異構體之混合物;或其醫藥上可接受之鹽、溶 劑合物、水合物或前藥);及一或多種醫藥上可接;之賦 形劑或載劑。 本文所提供之醫藥組合物可以單位劑型或多纟劑型來& 供。本文所用之單位劑型係指業内已知適於投與人類及動 物個體且單獨包裝之物理離散單位。每一單位劑量含有足 以產生期望治療效應之狀量的活性成份以及所需醫藥載 劑或賦形劑。單位劑型之實例包括安瓶(ampGuie)、注射器 及單獨包裝线劑及㈣4㈣型可分數份投與或多次 才又與。多次劑型係複數份相同單位劑型,其包裝於單一容 =中以供以分開之單位劑型投與。多次劑型之實例包括小 藥瓶、成瓶錠劑或膠囊、或品脫瓶或加侖瓶。 本文所提供醫藥組合物可—次投與或以—定時間間隔多 次投與。應理解,準確劑量及治療持續時間可根據所治療 〜者之年齡、ϋ重及健康狀況而有戶斤變化,&可根據經驗 使用已知測試方案來確定,或藉由活體内或活體外測試或 诊斷數據之外推來確定。亦應理解,對於彳卜特^個體而 言’具體劑量方案應根據個體需要及調配物投與者或調配 物投與監督者之專業判斷來隨時間進行調整。 154881.doc •73· 201134820 A.經口投與 本文所提供經口投與用醫藥組合物可以固體、半固體、 或液體劑型來提供以用於經口投與。本文所用之經口投與 亦包括含服、經舌及舌下投與。適宜口服劑型包括但不限 於錠劑、口崩片(fastmelt)、咀嚼錠劑、膠囊、丸劑、條形 劑(strip)、口含錠、菱形錠劑、軟錠劑、扁囊劑、片劑、 含藥口香糖、整裝粉劑、泡騰或非泡騰粉劑或粒劑、口腔 喷霧劑—1 mist)、溶液、乳液、懸浮液、糖米紙囊.劑、 喷灑劑、酏劑及糖漿。除活性成份外,醫藥組合物可含有 -或多種醫藥上可接受之載劑或賦形劑,包括但不限於黏 合劑、填充劑、稀釋劑、崩解劑、潤濕劑、潤滑劑、助流 劑、著色劑、染料遷移抑制劑、甜味劑、矯味劑、乳化 劑、懸洋及分㈣、防腐劑、溶劑、非水性液體、有機酸 及'一氧化碳來源。 黏合劑或製粒劑賦予錠劑黏著性以確保錠劑在壓縮後保 持完整。適宜黏合劑或製粒劑包括但不限於澱粉,例如玉 米澱粉、馬鈐薯澱粉及預膠化澱粉(例如starch 15〇〇); 月膠,糖類,例如嚴糖、葡萄糖、右旋糖、糖蜜及乳糖; 天然及合成樹膠,例如阿拉伯膠、海㈣、海藻酸鹽、角 又菜提取物、潘瓦爾膠(panwar gum)、印度膠⑴ g m)依粆貝果(isabgol)殼膠黏劑、羧甲基纖維素、甲基 纖維素、聚乙烯料相(pvp)、㈣鎮铭(veegum)、落 葉松阿拉伯半乳聚糖、粉狀黃蓍膠及瓜爾冑;纖維素,例 如乙基纖維素、乙酸纖維素、缓甲基纖維㈣、叛甲基纖 15488 丨.doc -74- 201134820 維素鈉、甲基纖維素、羥乙基纖維素(HEC)、羥丙基纖維 素(HPC)、羥丙基甲基纖維素(HPMC);微晶纖維素,例如 AVICEL-PH-101、AVICEL-PH-103、AVICEL RC-581、 AVICEL-PH-105(FMC公司,Marcus Hook,PA);及其混合 物。適宜填充劑包括但不限於滑石粉、碳酸鈣、微晶纖維 素、粉狀纖維素、右旋糖類(dextrates)、高嶺土、甘露 醇、矽酸、山梨醇、澱粉、預膠化澱粉及其混合物。本文 所提供醫藥組合物中之黏合劑或填充劑之量根據調配物之 類型而變化’且彼等熟習此項技術者可容易地確認。本文 所提供醫藥組合物中可存在約50重量%至約99重量%之黏 合劑或填充劑。 適宜稀釋劑包括但不限於磷酸二鈣、硫酸鈣、乳糖、山 梨醇、蔗糖、肌醇、纖維素、高嶺土、甘露醇、氣化鈉、 乾澱粉及糖粉。某些稀釋劑(例如甘露醇、乳糖、山梨 醇、嚴糖及肌醇)在以足量存在時可賦卜些壓縮鍵劑以 容許在口中藉由。且嚼而崩解之性f。該等壓縮錠劑可用作 口且嚼錠劑。本文所提供醫藥組合物中之稀釋劑之量根據調 配物之類型而有所變化,且彼等熟習此項技術者可容易地 確認。 ;膨潤土;纖維素,例如 質產品;天然海綿;陽離 例如瓜爾膠及矽酸鎂鋁 適宜崩解劑包括但不限於瓊脂 甲基纖維素及羧曱基纖維素;木 子交換樹脂;海藻酸;樹膠, HV;掛橘果肉;交聯纖維素’例如交聯叛甲纖维素;交 聯聚合物’例如交聯聚維酮;交聯殿粉;碳_ ;微晶纖 154881.doc -75- 201134820 維素’例如經基乙酸殿粉納;聚克立林奸(p〇lacriHn potassium) ;殿粉,例如玉米澱粉、馬鈴薯澱粉、木薯澱 粉及預膠化澱粉;黏土;藻膠;及其混合物。本文所提供 醫藥組合物中之崩解劑之量根據調配物之類型而有所變 化,且彼等熟習此項技術者可容易地確認。本文所提供醫 藥組合物中之崩解劑之量根據調配物之類型而有所變化, 且彼等熟習此項技術者可容易地確認。本文所提供醫藥組 合物可含有約0.5重量%至約15重量%或約i重量%至約5重 量%之崩解劑。 適宜潤滑劑包括但不限於硬脂酸鈣;硬脂酸鎂;礦物 油,輕礦物油;甘油;山梨醇;甘露醇;二醇類,例如山 茶酸甘油醋及聚乙二醇;硬脂酸;十二烷基硫酸 鈉,滑石粉;氫化植物油,包括花生油、棉籽油、葵花籽 油、芝麻油、橄欖油、玉米油及大豆油;硬脂酸鋅;油酸 乙酯;月桂酸乙酯;瓊脂;澱粉;石松子;二氧化矽或矽 膠,例如 AEROSIL® 200(W.R. Grace公司,Baltim〇re,MD) 及CAB-〇-SIL®(Cabot公司,Boston,MA);及其混合物。 本文所提供醫藥組合物可含有約〇」重量%至約5重量%之 潤滑劑。 適宜助流劑包括但不限於膠狀二氧化矽' cab_〇 sil® (Cabot公司,Boston,MA)、及無石棉滑石粉。適宜著色劑 包括但不限於任一種經批准鑒定之水溶性FD&C染料、及 懸浮於氧化鋁水合物上之水不溶性FD&C染料、及色澱及 其混合物。色澱係藉由將水溶性染料吸附至重金屬之水合 15488l.doc -76- 201134820 氧化物上而產生染料之不溶性形式之組合。適宜繙味劑包 括但不限於自植物(例如果實)提取之天然矯味劑、及可產 生令人愉快之味覺的化合物之合成摻合物,例如薄荷及水 揚酸甲酯。適宜甜味劑包括但不限於蔗糖、乳糖、甘露 醇糖梁、甘油及人工甜味劑,例如糖精及阿司帕坦 (aspartame)。適宜乳化劑包括但不限於明膠、阿拉伯膠、 黃蓍膠、膨潤土及表面活性劑,例如聚氧乙烯山梨醇酐單 油酸醋(TWEEN® 20)、聚氧乙烯山梨醇野單油酸醋8〇 (TWEEN 8G)、及二乙醇胺油酸g旨。冑宜懸浮及分散劑包 括但不限於缓甲基纖維素納、果膠、黃蓍膠、料鎮銘、 阿拉伯膠、缓甲基纖維素納、經丙基曱基纖維素及聚乙稀 吡咯啶酮。適宜防腐劑包括但不限於甘油、對羥基苯甲酸 甲酯及對羥基苯甲酸丙酯、苯甲酸、苯甲酸鈉及醇類。適 宜潤濕劑包括但不限於丙二醇單硬脂酸酯、山梨醇酐單油 酸酯、二甘醇單月桂酸酯及聚氧乙烯月桂醇醚。適宜溶劑 包括但不限於甘油、山梨醇、乙醇及糖漿。乳液中採用之 適宜非水性液體包括但不限於礦物油及棉籽油。適宜有機 酸包括但不限於檸檬酸及酒石酸,適宜二氧化碳來源包括 但不限於碳酸氫鈉及碳酸鈉。 應理解’即使在相同調配物中許多載劑及賦形劑亦可發 揮若干種功能。 本文所提供經口投與用醫藥組合物可以以下形式來提 供:壓縮錠劑、模印錠劑、可咀嚼菱形錠劑、速溶錠劑、 多重壓縮錠劑、或腸溶錠劑、糖衣錠劑或薄膜衣錠劑。腸 154881.doc •77· 201134820 溶錠劑係壓縮錠劑’其經可抵抗胃酸作用但在腸中溶解或 朋解之物質塗覆,由此保護活性成份免受胃中酸性環境的 侵蝕。腸溶包衣包括但不限於脂肪酸、脂肪、水揚酸苯 酯、蠟、蟲膠、胺化蟲膠及乙酸鄰苯二甲酸纖維素。糖衣 錠劑係由糖衣包圍之壓縮錠劑,糖衣可有益於隱藏令人不 愉快之味道或氣味並防止錠劑氧化。薄膜衣錠劑係壓縮錠 劑’其經水溶性材料之薄層或薄膜覆蓋。薄膜衣包括但不 限於經乙基纖維素、敌曱基纖維素鈉、聚乙二醇、及 乙酸鄰苯二甲酸纖維素。薄膜衣可賦予與糖衣相同之一般 特性。多重壓縮錠劑係藉由一個以上壓縮循環製成之壓縮 旋劑,包括多層錠劑及壓製包衣錠劑或乾壓包衣錠劑。 叙劑劑型可自呈粉狀、結晶或粒狀形式之活性成份製 備’該等活性成份係單獨使用或與一或多種本文所述之載 劑或賦形劑組合,包括黏合劑、崩解劑、受控釋放聚合 物、潤滑劑、稀釋劑及/或著色劑。橋味劑及甜味劑尤其 可用於形成咀嚼錠劑及菱形錠劑。 本文所提供經口投與用醫藥組合物可以軟質或硬質膠囊 形式來提供,其可由明膠、甲基纖維素、澱粉或海藻酸鈣 製備。硬質明膠膠囊(亦稱為乾填充膠囊(DFC))係由兩部 分組成’一部分套在另一部分上,由此完全封閉活性成 份。軟質彈性膠囊(SEC)係軟質球形外殼,例如明膠外 殼’其藉由添加甘油、山梨醇、或類似多元醇而塑化。軟 質明膠外殼可含有防腐劑以防止微生物生長。適宜防腐劑 係彼等本文所述者’包括對羥基苯曱酸甲酯及對羥基苯甲 154881.doc -78- 201134820 酸丙醋及山梨酸。可將本文所提供之液體、半固體及固體 劑型囊封於膠囊中。適宜液體及半固體劑型包括存於碳酸 丙二醋、植物油或甘油三酯中之溶液及懸浮液《含有該等 溶液之膠囊可如美國專利第4,328,245號、第4,409,239號及 第4,410,545號中所述來製備。亦可根據彼等熟習此項技術 者習知之方法來塗覆膠囊以改變或維持活性成份之溶解。 本文所提供經口投與用醫藥組合物可以液體及半固體劑 型來提供,包括乳液、溶液、懸浮液、酏劑及糖漿。乳液 為兩相系統’其中一種液體以小球體形式遍佈分散於另一 種液體中’其可為水包油或油包水。乳液可包括醫藥上可 接受之非水性液體或溶劑、乳化劑及防腐劑。懸浮液可包 括醫藥上可接受之懸浮劑及防腐劑。水性醇溶液可包括醫 藥上可接受之縮酸,例如低碳烷基醛之二(低碳烷基)縮 酸,例如乙路縮一乙醇;及具有一或多個經基之水可混溶 溶劑’例如丙二醇及乙醇。酏劑係澄清的甜味化水醇性溶 液。糖漿係諸如蔗糖等糖之濃縮水溶液,且亦可含有防腐 劑。對於液體劑型而言,舉例而言,存於聚乙二醇中之溶 液可經足量醫藥上可接受之液體載劑(例如水)稀釋以便於 量測後投與。 其他可用液體及半固體劑型包括但不限於彼等含有本文 所提供活性成份及二烷基化單_或聚-伸烷基二醇者,包括 1,2-一甲氧基甲烷、二乙二醇二曱醚、三甘醇二甲醚、四 乙醇二曱醚、聚乙二醇·35〇·二曱醚、聚乙二醇_55〇_二甲 醚、聚乙二醇-750-二甲醚,其中35〇、55〇及75〇係指聚乙 154881.doc -79- 201134820 二醇之近似平均分子量。該等調配物可另外包含一或多種 抗氧化劑’例如丁羥甲苯(BHT)、丁羥茴醚(BHA)、沒食 子酸丙酯、維他命E、氫醌、羥基香豆素、乙醇胺、卵磷 脂' 腦磷脂、抗壞血酸、蘋果酸、山梨醇、磷酸、亞硫酸 氫鹽、偏亞硫酸氫鈉、硫二丙酸及其酯,及二硫代胺基甲 酸鹽。 本文所提供經口投與用醫藥組合物亦可以脂質體、膠 粒、微球體或奈米系統形式來提供。膠粒劑型可根據美國 專利第6,350,458號中所述來製備。 本文所提供、經口投與用冑藥組合物可以^重構成液體劑 型之非泡騰或泡騰粒劑及粉劑形式來提供。用於非泡騰粒 劑或粉劑之醫藥上可接受之載劑及賦形劑可包括稀釋劑、 甜味劑及潤劑。用於泡騰粒劑或粉劑中之醫藥上可接受 之載劑及賦形劑可包括有機酸及二氧化碳來源。 著色劑及矯味劑可用於所有上述劑型中。 文所提供經口投與用醫藥組合物可調配成直接或改良 釋放劑型,包括延遲_、持續_、脈衝-、受控-、靶向-及程 式化釋放形式》 B ·非經腸投與 /本文所提供醫藥組合物可以非經腸方式藉由注射、輸注 =植入投與以供局部或全身性投與。本文所用非經腸投與 靜脈内、動脈内、腹膜腔内、勒,内、心室内、尿道 =胸骨内、顧内、肌内、滑囊腔内、膀胱内及皮下投 15488l.doc 201134820 可以適於非經腸投與之任何劑型冑配本文所提供非經腸 投與用醫藥組合物’包括溶液、懸浮液、乳液、膠粒、脂 質體、微球體、奈米系統及適於在注射前於液體中形成溶 液或懸浮液之固體形式。該等劑型可根據彼等熟習藥物科 學技術者已知之習用方法來製備(參見Remington: The Science and practice of Pharmacy,如上所述)。 意欲用於非經腸投與之醫藥組合物可包括—或多種醫藥 上可接受之制及賦形劑’包括但不限於水性媒劑、水可 混溶媒劑、非水性媒劑、防止微生物生長之抗微生物劑或 防腐劑、穩定劑、促溶劑、等渗劑、緩衝劑、抗氧化劑、 局部麻醉劑、懸浮及分散劑、濁濕劑或乳化劑、錯合劑、 掩蔽劑或螯合劑、冷凌保護劑、康乾保護劑、增稠劑、pH 調節劑及惰性氣體。 適宜水性媒劑包括但不限於水、鹽水、生理鹽水或構酸 鹽緩衝鹽水(PBS)、氣化鈉注射液、林格氏注射液(㈣⑽ 咖㈣、等滲右旋糖注射液、無菌水注射液、右旋糖及 乳酸化林格氏注射液。適宜非水性媒劑包括但不限於植物 源不揮發油、!麻油、玉米油、棉軒油、橄欖油、花生 油、薄荷油、紅花油、芝麻油、大豆油、氫化植物油、敷 化大豆油、及椰子油之中鏈甘油三6|、及㈣籽油。適宜 水可混溶媒劑包括但不限於乙醇、丁二醇、液體聚乙 二醇(例如聚乙二醇300及聚乙二醇4〇〇)、丙二醇、甘油、 N-甲基-2-吡咯啶酮、N,N-二甲基乙醯胺及二曱亞砜。 適宜抗微生物劑或防腐劑包括但不限於酚類、曱酚類、 154881.doc -81 - 201134820 汞製劑、苯甲醇、氯丁醇、對羥基苯甲酸甲酯及對羥基苯 甲酸丙酯、硫柳汞、苯紮氣敍(benzalkonium chloride)(例 如苄索氯敍(benzethonium chloride))、對經基苯甲酸甲酯 及對羥基苯曱酸丙酯、及山梨酸。適宜等滲劑包括但不限 於氯化鈉、甘油及右旋糖。適宜緩衝劑包括但不限於磷酸 鹽及檸檬酸鹽。適宜抗氧化劑係彼等本文所述者,包括亞 硫酸氫鹽及偏亞硫酸氮納。適宜局部麻醉劑包括但不限於 鹽酸普魯卡因(procaine hydrochloride)。適宜懸浮及分散 劑係彼等本文所述者,包括羧甲基纖維素鈉、羥丙基甲基 纖維素及聚乙烯吡咯啶酮。適宜乳化劑係彼等本文所述 者,包括聚氧乙烯山梨醇酐單月桂酸酯、聚氧乙烯山梨醇 酐單油酸酯80及三乙醇胺油酸酯。適宜掩蔽劑或螯合劑包 括但不限於EDTA ^適宜PH調節劑包括但不限於氫氧化 鈉鹽I、彳宁彳豕酸、及乳酸。適宜錯合劑包括但不限於環 糊精類,包括(X-環糊精、β_環糊精、羥丙基_p_環糊精、磺 丁基醚-β-環糊精、及磺丁基醚_7_p_環糊精(CApTis〇L®, CyDex, Lenexa, KS) ° 备本文所提供醫藥組合物係經調配以用於多劑量投與 時,多劑量非經腸調配物應含有細菌抑制濃度或真菌抑制 濃度之抗微生物劑。如業内已知及實踐,所有非經腸調配 物必須為無菌的。 在一實施例中,非經腸投與用醫藥組合物係以即用無菌 洛液形式來提供。在另-實施例中,f藥組合物係以可在 使用則用媒劑重構成之無菌乾燥可溶產物形式來提供,包 154881.doc •82- 201134820 括凍乾粉劑及皮下注射 物係以即用無菌懸浮液丄: 醫藥組合 藥組合物係以可在使用在另一實施例中,醫 產物形式來提供。在又—^ 之無菌乾燥不可溶 在又一貫施例中,醫藥組合物係以即用 無菌乳液形式來提供。 本文所提供非經腸投與用醫藥組合物可調配成直接或改 良釋放劑型’包括延遲·、持續…脈衝_、受控_、靶向·及 程式化釋放形式。 可將本文所冑供非經腸投與用#帛組合物調配成懸浮 液、固體、半固體或觸變液體以供作為植入儲積物來投 與。在—實施{列中,冑本文所提供醫藥组合物分散於固體 内基質中’其由外層聚合物膜包圍,該膜在體液中不溶但 允許醫藥組合物中之活性成份擴散通過。 適宜内基質包括但不限於聚甲基丙烯酸甲酯、聚曱基丙 烯酸丁酯、塑化或未塑化聚氯乙烯、塑化耐綸、塑化聚對 苯二甲酸乙二酯'天然橡膠、聚異戊二烯、聚異丁烯、聚 丁二烯、聚乙烯、乙烯-乙酸乙烯酯共聚物、聚矽氧橡 膠、聚二曱基矽氧烷、聚矽氧碳酸酯共聚物、親水聚合物 (例如丙烯酸及曱基丙烯酸之酯之水凝膠)、膠原、交聯聚 乙烯醇、及交聯且部分水解之聚乙酸乙烯酯。 適宜外層聚合膜包括但不限於聚乙烯、聚丙烯、乙稀/ 丙烯共聚物、乙烯/丙烯酸乙酯共聚物、乙烯/乙酸乙烯酯 共聚物、聚矽氧橡膠、聚二曱基矽氧烷、氯丁橡膠、氣化 聚乙烯、聚氣乙烯、與乙酸乙烯酯之氯乙烯共聚物、二氣 154881.doc •83· 201134820 亞乙烯、乙烯及丙烯、聚對苯二甲酸乙二酯離子聚合物、 丁基橡膠環氧氣丙烧橡膠、乙稀/乙烯醇共聚物、乙烯/乙 酸乙烯酯/乙烯醇三元共聚物、及乙烯/乙烯氧基乙醇共聚 物。 c ·局部投與 可將本文所提供醫藥組合物局部投與至皮膚、孔口或黏 膜。本文所用之局部投與包括經真皮(内)、經結膜、角膜 内、眼内、經眼'經耳、經皮、經鼻、經陰道、經尿道、 經呼吸器官及經直腸投與。 可以適於局部投與以達成局部或全身性效應之任何劑型 調配本文所提供醫藥組合物,包括乳液、溶液、懸浮液、 乳膏、凝膠、水凝膠、軟膏、撒粉劑、敷料、酏劑、洗 劑、懸浮液、酊劑、糊劑、發泡劑、薄膜、氣溶膠、灌洗 劑、噴霧劑、栓劑、繃帶及皮膚貼劑。本文所提供醫藥組 合物之局部調配物亦可包含脂質體、膠粒'微球體、奈米 系統及其混合物。 適用於本文所提供局部調配物之醫藥上可接受之載劑及 賦形劑包括但不限於水性媒劑、水可混溶媒劑、非水性媒 劑、防止微生物生長之抗微生物劑或防腐劑、穩定劑、促 令劑、等滲劑、緩衝劑、抗氧化劑、局部麻醉劑、懸浮及 散齊丨潤/最劑或乳化劑、錯合劑、掩蔽劑或螯合劑、渗 透促進劑、冷柬保護劑、凍乾保護劑、增稠劑及惰性氣 體。 亦可藉由以下方式局部投與醫藥組合物:電穿孔、離子 154881.doc • 84 · 201134820 導入法、超音波導入法、超音促滲、或微型針或無針注 射,例如POWDERJECTTM(Chiron公司,Emeryville,CA)及 BIOJECTTM(Bioject Medical Technologies公司,Tualatin OR)。 本文所提供醫藥組合物可以軟膏、乳膏及凝膠形式來提 供。適宜軟膏媒劑包括油狀或烴類媒劑,包括豬油、安息 香化猪油、撤禮油、棉杆油及其他油、白礦脂;可乳化戍 吸收性媒劑,例如親水礦脂、硫酸羥基硬脂精及無水羊毛 脂;水可去除媒劑,例如親水軟膏;水溶性軟膏媒劑,包 括不同分子量之聚乙一醇,乳液媒劑,亦即油包水(w/〇) 乳液或水包油(0/W)乳液’包括鯨蠟醇、單硬脂酸甘油 醋、羊毛脂及硬脂酸(參見Remington: The Science and Practice of Pharmacy,如上所述卜該等媒劑係軟化劑,但 通常需要添加抗氧化劑及防腐劑。 適且乳膏基質可為水包油或油包水。適宜乳膏媒劑可為 水可洗媒劑,且含有油相、乳化劑及水相。油相亦稱為 「内部」相,其通常包含礦脂及脂肪醇(例如鯨蠟醇或硬 脂醇)。水相之體積通常(但不一定)大於油相,且通常含有 保濕劑。乳膏調配物中之乳化劑可為非離子型、陰離子 型、陽離子型或兩性表面活性劑。 凝膠為半固體懸浮液型系統。單相凝膠含有實質上均勻 分佈於整個液體載劑中之有機大分子。適宜膠凝劑包括但 不限於交聯丙烯酸聚合物,例如卡波姆(carb〇mer)、羧基 聚稀L及CARB〇P〇L® ;親水聚合物,例如聚環氧乙 154881.doc -85- 201134820 貌、聚氧乙婦-聚氧丙烯共聚物、及聚乙歸醇;纖維質聚 合物,例如經丙基纖維素、經乙基纖維素、經丙基甲基纖 維素、鄰苯二甲酸羥丙基甲基纖維素、及甲基纖維素;樹 膠’例如黃蓍膠及黃原膠;海藻酸納;及明膠。為製備均 勻凝膠,可添加諸如醇或甘油等分散劑,或可藉由研磨、 機械混合、及/或攪拌來分散膠凝劑。 本文所提供醫藥組合物可以經直腸、經尿道、經陰道、 或經陰道周圍方式使用以下形式來投與:检劑、陰道環、 探條、泥秦劑或泥敷劑、糊劑、粉劑、敷料、乳膏、硬膏 劑、避孕劑、軟f、溶液、乳液、懸浮液、陰道塞、凝 膠、發泡劑、喷霧劑或灌腸劑。該等劑型可使用以下文獻 中所述之習用製程製得:Remingt〇n: The以丨印⑶ Practice of Pharmacy ,如上所述。 直腸、尿道及陰道栓劑係插入身體孔口之固體,其在常 溫下為固態但在體溫下熔化或軟化以在孔口内釋放活性成 份。用於直腸及陰道栓劑之醫藥上可接受之載劑包括基質 或媒劑,例如硬化劑,其在與本文所提供醫藥組合物一起 調配時可使溶點接近體溫;及本文所述抗氧化劑,包括亞 硫酸氫鹽及偏亞硫酸氫鈉《適宜媒劑包括但不限於可可脂 (可可油)、甘油-明膠、碳蠟(聚氧乙稀二醇)、鯨蠟、石 蠟、黃白色蠟、及脂肪酸單·、二·及三甘油酯之適宜混合 物、及水凝膠,例如聚乙烯醇、甲基丙稀酸羥乙基酯及聚 丙烯酸。亦可使用各種媒劑之組合。直腸及陰道栓劑可藉 由壓縮或模製來製備。直腸及陰道栓劑之典型重量為約2 \5mi.doc • 86 - 201134820 g至約3 g。 本文所提供醫藥組合物可以以下形 肜式經眼投與:溶液、 L序夜、軟膏、乳液、凝膠形成溶々 腺· nB 1 /谷液用粉劑、凝 勝、眼插入物及植入體。 本文所提供醫藥組合物可以鼻内方 A或藉由吸入投盘至 醫藥組合物可以遞送用氣溶膠或溶液形式使用、: 裝置單獨提供或與適宜推進劑(例 1 ! , m2-四氟乙烷或 ,,:3’3’3-七氟丙烷)之組合來提供:增壓容器幫浦、 噴射器、霧化器(例如使用電流體動力 ^ X , U產生細霧之霧化 摇广麗器。醫藥組合物亦可以吹藥用乾粉劑形式單獨 k供或與惰性載劑(例如乳糖或鱗脂)及滴鼻劑組合提供。 2鼻内使用,粉劑可包含生物黏著劑,包括殼聚糖或環 糊精。 用於增壓容器、幫浦、喷射器、霧化器或伽之溶液 :戈懸洋液可經調配以含有乙醇、乙醇水溶液、或用於分 散、增溶或延續釋放本文所提供活性成份之適宜替代劑、 作為溶劑之推進劑、及/或表面活性劑,例如三油酸山梨 坦、油酸或寡聚乳酸。 可將本文所提供醫藥、组合物微粒化為適合吸入遞送之大 小,例如約50微米或更小,或約10微米或更小。具有該等 大小之顆粒可使用彼等熟習此項技術者已知之粉碎方法來 製備’例如螺旋噴射研磨、流化床喷射研磨、形成奈米顆 粒之超£&界流體處理、高壓勻漿或喷霧乾燥。 用於吸人器或吹藥器中之膠囊、泡罩及藥筒可經調配而 154881.doc -87- 201134820 含有本文所提供醫藥組合物之粉末混合物;適宜粉末基 質,例如乳糖或殿粉;及性能改良劑,例如^白㈣、甘 露醇或硬脂酸鎖。乳糖可為無水乳糖或呈單水合物形式。 其他適宜賦形劑或載劑包括但不限於右旋糖野、葡萄糖、 麥芽糖、山梨醇、木糖醇、果糖、嚴糖及海藻糖。本文所 提供用於吸人/鼻内投與之醫藥組合物另外可包含適宜橋 味劑⑼如薄荷腦及左薄荷腦)、及/或甜味劑(例如糖精及 糖精鈉)。 本文所提供用於局部投與之醫藥組合物可經調配以可直 接釋放或改良釋放,包括延遲…持續…脈衝_、受控… 靶向-及程式化釋放。 D.改良釋放 可將本文所提供醫藥組合物調配成改良釋放劑型。本文 所用之術語「改良釋放」係指在藉由相同途徑投與時活性 成份之釋放速率或位置與直接釋放劑型不同之劑型。改良 釋放劑型包括但不限於延遲-、延續-、延長…持續-、間 斷-、文控-、加速-及快速_、靶向_、程式化釋放及胃滯留 劑型。呈改良釋放劑型之醫藥組合物可使用彼等熟習此項 技術者習知之各種改良釋放裝置及方法來製備,包括但不 限於基質控制釋放裝置、滲透控制釋放裝置、多顆粒控制 釋放裝置、離子交換樹脂、腸溶包衣、多層包衣、微球 體、脂質體及其組合。活性成份之釋放速率亦可藉由改變 活性成份之粒徑及多態性來改變。 改良釋放之實例包括但不限於彼等以下美國專利中所述 154881.doc •88· 201134820 者:第 3,845,770號、第 3,916,899號、第 3,536,809號、第 3,598,123 號、第 4,008,719 號、第 5,674,533 號、第 5,059,595 號、第 5,591,767 號、第 5,120,548 號、第 5,073,543 號、第 5,639,476 號、第 5,354,556 號、第 5,639,480 號、第 5,733,566 號、第 5,739,108 號、第 5,891,474 號、第 5,922,356 號、第 5,972,891 號、第 5,980,945 號、第 5,993,855 號、第 6,045,830 號、第 6,087,324 號、第 6,113,943 號、第 6,197,350 號、第 6,248,363 號、第 6,264,970 號、第 6,267,981 號、第 6,376,461 號、第 6,419,961 號、第 6,589,548 號、第 6,613,358 號及第 6,699,500 號。 1.基質控制釋放裝置 呈改良釋放劑型之本文所提供醫藥組合物可使用彼等熟 習此項技術者已知之基質控制釋放裝置來製備(參見
