1-(3-methoxyphenyl)-3-(4-nitrophenyl)urea
中文名称
——
中文别名
——
英文名称
1-(3-methoxyphenyl)-3-(4-nitrophenyl)urea
英文别名
N-(3-methoxy-phenyl)-N'-(4-nitro-phenyl)-urea;N-(3-Methoxy-phenyl)-N'-(4-nitro-phenyl)-harnstoff
CAS
——
化学式
C14H13N3O4
mdl
——
分子量
287.275
InChiKey
SEYMHGVSIYPZRG-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):2.5
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重原子数:21
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可旋转键数:3
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环数:2.0
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sp3杂化的碳原子比例:0.07
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拓扑面积:96.2
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氢给体数:2
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氢受体数:4
上下游信息
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下游产品
中文名称 英文名称 CAS号 化学式 分子量 1-(3-羟基苯基)-3-(4-硝基苯基)脲 1-(3-hydroxyphenyl)-3-(4-nitrophenyl)urea 1005450-90-7 C13H11N3O4 273.248 —— 1-(4-aminophenyl)-3-(3-methoxyphenyl)urea 1156595-08-2 C14H15N3O2 257.292
反应信息
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作为反应物:描述:1-(3-methoxyphenyl)-3-(4-nitrophenyl)urea 在 盐酸 、 铁粉 、 氯化铵 作用下, 以 乙醇 、 水 、 正丁醇 为溶剂, 反应 3.83h, 生成 1-(3-methoxyphenyl)-3-[4-(1H-pyrazolo[3,4-d]pyrimidin-4-ylamino)phenyl]urea参考文献:名称:Structure–Activity Relationship Studies of Pyrazolo[3,4-d]pyrimidine Derivatives Leading to the Discovery of a Novel Multikinase Inhibitor That Potently Inhibits FLT3 and VEGFR2 and Evaluation of Its Activity against Acute Myeloid Leukemia in Vitro and in Vivo摘要:We describe the structural optimization of a hit compound, 1-(4-(1H-pyrazolo[3,4-d]pyrimidin-4-ylamino)phenyl)-3-(3-methoxyphenyl)urea (1), which exhibits inhibitory activity but low potency against FLT3 and VEGFR2. A series of pyrazolo [3,4-d]pyrimidine derivatives were synthesized, and structure-activity relationship analysis using cell- and transgenic-zebrafish-based assays led to the discovery of a number of compounds that exhibited both high potency against FLT3-driven human acute myeloid leukemia (AML) MV4-11 cells and a considerable antiangiogenic effect in transgenic-zebrafish-based assays. The compound 1-(4-(1H-pyrazolo[3,4-d]pyrimidin-4-yloxy)phenyl)-3-(4-chloro-3-(trifluoromethyl)phenyl)urea (33), which exhibited the highest activity in preliminary in vivo anti-AML assays, was chosen for further anti AML studies. The results demonstrated that compound 33 is a multikinase inhibitor that potently inhibits FLT3 and VEGFR2. In an MV4-11 xenograft mouse model, a once daily dose of compound 33 at 10 mg/kg for 18 days led to complete tumor regression without obvious toxicity. Western blot and immunohistochemical analyses were performed to determine the mechanism of action of compound 33.DOI:10.1021/jm301537p
