4-氯-7-(三氟甲氧基)喹啉-3-羧酸乙酯 | 890841-23-3
中文名称
4-氯-7-(三氟甲氧基)喹啉-3-羧酸乙酯
中文别名
——
英文名称
ethyl 4-chloro-7-(trifluoromethoxy)quinoline-3-carboxylate
英文别名
4-Chloro-7-(trifluoromethoxy)quinoline-3-carboxylic acid ethyl ester
CAS
890841-23-3
化学式
C13H9ClF3NO3
mdl
——
分子量
319.668
InChiKey
XQRIHVPOLQTQIZ-UHFFFAOYSA-N
BEILSTEIN
——
EINECS
——
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物化性质
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计算性质
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ADMET
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安全信息
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SDS
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制备方法与用途
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上下游信息
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文献信息
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表征谱图
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同类化合物
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相关功能分类
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相关结构分类
计算性质
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辛醇/水分配系数(LogP):4.2
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重原子数:21
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可旋转键数:4
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环数:2.0
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sp3杂化的碳原子比例:0.23
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拓扑面积:48.4
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氢给体数:0
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氢受体数:7
SDS
上下游信息
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上游原料
中文名称 英文名称 CAS号 化学式 分子量 4-氧代-7-(三氟甲氧基)-1H-喹啉-3-羧酸乙酯 4-Hydroxy-7-trifluoromethoxy-quinoline-3-carboxylic acid ethyl ester 53985-73-2 C13H10F3NO4 301.222 -
下游产品
中文名称 英文名称 CAS号 化学式 分子量 —— ethyl 2-(3-methoxyphenyl)-4-oxo-7-(trifluoromethoxy)-1,4-dihydroquinoline-3-carboxylate 1373767-09-9 C20H16F3NO5 407.346 —— ethyl 4-oxo-7-(trifluoromethoxy)-2-(3-(trifluoromethoxy)phenyl)-1,4-dihydroquinoline-3-carboxylate 1373767-10-2 C20H13F6NO5 461.317 —— ethyl 2-(benzo[d][1,3]dioxol-5-yl)-4-oxo-7-(trifluoromethoxy)-1,4-dihydroquinoline-3-carboxylate 1373767-08-8 C20H14F3NO6 421.329
反应信息
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作为反应物:描述:4-氯-7-(三氟甲氧基)喹啉-3-羧酸乙酯 在 三乙基硅烷 、 bis-triphenylphosphine-palladium(II) chloride 、 lithium hydroxide monohydrate 、 N,N-二异丙基乙胺 、 N-[(dimethylamino)-3-oxo-1H-1,2,3-triazolo[4,5-b]pyridin-1-yl-methylene]-N-methylmethanaminium hexafluorophosphate 作用下, 以 四氢呋喃 、 水 、 N,N-二甲基甲酰胺 、 乙腈 为溶剂, 反应 20.08h, 生成 N-(trans-4-(2-hydroxypropan-2-yl)cyclohexyl)-7-(trifluoromethoxy)quinoline-3-carboxamide参考文献:名称:喹啉-3-羧酰胺作为造血前列腺素D合酶(H-PGDS)抑制剂的发现。摘要:为了发现比COX抑制剂更具选择性的消炎药,以减弱前列腺素信号传导,进行了基于片段的造血前列腺素D合酶筛选。将76个晶体学命中物分为相似的组,其中3-氰基喹啉1a(FP IC50 = 220,000 nM,LE = 0.43)是6,6-稠合杂环簇的有效成员。利用从其他H-PGDS片段结合模式簇的结构比较中获得的SAR洞察力,将初始命中1a转化为更有效的喹啉1d(IC50 = 3,100 nM,LE = 0.49)。利用结构信息和阵列化学方法,系统修饰1d的胺部分,并进行修饰以改善抑制剂的稳定性,结果鉴定出具有300倍活性的H-PGDS抑制剂工具化合物1bv(IC50 = 9.9 nM,LE = 0.42)。这种选择性抑制剂在肥大细胞脱粒试验中表现出良好的鼠药代动力学,剂量依赖性地减弱了PGD2的产生,应该适合于进一步研究H-PGDS生物学。DOI:10.1016/j.bmc.2019.02.017
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作为产物:描述:参考文献:名称:喹啉-3-羧酰胺作为造血前列腺素D合酶(H-PGDS)抑制剂的发现。摘要:为了发现比COX抑制剂更具选择性的消炎药,以减弱前列腺素信号传导,进行了基于片段的造血前列腺素D合酶筛选。将76个晶体学命中物分为相似的组,其中3-氰基喹啉1a(FP IC50 = 220,000 nM,LE = 0.43)是6,6-稠合杂环簇的有效成员。利用从其他H-PGDS片段结合模式簇的结构比较中获得的SAR洞察力,将初始命中1a转化为更有效的喹啉1d(IC50 = 3,100 nM,LE = 0.49)。利用结构信息和阵列化学方法,系统修饰1d的胺部分,并进行修饰以改善抑制剂的稳定性,结果鉴定出具有300倍活性的H-PGDS抑制剂工具化合物1bv(IC50 = 9.9 nM,LE = 0.42)。这种选择性抑制剂在肥大细胞脱粒试验中表现出良好的鼠药代动力学,剂量依赖性地减弱了PGD2的产生,应该适合于进一步研究H-PGDS生物学。DOI:10.1016/j.bmc.2019.02.017