Takada 等人,「Encyclopedia of Controlled Drug Delivery」,第 2卷,Mathiowitz編輯,Wiley,1999)。 在某些實施例中,呈改良釋放劑型之本文所提供醫藥組 合物係使用可蝕基質裝置來調配,其係水可膨脹、可蝕或 可溶聚合物,包括但不限於合成聚合物及天然存在聚合物 及衍生物’例如多糖及蛋白質。 :用於形成可蝕基質之材料包括但不限於殼多糖、脫乙 醯’又多糖 '右旋糖針及支鍵澱粉;瓊脂樹膠、阿拉伯樹 膠、刺梧桐樹膠、刺槐豆膠、黃蓍膠、角又菜膠、印度樹 膠、瓜爾膠、黃原膠及硬葡聚糖;澱粉,例如糊精及:芽 154881.doc •89· 201134820 糖糊精;親水膠體’例如果膠;磷脂,例如卵磷脂;海藻 酸鹽;海藻酸丙二醇酯;明膠;膠原;纖維質,例如乙基 纖維素(EC)、甲基乙基纖維素(Mec)、羧甲基纖維素 (CMC)、CMEC、羥乙基纖維素(HEC)、羥丙基纖維素 (HPC)、乙酸纖維素(CA)、丙酸纖維素(CP)、丁酸纖維素 (CB)、乙酸丁酸纖維素(cab)、CAP、CAT、羥丙基曱基 纖維素(HPMC)、HPMCP、HPMCAS、羥丙基曱基乙酸偏 苯三酸纖維素(HPMCAT)、及乙基羥乙基纖維素(EHEC); 聚乙烯"比咯啶酮;聚乙烯醇;聚乙酸乙烯酯;甘油脂肪酸 醋;聚丙烯酿胺;聚丙烯酸;乙基丙烯酸或曱基丙烯酸之 共聚物(EUDRAGIT® ’ Rohm America公司,Piscataway, NJ);聚(2-羥乙基-甲基丙烯酸酯);聚交酯;L_麩胺酸及 L-麩胺酸乙酯之共聚物;可降解乳酸-乙醇酸共聚物;聚_ D-(-)-3-羥丁酸;及其他丙稀酸衍生物’例如甲基丙烯酸 丁酯、甲基丙烯酸甲酯、曱基丙烯酸乙酯、丙烯酸乙酯、 甲基丙烯酸(2-二甲基胺基乙基)酯、及(三曱基胺基乙基) 曱基丙稀醯氯之均聚物及共聚物。 在某些實施例中,本文所提供醫藥組合物可與不可蝕基 質裝置一起調配。將活性成份溶解或分散於惰性基質中, 且在投與後主要藉由穿過惰性基質擴散而立即釋放。適宜 用作不可餘基質裝置之材料包括但不限於不溶性塑膠,例 如聚乙烯、聚丙烯、聚異戊二烯、聚異丁烯、聚丁二烯、 聚甲基丙烯酸曱酯、聚曱基丙烯酸丁酯、氣化聚乙烯、聚 氯乙烯、丙烯酸曱酯-甲基丙浠酸甲酯共聚物、乙烯-乙酸 154881.doc •90· 201134820 乙烯酯共聚物、乙烯/丙烯共聚物、乙烯/丙烯酸乙酯共聚 物、與乙酸乙烯酯之氣乙烯共聚物、二氯亞乙烯、乙烯及 丙烯、聚對苯二曱酸乙二酯離子聚合物、丁基橡膠、環氧 氯丙烷橡膠、乙烯/乙烯醇共聚物、乙烯/乙酸乙烯酯/乙烯 醇三元共聚物、乙烯/乙烯氧基乙醇共聚物、聚氣乙烯、 塑化耐綸、塑化聚對笨二甲酸乙二酯、天然橡膠、聚矽氧 橡膠、聚二曱基矽氧烷、及聚矽氧碳酸酯共聚物;親水聚 合物,例如乙基纖維素、乙酸纖維素、交聯聚維酮、及交 聯且部分水解之聚乙酸乙烯酯;及脂肪族化合物,例如巴 西棕櫚蠟、微晶蠟及甘油三醋。 在基質控制釋放系統中,可經由(例如)以下因素來控制 期望之釋放動力學:所用聚合物類型、聚合物黏度、聚合 物及/或活性成份之粒徑、活性成份與聚合物之比率、及 組合物中之其他賦形劑或載劑。 呈改良釋放劑型之本文所提供醫藥組合物可藉由彼等熟 習此項技術者習知之方法來製備,包括直㈣縮、乾法或 濕法製粒後壓縮、及熔體製粒後壓縮。 2·滲透控制釋放裝置 呈改良釋放劑型之本文所提供醫藥組合物可使用渗透控 制釋放裝置來製備,包括但不限於單室系統、二室系統、 不對稱膜技術(AMT)及擠出核心系統(ECs)。通常’,該等 裝置具有至少兩個組件:⑷含有活性成份之核心;及⑻ :有至少-個遞送口之半通透性膜,其囊封該核心。半通 透性膜控制水自應用水性環境流入核心,從而經由遞送口 15488 丨.doc 201134820 藉由擠出使藥物釋放。 除活性成份外,滲透裝置之核心視需要包括滲透劑,其 產生將水自應用環境輸送至裝置核心中之驅動力。一類滲 透劑係水可膨脹親水聚合物’其亦稱為「滲透聚合物」及 「水凝膠」。作為滲透劑之適宜水可膨脹親水聚合物包括 但不限於親水乙烯基及丙稀酸聚合物、諸如海藻酸鈣等多 糖、聚環氧乙烷(PEO)、聚乙二醇(PEG)、聚丙二醇 (PPG)、聚(甲基丙烯酸2_羥乙基酯)、聚(丙烯)酸、聚(曱基 丙烯)酸、聚乙烯吡咯啶酮(PVP)、交聯PVP、聚乙烯醇 (PVA) ' PVA/PVP共聚物、具有諸如甲基丙烯酸曱酯及乙 酸乙烯酯等疏水單體之PVA/PVP共聚物、含有大型peo嵌 段之親水聚胺基曱酸酯、交聯羧甲纖維素鈉、角叉菜膠、 細乙基纖維素(HEC)、羥丙基纖維素(HPC)、羥丙基甲基纖 維素(HPMC)、羧甲基纖維素(CMC)及羧乙基纖維素 (CEC)、海藻酸鈉、聚卡波非(polycarbophil)、明膠、黃原 膠及羥基乙酸澱粉鈉。 另類’參透劑係渗透壓調節物質(osmogen),其能夠吸 收水來影響周圍包衣障壁兩侧之滲透壓梯度。適宜滲透壓 調節物質包括但不限於無機鹽,例如硫酸鎂、氣化鎂、氣 化辦、氣化納、氣化鋰、硫酸鉀、磷酸鉀、碳酸鈉、亞硫 酸納、硫酸裡、氣化鉀及硫酸鈉;糖類,例如右旋糖、果 糖、葡萄糖、肌醇、乳糖、麥芽糖、甘露醇、棉子糖、山 梨醇、蔬糖、海藻糖及木糖醇;有機酸,例如抗壞血酸、 苯甲酸、富馬酸、檸檬酸、馬來酸、癸二酸、山梨酸、己 154881.doc -92· 201134820 二酸、乙二胺四乙酸、麩胺酸、對甲苯磺酸、琥珀酸及酒 石酸;尿素;及其混合物。 具有不同溶解速率之滲透劑可用於影響最初自劑型所遞 送活性成份之速率。舉例而言,非晶型糖(例如 MANN〇GEMtmEZ (SPI Pharma, Lewes, DE))可用於在最初 邊j時内it供較快遞送以促進產生期望治療效應,且在延 長時間内使剩餘量逐漸持續釋放以維持期望程度之治療效 應或預防效應。在此情況下,以此一速率釋放活性成份以 補充經代謝及排泄之活性成份之量。 核心亦可包括眾多種本文所述之其他賦形劑及載劑以增 強劑型之性能或促進穩定性或處理。 用於形成半通透性膜之材料包括各種等級之丙烯酸系 物、乙烯類、醚類、聚醯胺類、聚酯類及纖維質衍生物’ 其在生理相關pH下為水通透性及水不溶性,或易於因化學 改變(例如交聯)而具有水不溶性。可用於形成包衣之適宜 聚合物之實例包括塑化、非塑化及強化乙酸纖維素(CA)、 二乙酸纖維素、三乙酸纖維素、丙酸CA、硝酸纖維素、 乙酸丁酸纖維素(CAB)、乙基胺基甲酸CA、CAP、曱基胺 基甲酸CA、琥珀酸CA、偏苯三酸乙酸纖維素(CAT)、二甲 胺基乙酸CA、乙基碳酸CA、氯乙酸CA、乙基草酸CA、 曱基磺酸CA、丁基磺酸CA、對甲苯磺酸CA、瓊脂乙酸 酯、直鏈澱粉三乙酸酯、β-葡聚糖乙酸酯、β-葡聚糖三乙 酸酯、乙醛二曱基乙酸酯、刺槐豆膠之三乙酸酯、羥基化 乙烯-乙酸乙烯酯、EC、PEG、PPG、PEG/PPG共聚物、 154881.doc -93- 201134820 PVP、HEC、HPC、CMC、CMEC、HPMC、HPMCP、 HPMCAS、HPMCAT、聚(丙烯)酸及酯及聚·(甲基丙烯)酸 及其酯及共聚物、澱粉、右旋糖酐、糊精、脫乙醯殼多 糖、膠原、明膠、聚烯烴、聚醚、聚砜、聚醚砜、聚苯乙 烯、聚齒代乙烯、聚乙烯酯及醚、天然蠟及合成蠛。 半通透性膜亦可為疏水微孔膜,其中該等孔實質上經氣 體填充且未經水性介質潤濕但對水蒸氣具有通透性,如美 國專利第5,7 9 8,119號中所揭示。該疏水但水蒸氣可通透之 膜通常包含疏水聚合物,例如聚烯烴、聚乙烯、聚丙稀、 聚四氟乙稀、聚丙烯酸衍生物、聚趟、聚颯、聚謎颯、聚 笨乙稀、聚鹵代乙稀、聚二氟亞乙稀、聚乙烯酯及趟、天 然蠟及合成蠟。 半通透性膜上之遞送口可在塗覆後藉由機械或雷射鑽孔 來形成。遞送口亦可藉由水溶性材料塞之侵蝕或藉由核心 凹陷處之膜上較薄部分之破裂而原位形成。此外,遞送口 可在塗覆過程期間形成,如在美國專利第5,612,059號及第 5,698,220號中所揭示類型之不對稱膜包衣情況下。 所釋放活性成份之總量及釋放速率實質上可經由半通透 性膜之厚度及孔隙率、核心之組成、及遞送口之數量、大 小及位置來調節。 滲透控制釋放劑型中之醫藥組合物可另外包含本文所述 之額外習用賦形劑或載劑以促進調配物之性能或處理。 滲透控制釋放劑型可根據彼等熟習此項技術者習知之習 用方法及技術來製備(參見Remingt〇n: The Science and 134881.doc -94· 201134820
Practice of Pharmacy,如上所述;Santus 及 Baker,J. Controlled Release 1995,35,1-21 ; Verma 等人,Drug Development and Industrial Pharmacy 2000, 26, 695-708 ; Verma等人,J. Controlled Release 2002,79,7-27)。 在某些實施例中,本文所提供醫藥組合物係調配成amt 控制釋放劑型,其包含包覆核心之不對稱滲透膜,該核心 包含活性成份及其他醫藥上可接受之賦形劑或載劑。參見 美國專利第5,6 12,059號及WO 2002/17918。AMT控制釋放 劑型可根據彼等熟習此項技術者習知之習用方法及技術來 製備,包括直接壓縮、乾法製粒、濕法製粒及浸塗法。 在某些實施例中,本文所提供醫藥組合物係調配成ESC 控制釋放劑型,其包含包覆核心之滲透膜,該核心包含活 性成份、羥乙基纖維素及其他醫藥上可接受之賦形劑或載 劑。 3.多顆粒控制釋放裝置 呈改良釋放劑型之本文所提供醫藥組合物可藉由多顆粒 控制釋放裝置來製備,其包含眾多顆粒、粒劑或片劑,其 直徑範圍為約10 μπι至約3 mm、約50 μιη至約2.5 mm或約 1 00 μπι至約1 mm。該等多顆粒可藉由彼等熟習此項技術 者已知之方法來製備,包括濕法及乾法製粒、擠出/滾 圓、碾壓、熔體凍結,及藉由噴塗種核來製備。舉例而 言,參見 Multiparticulate Oral Drug Delivery ; Marcel Dekker: 1994 ;及 Pharmaceutical Pelletization Technology ; Marcel Dekker: 1989 o lS4881.doc -95- 201134820 可將本文所述其他賦形劑或載劑與醫藥組合物摻和在一 起以幫助處理及形成多n所得粒子可自身構成多顆粒 裝置或可經不同薄膜形成材料塗覆,例如腸溶聚合物、水 可膨脹及水溶性聚合物。可將多顆粒進__步處理為膠囊或 旋劑。 4.靶向遞送 本文所提供醫藥組合物亦可經調配以靶向欲治療個體身 體之特定組織、受體或其他區域,包括基於脂質體、重密 封紅細胞及抗體之遞送系統。實例包括但不限於彼等揭示 於以下美國專利中者:第6,316,652號、第6,274,552號、第 6,271,359 號、第 6,253,872 號、第 6,139,865 號、第 6,131,570 號、第 6,120,751 號、第 6,071,495 號、第 6,〇60,082 號、第 6,048,736 號、第 6,039,975 號、第 M〇4,534 號、第 5,985,307 號、第 5,972,366 號、第 5,900,252 號、第 5,840,674 號、第 5,759,542 號及第 5,7〇9,874 號。 使用方法 在一實施例中,提供治療、預防或改善個體之與CCR3 有關之病症、疾病或病狀之一或多種症狀的方法,其包含 向個體投與治療有效量之本文所提供化合物,例如,式I 或II化合物,包括其對映異構體、對映異構體之混合物、 兩種或更多種非對映異構體之混合物、互變異構體或兩種 或更多種互變異構體之混合物;或其醫藥上可接受之鹽、 溶劑合物、水合物或前藥。在一實施例中’個體係哺乳動 154881.doc •96· 201134820 物。在另一實施例中,個體係人類。 在另一實施财,提供治療、預防或改善個體因應 CCR3活性調節之病症、疾病或病狀之—或多種症狀的方 法’其包含向個體投與治療有效量之本文所提供化合物, 例如,式bin化合物,包括其對映異構體、對映異構體之 混合物、兩種或更多種非對映異構體之混合物、互變異構 體或兩種或更多種互變異構體之混合物;或其醫藥上可接 受之鹽、溶劑合物、水合物或前藥。在一實施例中,個體 係哺乳動物。在另一實施例中,個體係人類。 在再一實施例中,提供治療、預防或改善個體中由 CCR3受體介導之病症、疾病或病狀之一或多種症狀的方 法’其包含向個體投與治療有效量之本文所提供化合物, 例如,式I或II化合物,包括其對映異構體、對映異構體之 混合物、兩種或更多種非對映異構體之混合物、互變異構 體或兩種或更多種互變異構體之混合物;或其醫藥上可接 受之鹽、溶劑合物、水合物或前藥。在一實施例中,個體 係哺乳動物。在另一實施例中,個體係人類》 在再一實施例中,提供治療、預防或改善個體之嗜酸性 球相關性病症、疾病或病狀之一或多種症狀的方法,其包 含向個體投與治療有效量之本文所提供化合物,例如,式 I或II化合物’包括其對映異構體、對映異構體之混合物、 兩種或更多種非對映異構體之混合物、互變異構體或兩種 或更多種互變異構體之混合物;或其醫藥上可接受之鹽、 溶劑合物'水合物或前藥。在一實施例中’個體係哺乳動 154881.doc •97- 201134820 物。在另一實施例中,個體係人類。 在再一實施例中’提供治療、預防或改善個體之嗜驗性 球相關性病症、疾病或病狀之一或多種症狀的方法,其包 含向個體投與治療有效量之本文所提供化合物,例如,式 I或II化合物,包括其對映異構體、對映異構體之混合物、 兩種或更多種非對映異構體之混合物、互變異構體 或更多種互變異構體之混合物;或其醫藥上可接受之越、 溶劑合物、水合物或前藥❶在一實施例中,個體係哺乳動 物。在另一實施例中,個體係人類。 在再一實施例中,提供治療、預防或改善個體之肥大細 胞相關性病症、疾病或病狀之一或多種症狀的方法,其包 含向個體投與治療有效量之本文所提供化合物,例如,式 I或II化合物,包括其對映異構體、對映異構體之混合物、 兩種或更多種非對映異構體之混合物、互變異構體或兩種 或更多種互變異構體之混合物;或其醫藥上可接受之鹽、 溶劑合物、水合物或前藥。在一實施例中’個體係哺乳動 物。在另一實施例中,個體係人類。 在另貫施例中,提供治療、預防或改善個體之炎性疾 病之一或多種症狀的方法,其包含向個體投與治療有效量 之本文所提供化合物,例如,式化合物,包括其對映 異構體、董十映異才冓體之混合4勿、兩帛或更多種非對映異構 體之混合物、互變異構體或兩種或更多種互變異構體之混 合物;或其醫藥上可接受之鹽、溶劑合物'水合物或前 藥。在一實施例中,個體係哺乳動物。在另一實施例中, 154881.doc -98- 201134820 個體係人類。 可用本文所提供化合物(例如,式工或卩化合物,包括其 對映異構體、對映異構體之混合物、兩種或更多種非對映 異構體之混合物.、互變異構體或兩種或更多種互變異構體 之混口物,或其醫藥上可接受之鹽、溶劑合物、水合物或 月j藥)⑺療之病症、疾病、或病狀包括但不限於:⑴炎性 或過敏性疾病,包括全身性過敏及過敏病症、異位性皮 炎、蓴麻疹、藥物過敏、蟲螫過敏、食物過敏(包括腹腔 疾病及諸如此類)、及肥大細胞增生;(2)炎性腸病,包括 克羅恩氏病(Crohn’s diSease)、潰瘍性結腸炎、回腸炎及腸 炎’(3)血g火及貝切特氏症候群(Behcetis Syn£jr〇nie) ; (4) 牛皮癖及炎性皮膚病,包括皮炎、濕疹、異位性皮炎、過 敏性接觸性皮炎、蓴麻疹、病毒性皮膚病(包括彼等得自 人類乳頭瘤病毒、HIV或RLV感染者)、細菌性、真菌性及 其他寄生蟲性皮膚病、及皮膚紅斑狼瘡;(5)哮喘及呼吸道 過敏性疾病,包括過敏性哮喘、運動誘發之哮喘、過敏性 鼻炎、中耳炎、過敏性結膜炎、過敏性肺病及慢性阻塞性 肺病;(6)自身免疫疾病,包括關節炎(包括類風濕性及牛 皮癖性關節炎)、全身性紅斑狼瘡、I型糖尿病、重症肌無 力、多發性硬化症、葛雷夫斯氏病(Graves' disease)及腎小 球腎炎;(7)移植排斥(包括同種異體移植排斥及移植物抗 宿主病),例如皮膚移植排斥、實體器官移植排斥、骨騎 移植排斥;(8)發燒;(9)心血管病症’包括急性心臟衰 竭、低血壓、高血壓、心絞痛、心肌梗塞、心肌病、充血 154881.doc -99- 201134820 性心臟哀竭、動脈粥樣硬化、冠狀動脈病、再狹窄症及血 管狹窄;(1 〇)腦血管病症’包括外傷性腦損傷、中風、缺 血再灌注損傷及動脈瘤;(11)乳癌、皮膚癌、前列腺癌、 子宮頸癌、子宮癌、卵巢癌、睾丸癌' 膀胱癌、肺癌、肝 癌、喉癌、口腔癌、結腸癌及胃腸道癌(例如,食道癌、 胃癌、胰腺癌)、腦癌、甲狀腺癌、血癌及淋巴系統癌 症;(12)纖維化、結締組織疾病及結節病;(13)生殖及繁 殖病狀,包括勃起功能障礙;(14)胃腸道病症,包括胃 炎、潰瘍、噁心、胰腺炎及嘔吐;(15)神經性病症,包括 阿4海默氏症(Alzheimer’s disease) ; (16)睡眠障礙,包括 失眠、嗜眠症、睡眠呼吸暫停症候群、及匹克威克症候群 (Pickwick Syndrome); (17)疼痛;(18)腎臟病症;(19)眼部 病症,包括青光眼;及(2〇)傳染病,包括HIV。 在某些貫施例中,病症、疾病或病狀選自由以下組成之 群:哮喘、過敏性哮喘、運動誘發之哮喘、過敏性鼻炎、 常年性過敏性鼻炎、季節性過敏性鼻炎、異位性皮炎、接 觸性過敏、接觸性皮炎、結膜炎、過敏性結膜炎、嗜酸性 球性枝氣管炎、食物過敏、嗜酸性球性胃腸炎、炎性腸 病、肩瘍性結腸炎、克羅恩氏病、肥大細胞增生、高 症候群、全身性紅斑狼瘡、牛皮癬、痤瘡、多發性硬化 症、同種異體移植排斥、再灌注損傷、慢性阻塞性肺病、 丘施氏症候群(Churg-Strauss syndrome)、鼻竇炎、嗜驗性 球性白血病、慢性蓴麻疹、嗜鹼性球性白細胞增多、牛皮 癣、濕療、COPD(慢性阻塞性肺病)、關節炎、類風濕性 154881.doc •100· 201134820 關節炎、牛皮癣性關節炎及骨關節炎。 在某-實施例中,病症、疾病或病狀係哮喘、運動绣發 U喘 '㈣性鼻炎 '異位性皮炎、慢性阻塞性肺病或過 敏性結膜炎。 ^、見欲/。療之病症、疾病或病狀及個體狀況,本文所提 供化合物或醫藥組合物可藉由以下投與途徑來投與:經 口、非經腸(例如’肌内、腹膜腔内、靜脈内、icv、腦池 内注射或輸注、皮下注射或植入)、吸入.、經鼻、經陰 道經直腸、舌下或局部(例如經皮或局部),且可單獨或 與醫藥上可接受且適於每種投與途徑之賦形劑、載劑、佐 劑及媒劑一起調配成適宜劑量單元。本發明亦提供存於儲 積調配物中之本文所提供化合物或醫藥組合物之投與,其 中活性成份係在預定時期内釋放。 在哮喘、過敏性鼻炎、濕疹、牛皮癖、異位性皮炎、發 燒、敗血症、全身性紅斑狼瘡、糖尿病、類風濕性關節 炎、多發性硬化症'動脈粥樣硬化、移植排斥、炎性腸 病、癌症、或與CCR3受體有關之其他病狀、病症或疾病 之一或多種症狀之治療、預防或改善中,適宜劑量量通常 介於約0.001 mg/kg個體體重/天至1〇〇 mg/kg個體體重/天 (mg/kg/天)之間、約 〇·〇ι mg/kg/天至約 75 mg/kg/天、約 〇.1 mg/kg/天至約 50 mg/kg/天、約 0.5 mg/kg/天至約 25 mg/kg/ 天、或約1 mg/kg/天至約20 mg/kg/天之間’其可以單次或 多次劑量投與。在該範圍内,劑量可介於約0.005 mg/kg/ 天至約 0.05 mg/kg/天、約 0.05 mg/kg/天至約 0.5 mg/kg/ 154881.doc • 101 - 201134820 天、約0·5 mg/kg/天至約5.0 mg/kg/天、約1 mg/kg/天至約 15 mg/kg/天、約 1 mg/kg/天至約 20 mg/kg/天、或約 1 mg/kg/天至約50 mg/kg/天之間。在某些實施例中,劑量量 介於約0.001 mg/kg/天至約100 mg/kg/天之間。