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作为产物:描述:参考文献:名称:Structure–Activity Relationship Studies of Pyrazolo[3,4-d]pyrimidine Derivatives Leading to the Discovery of a Novel Multikinase Inhibitor That Potently Inhibits FLT3 and VEGFR2 and Evaluation of Its Activity against Acute Myeloid Leukemia in Vitro and in Vivo摘要:We describe the structural optimization of a hit compound, 1-(4-(1H-pyrazolo[3,4-d]pyrimidin-4-ylamino)phenyl)-3-(3-methoxyphenyl)urea (1), which exhibits inhibitory activity but low potency against FLT3 and VEGFR2. A series of pyrazolo [3,4-d]pyrimidine derivatives were synthesized, and structure-activity relationship analysis using cell- and transgenic-zebrafish-based assays led to the discovery of a number of compounds that exhibited both high potency against FLT3-driven human acute myeloid leukemia (AML) MV4-11 cells and a considerable antiangiogenic effect in transgenic-zebrafish-based assays. The compound 1-(4-(1H-pyrazolo[3,4-d]pyrimidin-4-yloxy)phenyl)-3-(4-chloro-3-(trifluoromethyl)phenyl)urea (33), which exhibited the highest activity in preliminary in vivo anti-AML assays, was chosen for further anti AML studies. The results demonstrated that compound 33 is a multikinase inhibitor that potently inhibits FLT3 and VEGFR2. In an MV4-11 xenograft mouse model, a once daily dose of compound 33 at 10 mg/kg for 18 days led to complete tumor regression without obvious toxicity. Western blot and immunohistochemical analyses were performed to determine the mechanism of action of compound 33.DOI:10.1021/jm301537p
文献信息
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Über den Umsatz aromatischer Isocyansäure-ester mit aromatischen Aminen作者:C. Naegeli、A. Tyabji、L. ConradDOI:10.1002/hlca.193802101140日期:——1. Wenn aromatische Isocyansäure-ester mit aromatischen Aminen in aromatischen Kohlenwasserstoffen sich miteinander umsetzen, so ordnen sich die Substituenten bezüglich ihres Einflusses auf die Aktivität der Isocyansäure-Gruppe in die Reihe1.当芳族异氰酸酯与芳烃中的芳族胺反应时,取代基将根据其对异氰酸酯基活性的影响进行排序
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Design, synthesis and molecular modeling study of certain VEGFR-2 inhibitors based on thienopyrimidne scaffold as cancer targeting agents作者:Amna Ghith、Khairia M. Youssef、Nasser S.M. Ismail、Khaled A.M. AbouzidDOI:10.1016/j.bioorg.2018.10.008日期:2019.3compound 10a. Flow cytometric analysis on both MCV-7 and PC-3 cancer cells revealed that it induced cell-cycle arrest in the G0-G1phase and reinforced apoptosis via activation of caspase-3. Furthermore, molecular modeling studies have been carried out to gain further understanding of the binding mode in the active site of VEGFR-2 enzyme and predict pharmacokinetic properties of all the synthesized inhibitors设计,合成和评价了不同系列的新型噻吩并[2,3- d ]嘧啶衍生物(9a-d,10a-f,l,m和15a-m)在体外抑制VEGFR-2酶的能力。