文献信息
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Lead Optimization of 3-Carboxyl-4(1<i>H</i>)-Quinolones to Deliver Orally Bioavailable Antimalarials作者:Yiqun Zhang、Julie A. Clark、Michele C. Connelly、Fangyi Zhu、Jaeki Min、W. Armand Guiguemde、Anupam Pradhan、Lalitha Iyer、Anna Furimsky、Jason Gow、Toufan Parman、Farah El Mazouni、Margaret A. Phillips、Dennis E. Kyle、Jon Mirsalis、R. Kiplin GuyDOI:10.1021/jm201642z日期:2012.5.10Malaria is a protozoal parasitic disease that is widespread in tropical and subtropical regions of Africa, Asia, and the Americas and causes more than 800,000 deaths per year. The continuing emergence of multidrug-resistant Plasmodium falciparum drives the ongoing need for the development of new and effective antimalarial drugs. Our previous work has explored the preliminary structural optimization of 4(1H)-quinolone ester derivatives, a new series of antimalarials related to the endochins. Herein, we report the lead optimization of 4(1H)-quinolones with a focus on improving both antimalarial potency and bioavailability. These studies led to the development of orally efficacious antimalarials including quinolone analogue 20g, a promising candidate for further optimization.
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QUINOLINE-3-CARBOXAMIDES AS H-PGDS INHIBITORS申请人:Astex Therapeutics Limited公开号:EP3390384B1公开(公告)日:2021-09-15
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CHEMICAL COMPOUNDS申请人:GlaxoSmithKline Intellectual Property Development Limited公开号:US20210238162A1公开(公告)日:2021-08-05The present invention relates to compounds of Formula (XI): wherein R 1a , R 2a , R 3a , R 4a , R 5a , R 6a , and Aa are as defined herein, and pharmaceutically acceptable salts thereof. The compounds of the present invention are inhibitors of hematopoietic prostaglandin D synthase (H-PGDS) inhibitors and can be useful in the treatment of Duchenne Muscular Dystrophy. Accordingly, the invention is further directed to pharmaceutical compositions comprising a compound of the invention. The invention is still further directed to methods of inhibiting H-PGDS activity and treatment of disorders associated therewith using a compound of the invention or a pharmaceutical composition comprising a compound of the invention.
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[EN] QUINOLINE-3-CARBOXAMIDES AS H-PGDS INHIBITORS<br/>[FR] QUINOLÉINE-3-CARBOXAMIDES UTILISÉS COMME INHIBITEURS DE H-PGDS申请人:ASTEX THERAPEUTICS LTD公开号:WO2017103851A1公开(公告)日:2017-06-22The present invention relates to compounds of Formula (XI) wherein R1a, R2a, R3a, R4a, R5a, R6a, and Aa are as defined herein, and pharmaceutically acceptable salts thereof. The compounds of the present invention are inhibitors of hematopoietic prostaglandin D synthase (H-PGDS) inhibitors and can be useful in the treatment of Duchenne Muscular Dystrophy. Accordingly, the invention is further directed to pharmaceutical compositions comprising a compound of the invention. The invention is still further directed to methods of inhibiting H-PGDS activity and treatment of disorders associated therewith using a compound of the invention or a pharmaceutical composition comprising a compound of the invention.
