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    首页 分子通 1-[2-(三氟甲基)苯基]哌嗪盐酸盐

    1-[2-(三氟甲基)苯基]哌嗪盐酸盐 | 40160-26-7

    分子结构分类

    有机化合物 - 有机杂环化合物 - 二嗪烷类
    中文名称
    1-[2-(三氟甲基)苯基]哌嗪盐酸盐
    中文别名
    ——
    英文名称
    1-(2-(trifluoromethyl)phenyl)piperazine hydrochloride
    英文别名
    1-[2-(Trifluoromethyl)phenyl]piperazinium chloride;1-[2-(trifluoromethyl)phenyl]piperazine;hydrochloride
    1-[2-(三氟甲基)苯基]哌嗪盐酸盐化学式
    CAS
    40160-26-7
    化学式
    C11H13F3N2*ClH
    mdl
    ——
    分子量
    266.694
    InChiKey
    OKQSPACLVSNVBL-UHFFFAOYSA-N
    BEILSTEIN
    ——
    EINECS
    ——
    • 物化性质
    • 计算性质
    • ADMET
    • 安全信息
    • SDS
    • 制备方法与用途
    • 上下游信息
    • 反应信息
    • 文献信息
    • 表征谱图
    • 同类化合物
    • 相关功能分类
    • 相关结构分类

    物化性质

    • 溶解度:
      DMSO:10mg/mL; PBS(pH 7.2):10 mg/mL

    计算性质

    • 辛醇/水分配系数(LogP):
      -2.17
    • 重原子数:
      17
    • 可旋转键数:
      1
    • 环数:
      2.0
    • sp3杂化的碳原子比例:
      0.45
    • 拓扑面积:
      16.5
    • 氢给体数:
      2
    • 氢受体数:
      5

    SDS

    SDS:cbf8823014853e99f0491696f20c1929
    查看

    反应信息

    • 作为反应物:
      描述:
      1-[2-(三氟甲基)苯基]哌嗪盐酸盐4-二甲氨基吡啶potassium carbonate一水合肼 作用下, 以 甲醇乙腈 为溶剂, 反应 9.17h, 生成
      参考文献:
      名称:
      设计,合成,构效关系研究,和三维定量构效关系的一系列的(3D-QSAR)建模Ø联苯氨基甲酸酯作为多巴胺D3受体的双重调节剂和脂肪酸酰胺水解酶
      摘要:
      我们最近报道了根据多靶标定向配体范例设计的分子,以对人脂肪酸酰胺水解酶(FAAH)和多巴胺受体D3亚型(D3R)发挥联合活性。这两个目标都与解决几种类型的成瘾(最著名的是尼古丁成瘾)和其他强迫行为有关。在这里,我们报告了一系列联苯-N- [4- [4-(4-(2,3-取代-苯基)哌嗪-1-基]烷基]氨基甲酸酯的SAR勘探,这是一类新颖的分子,已显示出有希望的活性在FAAH–D3R目标组合中进行初步研究。我们已经合理化了有利于主要目标活动的结构特征,并研究了两个非目标活动:多巴胺受体D2亚型和内源性大麻素受体CB 1。为了了解对CB 1受体的意外亲和力,我们设计了一个3D-QSAR模型,然后对其进行了前瞻性验证。选择化合物33进行PK研究是因为它对主要靶标显示出平衡的亲和力,并且在两个非靶标上均具有明显的选择性。33具有良好的稳定性和口服生物利用度,可以穿越血脑屏障。
      DOI:
      10.1021/acs.jmedchem.6b01578
    • 作为产物:
      描述:
      tert-butyl 4-(2-(trifluoromethyl)phenyl)piperazine-1-carboxylate盐酸 作用下, 以 乙酸乙酯 为溶剂, 反应 2.0h, 生成 1-[2-(三氟甲基)苯基]哌嗪盐酸盐
      参考文献:
      名称:
      RUVBL1/2 ATPase 小分子抑制剂的发现
      摘要:
      RUVBL1 和 RUVBL2 是高度保守的 AAA ATP 酶(与各种细胞活动相关的 ATP 酶)并且与癌症的进展高度相关,这使它们成为新型治疗性抗癌药物的有吸引力的靶标。在这项工作中,进行了基于对接的虚拟筛选以识别对 RUVBL1/2 复合物具有活性的化合物。七种化合物在酶促和细胞测定中均显示出对该复合物的抑制活性。基于化合物15的支架合成了一系列吡唑并[1,5- a ]嘧啶-3-甲酰胺类似物,具有抑制活性和良好的结构操作潜力。构效关系分析确定了 R 2上的苄基R 4上的芳环取代哌嗪基对 RUVBL1/2 复合物的抑制活性至关重要。其中,化合物18对 RUVBL1/2 复合物和 RUVBL1的 IC 50值分别为 6.0 ± 0.6 μM 和 7.7 ± 0.9 μM,在细胞系 A549、H1795、HCT116 和 MDA-MB-231 中表现出最有效的抑制作用IC 50值分别为 15
      DOI:
      10.1016/j.bmc.2022.116726
    点击查看最新优质反应信息

