3'-氯-2'-氟乙酰苯胺 | 395-36-8
中文名称
3'-氯-2'-氟乙酰苯胺
中文别名
——
英文名称
N-(3-chloro-2-fluorophenyl)acetamide
英文别名
acetic acid-(3-chloro-2-fluoro-anilide);Essigsaeure-(3-chlor-2-fluor-anilid)
CAS
395-36-8
化学式
C8H7ClFNO
mdl
MFCD03094496
分子量
187.601
InChiKey
CBJRXPIMTXGGAT-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
物化性质
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沸点:318.2±32.0 °C(Predicted)
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密度:1.352±0.06 g/cm3(Predicted)
计算性质
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辛醇/水分配系数(LogP):1.8
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重原子数:12
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可旋转键数:1
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环数:1.0
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sp3杂化的碳原子比例:0.125
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拓扑面积:29.1
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氢给体数:1
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氢受体数:2
SDS
上下游信息
反应信息
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作为反应物:描述:参考文献:名称:Tandem optimization of target activity and elimination of mutagenic potential in a potent series of N-aryl bicyclic hydantoin-based selective androgen receptor modulators摘要:Pharmacokinctic studies in cynomolgus monkeys with a novel prototype selective androgen receptor modulator revealed trace amounts of an aniline fragment released through hydrolytic metabolism. This aniline fragment was determined to be mutagenic in an Ames assay. subsequent concurrent optimization for target activity and avoidance of mutagenicity led to the identification of a pharmacologically superior clinical candidate without mutagenic potential. (c) 2007 Elsevier Ltd. All rights reserved.DOI:10.1016/j.bmcl.2007.01.076
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作为产物:参考文献:名称:对抗甲型流感病毒H1N1:苯并呋喃山衍生物作为病毒RNA聚合酶抑制剂的合成,分子建模和生物学评估摘要:由PA,PB1和PB2三个亚基组成的流感RNA聚合酶复合物是开发新抗病毒药物的有希望的目标。合成了庞大的苯并呋喃化合物文库,并针对流感病毒A / WSN / 33(H1N1)进行了分析。发现大多数新衍生物通过破坏亚基PA和PB1之间形成的复合物来抑制病毒RNA聚合酶复合物而发挥作用。还进行了对接研究,以阐明PA中PB1结合位点内苯并呋喃类的结合方式,并鉴定参与其作用机理的氨基酸。预测的结合姿势与生物学数据完全一致,为合理开发更有效的PA–PB1抑制剂奠定了基础。DOI:10.1002/cmdc.201300378
文献信息
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[EN] INHIBITORS OF RECEPTOR INTERACTING PROTEIN KINASE I FOR THE TREATMENT OF DISEASE<br/>[FR] INHIBITEURS DE LA PROTÉINE KINASE I INTERAGISSANT AVEC LE RÉCEPTEUR POUR LE TRAITEMENT D'UNE MALADIE申请人:UNIV TEXAS公开号:WO2021046515A1公开(公告)日:2021-03-11Disclosed herein are compounds which inhibit RIPK1, pharmaceutical compositions, and methods of treatment of RIPK1 -mediated diseases, such as neurodegenerative disorders, inflammatory disorders, and cancer.本文披露了一些抑制RIPK1的化合物、药物组合物和治疗RIPK1介导疾病的方法,如神经退行性疾病、炎症性疾病和癌症。
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Transition-Metal-Free Synthesis of Benzimidazoles Mediated by KOH/DMSO作者:Hannah Baars、Astrid Beyer、Stefanie V. Kohlhepp、Carsten BolmDOI:10.1021/ol403414v日期:2014.1.17Benzimidazoles are prepared by intramolecular N-arylations of amidines mediated by potassium hydroxide in DMSO at 120 degrees C. In this manner, diversely substituted products have been obtained in moderate to very good yields.
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The Fight against the Influenza A Virus H1N1: Synthesis, Molecular Modeling, and Biological Evaluation of Benzofurazan Derivatives as Viral RNA Polymerase Inhibitors作者:Mafalda Pagano、Daniele Castagnolo、Martina Bernardini、Anna Lucia Fallacara、Ilaria Laurenzana、Davide Deodato、Ulrich Kessler、Beatrice Pilger、Lilli Stergiou、Stephan Strunze、Cristina Tintori、Maurizio BottaDOI:10.1002/cmdc.201300378日期:2014.1The influenza RNA polymerase complex, which consists of the three subunits PA, PB1, and PB2, is a promising target for the development of new antiviral drugs. A large library of benzofurazan compounds was synthesized and assayed against influenza virus A/WSN/33 (H1N1). Most of the new derivatives were found to act by inhibiting the viral RNA polymerase complex through disruption of the complex formed由PA,PB1和PB2三个亚基组成的流感RNA聚合酶复合物是开发新抗病毒药物的有希望的目标。合成了庞大的苯并呋喃化合物文库,并针对流感病毒A / WSN / 33(H1N1)进行了分析。发现大多数新衍生物通过破坏亚基PA和PB1之间形成的复合物来抑制病毒RNA聚合酶复合物而发挥作用。还进行了对接研究,以阐明PA中PB1结合位点内苯并呋喃类的结合方式,并鉴定参与其作用机理的氨基酸。预测的结合姿势与生物学数据完全一致,为合理开发更有效的PA–PB1抑制剂奠定了基础。
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Tandem optimization of target activity and elimination of mutagenic potential in a potent series of N-aryl bicyclic hydantoin-based selective androgen receptor modulators作者:Lawrence G. Hamann、Mark C. Manfredi、Chongqing Sun、Stanley R. Krystek、Yanting Huang、Yingzhi Bi、David J. Augeri、Tammy Wang、Yan Zou、David. A. Betebenner、Aberra Fura、Ramakrishna Seethala、Rajasree Golla、Joyce E. Kuhns、John A. Lupisella、Celia J. Darienzo、Laura L. Custer、Jennifer L. Price、James M. Johnson、Scott A. Biller、Robert Zahler、Jacek OstrowskiDOI:10.1016/j.bmcl.2007.01.076日期:2007.4Pharmacokinctic studies in cynomolgus monkeys with a novel prototype selective androgen receptor modulator revealed trace amounts of an aniline fragment released through hydrolytic metabolism. This aniline fragment was determined to be mutagenic in an Ames assay. subsequent concurrent optimization for target activity and avoidance of mutagenicity led to the identification of a pharmacologically superior clinical candidate without mutagenic potential. (c) 2007 Elsevier Ltd. All rights reserved.
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