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The discovery of quinoline-3-carboxamides as hematopoietic prostaglandin D synthase (H-PGDS) inhibitors作者:David N. Deaton、Young Do、Jason Holt、Michael R. Jeune、H. Fritz Kramer、Andrew L. Larkin、Lisa A. Orband-Miller、Gregory E. Peckham、Chuck Poole、Daniel J. Price、Lee T. Schaller、Ying Shen、Lisa M. Shewchuk、Eugene L. Stewart、J. Darren Stuart、Stephen A. Thomson、Paris Ward、Joseph W. Wilson、Tianshun Xu、Jeffrey H. Guss、Caterina Musetti、Alan R. Rendina、Karen Affleck、David Anders、Ashley P. Hancock、Heather Hobbs、Simon T. Hodgson、Jonathan Hutchinson、Melanie V. Leveridge、Harry Nicholls、Ian E.D. Smith、Don O. Somers、Helen F. Sneddon、Sorif Uddin、Anne Cleasby、Paul N. Mortenson、Caroline Richardson、Gordon SaxtyDOI:10.1016/j.bmc.2019.02.017日期:2019.4converted into the 70-fold more potent quinoline 1d (IC50 = 3,100 nM, LE = 0.49). A systematic substitution of the amine moiety of 1d, utilizing structural information and array chemistry, with modifications to improve inhibitor stability, resulted in the identification of the 300-fold more active H-PGDS inhibitor tool compound 1bv (IC50 = 9.9 nM, LE = 0.42). This selective inhibitor exhibited good murine pharmacokinetics为了发现比COX抑制剂更具选择性的消炎药,以减弱前列腺素信号传导,进行了基于片段的造血前列腺素D合酶筛选。将76个晶体学命中物分为相似的组,其中3-氰基喹啉1a(FP IC50 = 220,000 nM,LE = 0.43)是6,6-稠合杂环簇的有效成员。利用从其他H-PGDS片段结合模式簇的结构比较中获得的SAR洞察力,将初始命中1a转化为更有效的喹啉1d(IC50 = 3,100 nM,LE = 0.49)。利用结构信息和阵列化学方法,系统修饰1d的胺部分,并进行修饰以改善抑制剂的稳定性,结果鉴定出具有300倍活性的H-PGDS抑制剂工具化合物1bv(IC50 = 9.9 nM,LE = 0.42)。这种选择性抑制剂在肥大细胞脱粒试验中表现出良好的鼠药代动力学,剂量依赖性地减弱了PGD2的产生,应该适合于进一步研究H-PGDS生物学。
同类化合物
(S)-4-(叔丁基)-2-(喹啉-2-基)-4,5-二氢噁唑
(SP-4-1)-二氯双(喹啉)-钯
(E)-2-氰基-3-[5-(2,5-二氯苯基)呋喃-2-基]-N-喹啉-8-基丙-2-烯酰胺
(8α,9S)-(+)-9-氨基-七氢呋喃-6''-醇,值90%
(6,7-二甲氧基-4-(3,4,5-三甲氧基苯基)喹啉)
(1-羟基-5-硝基-8-氧代-8,8-dihydroquinolinium)
黄尿酸 8-甲基醚
麻保沙星EP杂质D
麻保沙星EP杂质B
麻保沙星EP杂质A
麦角腈甲磺酸盐
麦角腈
麦角灵
麦皮星酮
麦特氧特
高铁试剂
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马波沙星
马来酸茚达特罗
马来酸维吖啶
马来酸来那替尼
马来酸四甲基铵
香草木宁碱
颜料红R-122
颜料红210
颜料红
顺式-苯并(f)喹啉-7,8-二醇-9,10-环氧化物
顺式-(alphaR)-N-(4-氯苯基)-4-(6-氟-4-喹啉基)-alpha-甲基环己烷乙酰胺
非那沙星
非那沙星
青花椒碱
青色素863
雷西莫特
隐花青
阿莫地喹-d10
阿莫地喹
阿莫吡喹N-氧化物
阿美帕利
阿米诺喹
阿立哌唑溴代杂质
阿立哌唑杂质38
阿立哌唑杂质1750
阿立哌唑杂质13
阿立哌唑杂质
阿尔马尔
阿加曲班杂质43
阿加曲班杂质13
阿克罗宁
铽(3+)十氧化五硼镁
银(1+)1-乙基-6-氟-4-氧代-7-(1-哌嗪基)-1,4-二氢-3-喹啉羧酸酯
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