在某些實施 例中,劑量量介於約0.01 mg/kg/天至約75 mg/kg/天之間。 在某些實施例中,劑量量介於約0.1 mg/kg/天至約50 mg/kg/天之間。在某些實施例中,劑量量介於約〇.5 mg/kg/天至約25 mg/kg/天之間。在某些實施例中,劑量量 介於約1 mg/kg/天至約20 mg/kg/天之間。 對於經口投與,本文所提供醫藥組合物可調配成錠劑形 式’該等錢劑含有約1 ·〇 mg至約1,〇〇〇 mg活性成份,在一 實施例中,含有約1 mg、約5 mg、約! 〇 mg、約j 5 mg、約 20 mg、約 25 mg、約 50 mg、約 75 mg、約 100 mg、約 150 mg、約 200 mg、約 250 mg、約 300 mg、約 400 mg、約 500 mg、約 600 mg、約 750 mg、約 800 mg、約 900及約 1,000 mg活性成份’根據症狀來調節投與欲治療患者之劑量。醫 藥組合物可以每天1至4次之方案來投與,包括每天一次、 兩次、三次及四次。 然而’應理解’對於任一特定患者,特定劑量量及給藥 頻率可能會有所不同且應端視各種因素而定,該等因素包 括所用具體化合物之活性、該化合物之代謝穩定性及作用 時間長度、年齡、體重、一般健康狀況、性別、飲食、投 與模式及時間、排泄速率、藥物組合、特定病狀之嚴重程 度及接受療法之主體。 154881.doc 201134820 本發明亦提供調節CCR3活性之方法,其包含使⑽巧 體與本文所提供化合物接觸,該化合物係(例如)式_之 化合物’包括其對映異構體、對映異構體混合物、兩種或 更多種非對映異構體之混合物'互變異構體、或兩種或更 多種互變異構體之混合物;或其醫藥上可接受之鹽、溶劑 合物'水合物或前藥。在—實施例中,細胞表現咖3受 體。 本文所提供化合物(例如,式丨或丨〗化合物,包括其對映 異構體、對映異構體之混合物、兩種或更多種非對映異構 體之混合物、互變異構體或兩種或更多種互變異構體之混 合物;或其醫藥上可接受之鹽、溶劑合物、水合物或前 藥)亦可與其他藥劑組合或組合使用,該等其他藥劑可用 於治療、預防或改善本文所提供化合物有用之病症、疾病 或病狀之一或多種症狀,包括哮喘、過敏性鼻炎、濕疹、 牛皮癬、異位性皮炎、發燒、敗血症、全身性紅斑狼瘡、 糖尿病、類風濕性關節炎、多發性硬化症、動脈粥樣硬 化、移植排斥、炎性腸病、癌症、傳染病及彼等上文所述 病況。 在某些實施例中,本文所提供化合物可與業内已知之一 或多種類固醇藥物組合,包括但不限於包括以下藥物之 群:醛固酮(aldosterone)、倍氣米松(beclornetasone)、倍他 米松(betamethasone)、乙酸去氧皮質固酮(de〇xyc〇rtic〇ster〇ne acetate)、氟氫可的松(fludrocortisone)、氫化可的松 (hydrocortisone)(考的松(cortisol))、潑尼松龍(prednisolone)、 154881.doc -103· 201134820 潑尼松(prednisone)、甲基潑尼松龍、地塞米松(dexamethasone) 及曲安西龍(triamcinolone)。 在某些實施例中,本文所提供化合物可與業内已知之一 或多種抗細菌藥組合,包括但不限於包括以下藥物之群: 阿米卡星(amikacin)、阿莫西林(amoxicillin)、胺苄青黴素 (ampicillin)、胂凡納明(arsphenamine)、阿爾奇黴素 (azithromycin)、胺曲南(aztreonam)、阿洛西林(azlocillin)、 桿菌肽(bacitracin)、叛苄西林(carbenicillin)、頭抱克洛 (cefaclor)、頭抱經胺节(cefadroxil)、頭抱孟多(cefamandole)、 頭孢°坐林(cefazolin)、頭孢氨苄(cephalexin)、頭抱地尼 (cefdinir)、頭抱托余(cefditorin)、頭孢0比肪(cefepime)、 頭孢克肪(cefixime)、頭抱11 底酮(cefoperazone)、頭抱。塞肪 (cefotaxime)、頭孢西丁(cefoxitin)、頭抱泊肪(cefpodoxime)、 頭抱羅齊(cefprozil)、頭抱他咬(ceftazidime)、頭孢布稀 (ceftibuten)、頭孢。坐肪(ceftizoxime)、頭抱曲松(ceftriaxone)、 頭抱0夫辛(cefuroxime)、氣黴素(chloramphenicol)、西拉司 丁(cilastin)、環丙沙星(ciprofloxacin)、克拉黴素 (clarithromycin)、克林黴素(clindamycin)、氣0坐西林 (cloxacillin)、黏菌素(colistin)、達福普汀(dalfopristin)、 地美環素(demeclocycline)、雙氣西林(dicloxacillin)、地紅 黴素(dirithromycin)、多西環素(doxycycline) ' 紅黴素 (erythromycin)、恩氟沙星(enrofloxacin)、厄他培南 (ertepenem)、乙胺丁醇(ethambutol) 、 II 氯西林 (flucloxacillin)、填徽素(fosfomycin)、吱喃。坐酮 154881.doc 201134820 (furazolidone)、加替沙星(gatifloxacin)、格爾德黴素 (geldanamycin)、慶大黴素(gentamicin)、除莠黴素 (herbimycin)、亞胺培南(imipenem)、異煙肼(isoniazid)、 卡那黴素(kanamycin)、左氧氟沙星(levofloxacin)、利奈唑 胺(linezolid)、洛美沙星(lomefloxacin)、氣碳頭孢 (loracarbef)、 續胺米隆(mafenide)、 莫西沙星 (moxifloxacin)、美羅培南(meropenem)、曱硝。坐 (metronidazole)、美洛西林(mezlocillin)、米諾環素 (minocycline)、莫匹羅星(mupirocin)、萘夫西林 (nafcillin)、新黴素(neomycin)、奈替米星(netilmicin)、》夫 喃妥因(nitrofurantoin)、法氟沙星(norfloxacin)、氧氟沙星 (ofloxacin) 、土 黴素(oxytetracycline)、盤尼西林 (penicillin)、旅拉西林(piperacillin)、平板徽素 (platensimycin)、多黏菌素 B (polymyxin B)、百浪多息 (prontocil)、D比。秦醯胺(pyrazinamide)、奎奴普丁 (quinupristine)、利福平(rifampin)、羅紅黴素 (roxithromycin)、壯觀黴素(spectinomycin)、键黴素 (streptomycin)、項胺醋酿(sulfacetamide)、績胺甲售二 〇坐 (sulfamethizole)、確胺甲0惡0圭(sulfamethoxazole)、替考拉 寧(teicoplanin)、泰利黴素(telithromycin)、四環素 (tetracycline)、替卡西林(ticarcillin)、妥布拉黴素 (tobramycin)、甲氧苄咬(trimethoprim)、醋竹桃黴素 (troleandomycin)、曲伐沙星(trovafloxacin)及萬古黴素 (vancomycin) 〇 154881.doc -105- 201134820 在某些實施例中,本文所提供化合物可與業内已知之一 或多種抗真菌藥組合’包括但不限於包括以下藥物之群: 阿莫羅芬(amorolfine)、兩性黴素 b (amphotericin B)、阿 尼芬淨(anidulafungin) '聯苯苄唑(bifonaz〇le)、布替萘芬 (butenafine)、布康唑(but〇conaz〇le)、卡泊芬淨(casp〇fungin)、 環 °比酮(ciclopirox)、克黴唑(ci〇trimaz〇ie)、益康唾 (econazole)、芬替康唑(fenticonaz〇ie)、非律平(fiUpin)、 氟康0坐(fluconazole)、異康 〇坐(isoconaz〇ie)、伊曲康 〇坐 (itraconazole)、酮康唑(ketoconazole)、米卡芬淨 (micafungin)、咪康唑(miconazole)、萘替芬(nafUfine)、納 他黴素(natamycin)、製黴菌素(nyStatin)、奥昔康。坐 (oxyconazole)、雷夫康 坐(ravuconazole)、泊沙康 0坐 (posaconazole)、龜裂殺菌素(rimocidin)、舍他康唾 (sertaconazole)、硫康 °坐(sulconazole)、特比萘芬 (terbinafine)、特康唑(terconazole)、噻康唑(tioconazole) 及伏立康唾(voriconazole)。 在某些實施例中,本文所提供化合物可與業内已知之一 或多種抗凝血藥組合,包括但不限於包括以下藥物之群: 醋确香豆醇(acenocoumarol)、阿加曲班(argatroban)、比伐 盧定(bivalirudin)、來匹盧定(lepirudin)、續達肝素 (fondaparinux)、肝素、苯茚二酮、華法林(warfarin)及希 美加群(ximelagatran)。 在某些實施例中,本文所提供化合物可與業内已知之__ 或多種溶血栓藥組合,包括但不限於包括以下藥物之群: 154881.doc -106· 201134820 阿尼普酶(anistreplase)、瑞替普酶(reteplase)、t-PA(阿替 普酶激活酶(alteplase activase))、鏈激酶、替奈普酶 (tenecteplase)及尿激酶。 在某些實施例中,本文所提供化合物可與業内已知之一 或多種非類固醇類消炎藥組合,包括但不限於:醋氣芬酸 (aceclofenac)、阿西美辛(acemetacin)、阿洛普令(amoxiprin)、 阿司匹林(aspirin)、阿紮丙宗(azapropazone)、貝諾酯 (benorilate)、溴芬酸(bromfenac)、卡洛芬(carprofen)、塞 來考昔(celecoxib)、三水揚酸膽驗鎂、雙氯芬酸 (diclofenac)、二氟尼柳(diflunisal)、依乾度酸(etodolac)、 艾托考昔(etoricoxib)、法拉胺(faislamine)、芬布芬 (fenbufen)、非諾洛芬(fenoprofen)、氟比洛芬(flurbiprofen)、 布洛芬(ibuprofen)、吲哚美辛(indometacin)、酮洛芬 (ketoprofen)、酮咯酸(ketorolac)、氣諾昔康(lornoxicam)、 洛索洛芬(loxoprofen)、魯米考昔(lumiracoxib)、甲氣芬那 酸(meclofenamic acid)、甲芬那酸(mefenamic acid)、美洛 昔康(meloxicam)、安替比林甲胺甲烷(metamizole)、水楊 酸曱醋、水揚酸鎮、萘丁美網(nabumetone)、萘普生 (naproxen)、尼美舒利(nimesulide)、羥布宗(OXyphenbutazone)、 帕瑞考昔(parecoxib)、保泰松(phenylbutazone)、吡羅昔康 (piroxicam)、雙水楊酯、舒林酸(suiindac)、磺吡酮 (sulfinpyrazone)、舒洛芬(suprofen)、替諾昔康 (tenoxicam)、噻洛芬酸(tiaprofenic acid)及托美丁 (tolmetin) 〇 154881.doc •107- 201134820 在某些實施例中,本文所提供化合物可與業内知己之— 或多種抗血小板藥組合,包括但不限於:阿昔單抗 (abciximab)、西洛他唑(cilostazol)、氣吡格雷(cl〇pid〇grel)、 雙嘧達莫(dipyridamole)、噻氯匹定(ticlopidine)及替羅非 班(tironbin)。 本文所提供化合物亦可與其他類化合物組合投與,包括 但不限於(1) α·腎上腺素能藥;(2)抗心律不齊藥;(3)抗動 脈粥樣硬化藥’例如ACAT抑制劑;(4)抗生素,例如蒽環 (anthracycline)、博來黴素(bleomycin)、絲裂黴素 (mitomycin)、放線菌素D (dactinomycin)及普利黴素 (plicamycin) ; (5)抗癌藥及細胞毒性劑,例如,烧基化 劑’例如氮芥、烷基磺酸鹽、亞硝基脲(nitros〇urea)、氮 丙α定及二氛稀’(6)抗凝血樂’例如醋硝香豆醇、阿加曲 班、比伐盧定、來匹盧定、磺達肝素、肝素、苯茚二酮、 華法林及及希美加群;(7)抗糖尿病藥,例如雙胍(例如, 二甲雙胍(metformin))、葡糖苷酶抑制劑(例如,阿卡波糖 (acarbose))、胰島素、美格替耐(meglitinide)(例如,瑞格 列奈(repaglmide)) '磺醯基脲(例如,格列美脲(gHmepiride)、 格列本脲(glyburide)及格列吡嗪(glipizide))、噻唑啶二酮 (例如,曲格列酮(troglitazone)、羅格列酮(r〇siglhaz〇ne) 及吡格列酮(Pi〇glitazone))及ΡΡΑΚ·γ激動劑;(8)抗真菌 藥,例如阿莫羅芬、兩性黴素Β、阿尼芬淨、聯苯苄唑、 布替萘芬、布康唾、卡泊芬淨、環賴、克黴唾、益康 唑、芬替康唑、非律平、氟康唑、異康唑、伊曲康唑、酮 154881.doc -108- 201134820 康唑、米卡芬淨、唓忠1 ^ ’、唑、奈替芬、納他黴素、製黴菌 素、奥昔康唾、雷夫廉η4ί >Α 由天康坐、泊沙康唑、龜裂殺菌素、舍他 康坐,Γ康坐、特比蔡芬、特康。坐、°塞康嗤及伏立康0坐; ()肖炎藥例如’非類固醇類消炎藥’例如醋氯芬酸、阿 西美辛、阿洛普令、阿§lm;*Wr j*- . .叮刁匹林、阿紮丙宗、貝諾酯、溴芬 酸、卡洛芬、塞來考昔、三水楊酸膽鹼鎂、雙氯芬酸、二 *氟尼柳、依託度酸、艾托考昔、法拉胺、芬布芬、非諾洛 芬、氟比洛芬、布洛芬、十朵美辛、酮洛芬、嗣嘻酸、氣 諾昔康、洛索洛芬、魯米考昔、甲氣芬那酸、甲芬那酸、 美洛昔康、安替比林甲胺甲烷、水揚酸甲酯、水揚酸鎂、 萘丁美酮、萘普生、尼美舒利、羥布宗、帕瑞考昔、保泰 松、°比羅昔康、雙水揚醋、舒林酸、項。比_、舒洛芬、替 諾昔康、噻洛芬酸及托美丁 ;(10)抗代謝藥,例如葉酸拮 抗劑、嘌呤類似物及嘧啶類似物;(11)抗血小板藥,例如 GPIIb/IIIa阻斷劑(例如,阿昔單抗、依替巴肽 (eptifibatide)及替羅非班)、P2Y(AC)拮抗劑(例如,氯吡格 雷 '嚷氣匹定及CS-747)、西洛他β坐、雙嘴達莫及阿司匹 林;(12)抗增殖藥,例如甲胺蝶吟(methotrexate)、FK506 (他克莫司(tacrolimus))及嗎替麥考酚酯(mycophenolate mofetil) ; (13)抗TNF抗體或可溶性TNF受體,例如依那西 普(etanercept)、雷帕黴素(rapamycin)及來氣米特 (leflunimide); (14) aP2抑制劑;(15) β_腎上腺素能藥,例 如卡維地洛(carvedilol)及美托洛爾(metoprolol) ; (16)膽汁 酸多價螯合劑,例如消膽胺(questran) ; (17)好通道阻斷 154881.doc -109- 201134820 劑,例如苯確酸胺氣地平(amlodipine besylate); (18)化學 治療劑;(19)環氧化酶-2 (COX-2)抑制劑,例如塞來考昔 及羅非昔布(rofecoxib) ; (20)環抱菌素;(21)細胞毒性藥 物,例如硫唑嘌呤(azathioprine)及環磷醯胺(cyclophosphamide); (22) 利尿藥,例如氣"塞嗓(chlorothiazide)、氫氣嗟嗪 (hydrochlorothiazide)、氟甲售嗓(flumethiazide)、氫敗 0塞 嗪(hydroflumethiazide)、苄氟嗟唤(bendroflumethiazide)、 曱基氯嘆嗓(methylchlorothiazide)、 三氣0塞嗪 (trichloromethiazide)、泊利0塞 °秦(polythiazide)、苄0塞0秦 (benzothiazide)、依他尼酸(ethacrynic acid)、替尼酸 (ticrynafen)、氯0塞酮(chlorthalidone)、0夫塞米(furosenide)、 莫0坐胺(muzolimine)、布美他尼(bumetanide)、胺苯嗓咬 (triamterene)、阿米洛利(amiloride)及螺内醋(spironolactone); (23) 内皮素轉化酶(ECE)抑制劑,例如膦醯二肽 (phosphoramidon); (24)酶,例如L-天冬醯胺酶;(25)因子 Vila抑制劑及因子Xa抑制劑;(26)法呢基蛋白轉移酶抑制 劑;(27)貝特類(fibrates) ; (28)生長因子抑制劑,例如 PDGF活性調節劑;(29)生長激素促分泌劑;(30) HMG輔 酶A還原酶抑制劑,例如普伐他彡丁(pravastatin)、洛伐他江 (lovastatin)、阿托伐他汀(atorvastatin)、辛伐他 $丁 (simvastatin)、NK-104(亦稱為伊伐他汀(itavastatin)、尼伐 他汀(nisvastatin)或尼巴他汀(nisbastatin))及 ZD-4522(亦稱 為羅舒伐他汀(rosuvastatin)、阿他伐他汀(atavastatin)或維 薩他汀(visastatin));中性肽鍵内切酶(NEP)抑制劑;(3 1) 154881.doc -110- 201134820 激素性藥物’例如糠皮質激素類(例如,可的松 (cortisone))、雌激素/抗雌激素藥、及雄激素/抗雄激素 藥、孕激素(pr0gestin)及促黃體生成素_釋放激素拮抗劑、 及乙酸奥曲肽(octreotide acetate)(32)免疫抑制劑;(33)鹽 皮質激素受體拮抗劑,例如螺内酯及依普利酮 (eplerenone) ; (34)微管破壞劑,例如海鞘素(ecteinascidin); (35)微管穩定劑,例如紫杉醇(pacitaxel)、多西他赛 (docetaxel)及埃坡黴素(ep〇thilone) A-F ; (36) MTP抑制 劑;(37)尼亞新(niacin) ; (38)磷酸二酯酶抑制劑,例如 PDE III抑制劑(例如,西洛他嗤(cilostazol))及PDE V抑制 劑(例如,西地那非(sildenafil)、他達拉非(tadalafil)及伐 地那非卜&[(^1^打1));(39)源於植物之產物,例如長春花生 物鹼(vinca alkaloid)、表鬼臼毒素(epipodophyllotoxin)及 紫杉烷(taxane) ; (40)血小板活化因子(PAF)拮抗劑;(41) 鉑配位錯合物,例如順鉑(cisplatin)、沙鉑(satraplatin)及 卡鉑(carboplatin) ; (42)鉀通道開放劑;(43)異戊二烯蛋白 轉移酶抑制劑;(44)蛋白酪胺酸激酶抑制劑;(45)腎素抑 制劑;(46)角鯊烯合成酶抑制劑;(47)類固醇’例如醛固 酮、倍氯米松、倍他米松、匕酸去氧皮質固晒、氟氫可的 松、氫化可的松(考的松)、潑尼松龍、潑尼松、曱基潑尼 松龍 '地塞米松及曲安西龍;(48) TNF-α抑制劑,例如替 尼達普(tenidap) ; (49)凝血酶抑制劑,例如水蛭素;(50)溶 血栓藥,例如阿尼普酶、瑞替普酶、替奈普酶、組織纖溶 酶原激活物(tPA)、重組tPA、鍵激酶、尿激酶、尿激酶原 154881.doc -111- 201134820 及茴醯化纖溶酶原鏈激酶激活物複合物(APSAC) ; (51)血 栓素受體拮抗劑,例如伊非曲班(ifetroban) ; (52)拓撲異構 酶抑制劑;(53)血管肽酶抑制劑(雙重νερ-ACE抑制劑), 例如奥馬曲拉(omapatrilat)及古莫曲拉(gem〇patrilat);及 (54)各種其他藥劑,例如羥基脲、丙卡巴肼 (procarbazine)、米托坦(mitotane)、六曱喊胺及金化合 物。 該等其他藥劑或藥物可藉由一種途徑並以其常用量與本 文所提供化合物(例如式I或II化合物)同時或依序投與,該 等化合物包括其單一對映異構體、對映異構體之混合物、 或非對映異構體之混合物;或其醫藥上可接受之鹽、溶劑 合物或前藥。在本文所提供化合物與一或多種其他藥物同 時使用時,可使用除含有本文所提供化合物外亦含有該等 其他藥物之醫藥組合物,但並非必須。因此,本文所提供 醫藥組合物包括彼等除本文所提供化合物外亦含有一或多 種其他活性成份或治療劑之醫藥組合物。 本文所提供化合物與第二活性成份之重量比可有所變 化且其取決於母一種成份之有效劑量。一般而言,應使 用每一種成份之有效劑量。因此,舉例而言,在本文所提 供化合物與NSAID組合時,該化合物與Nsaid之重量比可 介於約1,000:1至約1:1,麵之間,或介於約2〇〇:1至約1:2〇〇 之間。通常’本文所提供化合物與其他活性成份之組合亦 應屬於上述範圍内,但在每一情況下皆應使用每一種活性 成份之有效劑量。 154881.doc •112· 201134820 本文所提供化合物亦可使用彼等熟習此項技術者熟知之 包裝材料以製品形式提供。例如,參見美國專利第 5,323,907號;第 5,052,558號;及第 5,033,252號。醫藥包 裝材料之實例包括但不限於泡罩包裝、瓶子、管、吸入 器、幫浦、袋子、小瓶、容器、注射器及適於所選調配物 及擬定治療及投與方式之任何包裝材料。 本發明亦提供套組,當從業醫師使用時其可簡化適量之 活性成份至個體之投與。在某些實施例中,本文所提供套 組包括容器及本文所提供化合物之劑型,該化合物包括其 單一對映異構體或非對映異構體之混合物;或其醫藥上可 接受之鹽、溶劑合物或前藥。 在某些實施例中,該套組在包含一或多種本文所述其他 治療劑之容器中包括一容器,其包含本文所提供化合物之 劑型,該化合物包括其單一對映異構體或非對映異構體之 混合物;或其醫藥上可接受之鹽、溶劑合物或前藥。 本文所提供套組可進一步包括用以投與活性成份之裝 置。該等裝置之實例包括但不限於注射器、無針注射器、 滴袋、貼片及吸人器。本文所提供套組亦可包括用於投與 活性成份之保險套。 本文所提供套組m包括可用於投與—或多種活性 成份之醫藥上可接受之媒劑。舉例而言,若活性成份以須 經重構以用於非經腸投與之固體形式提供,則該套組可包 含適宜媒劑之密封容器,可將活性成份溶解於其中以形成 適於非經腸投與之無顆粒無菌溶液。醫藥上可接受之媒劑 154881.doc •113- 201134820 之實例包括但不限於:水性媒劑,包括但不限於usp注射 用水、氣化鈉注射液、林格氏注射液、右旋糖注射液右 旋糖及氣化鈉注射液、及乳酸化林格氏注射液;水可混溶 媒劑’包括但不限於乙醇、聚乙二醇及聚丙二醇;及非水 性媒劑,包括但不限於玉米油、棉籽油、花生油、芝麻 油、油酸乙酯、肉豆蔻酸異丙酯及苯曱酸苄酯。 藉由以下非限制性實例來進一步理解本發明。 實例 如本文所用,不管是否具體定義特定之縮寫,該等方 法、反應圖及實例中所用之符號及慣例應與彼等用於當前 科學文獻中者保持一致,例如,Journal of the AmeHcan Chemical Society 或 J0urnal ofBi〇1〇gical chemistry。具體 而言(但並非加以限制),可在實例及說明書通篇中使用以 下縮寫:g(克);mg(毫克);mL(毫升);(微升);mM(毫 莫耳);μΜ(微莫耳);Hz(赫兹);mhz(死赫兹);_〇1(毫 莫耳);hr或hrs(小時);min(分鐘);MS(質譜),ESI(電喷 射離子化);TLC(薄層層析);HPLC(高壓液相層析); THF〇氫咬喃);CDCh(氘化氯仿);DMS0(二曱亞砜); DMS0-d6(沉化一曱亞;ε風);EtOAc(乙酸乙酯);MeOH(曱 醇);及BOC(第三丁氧基羰基)。 對於所有以下實例,可利用彼等熟習此項技術者已知之 標準處理及純化方法《除非另有說明’否則所有溫度皆以 °C (攝氏度)表示。除非另有注明,否則所有反應均在室溫 下實施。本文所揭示之合成方法意欲經由使用具體實例來 154881.doc •114· 201134820 例示可應用之化學方法,日卄x扣+ 士 ^ 且並不知不本發明之範圍。 實例1 N-(1-(S-氰基·2·(3,5_二氣苯氧基)苯基伽基)六氫咐咬心 基)·3-氟笨磺醯胺(25)之製備