而且,通过NCI对60种不同的人类癌细胞系进行了测试,以测试最终化合物的细胞毒性。VEGFR-2酶的抑制结果表明,化合物10d,15d和15 g是活性最高的抑制剂,IC 50值分别为2.5、5.48和2.27 µM,而化合物10a显着显示出最高的细胞生长抑制率,平均生长抑制率(GI)为31.57%。它对几种NCI细胞系表现出广谱的抗增殖活性,特别是对人乳腺癌(T7-47D)和肾癌(A498)细胞系分别具有85.5%和77.65%的抑制作用。为了研究该活性的机制,对化合物10a进行了进一步的生物学研究,例如流式细胞术细胞周期与caspase-3比色测定。对MCV-7和PC-3癌细胞的流式细胞仪分析表明,它诱导了G0-G1期的细胞周期停滞,并通过激活c
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3D-QSAR pharmacophore modelling, virtual screening and docking studies for lead discovery of a novel scaffold for VEGFR 2 inhibitors: Design, synthesis and biological evaluation作者:Mahitab K. Sobhy、Samar Mowafy、Deena S. Lasheen、Nahla A. Farag、Khaled A.M. AbouzidDOI:10.1016/j.bioorg.2019.102988日期:2019.8modelling protocols prior to the synthesis and biological evaluation of the derivatives. First, sorafenib was docked in the binding site of VEGFR 2 to study its binding orientation and affinity, followed by the generation of a valid 3D QSAR pharmacophore model for use in the virtual screening of different 3D databases. Structures with promising pharmacophore-based virtual screening results were refined using成功设计,合成和评估了一系列新颖的6,7-二氢-5H-环戊[d]嘧啶衍生物,作为具有血管内皮生长因子受体(VEGFR 2)抑制活性的新型化学支架。化合物6c和6b在10 µM时分别显示97%和87%的酶抑制,并显示出有效的剂量相关VEGFR 2抑制,IC50值分别为0.85 µM和2.26 µM。6,7-二氢-5H-环戊[d]嘧啶骨架的设计是通过连续的分子建模方案进行的,然后进行衍生物的合成和生物学评估。首先,将索拉非尼停靠在VEGFR 2的结合位点以研究其结合方向和亲和力,然后生成有效的3D QSAR药效团模型,用于虚拟筛选不同的3D数据库。通过在VEGFR 2的结合位点进行分子对接研究,对具有前景的基于药效团的虚拟筛选结果的结构进行了改进。通过结合药效团模型生成和分子对接研究的结果,设计了一种新型支架。新的支架显示出与激酶前袋的疏水相互作用,这可能归因于在VEGFR 2中的停留时间增加
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Molecular design, synthesis and <i>in vitro</i> biological evaluation of thienopyrimidine–hydroxamic acids as chimeric kinase HDAC inhibitors: a challenging approach to combat cancer作者:Mona M. Abdel-Atty、Nahla A. Farag、Rabah A. T. Serya、Khaled A. M. Abouzid、Samar MowafyDOI:10.1080/14756366.2021.1933465日期:2021.1.1pharmacophore of EGFR, VEGFR2 into the inhibitory functionality of HDAC6. Three compounds (12c, 15b and 20b) were promising hits, whereas (12c) exhibited potent VEGFR2 inhibition (IC50=185 nM), potent EGFR inhibition (IC50=1.14 µM), and mild HDAC6 inhibition (23% inhibition). Moreover, compound (15c) was the most potent dual inhibitor among all the synthesised compounds, as it exhibited potent EGFR and VEGFR2抽象的 通过将EGFR、VEGFR2的药效团结合到HDAC6的抑制功能中,设计并合成了一系列基于噻吩并[2,3- d ]嘧啶的异羟肟酸杂合体作为多靶点抗癌药物。