    文献信息

    • [EN] PHENYL CARBAMATES AND THEIR USE AS INHIBITORS OF THE FATTY ACID AMIDE HYDROLASE (FAAH) ENZYME AND MODULATORS OF THE D3 DOPAMINE RECEPTOR (D3DR)<br/>[FR] PHENYL CARBAMATES ET LEUR UTILISATION COMME INHIBITEURS DE L'ENZYME HYDROLASE D'AMIDES D'ACIDES GRAS (FAAH) ET MODULATEURS DU RÉCEPTEUR D3 DE LA DOPAMINE (D3DR)
      申请人:FOND ISTITUTO ITALIANO DI TECNOLOGIA
      公开号:WO2015007615A1
      公开(公告)日:2015-01-22
      The invention provides compounds of Formula (I) or pharmaceutically acceptable salts thereof wherein Ar', R1, R2, R3, R4, X, Y are as defined in the description of invention, as multi-target directed ligands (MTDLs) that are at the same time inhibitors of the fatty acid amide hydrolase (FAAH) enzyme and modulators of the D3 dopamine receptor (D3DR), their methods of preparation, formulations and therapeutic applications thereof.
      该发明提供了式(I)的化合物或其药用可接受的盐,其中Ar',R1,R2,R3,R4,X,Y如发明描述中所定义,作为多靶点定向配体(MTDLs),同时是脂肪酸酰胺水解酶(FAAH)酶的抑制剂和D3多巴胺受体(D3DR)的调节剂,以及它们的制备方法、配方和治疗应用。
    • PHENYL CARBAMATES AND THEIR USE AS INHIBITORS OF THE FATTY ACID AMIDE HYDROLASE (FAAH) ENZYME AND MODULATORS OF THE D3 DOPAMINE RECEPTOR (D3DR)
      申请人:FONDAZIONE ISTITUTO ITALIANO DI TECNOLOGIA
      公开号:US20160194296A1
      公开(公告)日:2016-07-07
      The invention provides compounds of Formula (I) or pharmaceutically acceptable salts thereof wherein Ar′, R 1 , R 2 , R 3 , R 4 , X, Y are as defined in the description of invention, as multi-target directed ligands (MTDLs) that are at the same time inhibitors of the fatty acid amide hydrolase (FAAH) enzyme and modulators of the D3 dopamine receptor (D3DR), their methods of preparation, formulations and therapeutic applications thereof.
      本发明提供了化合物I或其药学上可接受的盐,其中Ar′、R1、R2、R3、R4、X、Y的定义如本发明描述中所述,作为多靶点定向配体(MTDLs),同时作为脂肪酸酰胺水解酶(FAAH)酶的抑制剂和D3多巴胺受体(D3DR)的调节剂,以及它们的制备方法、配方和治疗应用。
    • Bicyclic [3.3.0]-Octahydrocyclopenta[<i>c</i>]pyrrolo Antagonists of Retinol Binding Protein 4: Potential Treatment of Atrophic Age-Related Macular Degeneration and Stargardt Disease
      作者:Christopher L. Cioffi、Boglarka Racz、Emily E. Freeman、Michael P. Conlon、Ping Chen、Douglas G. Stafford、Daniel M. C. Schwarz、Lei Zhu、Douglas B. Kitchen、Keith D. Barnes、Nicoleta Dobri、Enrique Michelotti、Charles L. Cywin、William H. Martin、Paul G. Pearson、Graham Johnson、Konstantin Petrukhin
      DOI:10.1021/acs.jmedchem.5b00423
      日期:2015.8.13
      Antagonists of retinol-binding protein 4 (RBP4) impede ocular uptake of serum all-trans retinol (1) and have been shown to reduce cytotoxic bisretinoid formation in the retinal pigment epithelium (RPE), which is associated with the pathogenesis of both dry age-related macular degeneration (AIVID) and Stargardt disease. Thus, these agents show promise as a potential pharmacotherapy by which to stem further neurodegeneration and concomitant -vision loss associated with geographic atrophy of the macula. We previously disdosed the discovery of a novel series of nonretinoid RBP4 antagonists, represented by bicyclic [3.3.0]-octahydrocydopenta[c]pyrrolo analogue 4. We describe herein the utilization of a pyrimidine-4-carboxylic acid fragment as a suitable isostere for the anthranilic acid appendage of 4, which led to the discovery of standout antagonist 33. Analogue 33 possesses exquisite in vitro RBP4 binding affinity and favorable drug-like characteristics and was found to reduce circulating plasma RBP4 levels in vivo in a robust manner (>90%).
    • Structure–Functional Selectivity Relationship Studies of β-Arrestin-Biased Dopamine D<sub>2</sub>Receptor Agonists
      作者:Xin Chen、Maria F. Sassano、Lianyou Zheng、Vincent Setola、Meng Chen、Xu Bai、Stephen V. Frye、William C. Wetsel、Bryan L. Roth、Jian Jin
      DOI:10.1021/jm300603y
      日期:2012.8.23
      Functionally selective G protein-coupled receptor (GPCR) ligands, which differentially modulate canonical and noncanonical signaling, are extremely useful for elucidating key signal transduction pathways essential for both the therapeutic actions and side effects of drugs. However, few such ligands have been created, and very little purposeful attention has been devoted to studying what we term: "structure-functional selectivity relationships" (SFSR). We recently disclosed the first beta-arrestin-biased dopamine D-2 receptor (D2R) agonists UNC9975 (44) and UNC9994 (36), which have robust in vivo antipsychotic drug-like activities. Here we report the first comprehensive SFSR studies focused on exploring four regions of the aripiprazole scaffold, which resulted in the discovery of these beta-arrestin-biased D2R agonists. These studies provide a successful proof-of-concept for how functionally selective ligands can be discovered.
    • US9828352B2
      申请人:——
      公开号:US9828352B2
      公开(公告)日:2017-11-28
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