α C102S
CN 將市售4-氣-3-节腈溶於4份前中。添加i份水以及硫氮 化鈉(3當量)並在4代下_過夜。ΤΙχ(存於己烧中之25% EtOAc)也實反應已完成。在真空中蒸發且沉澱出產 ㈣心㈣㈣白色㈣,使用水洗滌並在輕微加 熱下於真空烘箱中乾燥(產率為97〇%)。 在研蛛及研杵中研磨笨胺產物並溶於11份HQ及4份乙酸 之混。物中。在單獨器凰中,在s〇2氣體下攪拌5〇份乙酸 直至飽和為止(藉由重量予以證實)。將HC1 :乙酸:苯胺 此。物在10 C下放置於乾冰/乙醇浴中。將亞硝酸鈉(丨j當 量)溶於最小量水中並逐滴添加至肥:乙酸:苯胺混合物 中’同時不能使溫度升至高於約· 5。〔。將所得混合物擾摔 45刀鐘以形成重I鹽離子。將氯化亞銅(1)(0.1當量)及氣化 154881.doc •115· 201134820 銅(11)(0.25當量)添加至s〇2/乙酸溶液中且授拌3〇分鐘並在 冰浴中冷卻至HTC。將重氮鹽混合物逐份添加至氣化亞鋼 (I)/氣化銅(II)懸浮液中,同時將溫度維持於3(rc或更低。 完全合併後,攪拌混合物直至氣體逸出停止為止,從而形 成暗綠色溶液。然後在攪拌下將混合物緩慢傾倒至2〇〇份 冰水中直至冰融化為止。藉由真空過濾收集所得白色沉澱 物並使用水洗滌(產率為72.9%)。
將2-氣氰基苯_ι_磺醯氯(8〇〇 g)溶於1〇〇 ml ΤΗρ中且 添加N-BOC-4-胺基六氫吡啶(5 79 g)。緩慢添加6當量之 κζ(:〇3並將混合物在室溫下攪拌丨小時。添加3,5_二氣苯酚 (11.06 g)及18-冠-6 (4.66 g)並將反應在回流下(75。〇攪拌4 天。冷卻混合物並真空過濾,在真空中濃縮濾液,再次溶 於二氣曱统中’使用水進行分配並使用二氯甲烷將水層萃 取二次。使用飽和碳酸氫鈉、水及鹽水洗滌合併之有機層 並藉由MgS〇4乾燥。在真空中濃縮濾液,使用二氣曱烷/二 異丙基驗研磨並真空過濾以提供黃色粉末。將粉末在 MeOH中重結晶以提供白色粉末產物(14 5〇 g,87 3%)。
154881.doc •116- 201134820 將經BOC保護之胺(11.00 g)懸浮於二氣甲燒(400 mL)中 且添加11.0 ml三氟乙酸。撥拌22小時之後,起始材料耗盡 (藉由HPLC證實)。在真空中濃縮混合物並藉由添加3N NaOH (36·0 mL)使所得油狀物達到pH 7。在真空中過滤白 色懸浮液,並將固體在MeOH中重結晶以提供白色粉末 (6.51 g,73.0%)。 將胺起始材料3-(4-胺基六氣》»比咬_ι_基續酿基)_4_(3,5_二 氯苯氧基)苄腈(100 mg)溶於3.0 mL二氯甲烧中,且依次添 加三乙胺(0.042 mL,1.3當量)以及3-氟苯磺醯氣(58 mg, 1.3當量)。攪拌3.5小時之後,起始材料耗盡,如藉由tlC 所證實(50% EtOAc/己烷)。藉由正相矽膠層析(〗4%,35% EtOAc/己烷)實施純化以提供期望產物,使用二異丙基醚 研磨並真空過濾以得到白色粉末(61 mg,44.5%)。4 NMR (500 MHz, CDC13) δ: 8.24 (d, J=2 Hz, 1H), 7.78 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.53 (m, 2H), 7.41 (m, 1H), 7.31 (m, 2H),6.99 (m,3H),4.93 (t,J=7 Hz,1H), 3.26 (m,1H), 2.46 (m,2H),1_89 (m,2H),1.65 (m,2H)。MS(ESI+離子, m/z) : 585。 實例2 1-(1-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫啦啶_4-基)_3-(3-氟苯基)脲(4)之製備
154S81.doc •117- 201134820
根據實例1之程序來製備3_(4·胺基六氫。比啶_丨_基磺醯 基)·4-(3,5·二氣苯氧基)苄腈。藉由向存於二氯甲烷〇 mL)中之3-(4-胺基六氫吡啶基磺醯基)_4_(3,5_二氯笨氣 基)苄腈(102 mg)的溶液中依次添加三乙胺(〇 42 mL)以及 異氰酸3 -氣本基醋來製備最終產物。攪拌3小時之後’起 始材料耗盡,如藉由TLC所證實(5〇% EtOAc/己烷)。添加4 mL己烷且藉由真空過濾收集產物並使用1 n HC1洗滌。獲 得白色粉末形式之期望產物(99 mg,73.3%) » 4 NMR (500 MHz, DMS0-d6) δ: 8.61 (s, 1Η), 8.28 (d, J=2 Hz, 1H), 8.13 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.55 (t, J=2 Hz, 2H), 7.42 (m, 1H), 7.37 (d,J=2 Hz,2H), 7.34 (d,J=9 Hz,1H),7.22 (m, 1H),6.99 (m,1H),6.68 (m,1H),6.33 (d,J=8 Hz,1H),3.61 (m, 3H), 2.96 (m, 2H), 1.88 (m, 2H), 1.40 (m, 2H)。 MS(ESI +離子,m/z) : 564。 實例3 N-(l-(5-氰基-2-(3,5-二氯苯氧基)苯基磺醮基)六氫吨啶-4- 基)苯甲醯胺(1)
154881.doc -Π8- 201134820 根據本文所述之方法來製備化合物1。iH NMR (500 MHz, CDC13) δ: 8.32 (d, J=1 Hz, 1H), 7.79 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.74 (d, J=8 Hz, 2H), 7.52 (m, 1H), 7.44 (m, 2H), 7.30 (s, 1H), 7.04 (d, J=9 Hz, 1H), 7.00 (s, 2H), 5.98 (J=7 Hz, 1H), 4.12 (m, 1H), 3.96 (m, 2H), 2.92 (m, 2H), 2.14 (m,2H),1.62 (m,2H)。MS(ESI+離子,m/z) : 531。 實例4 N-(l-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫吼啶-4- 基)甲烷磺醯胺(3)
根據本文所述之方法來製備化合物3。NMR (500 MHz, CDCI3) δ: 8.30 (d, J=2 Hz, 1H), 7.79 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.30 (t, J=2 Hz, 1H), 7.03 (d, J=9 Hz, 1H), 6.98 (d, J=2 Hz, 2H), 4.19 (m, 1H), 3.85 (m, 2H), 3.47 (m, 1H), 2.99 (s, 3H), 2.91 (m, 1H), 2.09 (m, 2H), 1.63 (m, 2H)。MS(ESI+離子,m/z) : 505。 實例5 N-(l-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫啦啶-4- 基)乙醯胺(5) 154881.doc •119- 201134820
根據本文所述之方法來製備化合物5。iH NMR (500 MHz, DMSO-d6) δ: 8.27 (d, J=2 Hz, 1H), 8.12 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.82 (d, J=8 Hz, 1H), 7.55 (t, J=2 Hzs 1H), 7.36 (d, J=2 Hz, 2H), 7.32 (d, J=9 Hz, 1H), 3.67 (m, 1H), 3.61 (m, 2H), 2.91 (m, 2H),1.77 (m, 5H),1.36 (m,2H)。 MS(ESI+離子,m/z) : 469。 實例6 N-(l-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫吼啶-4- 基)異丁醯胺(6)
根據本文所述之方法來製備化合物6。4 NMR (500 MHz, DMSO-d6) δ: 8.25 (s, 1H), 8.10 (d, J=9 Hz, 1H), 7.68 (s, 1H), 7.52 (s, 1H), 7.34 (s, 1H), 7.30 (d, J=9 Hz, 1H), 3.64 (m, 3H), 2.90 (m, 2H), 1.76 (m, 2H), 1.36 (m, 2H), 0.96 (d,J=7 Hz,6H)。MS(ESI+離子 ’ m/z) : 497。 實例7 154881.doc -120· 201134820 N-(l-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫nfc咬-4-基)-4-甲基-l,2,3-噻二唑-5·甲醯胺(7)
根據本文所述之方法來製備化合物7。NMR (500 MHz, DMSO-d6) δ: 8.76 (d, J=8 Hz, 1H), 8.28 (d, J=2 Hz, 1H), 8.12 (dd, Π=2 Hz, J2=9 Hz, 1H), 7.56 (t, J=2 Hz, 1H), 7.38 (d, J=2Hz, 2H), 7.33 (d, J=9 Hz, 1H), 3.93 (m, 1H), 3.69 (m, 2H), 2.96 (m, 2H), 2.74 (s, 3H), 1.91 (m, 2H), 1.51 (m,2H)。MS(ESI+離子,m/z) : 553。 實例8 4-氣-N-(l-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫吼 啶-4-基)丁醢胺(8)
根據本文所述之方法來製備化合物8。1H NMR (500 MHz, DMSO-d6) 8.27 (d, J=2 Hz, 1H), 8.12 (dd, Jl=2 Hz, J2=9 Hz, 1H), 7.87 (d, J=8 Hz, 1H), 7.55 (t, J=2 Hz, 1H), 7.36 (d, J=2Hz, 2H), 7.32 (d, J=9 Hz, 1H), 3.70 (m, 1H), 154881.doc -121 - 201134820 3.61 (m, 4H), 2.92 (m, 2H), 2.20 (m, 2H), 1.91 (m, 2H), 1.78 (m,2H),1.37 (m,2H)。 實例9 N-(l-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫》比啶-4- 基)環丁烷甲醢胺(9)
根據本文所述之方法來製備化合物9。NMR (500 MHz, DMSO-de) δ: 8.26 (d, J=2 Hz, 1H), 8.11 (dd, Jl = 9 Hz, J2 = 2 Hz, 1H), 7.60 (d, J=8 Hz, 1H), 7.55 (t, J=2 Hz, 1H), 7.37 (d, J=2 Hz, 2H), 7.31 (d, J=9 Hz, 1H)} 3.68 (m, 1H), 3.62 (m, 2H), 2.91 (m, 3H), 2.08 (m, 2H), 1.97 (m, 2H), 1_86 (m,1H), 1.76 (m,3H),1.35 (m, 2H)。 實例10 N-(l-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醢基)六氫”比啶-4- 基)-4-甲基苯甲醯胺(10)
H3C 根據本文所述之方法來製備化合物10。NMR (500 154881.doc -122· 201134820 MHz, DMSO-d6) δ: 8.28 (dj J=2 Hz, 1H), 8.22 (d, J=8 Hz, 1H),8.12 (dd, Jl=9 Ήζ,J2=2 Hz,1H),7 73 (d, J=8 Hz, 2H),7.55 (t,J=2 Hz,7 39 (d,J=2 Hz,2H), 7.32 (d, J=9 Hz,1H),7.25 (d,j=8 Hz,2H),3 94 (m,1H),3 73 (m, 2H), 2.93 (m, 2H),2.34 (s,3H),187 (m,2H), 1.56 (m, 2H)。 實例11 ~(1-(5-氮基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫哺啶_4· 基氟苯甲醯胺(11)
根據本文所述之方法來製備化合物丨丨。lH NMr (500 MHz,DMSO-d6) δ: 8·4〇 (d,J=8 Hz,1H),8 28 (d,J=2 Hz, 1H),8.12 (dd,Jl=9 Hz,J2=2 Hz,1H),7.68 (d,J=7 Hz,1H), 7.55 (t, J=2 Hz, 1H), 7.52 (m, 1H), 7.39 (d, J=2 Hz, 2H), 7.37 (m,1H)’ 7.33 (d,J=9 Hz,1H),3 95 (m,1H),3 73 (m, 2H),2.94 (m,2H),1.88 (m,2H),1.56 (m,2H)。 實例12 1-(1-(5-氛基-2-(3,5-一氛苯氧基)苯基項酿基)六氫ejt咬_4_ 基)-3·異丙基腿(12) 154881.doc -123- 201134820 根據本文所述之方 Λ,
CN MHz, DMSO-d ., 來製備化合物 12。NMR (500 6; ό: 8.26 (a j2 = 9 Hz, 1H) 7 54 (d> J=2 Hz, 1H), 8.12 (dd, Jl=2 Hz, 7-33 (d, J=9 Hz, lH)(t,HZ,1H)j 7·36 (di J=2HZi 2H)i 1ΗΛ 3 6〇 , , 5 5,75 (d, J=8 Hz, 1H), 5.55 (d, J=8 Hz, 1H), 3.63 (m, lH)j 3 2H), 1.79 (m 2m (m, 2H), 3.50 (m, 1H), 2.91 (m, ’ Ή·),1 · 3 q 1-烯丙基-3-(1你氖基2 ⑽,2H),0.99 (d,J=6 Hz,6H) 〇 實例13 (3,5-二氣苯氧基)苯基磺酿基)六 氟吡啶、4-基)脲(13)
Λ〇, 根據本文所述之方 man 决來製備化合物13。4 NMR (500 MHz, DMSO-d6) δ: 8 J2=2 Ηζ,1Η),7 54、(<3, J=2 ΗΖ,1Η),812 _,11=9 ΗΖ, 7.33 (d,J=9 % (t,Ηζ,1Η),7 36 (d,J=2HZ,2Η), 5.07 (m,1H),5’.〇 ,5·95 (d,J=8 Hz,1H),5 84 (m,1H), 2.91 (m’ 2H)’ h8l (mm,⑴),3 61 (m,3H),3 52 (m,2H), 取’ 2ii),1.31 (m,2H)。 15488 丨doc ' 124- 201134820 實例14 1-(1-(5-氰基-2-(3,5-二氣苯氧基)苯基磺酿基)六氫咕啶_4_ 基)·3-對甲苯基脲(14)
根據本文所述之方法來製備化合物14〇 1h Nmr (500 DMSO-d6) δ: 8.28 (d, J=2 Hz, 1H), 8.18 (s, 1H), 8.13 (dd, Jl = 9 Hz, J2=2 Hz, 1H), 7.55 (t5 J=2 Hz, 1H), 7.37 (d, J-2Hz,2H),7.34 (d,J=9 Hz,1H),7.23 (d,J=8 Hz,2H), 7.00 (d,J=8 Hz,2H),6.13 (d,J=8 Hz, 1H),3.60 (m,3H), 2.95 (m,2H),2.20 (s,3H),1.87 (m,2H),1.39 (m,2H)。 MS(ESI+離子,m/z): 560 ; MS(ESI-離子 ’ m/z): 558。 實例15 1-(1-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫”比啶_4_ 基)-3-(4-甲氧基苯基)脲(15)
根據本文所述之方法來製備化合物丨5 ^ ijj NMR (500 MHz, DMSO-d6) δ: 8.28 (d, j=2 Hz, 1H), 8.13 (dd, Jl=9 Hz, 154881.doc -125- 201134820 J2 = 2 Hz, 1H), 8.10 (s, 1H), 7.55 (t, J=2 Hz, 1H), 7.37 (d, J=2Hz, 2H), 7.34 (d, J=9 Hz, 1H), 7.25 (dd, Jl=7 Hz, J2=2 Hz, 2H), 6.79 (dd, Jl=7 Hz, J2=2 Hz, 2H), 6.08 (d, J=8 Hz, 1H), 3.68 (s, 3H), 3.59 (m, 3H), 2.95 (m, 2H), 1.87 (m, 2H), 1.38 (m,2H)。MS(ESI+離子,m/z): 576。MS(ESI-離子, m/z): 574。 實例16 1-(1-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫《Λ啶-4-基)-3-(呋喃-2-基甲基)脲(16)
根據本文所述之方法來製備化合物16。1H NMR (500 MHz, DMSO-d6) δ: 8.27 (d, J=2 Hz, 1H), 8.12 (dd, Jl=9 Hz, J2 = 2 Hz, 1H), 7.54 (m, 2H), 7.36 (d, J=2Hz, 2H), 7.33 (d, J=9 Hz,1H),6.36 (m,1H),6.16 (m,1H),6.12 (m,1H),5.98 (d, J=8 Hz, 1H), 4.16 (d, J=6 Hz, 1H), 3.54 (m, 3H), 2.91 (m,2H),1.81 (m,2H),1.31 (m,2H)。MS(ESI+離子,m/z): 550。MS(ESI-離子,m/z): 548。 實例17 1-(1-(5-氣基-2-(3,5-二氣苯氧基)苯基確酿基)六氩1»比咬-4- 基)-3-異丙基硫脲(17) 154881.doc -126- 201134820
根據本文所述之方法來製備化合物17» iH NMR (500 MHz, DMSO-d6) δ: 8.27 (d, J=2 Hz, 1H), 8.12 (dd, Jl=2 Hz, J2=9 Hz, 1H), 7.54 (t, J=2 Hz, 1H), 7.34 (m, 3H), 7.19 (m, 1H), 7.12 (m, 1H), 4.22 (m, 1H), 4.10 (m5 1H), 3.61 (m, 2H), 2.90 (m, 2H), 1.93 (m, 2H), 1.39 (m, 2H), l.〇8 (d, J=7 Hz, 6H)。MS(ESI+離子,m/z): 529。MS(ESI-離子,m/z)· 525 » 實例18 1-(1-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氩„比咬_4_ 基)-3-(3-(甲硫基)丙基)硫腺(is)