三种化合物(12c、15b 和 20b)是有希望的命中,而(12c)表现出有效的 VEGFR2 抑制(IC 50 = 185 nM)、有效的 EGFR 抑制(IC 50 = 1.14 µM)和轻度 HDAC6 抑制(抑制 23%)。此外,化合物(15c)是所有合成化合物中最有效的双重抑制剂,因为它分别表现出有效的EGFR和VEGFR2抑制作用(IC 50 =19 nM)和(IC 50 =5.58 µM)。而化合物(20d)和(7c)分别表现出纳摩尔选择性激酶抑制作用,EGFR IC 50 = 68 nM,VEGFR2 IC 50 = 191 nM。所有合成的化合物均在体外筛选其对 60 种人类 NCI 肿瘤细胞系的细胞毒作用。此外,还进行了分子对接研究和
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Über die Einwirkung von Wasser auf aromatische lsocyansäure-ester作者:C. Naegeli、A. Tyabji、L. Conrad、F. LitwanDOI:10.1002/hlca.193802101139日期:——1. Die Reaktionswege, die bei Umsatz aromatischer Isocyansäure-ester mit Wasser zum zugehörigen Diarylharnstoff bzw. zum entsprechenden Arylamin führen, wurden systematisch untersucht: (a) durch den Umsatz der Isocyanate mit Wasser unter verschiedenartigen Bedingungen; (b) durch den Umsatz mit Arylaminen in Benzol-Toluol-Lösung; (c) durch den gleichzeitigen Umsatz mit Wasser und Arylamin in Aceton;1.已经系统地研究了使芳族异氰酸酯与水反应时导致缔合的二芳基脲或相应的芳基胺的反应途径:(a)通过在不同条件下使异氰酸酯与水反应;(b)通过与芳胺在苯-甲苯溶液中的转化;(c)与水和芳基胺在丙酮中同时反应;(d)通过转换获得2%的收益。钾碱液和不同浓度的盐酸;(e)通过用甲醇转化。实验结果为z。部分内容在表1(p。1102)中,然后用文字简要概述。参考了实验的制备重要性(第1101、1118和1125页)。
同类化合物
(βS)-β-氨基-4-(4-羟基苯氧基)-3,5-二碘苯甲丙醇
(S)-(-)-7'-〔4(S)-(苄基)恶唑-2-基]-7-二(3,5-二-叔丁基苯基)膦基-2,2',3,3'-四氢-1,1-螺二氢茚
(S)-盐酸沙丁胺醇
(S)-3-(叔丁基)-4-(2,6-二甲氧基苯基)-2,3-二氢苯并[d][1,3]氧磷杂环戊二烯
(S)-2,2'-双[双(3,5-三氟甲基苯基)膦基]-4,4',6,6'-四甲氧基联苯
(S)-1-[3,5-双(三氟甲基)苯基]-3-[1-(二甲基氨基)-3-甲基丁烷-2-基]硫脲
(R)富马酸托特罗定
(R)-(-)-盐酸尼古地平
(R)-(+)-7-双(3,5-二叔丁基苯基)膦基7''-[((6-甲基吡啶-2-基甲基)氨基]-2,2'',3,3''-四氢-1,1''-螺双茚满
(R)-3-(叔丁基)-4-(2,6-二苯氧基苯基)-2,3-二氢苯并[d][1,3]氧杂磷杂环戊烯
(R)-2-[((二苯基膦基)甲基]吡咯烷
(N-(4-甲氧基苯基)-N-甲基-3-(1-哌啶基)丙-2-烯酰胺)
(5-溴-2-羟基苯基)-4-氯苯甲酮
(5-溴-2-氯苯基)(4-羟基苯基)甲酮
(5-氧代-3-苯基-2,5-二氢-1,2,3,4-oxatriazol-3-鎓)
(4S,5R)-4-甲基-5-苯基-1,2,3-氧代噻唑烷-2,2-二氧化物-3-羧酸叔丁酯
(4-溴苯基)-[2-氟-4-[6-[甲基(丙-2-烯基)氨基]己氧基]苯基]甲酮
(4-丁氧基苯甲基)三苯基溴化磷
(3aR,8aR)-(-)-4,4,8,8-四(3,5-二甲基苯基)四氢-2,2-二甲基-6-苯基-1,3-二氧戊环[4,5-e]二恶唑磷
(2Z)-3-[[(4-氯苯基)氨基]-2-氰基丙烯酸乙酯
(2S,3S,5S)-5-(叔丁氧基甲酰氨基)-2-(N-5-噻唑基-甲氧羰基)氨基-1,6-二苯基-3-羟基己烷
(2S,2''S,3S,3''S)-3,3''-二叔丁基-4,4''-双(2,6-二甲氧基苯基)-2,2'',3,3''-四氢-2,2''-联苯并[d][1,3]氧杂磷杂戊环
(2S)-(-)-2-{[[[[3,5-双(氟代甲基)苯基]氨基]硫代甲基]氨基}-N-(二苯基甲基)-N,3,3-三甲基丁酰胺
(2S)-2-[[[[[[((1R,2R)-2-氨基环己基]氨基]硫代甲基]氨基]-N-(二苯甲基)-N,3,3-三甲基丁酰胺
(2-硝基苯基)磷酸三酰胺
(2,6-二氯苯基)乙酰氯
(2,3-二甲氧基-5-甲基苯基)硼酸
(1S,2S,3S,5S)-5-叠氮基-3-(苯基甲氧基)-2-[(苯基甲氧基)甲基]环戊醇
(1-(4-氟苯基)环丙基)甲胺盐酸盐
(1-(3-溴苯基)环丁基)甲胺盐酸盐
(1-(2-氯苯基)环丁基)甲胺盐酸盐
(1-(2-氟苯基)环丙基)甲胺盐酸盐
(-)-去甲基西布曲明
龙胆酸钠
龙胆酸叔丁酯
龙胆酸
龙胆紫
龙胆紫
齐达帕胺
齐诺康唑
齐洛呋胺
齐墩果-12-烯[2,3-c][1,2,5]恶二唑-28-酸苯甲酯
齐培丙醇
齐咪苯
齐仑太尔
黑染料
黄酮,5-氨基-6-羟基-(5CI)
黄酮,6-氨基-3-羟基-(6CI)
黄蜡,合成物
黄草灵钾盐
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