根據本文所述之方法來製備化合物18。NMR (500 MHz, DMSO-d6) δ: 8.28 (d, J=2 Hz, 1H), 7.78 (dd, Jl=2 Hz, J2=9 Hz, 1H), 7.29 (t, J=2 Hz, 1H), 7.02 (d, J=9 Hz, 1H), 7.00 (d, J=2 Hz, 2H), 6.20 (m, 1H), 5.98 (m, 1H), 4.35 (m, 1H), 3.91 (m, 2H), 3.46 (m, 2H), 2.88 (m, 2H), 2.57 (t, 154881.doc -127- 201134820 J=7 Hz, 2H), 2.19 (m, 2H), 2.10 (s, 3H), 1.87 (m, 2H), 1.57 (m,2H)。MS(ESI +離子,m/z): 573 » MS(ESI-離子,m/z): 572。 實例19 1^-(1-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫吼啶_4_ 基)-3,5-二甲基異噁唑-4-磺酿胺(19)
根據本文所述之方法來製備化合物19。NMR (500 MHz, DMSO-d6) δ: 8.24 (d, J=2 Hz, 1H), 8.12 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.54 (t, J=2 Hz, 1H), 7.34 (m, 3H), 3.54 (m, 2H), 3.16 (m, 1H), 2.88 (m, 2H), 2.57 (s, 3H), 2.31 (s, 3H), 1.61 (m,2H),1.39 (m, 2H)。MS(ESI_離子,m/z) : 583 » 實例20 N-(l-(5·氰基-2-(3,5-二氛苯氧基)苯基磺醯基)六氫nb啶-4- 基)嗎啉-4-甲醯胺(20)
154881.doc •128· 201134820 根據本文所述之方法來製備化合物20。NMR (500 MHz, DMSO-d6) δ: 8.26 (d, J=2 Hz, 1H), 8.11 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.55 (t, J=2 Hz, 1H), 7.36 (s, 2H), 7.31 (d, J=9 Hz, 1H), 6.30 (d, J=8 Hz, 1H), 3.67 (m, 1H), 3.57 (m, 1H), 3.52 (m, 4H), 3.23 (m, 4H), 2.85 (m, 2H), 1.79 (m, 2H),1.41 (m, 2H)。MS(ESI+離子,m/z) : 539。 實例21 氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫吼啶_4· 基)-3-丙基脲(21)
根據本文所述之方法來製備化合物21 ^ NMR (500 MHz, DMSO-d6) δ: 8.26 (d, j=2 Hz, 1H), 8.12 (dd, Jl=9 Hz, J2=2 Hz, 1H),7.54 (t,j=2 Hz,1H),7.36 (s,2H),7.32 (d, J=9 Hz,1H),5.83 (d,J=8 HZ,1H),5.71 (t,J=6 Hz,1H), 3.57 (m, 2H), 3.50 (m, iH)} 2.91 (m, 4H), 1.79 (m, 2H), 1.32 (m,4H),0.81 (t,J=7 Hz, 3H)。MS(ESI +離子,m/z): 511。 實例22 1-(1-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫咕啶_4· 基M-(2-嗎啉基乙基)脲(22) 154881.doc •129- 201134820
根據本文所述之方法來製備化合物22。NMR (500 MHz, DMSO-d6) δ: 8.27 (d,j=2 Hz,1H),8.12 (dd,Jl=9 Hz, J2 = 2 Hz, 1H), 7.54 (t, J=2 Hz, 1H), 7.35 (s, 2H), 7.33 (d, J=9 Hz, 1H), 6.07 (d, J=8 Hz, 1H), 5.62 (t, J=5 Hz, 1H), 3.56 (m,6H), 3.51 (m,1H),3.08 (m,2H), 2.91 (m,2H), 2.33 (m,4H),2.28 (m,2H), 1.80 (m,2H),1.29 (m,2H)。 MS(ESI+離子,m/z) : 582。 實例23 1-(1-(5-氟基-2·(3,5-二氣苯氧基)苯基磺醯基)六氫吼啶_4_ 基)-3-環己基脲(24)
根據本文所述之方法來製備化合物24。4 NMR (500 MHz, DMSO-d.'i X. Ο ίΑ Τ-Ο tr 1 ττχ 6) δ. 8.27 (d,J-2 Ηζ,1Η),8.12 (dd,Jl=9 Ηζ, J2=2 HZ,1H),7.55 (〖,Hz,1H),7.36 (d,Hz,2H), 7-32 (d, J=9 Hz> 1H), 5.74 (d, J=8 Hz, 1H)5 5.60 (d} J=8 Hz, 6H),3.54 (m,2H),3 49 (m,m),2 9〇 (m,2h),丄 π ⑼, 134881.doc • 130- 201134820 2H),1.71 (m,2H),1.61 (m, 2H),1.50 (m,1H),1.25 (m, 4H),1.05 (m,4H)。MS(ESI+離子,m/z) : 552。 實例24 4-(3,5-二氣苯硫基)-3-(4-(3,5-二甲基-4H-1,2,4-三唑-4-基) 六氫B比咬-1-基項酿基)节腈(26)
根據本文所述之方法來製備化合物26。1H NMR (500 MHz, DMSO-d6) δ: 8.29 (d, J=2 Hz, 1H), 7.93 (dd, Jl=9 Hz, J2=2 Hz,1H),7.84 (t,J=2 Hz,1H),7.71 (d,J=2 Hz,2H), 7.14 (d, J=9 Hz, 1H), 4.21 (m, 1H), 3.93 (m, 2H), 2.98 (m, 2H),2.35 (s,6H),2.04 (m,2H),1.93 (m,2H)。MS(ESI+離 子,m/z) : 522。 實例25 4_(3,5-二氣苯氧基)-3-(4-(3,5-二甲基_4H-1,2,4-三唑-4-基) 六氫*Λ咬-1-基項酿基)苄腈(27)
201134820 根據本文所述之方法來製備化合物27。4 NMR (500 MHz, DMSO-d6) δ: 8.33 (d, J=2 Hz, 1H), 8.16 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.55 (t, J=2 Hz, 1H), 7.40 (d, J=9 Hz, 1H), 7.35 (d5 J=2 Hz, 2H), 4.17 (m, 1H), 3.86 (m, 2H), 2.93 (m, 2H),2.33 (s,6H),2.01 (m,2H), 1.91 (m,2H) » MS(ESI+離 子,m/z) : 507。 實例26 3-(4-(3,5-二甲基-4H-1,2,4-三唑-4-基)六氫吡啶-1-基磺醯 基)-4-(3,5-二甲基苯氧基)苄腈(28)
根據本文所述之方法來製備化合物28。NMR (500 MHz, DMSO-d6) δ: 8.28 (d, J=2 Hz, 1H), 8.06 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.06 (d, J=9 Hz, 1H), 6.97 (s, 1H), 6.84 (s, 1H), 4.18 (m, 1H), 3.88 (m, 2H), 2.95 (m, 2H), 2.33 (s, 6H), 2.30 (s,6H),1.99 (m,2H),1.91 (m,2H)。MS(ESI+離子, m/z) : 466 o 實例27 3-(4-(3,5-二甲基-4H-1,2,4-三嗤-4-基)六氫0Λ咬-1-基續酿 基)-4-(3,5-二甲基苯硫基)苄腈(29) 154881.doc -132- 201134820
根據本文所述之方法來製備化合物29。1H NMR (500 MHz, DMSO-d6) δ: 8.27 (d, J=2 Hz, 1H), 7.89 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.24 (s, 1H), 6.94 (d, J=9 Hz, 1H), 4.22 (m, 1H), 3.97 (m, 2H), 3.00 (m, 2H), 2.33 (m, 12H), 2.04 (m, 2H),1.94 (m,2H)。MS(ESI+離子,m/z) : 482 » 實例28 5 -氛基-2-(3,5-—氣苯氧基)-甲苯項酿基六氮咬- 4-基)苯磺酿胺(30)
根據本文所述之方法來製備化合物30。1H NMR (500 MHz, DMSO-d6) δ: 8.22 (d, 1=2 Hz, 1H), 7.76 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.57 (d, J=8 Hz, 2H), 7.31 (d, J=8 Hz, 2H), 7.26 (m, 1H), 6.98 (m, 3H), 5.11 (d, J=8 Hz, 1H), 3.60 (m, 2H), 3.22 (m, 1H), 2.43 (s, 3H), 2.36 (m, 2H), 1.84 (m, 2H), 1.67 (m,2H)。MS(ESI+離子,m/z) : 482。 154881.doc •133· 201134820 實例29 5-氰基-2-(3,5-二甲基苯氧基)-Ν-(1-甲苯磺醢基六氫"比啶- 4-基)苯磺酿胺(31)
根據本文所述之方法來製備化合物31。NMR (500 MHz, DMSO-d6) δ: 8.19 (d, J=2 Hz, 1H), 7.67 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.58 (d, J=8 Hz, 2H), 7.31 (d, J=8 Hz, 2H), 6.95 (s} 1H), 6.89 (d, J=9 Hz, 1H), 6.68 (s, 1H), 4.97 (dd, Jl = 8 Hz, J2=2 Hz, 1H), 3.58 (m, 2H), 3.21 (m, 1H), 2.42 (s, 3H),2.38 (m,2H), 1.86 (m,2H),1.61 (m,2H)。MS(ESI +離 子,m/z) : 540。 實例30 5-氰基-2-(3,5-二氣苯氧基)·Ν-(1-(3-氟苯基磺酿基)六氫"比 啶-4-基)苯磺酿胺(32)
154881.doc -134 201134820 根據本文所述之方法來製備化合物32。NMR (500 MHz, DMSO-d6) δ: 8.24 (d, 3=2 Hz, 1H), 7.78 (dd, Jl=9 Hz, J2=2 Hz, 1H), 7.53 (m, 2H), 7.41 (m, 1H), 7.31 (m, 2H), 6.99 (m, 3H), 4.93 (t, J=7 Hz, 1H), 3.64 (m, 2H), 3.22 (m, 1H),2.46 (m,2H),1.89 (m,2H),1.65 (m, 2H)。MS(ESI+離 子,m/z) : 585。 實例31 1-(2-氣乙基)-3-(1-(5-氰基-2-(3,5_二氣苯氧基)-苯基磺酿 基)六氫吡啶-4-基)脲(46)之製備
根據實例1之程序來製備3-(4-胺基六氫咣啶_丨_基續醯 基)-4-(3,5-—乳本氧基)¥腈。藉由將3-(4-胺基六氫。比咬_ 1-基續酿基)·4-(3,5 - 一氣本氧基)卡腈(1.00 g)溶於THF (3 0 mL)中隨後逐滴添加碳酸#P (975 mg,3.〇當量)、然後添加 異氰酸2-氯乙基醋(496 mg ’ 2.0當量)來製備最終產物。搜 拌1小時之後,起始材料耗盡(藉由HPLC證實),且過灸混 134881.doc -135· 201134820 合物以去除碳酸鉀。在真空中濃縮所得濾液,使用二氯甲 烷及異丙基醚研磨固體,並過濾以獲得白色粉末(838 mg ’產率為67°/❶,純度為97%)。 實例32 1 (1 (5氦基-2-(3,5· —氣苯氧基)苯基項酿基)六氫”比咬_4_ 基)-3-(2-嗎琳基己基)服(22)之製備
將1-(2-氣乙基)-3-(1-(5-氰基-2-(3,5-二氯苯氧基)-苯基績 醯基)六氫吡啶-4-基)脲(83 8 mg)、碳酸鉀(655 mg,3.0當 量)及嗎啉(413 mg,3.0當量)溶於乙腈(25 mL)中並加熱至 回流。3小時之後,反應完成(藉由HPLC證實)》然後在真 空中濃縮混合物,使用二氣甲烷及異丙基醚研磨固體以獲 得白色粉末。將粉末懸浮於熱丙酮中,在冰浴中冷卻,過 濾,並使用水洗滌以獲得白色粉末產物(601 mg,產率為 65%,純度為97%)。 實例33 1-(1-(5-氰基-2-(3,5-二氣苯氧基)苯基項酿基)六氫吼咬_4· 154881.doc •136· 201134820 基)_3_(2_嗎啉基乙基)脲(22)之製備 h2n
0
CN
儿 N
CN
根據下列方法作為實例32方法之替代方式來製備卜(卜 (5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)_六氫。比啶 3-(2-嗎啉基乙基)脲(22)。將3-(4-胺基六氫吡啶_丨_基磺醯 基)-4-(3,5-二氯苯氧基)_苄腈(1〇〇2 g)(根據實例j製得广 及羰基二咪唑(420 mg,1.1當量)合併於丁出?(15 mL)中並 在室溫下攪拌。5小時之後,起始材料耗盡(藉由HpL(^^ 實)。添加4-(2-胺基乙基)嗎啉(512 mg,2 〇當量)且將混合 物攪拌19小時。在真空中濃縮以提供白色固體,將其再懸 浮於二氣甲烧中,使用水進行分配,並使用二氣曱炫將水 層萃取三次。使用鹽水洗滌合併之有機層,藉由無水硫酸 鎂乾燥,過濾並在真空中濃縮以得到白色固體。與異丙基 醚一起研磨得到96%純產物(根據HPLC)。將粉末懸浮於^ 少量的熱甲醇中,在6(TC下授拌3〇分鐘,在冰浴中冷卻並 真二過濾以獲得白色粉末產物(83丨,產率為,純 度為 98°/〇)。 154881.doc -137- 201134820 實例34 1-(1-(5 -氣基-2-(3,5-一氣苯氧基)苯基項酿基)六氫咕咬-4- 基)-3-(2-硫嗎琳基乙基)膝(47)
根據本文所述之方法來製備化合物47。丨《[ NMR (500 MHz, DMSO-d6) δ: 8.26 (d, J=2 Hz, 1H), 8.11 (dd, Jl = 7 Hz, J2-2 Hz, 1H), 7.54 (t, J=1 Hz, 1H), 7.35 (d, J=2Hz, 2H), 7.32 (d, J=9 Hz, 1H), 6.34 (m, 1H), 4.11 (t, J1=J2=9 Hz, 2H), 3.58 (m, 5H), 3.48 (m, 1H), 2.91 (m, 3H), 2.61 (m, 1H),1.87 (m,2H),1.41 (m,2H)° MS(ESI+離子,m/z): 599。 實例35 1-(1-(5 -氮基-2-(3,5-一氣苯氧基)苯基確酿基)六氫比咬- 4-基)-3-(2-(六氫吼啶_ι·基)乙基)腺(48)
根據本文所述之方法來製備化合物48。1H NMR (500 MHz, DMSO-d6) δ: 8.56 (d, J=2 Hz, 1H), 8.11 (dd, Jl=8 Hz, J2=2 Hz, 1H), 7.54 (t5 J=2 Hz, 1H), 7.35 (d, J=2Hz, 2H), 15488 丨.doc •138· 201134820 7.32 (d,J=9 Hz,1Η),6· 2H),3.54 (m,5H),3.46 2H),1.87 (m,2H),1.39 580 〇 36 (m, 1H), 4.11 (t, J1=J2=9 Hz, (m,1H),3.04 (m,3H),2.89 (m, (m,2H)。MS(ESI+離子,m/z): 實例36 1-(1-(5-氰基-2-(3,5_二 基)-3-(2-(六 氣笨氧基)苯基磺醯基)六氫吼啶-4-氧吡嗪-1-基)乙基)脲(49)
根據本文所述之方法 々來製備化合物49。iH-NMR : (500 MHz, DMSO-d6) δ· R ^ ' (d, J=2 Hz, 1H), 8.11 (dd, Jl = 6 Hz, J2=2 Hz, 1H), 7 54 (i U, Jl=J2=l Hz, 1H), 7.31 (d, J=6 Hz, 1H),4.11 (t,J1=j2=9 Hz,2H),3 55 (m,5H),2 9〇 (m,3H), 2.62 (m,3H),2.26 (m,iH),1.87 (m,2H),1.39 (m,2H)。 MS(ESI+離子,m/z) : 581。 實例37 1-(1-(5-氰基-2-(3,5-二氣苯氧基)苯基磺醯基)六氫吼啶-4-基)-3-(2-(4-氟六氫咕啶-1-基)乙基)脲(5〇)
154881.doc .139- 201134820 根據本文所述之方法來製備化合物50。NMR (500 MHz, DMS〇-d6) δ: 8.26 (d, J=2 Hz, 1H), 8.12 (dd, Jl=8 Hz, J2-2 Hz, 1H), 7.54 (t, J1=J2=1 Hz, 1H), 7.35 (s, 2H), 7.32 (d, J=9 Hz, 1H), 6.14 (d, J=8 Hz, 1H), 5.37 (m, 2H), 3.11 (m, 2H), 2.91 (m, 3H), 2.61 (m, 2H), 2.41 (m, 3H), 1.88 (m, 2H), 1.81 (m, 3H), 1.72 (m, 2H), 1.30 (m,2H)。MS(ESI+ 離子,m/z) : 598。 實例38 1-(1-(5 -氣基-2· (3,5-二氯苯氧基)苯基橫酿基)六氫啦咬_4· 基)-3-(2-(4-甲基六氫批嗪_1_基)乙基)脲(51)
根據本文所述之方法來製備化合物51。NMR (5〇0 MHz,DMSO-d6) δ: 8 26 (d,J=2 Hz’ 1H),811 (dd,Jl=7 Hz, J2=2 Hz, 1H), 7.35 (s, 2H), 7.32 (d, J=9 Hz, 1H), 6.36 (s, 1H), 4.11 (t, J1=J2=8 Hz, 2H), 3.56 (m, 5H), 3.40 (m, 2H), 3.39 (m,3H),2.29 (m,1H),1.87 (m,2H),1.39 (m,2H)。 MS(ESI+離子,m/z) : 596。 實例39 1-稀丙基-3-(1-(5-氰基_3,4,6-三乳-2-(3,5-二氣苯氧基)苯基 读酿基)六氣咬基)腺(S3) 154881.doc -140- 201134820
根據本文所述之大 法"來製備化合物54。4 NMR (500 MHz, DMSO-d6) δ: 7 54 r 04 (s, 1H), 7.35 (s, 2H), 5.96 (d, J=8 Hz, 1H), 5.86 (t T=fi tt ’ Hz> 1H), 5.78 (m, 1H), 5.07 (dd, Jl = 8 Z,J2 2 HZ,1H),4.99 (dd,Jl = 6 Hz,J2=2 Hz, 1H),3.60 (m,4H),3.51 (m,iH)’ 2 9l (⑺,2H),〗(⑺,2h),m (叫 2H)。MS(ESI+離子,m/z) : 534 實例40 1-(1-(5-氛基-3,4,6-三H(3,s_二氣苯氧基)苯基磺醯基)六 氮哺唆-4-基)_3-(2-(2,2,3,3,5,5,6,6_八氘-嗎啉基)乙基)脲 (54)
根據本文所述之方法來製備化合物53。NMR (500 MHz, DMSO-d6) δ: 7.35 (s, 2H), 6.08 (m, 1H), 5.63 (m, 1H), 4.14 (t, J1=J2=8 Hz, 2H), 3.57 (m, 3H), 3.40 (m, 2H), 2.91 (m,ih), 1.87 (m,2H),1.40 (m,2H)。MS(ESI+離子, 154881.doc -141 - 201134820 m/z) : 593 0 實例41 CCR3受體結合分析 用PBS將細胞洗滌一次並使其再懸浮於結合緩衝液(25 mM HEPES pH 7.6 ’ 5 mM MgCl2,1 mM CaCl2,0.5〇/〇 BSA,0.1% NaN3)中。將100 mL細胞懸浮液(2xl05個細胞/ 孔)與0.1 nM [125I]標記之人類嗜伊紅趨化因子/CCL11 (2000Ci/mmol比活性)混合於96孔U形底聚丙稀板中’並在 室溫下培育6 0 m i η以進行結合反應。然後將細胞懸浮液轉 移至過濾板(#MAFB,Millipore)中,並用含有〇.5MNaCl之 結合緩衝液洗滌3次,添加閃爍體,並在TopCount (Packard)上計數放射性。在測定非特異性結合時’將細胞 懸浮液及[1251]標記之人類嗜酸性球趨化因子…01^11在500 nM未經標記之人類嗜酸性球趨化因子/CCL11存在下進行 培育0 參見,lino等人 ’ r Molecular cloning and functional characterization of cynomolgus monkey (Macaca fascicularis) CC chemokine receptor, CCR3」,Cytokine 2002,19,276-286 ° 生物學結果匯總於表1中,其中A代表不大於50 nM之 值,且B代表大於50 nM但不大於500 nM之值,C代表大於 500 nM但不大於5 μΜ之值;且D代表大於5 μΜ之值。 154881.doc • 142- 表1
化合物編號 Kj 化合物編號 Ki 1 — 2 D 3 — 4 — 5 — 6 — 7 — 8 — 9 — 10 — 11 — 12 — 13 — 14 — 15 — 16 — 17 — 18 — 19 — 20 — 21 — 22 A 23 C 24 — 25 B 26 — 27 — 28 — 29 — 30 B 31 D 32 D 33 B 34 D 35 D 36 B 37 D 38 B 39 D 40 — 41 — 42 — 43 — 44 B 45 C 46 — 47 A 48 A 49 A 50 A 51 A 52 C 53 A 54 A 201134820 154881.doc -143- 201134820 實例42 hERG受體結合分析 藉由使用1251標記之肽BeKm-1改良平衡解離分析來以 中等通量篩選可與人類Ether-a-go-go相關基因(hERG)相互 作用之化合物。BeKm-1(來自 Central Asian scorpion Buthus eupeus之徵毒素)可選擇性阻斷hERG通道。Angelo, Κ·等人,2003,Pflugers Arch.-Eur. J. Physiol.,447: 55-63 ; Chiu, PJS.等人,J. Pharmacol. Sci” 2004, 95: 311-319。將來自含有轉染hERG通道之HEK-293細胞的分離膜 製劑(hERG K+ Channel Membrane Target SystemsTM ;目 錄號:RBHERGM400UA)(Perkin Elmer, Boston, MA)以 1:150 v/v之最終濃度懸浮於分析緩衝液A中》亦將篩選用 化合物、及未經放射性標記之BeKm-1、以及125I-BeKm-l 放射性配體(Perkin Elmer ;目錄號:NEX-412 ;比活性: 2,200 Ci/mmol)重構於緩衝液A中。以下列比率將分析組份 培育於96孔圓底聚丙烯板中: 25 μΐ適當濃度之化合物 25 μΐ 0.8 ηΜ放射標記之BeKm-1(最終濃度為〇·1 ηΜ) 150 μΐ膜製劑 在振動及室溫下將分析液培育1 hr。隨後,將孔内容物 轉移至96孔過濾板(GF/C多孔板,MultiScreenTM HTS ; Millipore, 290 Concord Road, Billerica, MA 01821 USA ; 目錄號:MSFBN6B-XX,於0.3%聚乙烯亞胺中預浸泡; Acros Organics, NJ ;目錄號:178571000)。去除未結合放 154881.doc 201134820 射性並在真空下使用冰冷緩衝液B將膜洗滌4次》將板風 乾,且在Packard Top-Count NXTTM微板閃爍及發光計數 器(Packard Instrument公司,Downers Grove, IL)上對結合 放射性進行計數。分析平衡解離且使用GraphPad Prism 4TM 軟體(GraphPad Software, San Diego,CA)計算 IC50 及 / 或Ki值。 分析緩衝液A :存於水中之20 nM Hepes(MP Biomedicals, LLC ; 29525 Fountain Parkway, Solon OH, 441389 ;目錄 號:1688449),pH為 7·2,具有 1M Tris (Fisher Chemicals, Fair Lawn,NJ 07410 ;目錄號:BP-1757-500) ; 100 μΜ KC1 (Fisher Chemicals,目錄號:BP-366-500) ; 0.1% BSA (Sigma Aldrich, 3050 Spruce Street, St. Louis, MO 63103 ; 目錄號:A3059)。 分析緩衝液B : 20 mM Tris HC1 ’ pH為 7_3 ; 150 mM NaCl(Fisher Chemicals ;目錄號:S78449)。 hERG結合分析結果匯總於表2中,其中A代表無量測之 活性(亦即,大於100 μΜ之值),且B代表大於10 μΜ但小於 100 μΜ之值且C代表小於10 μΜ之值。 表2
化合物編號 Ki 化合物編號 Ki 2 A 5 A 8 A 10 A 11 A 12 A 13 A 16 A 17 A 18 A 154881.doc -145· 201134820
化合物編號 Κί 化合物編號 κ8 25 A 30 A 33 A 36 B 38 A 52 A 本文所提供化合物與已知CCR3拮抗劑相比具有改良之 hERG特性,許多已知CCR3拮抗劑在hERG結合分析中之Ki 值小於10 μΜ。 提供上文所述實例以為彼等熟習此項技術者提供完整之 本發明及如何實施及利用所主張實施例之說明,且並不意 欲限制本文所揭示之範圍。對熟習此項技術者而言顯而易 見之修改意欲屬於以下申請專利範圍之範圍内。本說明書 中所提及之所有出版物、專利及專利申請案皆以引用方式 併入本文中,其併入程度如同明確地及單獨地指出將每一 該出版物、專利或專利申請案以引用方式併入本文中一 般。 154881.doc •146·
Claims (1)
- 201134820 七、申請專利範圍: 1. 一種式I或II化合物,⑴ (II) 或其對映異構體'對映異構體之混合物、兩種或更多種 非對映異構體之混合物、互變異構體或兩種或更多種互 變異構體之混合物;或其醫藥上可接受之鹽、溶劑合 物、水合物或前藥; 其中: R1、R2、R3、R4、R^R6各自獨立地為⑷氫、_基、 氰基、硝基或胍;(b) CN6烷基、C2_6烯基、C2.6炔基、 C3.7環烷基、C 6-14芳基、 C7.15芳烷基、雜芳基或雜環基; 或(c) -C(0)R丨a、-(:(0)01113、-C(0)NRlbRlc、-C(NRu)NRlbRu 、-ORla、_0C(0)Rla、_〇C(〇)〇Rla、_〇C(0)NRlbRlc、 •〇C(=NRla)NRlbRle、-〇S(0)Rla、-〇S(0)2Rla、-〇S(0)NRlbRlc 、-0S(0)2NRlbRlc、-NRlbRlc、-NRlaC(0)Rld、-NRlaC(0)0Rld 、-NRlaC(0)NRlbRle、-NRlaC(=NRld)NRlbRle、-NRlaS(0)Rld 、-NRlaS(0)2Rld、-NRlaS(0)NRlbRlc、-NRlaS(0)2NRlbRlc、 -SRla、-S(0)Rla、-S(0)2Rla、-S(0)NRlbR1(^_S(0)2NRlbRlc ; R7為(a)氫、鹵基、氰基、硝基、側氧基、或胍;(b) 154881.doc 201134820 Ci-6烧基、C2-6稀基、C2.6炔基、C3.7環炫基、〇6-14芳 基、C7.15芳坑基、雜芳基或雜環基;或(c) -(:(0)111 a、 -C(0)〇RIa ' -C(0)NRlbRlc . -C(NR,a)NR,bRlc ' -〇RU ' -0C(0)Rla' -0C(0)0R,a> -〇C(0)NR,bRlc ' -OC(=NR,a) NRlbRlc、_0S(0)Rla、_〇s(〇)2Rla、_〇s(〇)NRlbRlc、 -OS(0)2NRlbRlc ' -NRlbRlc、-NRlaC(0)Rld、-NR丨aC(0)0Rld ' -NRlaC(0)NRlbRlc > -NRlaC(=NRld)NRlbRlc > -NRlaS(0)Rld 、-NRlaS(0)2Rld、-NRlaS(0)NRlbRlc、_NRlaS(0)2NRlbRlc、 -SR〗a、-S(0)Ru、-S(0)2Rla、_S(〇)NRlbR1(^-S(0)2NRlbRlc ; X係o或s; Y係-C(0)Rla、-C(S)Rla、-C(0)NRlbRlc、-C(S)NRlbRlc、 -C(0)0Rle、-8(0)1113或-8(0)2尺13 ; 118係氫、(1!1.6烧基或€3-7環烧基;或 Y及R與其所連接之N原子一起形成包含至少一個額外 0、S、或N原子之雜芳基; Z係-C(0)Rla、-C(S)Rla、-C(0)NRlbRlc、-(:(8如11115111(:、 -S(0)Rla4-S(0)2Rla ; m係0至3之整數; R9係氫、Cw烷基或C3.7環烷基; m係0至3之整數; η係1至3之整數; ρ係1至4之整數;且 各Rla、Rib、Rk、Rid及Rle獨立地係氫、Cl-6烷基、 C2_6烯基、C2.6炔基、C3-7環烷基、C6-U芳基、雜芳基或 154881.doc 201134820 雜環基;或每對Rlb&Rlc與其所連接之n原子一起獨立形 成雜芳基或雜環基,前提係汉1«不為第三丁基或苄基; 其中各烷基、烯基、炔基、環烷基、芳基、芳烷基、 雜環基及雜芳基視需要經一或多個基團取代,其各自獨 立地選自(a)氰基、鹵基及硝基;(b) Ci-6烷基、烯 基C2-6炔基、C3.7環烷基、C6-14芳基、c7.15芳烷基、雜 芳基及雜環基,其各自視需要經一或多個、在一實施例 中1個、2個、3個或4個取代基Q取代;及⑷_c(〇)Ra、 -C(0)0Ra . -C(0)NRbRc ^ -C(NRa)NRbRc ^ -〇R^ . _〇C(〇)Ra . -OC(0)〇Ra , -〇C(0)NRbRc > -OC(=NRa)NRbRc χ -〇S(0)Ra > -OS(0)2Ra、_OS⑼NRbRC、_〇s⑼2NRbRC、NRbRC ' -NRaC(0)Rd . -NRaC(0)0Rd > -NRaC(0)NRbRc ^ -NRaC(=NRd) NR R、-NRaS(0)Rd、-NRaS(0)2Rd、-NRaS(〇)NRbRc、 -NR S(0)2NRbRe、-SRa、-S(0)Ra、-S(〇)2Ra、_s(〇)NRbRc 及-S(0)2NRbRc,其中V、Rb、Rd各自獨立地為:⑴ 氣’(ii) C〗_6烧基、C2-6婦基、C2-6炔基、〇3-7環烧基、C6.14 芳基、C?-μ芳院基、雜芳基或雜環基,其各自視需要經 一或多個、在一實施例中1個、2個、3個或4個取代基q 取代;或(iii) Rb&Re與其所連接之Ν原子一起形成雜環 基,其視需要經一或多個、在一實施例中1個、2個、3 個或4個取代基Q取代; 其中各Q獨立地選自由以下組成之群:(a)沉;(b)氰 基、鹵基、及墙基;(c) CN6院基、C2.6烯基、c2.6炔基、 C3·7環烧基、Ce-ΐ4芳基、C7·!5芳院基、雜芳基、及雜環 154881.doc 201134820 基;及(d) -C(0)Re、-C(0)0Re、-C(0)NRfRg、-C(NRe)NRfRg、 -ORe、-0C(0)Re、-0C(0)0Re、-0C(0)NRfRg ' -〇C(=NRe)NRfRg、 -〇S(0)Re、-〇S(0)2Re、-〇S(0)NRfRg、-〇S(0)2NRfRg、 -NRfRg、-NReC(0)Rh、-NReC(0)0Rh、-NReC(0)NRfRg、 -NReC(=NRh)NRfRg、-NReS(0)Rh、-NReS(0)2Rh、-NReS(0) NRfRS、-NReS(0)2NRfRg、-SRe、-S(0)Re、-S(0)2Re、 -S(0)NRfRg、及-S(0)2NRfRg ; 其中各Re、Rf、Rg、及Rh獨立地係⑴氫;(ii) c丨_6烷 基、C2-6稀基、C2-6炔基、C3-7環院基、C6·丨4芳基、C7-i5 芳烧基、雜芳基、或雜環基;或(iii) Rf&Rg與其所連接 之N原子一起形成雜環基。 2 ·如請求項1之化合物,其中 R1、R2、R3、R4及R5各自獨立地為氫、鹵基或Ci 6烷 •基; R6係氰基或硝基; R7係氫或C!_6烷基; R8係氫或Ck烷基; X係Ο或S ; m為0、1或2 ; η為1或2 ; ρ為1、2、3、或4 ;且 Υ係 _C(0)Rla、_C⑻Ria、_C(0)NRibRlc、_c⑻NRlbRU、 -C(0)0Rle、-8(〇)1113或_3(〇)21113 ;其中 R 、R及尺16各自獨立地係(a) Ci·6烷基,其視需要經 154881.doc 201134820 一或多個鹵基、Cw烷氧基、Cw烷硫基、雜環基或雜芳 基取代;(b) C2.6烯基,其視需要經一或多個鹵基取代; (C) C3-7環烷基,其視需要經一或多個鹵基、或一或兩個 Ci-6烧基取代,(d) 〇6-14方基’其視需要經一或多個鹵 基、Cw烷基取代,其中該烷基進一步視需要經1個、2 個或3個鹵基或(:1·6烷氧基取代,其中該烷氧基進一步視 需要經1個、2個或3個鹵基取代;(e)雜芳基,其視需要 經一或兩個Ci·6炫基取代;或(f) C7.ls芳燒基,其視需要 經一或多個鹵基、C!-6烷基取代,其中該烷基進一步視 需要經1個、2個或3個鹵基、或C,·6烷氧基取代,其中該 烷氧基進一步視需要經1個、2個或3個_基取代;且 Rlb係氫或甲基;或 Rlb&Rle與其所連接之N原子一起形成雜環基; 前提係RleF為第三丁基或苄基。 3. 如請求項1或2之化合物,其中 R7係氫; m為1 ; η為1 ;且 ρ為1、2、3、或4。 4. 如請求項1或2之化合物,其中 R8係氫或甲基; m為1 ; η為1 ;且 Υ係-C(〇)Rla或_c⑻Rla;其中 154881.doc 201134820 R係(a) Ck烷基,其視需要經一或多個鹵基取代; (b) C2.6烯基;(c) c3-7環烷基;或(d) C6丨々芳基其視需 要經一或多個鹵基、Ck烷基或c16烷氧基取代。 5. 如請求項1或2之化合物,其中 R8係氫或曱基; m為1 ; η為1 ; Υ係-C(〇)NRlbRlc或-C^NRUr1、其中 Rlb係氫;且 RUS(a) Cw烷基,其視需要經一或多個鹵基或ci6烷 氧基、Ck烷硫基、雜環基、或雜芳基取代;(b) 烯 基;(c) CP環烷基;或(d) (:6·μ芳基,其視需要經一或 多個函基、Cl·6烷基或C〗·6烷氧基取代;且 Rlb係氫或曱基;或 Rlb及Rle與其所連接之N原子一起形成雜環基。 6. 如請求項1或2之化合物,其中 R8係氫或曱基; m為1 ; η為1 ; Υ係-C(0)NRlbRlc4-C(S)NR丨bRlc;其中 Rlb係氫;且 Rle*(a) Cw烷基,其視需要經雜環基取代;且 Rlb係氫或甲基。 7. 如請求項1或2之化合物,其中 154881.doc -6 - 201134820 R8係氫或甲基; m為1 ; η為1 ;且 Υ係-S(〇)2Rla ;其中 R^(a) C,6^^;(b) 個函基、(^基或Cl.6烧氧基取代;或⑷雜芳基 需要經一或兩個CU6烷基取代。 、 8.如請求項1或2之化合物,其中 m為1 ; η為1 ;且 Υ及R8與其所連接之Ν原子—起形成5員㈣基,其中 該雜芳基包含至少一個額外〇、s、原子,其視需要 經一或兩個C!.6烷基取代。 9.如請求項8之化合物,其中¥及尺8與其所連接之Ν原子— 起形成視需要經一或兩個曱基取代之三唑基。 10_如請求項1之化合物,其中 R1、R2、R3、R4及R5各自獨立地為氫、齒基或q 6烷 基; R6係氰基或硝基; R7係氫或Cw烷基; R9係氫或(^_6烷基; X係〇或s; m為〇、1或2 ; η為1或2 ; 154881.doc 201134820 p為1、2、3、或4 ;且 Z係-C(0)Rla、-C(S)Rla、-C(〇)NR»bRlc、_c(s)NRlbRlc、 -C(0)0Rle、-S(0)Rla4-S(0)2Ru ;其中 Rla、Ric及Rle各自獨立地係:(a) Cl.6烷基,其視需要 經一或多個鹵基、Cw烷氧基、C!-6烷硫基、雜環基或雜 芳基取代;(b) C2·6烯基’其視需要經一或多個齒基取 代;(c) Ο:3-?環烷基’其視需要經一或多個鹵基、或一或 兩個C〗·6烧基取代;(d) (:6·〗4芳基’其視需要經一或多個 _基、Cl·6烧基取代’其中該烧基進一步視需要經1個、 2個或3個鹵基或Cw烷氧基取代’其中該烷氧基進一步 視需要經1個、2個或3個_基取代;(e)雜芳基,其視需 要經一或兩個Cw烷基取代;或⑴芳烷基,其視需 要經一或多個鹵基、Cw烷基取代,其中該烷基進一步 視需要經1個、2個或3個鹵基、或Cl.6烷氧基取代,其中 該烧氧基進一步視需要經1個、2個或3個齒基取代;且 Rlb係氫或甲基;或 R及R與其所連接之N原子一起形成雜環基; 前提係111<5不為第三丁基或苄基。 11.如請求項1或10之化合物,其中 R7係氫; R9係氫或甲基; m為1 ; π為1 ;且 Z 係-C(0)Rla4_C(S)Rla;其中 154881.doc 201134820 …系⑷一院基’其視需要經―或多個齒基取代; (b)c爾;⑷c3,7環院基;或⑷%芳基,立祝需 要經-或多個函基、cv6烷基或Ci.6烷氧基取代。 12.如請求項1或1〇之化合物,其中 R7係氫; R9係氫或甲基; m為1 ; η為1 ; ζ係-C(〇)NRlbRlc或-C(S)NRlbRic ;其中 Rlb係氫;且 R係(a) Ci.6炫基’其視需要唾一 -V ^ . 受丄或多個鹵基或C卜6烷 氧基、c丨.6烷硫基、雜環基、式雜 忒雜方基取代;(b) C2_6烯 基;(c) C3_7環烧基;或(d) 笔盆 )δ·丨4方基,其視需要經一或 多個鹵基、C!_6烷基或Ck烷氧基取代;且 Rlb係氫或甲基;或 起形成雜環基 Rlb及Rle與其所連接之N原子 13.如請求項1或10之化合物,其中 R7係氫; R9係氫或甲基; m為1 ; η為1 ;且 Ζ係-S(0)2Ru ;其中 其視需要經一或多 或(C)雜芳基,其視 RNMa) C丨-6烷基;(b) c6.u芳基 個_基、Cl-6烧基或Ci_6燒氣基取代. 154881.doc -9. 201134820 需要經一或兩個C 1 _6院基取代。 14·如請求項1、2、及10之化合物,其中 R1係氫; R2係氣或甲基; R3係氫; r4係氣或甲基; R5係氫; R6係氰基; R7係氫; x係〇或S ; m為1 ;且 η為1。 15. 16. 17. 如請求項1之化合物,其中Rl、R2、R3、R4、及尺5中之 二者係鹵基或C丨·6烷基,且其餘三者係氫。 如請求項1之化合物,其中Ri、R2、R3Hi: 者傳氣或Μ,且其餘三者錢。 一 如請求項卜2、1()、15及16中任—項之化合物,其中x 係0 〇 1 8 *如請求jg 1 、、10、15及16中任—項之化合物,其中X 係S 〇 19. 一種化入札 ®物,其選自由下列組成之群: 154881.doc 201134820154881.doc -11 - 201134820154881.doc • 12- 201134820154881.doc -13- 201134820154881.doc •14- 201134820154881.doc -15- 201134820及其對映異構體、對映異構體之混合物、兩種或更多種 非對映異構體之混合物、互變異構體、及兩種或更多種 互變異構體之混合物;及其醫藥上可接受之鹽、溶劑合 物、水合物、及前藥。 20. —種式la或Ila化合物,(la) (Ha) 或其對映異構體、對映異構體之混合物、兩種或更多種 非對映異構體之混合物、互變異構體或兩種或更多種互 變異構體之混合物;或其醫藥上可接受之鹽、溶劑合 物、水合物或前藥; 15488丨.doc -16- 201134820 其中: !^、112、113、1^、115及116各自獨立地為(3)氫、氘、豳 基、氰基、硝基或胍;(b) CN6烷基、c2-6烯基、c2.6炔 基、C3_7環烷基、C6_M芳基、(:7-15芳烷基、雜芳基或雜 環基;或(c) -C(0)Rla、-C(0)〇Rla、_c(〇)NRlbRlc、 -C(NRla)NRlbRlc、-〇Rla、_〇C(0)Ria、_〇c⑼〇Rla、 -0C(0)NRlbRlc、-OC(=NR丨a)NR丨bR丨c、-0S(0)Ria、_〇s(〇)2Ru、 -0S(0)NRlbRlc、-0S(0)2NRlbRlc、-NRlbRlc、-NRlaC(0)Rld、 -NRlaC(0)ORld、-NRlaC(0)NRlbRlc、_NRlaC(=NRld)NRlbRlc、 -NRlaS(0)Rld、_NRlaS(0)2Rld、-NRlaS(0)NRlbRle、-NRlaS(0)2 NRlbRlc、-SR丨a、_S(0)Rla、-S(0)2R丨a、_S(0)NRlbRlc 或-S(0)2NRlbRlc ; R7為(a)氫、鹵基、氰基、硝基、側氧基、或胍;(b) Cj-6烷基、C2-6烯基、C2-6炔基、C3-7環烷基、(:6.14芳 基、C7^5芳烧基、雜芳基或雜環基;或(c)-C(0)Rla、 -C(0)0Rla、-C(0)NRlbRlc、-C(NRla)NRlbRlc、-ORla、 -0C(0)Rla、-0C(0)0Rla ' -0C(0)NRlbRlc、-OC(=NRla) NRlbRlc、-0S(0)Rla、-0S(0)2Rla、-0S(0)NRlbRlc、 -0S(0)2NRlbRlc、-NRlbRlc、-NRlaC(0)Rld、-NRlaC(0)0Rld 、-NRlaC(0)NRlbRlc、-NRlaC(=NRld)NRlbRlc、-NRlaS(0)Rld 、-NRlaS(0)2Rld、-NRlaS(0)NRlbRlc、-NRlaS(0)2NR丨bRlc、 -SRla ' -S(0)Rla ' -S(0)2Rla ' -S(0)NRlbRlc^-S(0)2NRlbRlc ; X係O或S ; Y係-C(0)Rla、-C(S)Rla、-C(0)NRlbRlc、-C(S)NRlbRlc、 154881.doc • 17_ 201134820 -C(0)0Rle、-S(0)Rla4-S(0)2Rla ; R8係氫、Cw烷基或C3.7環烷基;或 Y及R8與其所連接之子一起形成包含至少—個額外 0、S、或N原子之雜芳基; Z係-C(0)Rla、-C(S)RU、-C(0)NRlbRlc、_C(s)NRlbRlc、 -S(0)Rla4-S(0)2Ru ; m係0至3之整數; R9係氫、Cu6烷基或C3._7環烷基; …係氘; m係0至3之整數; η係1至3之整數; Ρ係1至4之整數;且 q係0至3之整數, 各R丨a、R丨、吵、f及Ru獨立地係氫、^道美、 CM稀基、&快基、心環炫基、Ce.丨*芳基、雜芳1或 雜環基;或每對Rib及Ru與其所連接之崎子—起獨立形 成雜芳基或雜環基,前提係Rle不為第三丁基或节基; 其中各院基、稀基、炔基、環院基、芳基、芳院基、 雜環基及雜芳基視需要經—或多個基圏取代,其各自獨 立地選自⑷氰基、齒基及石肖基;⑻Ci 6院基、‘稀 基、c2.6炔基、C3-7環烧基、C6 i4芳基、芳烧基、雜 芳基及雜環基,其各自視需要經—或多個、在一實施例 個2個、3個或4個取代基Q取代;及(c) _c(〇)Ra、 ()〇R _C(〇)NR Rc、-C(NRa)NRbRc、_0Ra、_〇c(〇)Ra、 134881.doc 201134820 •0C(0)0Ra、-0C(0)NRbRc、-OC(=NRa)NRbRc、-0S(0)Ra、 -0S(0)2Ra、-0S(0)NRbRc、-0S(0)2NRbRc、-NRbRc、 -NRaC(0)Rd、-NRaC(0)0Rd、-NRaC(0)NRbRc、-NRaC(=NRd) NRbRc、-NRaS(0)Rd、-NRaS(0)2Rd、-NRaS(0)NRbRc、 -NRaS(0)2NRbRc、-SRa、-S(0)Ra、-S(0)2Ra、-S(0)NRbRc 及-S(0)2NRbRc,其中Ra、Rb、1^及Rd各自獨立地為:(i) 氫;(ii) Cw烷基、C2.6烯基、C2.6炔基、C3.7環烷基、C6_14 芳基、C7.15芳烷基、雜芳基或雜環基,其各自視需要經 一或多個、在一實施例中1個、2個、3個或4個取代基Q 取代;或(iii) Rb&Re與其所連接之N原子一起形成雜環 基’其視需要經一或多個、在一實施例中1個、2個、3 個或4個取代基Q取代; 其中各Q獨立地選自由以下組成之群:(a)氘;(b)氰 基、鹵基、及硝基;(c) CN6烷基、C2_6烯基、C2_6炔基、 C3_7環烷基、C6_14芳基、C7_15芳烷基、雜芳基、及雜環 基;及(d) -C(0)Re、-C(0)0Re、-C(0)NRfRg、-C(NRe)NRfRg 、-ORe、-OC(0)Re、-0C(0)0Re、-0C(0)NRfRg、-OC(=NRe) NRfRg、-〇S(0)Re、-0S(0)2Re、-0S(0)NRfRg、-0S(0)2 NRfRg、-NRfRg、-NReC(0)Rh、-NReC(0)0Rh、-NReC(0) NRfRg、-NReC(=NRh)NRfRg、-NReS(0)Rh、-NReS(0)2Rh 、-NReS(0)NRfRg、-NReS(0)2NRfRg、-SRe、-S(0)Re、 -S(0)2Re、-S(0)NRfRg、及-S(0)2NRfRg ; 其中各Re、Rf、Rg、及Rh獨立地係(i)氫;(ii) Cu烷 基、[2·6稀基、C2-6快基、C3-7壞烧基、C6-14芳基、C7-15 154881.doc -19- 201134820 芳烷基、雜芳基、或雜環基;或(iii) Rf&Rg與其所連接 之N原子一起形成雜環基。 21.如請求項20之化合物,其中該化合物具有式1&且其中: 尺1、尺2、113、114及115各自獨立地為氫、氘、_基或(:16 烷基; R6係氰基或硝基; R8係氫; Rd係氘; X係Ο或S ; m為0、1或2 ; η為1或2 ; ρ為 1、2、3、或 4 ; q為3 ;且 Y係-C(0)Rla、-C(S)Rla、-C(0)NRlbRlc、_C(S)NRibRu、 -C(0)0Rle、-S(0)R1{^-S(0)2Rla ;其中 Rla、Rlc及Rle各自獨立地係(a) Cl-6烷基,其視需要經 一或多個鹵基、C!·6烷氧基、C!_6烷硫基、雜環基或雜芳 基取代;(b) C:2·6烯基,其視需要經一或多個鹵基取代; (c) C3·7環院基’其視需要經一或多個鹵基、或一或兩個 C!·6烧基取代;(d) C;6·!4芳基’其視需要經一或多個齒 基、C〗_6烷基取代’其中該烷基進一步視需要經丨個、2 個或3個鹵基或匸^6烧氧基取代,其中該烷氧基進一步視 需要經1個、2個或3個齒基取代;(e)雜芳基,其視需要 經一或兩個Ci·6烧基取代;或(f) c?」5芳炫基,其視需要 154881.doc -20- 201134820 經一或多個齒基、Cl·6烷基取代,其中該烷基進—步視 需要經1個、2個或3個齒基、或Cw烷氧基取代,其中該 烧氧基進一步視需要經1個、2個或3個鹵基取代;且 Rlb係氫或甲基;或 R及R與其所連接之N原子一起形成雜環基。 22.如請求項20之化合物,其中該化合物具有式。且其中: R'RW'R4及R5各自獨立地為氫、氘、齒基或 燒基; R6係氰基; R8係氫; 1^係氘; X係Ο或S ; m為1 ; η為1 ; ρ為4 ; q為3 ;且 Y係-C(0)Rla、-C(S)Rla、-C(0)NRlbRlc、_c(S)NRlbRlc、 •C(0)0Rle、-S(0)Ru*_S(0)2Rla ;其中 Rla、Rlc^Rle各自獨立地係:(a) Cl 6烷基,其視需要 經一或多個鹵基、Cw烷氧基、Cw烷硫基、雜環基或雜 芳基取代;(b) C2·6稀基,其視需要經一或多個鹵基取 代;(c) C3·7環烷基,其視需要經一或多個鹵基、或一或 兩個Ck烷基取代;(d) 芳基,其視需要經一或多個 齒基、C1 -6院基取代’其中該烧基進一步視需要經1個、 154881.doc •21-. 201134820 2個或3個鹵基或匚!.6烷氧基取代,其中該院氧基進一步 視需要經1個、2個或3個函基取代;(e)雜芳基,其視需 要經一或兩個Cw烷基取代;或(f) C7-ls芳烷基,其視需 要經一或多個齒基、Cl_6烷基取代’其中該烷基進一步 視需要經1個、2個或3個鹵基、或C!.6烷氧基取代,其中 該烷氧基進一步視需要經1個、2個或3個_基取代;且 Rlb係氫或甲基;或 RIb及Rle與其所連接之N原子一起形成雜環基。 23.如請求項20之化合物,其中該化合物具有式1&且其中: R、R、R3、R4及R5各自獨立地為氫、_基或Cu烷 基; R6係氰基丨 R8係氫; Rd係氘; X係Ο或S ; m為1 ; η為1 ; ρ為4 ; q為3 ;且 Y係-C(0)NRlbRlc ;其中 111<:係(a)經雜環基取代之c Rlb係氫。 1-6院基;或(b) C2-6烯基; 且 24.如請求項20之化合物 R、R、R、R及R5各自獨立地為氫、 氘、齒基s 154881.doc •22- 201134820 烧基; R6係氰基或硝基; R7係氫或Cw烷基; R9係氫或Cm烷基; …係氘; X係〇或S ; m為0、1或2 ; η為1或2 ; ρ為1、2、3、或4;且 q為3 ;且 Z係-C(0)Rla、-C(S)Rla、_c(〇)NRlbRlc、、 -C(0)0Rle、-S(0)Rl!^_S(0)2Ru ;其中 Rla、Rlc&Rie各自獨立地係:(a) Ci 6烷基,其視需要 經一或多個函基、Cm烷氧基、Cl·6烷硫基、雜環基或雜 芳基取代;(b) C2·6烯基,其視需要經一或多個鹵基取 代;(c) Cm環烷基’其視需要經一或多個鹵基、或—或 兩個C!·6烷基取代;(d) Clm芳基’其視需要經一或多個 鹵基、C〗_6烷基取代,其中該烷基進一步視需要經1個、 2個或3個鹵基或(:〗_6烷氧基取代,其中該烷氧基進一步 視需要經1個、2個或3個鹵基取代;(e)雜芳基,其視需 要經一或兩個C!·6院基取代;或(f) C^-i5芳院基,其視需 要經一或多個鹵基、cN6烷基取代,其中該烷基進一步 視需要經1個、2個或3個鹵基、或CN6烷氧基取代,其中 該烷氧基進一步視需要經1個、2個或3個鹵基取代;且 154881.doc -23· 201134820 R係氫或曱基;或 一起形成雜環基。 及19至24中任一項之化合 尺^及尺卜與其所連接之^原子 25.如請求項 1、2、1〇、15、16、 物’其中該化合物係鹽酸鹽。 26. 一種醫藥組合物’其包含如請求項15_25中任一項之化 合物、或其醫藥上可接受之鹽、溶劑合物、水合物、立 體異構體、或互變異構體;及一或多種醫藥上可接受之 載劑或賦形劑。 27. 如請求項26之醫藥組合物,其進—步包含第二治療劑。 28. 如請求項26或27之醫藥組合物,其中該組合物係調配用 於單一劑量投與。 29.如請求項28之醫藥組合物 服、非經腸或靜脈内劑型。 3 0 ·如清求項2 9之醫樂組合物, 囊0 '其中該組合物係調配成口 其中該口服劑型係錠劑或膠 3 1 · —種如請求項1至25中任一項之仆人你―、, τ 1唄义化合物或如請求項26至 30中任一項之醫藥組合物的用途,其 ^ 舟用以製備用於治 療、預防、或改善個體的CCR3介導之病症、疾病、或病 狀之一或多種症狀的藥劑。 32. —種如請求項1至25中任一項之化合物或如請求項^至 30中任一項之醫藥組合物的用途’其用以製備用於治 療、預防、或改善個體的嗜酸性球相關性病症、疾病、 或病狀之一或多種症狀的藥劑。 33. —種如請求項1至25中任一項之化合物或如請求項^至 154881.doc •24· 201134820 対任-項之醫藥組合物的用途,其用以製備用於治 療、預防、或改善個體的嗜鹼性球相關性病症、疾病、 或病狀之一或多種症狀的藥劑。 ' ; 34. 35. 36. -種如請求項㈣中任一項之化合物或如請求項“至 30中任-項之醫藥組合物的用途,其用以製備用於治 療、預防、或改善個體的肥大細胞相關性病症、疾病、 或病狀之一或多種症狀的藥劑。 ’ 一種如請求項1至25中任-項之化合物或如請求項26至 30中任-項之醫藥組合物㈣途,其心製備用於治 療、預防 '或改善個體的炎性疾病之—或多種症狀的藥 劑。 如請求項31至35中任—項之用途,其中該病症疾病或 病狀選自由以下組成之群:哮喘、過敏性哮喘、運動誘 發之哮喘、過敏性鼻炎、常年性過敏性鼻炎、季節性過 敏性鼻炎、異位性皮炎、接觸性過敏、接觸性皮炎、結 膜炎、過敏性結膜炎、嗜酸性球性枝氣管炎、食物過 敏、嗜酸性球性胃腸炎、炎性腸病、潰瘍性結腸炎、克 羅恩氏病(Crohn's disease)、肥大細胞增生、高IgE症候 群、全身性红斑狼瘡、牛皮癬、痤瘡、多發性硬化症、 同種異體移植排斥、再灌注損傷、慢性阻塞性肺病、丘_ 施氏症候群(Churg-Strauss syndrome)、鼻竇炎、嗜鹼性 球性白血病、慢性蓴麻疹、嗜鹼性球性白細胞增多、牛 皮癬、濕疹、C0PD(慢性阻塞性肺病)、關節炎、類風濕 性關節炎、牛皮癬性關節炎、骨關節炎及心血管病症。 154881.doc •25- 201134820 37. 如請求項36之用途,其中該病症、疾病或病狀係哮喘、 運動誘發之哮喘、過敏性鼻炎、異位性皮炎、慢性阻塞 性肺病或過敏性結膜炎。 A 38. 如請求項31至35中任一項之用途 口、非經腸或局部投與。 39. 如請求項31至35中任一項 <用途’其十該化合物係與第 二治療劑組合使用。 其中該化合物係經 40. 一種調節CCR3活性之方法, 求項1至25中任一項之化合物 項之醫藥組合物接觸。 其包含使CCR3受體與如請 或如請求項26至30中任一 154881.doc 26· 201134820 四、指定代表圖: (一) 本案指定代表圖為:(無) (二) 本代表圖之元件符號簡單說明: 五、本案若有化學式時,請揭示最能顯示發明特徵的化學式:154881.doc
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JP (1) | JP5818873B2 (zh) |
CN (1) | CN102892754A (zh) |
AR (1) | AR080770A1 (zh) |
AU (1) | AU2011227232B2 (zh) |
CA (1) | CA2793391A1 (zh) |
IL (1) | IL222000A0 (zh) |
MX (1) | MX336559B (zh) |
TW (1) | TW201134820A (zh) |
WO (1) | WO2011116161A2 (zh) |
Families Citing this family (7)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
EP1997495B1 (en) | 2003-03-24 | 2013-01-02 | Axikin Pharmaceuticals, Inc. | 2-phenoxy- and 2-phenylsulfanyl-benzenesulfonamide derivatives with CCR3 antagonistic activity for the treatment of asthma and other inflammatory or immunological disorders |
SG10201505313RA (en) | 2009-04-22 | 2015-08-28 | Axikin Pharmaceuticals Inc | 2,5-Disubstituted Arylsulfonamide CCR3 Antagonists |
US8946197B2 (en) | 2009-11-16 | 2015-02-03 | Chdi Foundation, Inc. | Transglutaminase TG2 inhibitors, pharmaceutical compositions, and methods of use thereof |
JP2013543512A (ja) * | 2010-10-11 | 2013-12-05 | アクシキン ファーマシューティカルズ インコーポレーテッド | アリールスルホンアミドccr3アンタゴニストの塩 |
US8889716B2 (en) | 2011-05-10 | 2014-11-18 | Chdi Foundation, Inc. | Transglutaminase TG2 inhibitors, pharmaceutical compositions, and methods of use thereof |
CN104781240A (zh) | 2012-09-07 | 2015-07-15 | 埃克希金医药品有限公司 | 同位素富集的芳基磺酰胺ccr3拮抗剂 |
WO2014075124A1 (en) * | 2012-11-15 | 2014-05-22 | Victoria University | Methods and compositions for the treatment and/or prevention of bowel disorders |
Family Cites Families (82)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US2275354A (en) * | 1937-11-29 | 1942-03-03 | May & Baker Ltd | Preparation of new therapeutically useful heterocyclic compounds |
US3536809A (en) | 1969-02-17 | 1970-10-27 | Alza Corp | Medication method |
US3598123A (en) | 1969-04-01 | 1971-08-10 | Alza Corp | Bandage for administering drugs |
GB1368948A (en) * | 1970-11-11 | 1974-10-02 | Manuf Prod Pharma | Pyridine derivatives |
US3845770A (en) | 1972-06-05 | 1974-11-05 | Alza Corp | Osmatic dispensing device for releasing beneficial agent |
US3916899A (en) | 1973-04-25 | 1975-11-04 | Alza Corp | Osmotic dispensing device with maximum and minimum sizes for the passageway |
US4008719A (en) | 1976-02-02 | 1977-02-22 | Alza Corporation | Osmotic system having laminar arrangement for programming delivery of active agent |
US4233409A (en) * | 1979-07-05 | 1980-11-11 | Monsanto Company | Polymeric blend |
US4410545A (en) | 1981-02-13 | 1983-10-18 | Syntex (U.S.A.) Inc. | Carbonate diester solutions of PGE-type compounds |
US4328245A (en) | 1981-02-13 | 1982-05-04 | Syntex (U.S.A.) Inc. | Carbonate diester solutions of PGE-type compounds |
US4409239A (en) | 1982-01-21 | 1983-10-11 | Syntex (U.S.A.) Inc. | Propylene glycol diester solutions of PGE-type compounds |
KR890002631B1 (ko) | 1984-10-04 | 1989-07-21 | 몬산토 캄파니 | 생물학적으로 활성인 소마토트로핀을 지속적으로 유리하는 조성물 |
IE58110B1 (en) | 1984-10-30 | 1993-07-14 | Elan Corp Plc | Controlled release powder and process for its preparation |
JP2799327B2 (ja) | 1987-12-14 | 1998-09-17 | ザ ダウ ケミカル カンパニー | 三峰性のゴム粒子分布をもつabs組成物 |
US5033252A (en) | 1987-12-23 | 1991-07-23 | Entravision, Inc. | Method of packaging and sterilizing a pharmaceutical product |
US5052558A (en) | 1987-12-23 | 1991-10-01 | Entravision, Inc. | Packaged pharmaceutical product |
US5073543A (en) | 1988-07-21 | 1991-12-17 | G. D. Searle & Co. | Controlled release formulations of trophic factors in ganglioside-lipsome vehicle |
US5612059A (en) | 1988-08-30 | 1997-03-18 | Pfizer Inc. | Use of asymmetric membranes in delivery devices |
IT1229203B (it) | 1989-03-22 | 1991-07-25 | Bioresearch Spa | Impiego di acido 5 metiltetraidrofolico, di acido 5 formiltetraidrofolico e dei loro sali farmaceuticamente accettabili per la preparazione di composizioni farmaceutiche in forma a rilascio controllato attive nella terapia dei disturbi mentali organici e composizioni farmaceutiche relative. |
PH30995A (en) | 1989-07-07 | 1997-12-23 | Novartis Inc | Sustained release formulations of water soluble peptides. |
US5120548A (en) | 1989-11-07 | 1992-06-09 | Merck & Co., Inc. | Swelling modulated polymeric drug delivery device |
US5585112A (en) | 1989-12-22 | 1996-12-17 | Imarx Pharmaceutical Corp. | Method of preparing gas and gaseous precursor-filled microspheres |
US5041498A (en) * | 1990-01-02 | 1991-08-20 | The Dow Chemical Company | Trimodal ABS compositions having good gloss and reduced gloss sensitivity |
IT1246382B (it) | 1990-04-17 | 1994-11-18 | Eurand Int | Metodo per la cessione mirata e controllata di farmaci nell'intestino e particolarmente nel colon |
US5733566A (en) | 1990-05-15 | 1998-03-31 | Alkermes Controlled Therapeutics Inc. Ii | Controlled release of antiparasitic agents in animals |
US5543390A (en) | 1990-11-01 | 1996-08-06 | State Of Oregon, Acting By And Through The Oregon State Board Of Higher Education, Acting For And On Behalf Of The Oregon Health Sciences University | Covalent microparticle-drug conjugates for biological targeting |
US5580578A (en) | 1992-01-27 | 1996-12-03 | Euro-Celtique, S.A. | Controlled release formulations coated with aqueous dispersions of acrylic polymers |
US5323907A (en) | 1992-06-23 | 1994-06-28 | Multi-Comp, Inc. | Child resistant package assembly for dispensing pharmaceutical medications |
TW333456B (en) | 1992-12-07 | 1998-06-11 | Takeda Pharm Ind Co Ltd | A pharmaceutical composition of sustained-release preparation the invention relates to a pharmaceutical composition of sustained-release preparation which comprises a physiologically active peptide. |
US5591767A (en) | 1993-01-25 | 1997-01-07 | Pharmetrix Corporation | Liquid reservoir transdermal patch for the administration of ketorolac |
US6274552B1 (en) | 1993-03-18 | 2001-08-14 | Cytimmune Sciences, Inc. | Composition and method for delivery of biologically-active factors |
US5985307A (en) | 1993-04-14 | 1999-11-16 | Emory University | Device and method for non-occlusive localized drug delivery |
US5523092A (en) | 1993-04-14 | 1996-06-04 | Emory University | Device for local drug delivery and methods for using the same |
US6087324A (en) | 1993-06-24 | 2000-07-11 | Takeda Chemical Industries, Ltd. | Sustained-release preparation |
US6004534A (en) | 1993-07-23 | 1999-12-21 | Massachusetts Institute Of Technology | Targeted polymerized liposomes for improved drug delivery |
DE4404749A1 (de) * | 1994-02-15 | 1995-08-17 | Bayer Ag | ABS-Polymer-Zusammensetzungen mit gleichmäßiger matter Oberfläche |
IT1270594B (it) | 1994-07-07 | 1997-05-07 | Recordati Chem Pharm | Composizione farmaceutica a rilascio controllato di moguisteina in sospensione liquida |
US5759542A (en) | 1994-08-05 | 1998-06-02 | New England Deaconess Hospital Corporation | Compositions and methods for the delivery of drugs by platelets for the treatment of cardiovascular and other diseases |
US5660854A (en) | 1994-11-28 | 1997-08-26 | Haynes; Duncan H | Drug releasing surgical implant or dressing material |
DE19507749A1 (de) * | 1995-03-06 | 1996-09-12 | Bayer Ag | Thermoplastische Formmassen vom ABS-Typ |
DE19518025A1 (de) * | 1995-05-17 | 1996-11-21 | Bayer Ag | Thermoplastische ABS-Formmassen |
US6316652B1 (en) | 1995-06-06 | 2001-11-13 | Kosta Steliou | Drug mitochondrial targeting agents |
US5798119A (en) | 1995-06-13 | 1998-08-25 | S. C. Johnson & Son, Inc. | Osmotic-delivery devices having vapor-permeable coatings |
CA2224381A1 (en) | 1995-06-27 | 1997-01-16 | Takeda Chemical Industries, Ltd. | Method of producing sustained-release preparation |
TW448055B (en) | 1995-09-04 | 2001-08-01 | Takeda Chemical Industries Ltd | Method of production of sustained-release preparation |
JP2909418B2 (ja) | 1995-09-18 | 1999-06-23 | 株式会社資生堂 | 薬物の遅延放出型マイクロスフイア |
US6039975A (en) | 1995-10-17 | 2000-03-21 | Hoffman-La Roche Inc. | Colon targeted delivery system |
US5980945A (en) | 1996-01-16 | 1999-11-09 | Societe De Conseils De Recherches Et D'applications Scientifique S.A. | Sustained release drug formulations |
TW345603B (en) | 1996-05-29 | 1998-11-21 | Gmundner Fertigteile Gmbh | A noise control device for tracks |
US6264970B1 (en) | 1996-06-26 | 2001-07-24 | Takeda Chemical Industries, Ltd. | Sustained-release preparation |
US6419961B1 (en) | 1996-08-29 | 2002-07-16 | Takeda Chemical Industries, Ltd. | Sustained release microcapsules of a bioactive substance and a biodegradable polymer |
US6139865A (en) | 1996-10-01 | 2000-10-31 | Eurand America, Inc. | Taste-masked microcapsule compositions and methods of manufacture |
CA2217134A1 (en) | 1996-10-09 | 1998-04-09 | Sumitomo Pharmaceuticals Co., Ltd. | Sustained release formulation |
DE69730093T2 (de) | 1996-10-31 | 2006-07-20 | Takeda Pharmaceutical Co. Ltd. | Zubereitung mit verzögerter Freisetzung |
US6131570A (en) | 1998-06-30 | 2000-10-17 | Aradigm Corporation | Temperature controlling device for aerosol drug delivery |
DE19649249A1 (de) * | 1996-11-28 | 1998-06-04 | Bayer Ag | Verbesserte thermoplastische Formmassen vom ABS-Typ |
KR20000057693A (ko) | 1996-12-20 | 2000-09-25 | 다케다 야쿠힌 고교 가부시키가이샤 | 지효성 제제의 제조 방법 |
US5891474A (en) | 1997-01-29 | 1999-04-06 | Poli Industria Chimica, S.P.A. | Time-specific controlled release dosage formulations and method of preparing same |
US6120751A (en) | 1997-03-21 | 2000-09-19 | Imarx Pharmaceutical Corp. | Charged lipids and uses for the same |
US6060082A (en) | 1997-04-18 | 2000-05-09 | Massachusetts Institute Of Technology | Polymerized liposomes targeted to M cells and useful for oral or mucosal drug delivery |
US6350458B1 (en) | 1998-02-10 | 2002-02-26 | Generex Pharmaceuticals Incorporated | Mixed micellar drug deliver system and method of preparation |
US6613358B2 (en) | 1998-03-18 | 2003-09-02 | Theodore W. Randolph | Sustained-release composition including amorphous polymer |
EP1076557A1 (en) | 1998-04-27 | 2001-02-21 | Smithkline Beecham Corporation | Ccr-3 receptor antagonists |
US6048736A (en) | 1998-04-29 | 2000-04-11 | Kosak; Kenneth M. | Cyclodextrin polymers for carrying and releasing drugs |
KR19990085365A (ko) | 1998-05-16 | 1999-12-06 | 허영섭 | 지속적으로 약물 조절방출이 가능한 생분해성 고분자 미립구 및그 제조방법 |
WO2000042003A1 (en) | 1999-01-13 | 2000-07-20 | Warner-Lambert Company | Benzenesulfonamide derivatives and their use as mek inhibitors |
US6248363B1 (en) | 1999-11-23 | 2001-06-19 | Lipocine, Inc. | Solid carriers for improved delivery of active ingredients in pharmaceutical compositions |
US6271359B1 (en) | 1999-04-14 | 2001-08-07 | Musc Foundation For Research Development | Tissue-specific and pathogen-specific toxic agents and ribozymes |
AU5473800A (en) | 1999-06-11 | 2001-01-02 | Merck & Co., Inc. | Cyclopentyl modulators of chemokine receptor activity |
AU5600100A (en) | 1999-06-11 | 2001-01-02 | Merck & Co., Inc. | Cyclopentyl modulators of chemokine receptor activity |
CA2389773A1 (en) | 1999-11-05 | 2001-05-10 | Robert Glen | Activators of soluble guanylate cyclase |
DE10008420A1 (de) | 2000-02-23 | 2001-08-30 | Bayer Ag | Polymerzusammensetzungen mit verbesserter Eigenschaftskonstanz |
DE10008419A1 (de) | 2000-02-23 | 2001-08-30 | Bayer Ag | Polymerzusammensetzungen mit verbesserter Eigenschaftskonstanz |
AU2001276608A1 (en) | 2000-08-30 | 2002-03-13 | Pfizer Products Inc. | Sustained release formulations for growth hormone secretagogues |
JP2003081937A (ja) * | 2001-09-07 | 2003-03-19 | Bayer Ag | ベンゼンスルホンアミド誘導体 |
DE10145773A1 (de) | 2001-09-17 | 2003-04-03 | Bayer Ag | ABS-Zusammensetzungen mit verbesserten Eigenschaftskombinationen |
WO2003037271A2 (en) * | 2001-10-30 | 2003-05-08 | Millennium Pharmaceuticals,Inc. | Compounds, pharmaceutical compositions and methods of use therefor |
EP1997495B1 (en) * | 2003-03-24 | 2013-01-02 | Axikin Pharmaceuticals, Inc. | 2-phenoxy- and 2-phenylsulfanyl-benzenesulfonamide derivatives with CCR3 antagonistic activity for the treatment of asthma and other inflammatory or immunological disorders |
BRPI0514230A (pt) * | 2004-08-10 | 2008-06-03 | Incyte Corp | compostos de amido e seu uso como produtos farmacêuticos |
GB0513702D0 (en) * | 2005-07-04 | 2005-08-10 | Sterix Ltd | Compound |
JP5147401B2 (ja) * | 2005-09-06 | 2013-02-20 | 塩野義製薬株式会社 | Pgd2受容体アンタゴニスト活性を有するインドールカルボン酸誘導体 |
CA2758985A1 (en) * | 2009-04-22 | 2010-10-28 | Axikin Pharmaceuticals, Inc. | 2,5-disubstituted arylsulfonamide ccr3 antagonists |
-
2011
- 2011-03-17 WO PCT/US2011/028771 patent/WO2011116161A2/en active Application Filing
- 2011-03-17 CN CN2011800243474A patent/CN102892754A/zh active Pending
- 2011-03-17 AU AU2011227232A patent/AU2011227232B2/en not_active Ceased
- 2011-03-17 AR ARP110100873A patent/AR080770A1/es unknown
- 2011-03-17 JP JP2013500199A patent/JP5818873B2/ja not_active Expired - Fee Related
- 2011-03-17 CA CA2793391A patent/CA2793391A1/en not_active Abandoned
- 2011-03-17 EP EP11715094.6A patent/EP2547655B1/en not_active Not-in-force
- 2011-03-17 TW TW100109234A patent/TW201134820A/zh unknown
- 2011-03-17 MX MX2012010714A patent/MX336559B/es unknown
- 2011-03-17 US US13/050,831 patent/US8741894B2/en not_active Expired - Fee Related
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2012
- 2012-09-19 IL IL222000A patent/IL222000A0/en unknown
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2014
- 2014-04-22 US US14/258,906 patent/US20140221428A1/en not_active Abandoned
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AU2011227232B2 (en) | 2015-07-09 |
US20140221428A1 (en) | 2014-08-07 |
AU2011227232A1 (en) | 2012-10-11 |
US20110230487A1 (en) | 2011-09-22 |
MX336559B (es) | 2016-01-25 |
US8741894B2 (en) | 2014-06-03 |
MX2012010714A (es) | 2013-01-29 |
IL222000A0 (en) | 2012-12-02 |
CN102892754A (zh) | 2013-01-23 |
JP2013522316A (ja) | 2013-06-13 |
CA2793391A1 (en) | 2011-09-22 |
JP5818873B2 (ja) | 2015-11-18 |
WO2011116161A2 (en) | 2011-09-22 |
AR080770A1 (es) | 2012-05-09 |
WO2011116161A3 (en) | 2012-04-19 |
EP2547655B1 (en) | 2016-03-09 |
EP2547655A2 (en) | 2013-01-23 |
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