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5-溴-1H-吲哚-2-羧酸N-甲氧基-N-甲基酰胺 | 1016481-05-2

中文名称
5-溴-1H-吲哚-2-羧酸N-甲氧基-N-甲基酰胺
中文别名
——
英文名称
5-bromo-N-methoxy-N-methyl-1H-indole-2-carboxamide
英文别名
——
5-溴-1H-吲哚-2-羧酸N-甲氧基-N-甲基酰胺化学式
CAS
1016481-05-2
化学式
C11H11BrN2O2
mdl
——
分子量
283.125
InChiKey
FFNBRFXIDGYKSY-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

  • 沸点:
    475.4±25.0 °C(Predicted)
  • 密度:
    1.575±0.06 g/cm3(Predicted)

计算性质

  • 辛醇/水分配系数(LogP):
    2.6
  • 重原子数:
    16
  • 可旋转键数:
    2
  • 环数:
    2.0
  • sp3杂化的碳原子比例:
    0.18
  • 拓扑面积:
    45.3
  • 氢给体数:
    1
  • 氢受体数:
    2

上下游信息

  • 上游原料
    中文名称 英文名称 CAS号 化学式 分子量
  • 下游产品
    中文名称 英文名称 CAS号 化学式 分子量

反应信息

  • 作为反应物:
    描述:
    5-溴-1H-吲哚-2-羧酸N-甲氧基-N-甲基酰胺 在 sodium cyanoborohydride 、 溶剂黄146 作用下, 以 四氢呋喃乙醚乙醇 为溶剂, 反应 3.0h, 生成 tert-butyl (2-((1-(5-bromo-1H-indol-2-yl)ethyl)amino)ethyl)carbamate
    参考文献:
    名称:
    [EN] THERAPEUTIC COMPOUNDS AND METHODS TO TREAT INFECTION
    [FR] COMPOSÉS THÉRAPEUTIQUES ET MÉTHODES POUR TRAITER UNE INFECTION
    摘要:
    本文披露了化合物的结构式(I)或其盐,以及包含表现出抗菌活性的化合物的组合物的组合物,当单独测试和/或与细菌外排泵抑制剂结合时。还披露了治疗或预防动物细菌感染的方法,包括向动物单独或与细菌外排泵抑制剂的给药结合给动物的结构式(I)的化合物。
    公开号:
    WO2019099402A1
  • 作为产物:
    参考文献:
    名称:
    2-吲哚亚胺甲基化物催化对映选择性合成全碳季立构2,3'-双(吲哚基)甲烷
    摘要:
    描述了 2-乙烯基吲哚的有机催化对映选择性形式加氢芳基化,用于制备带有全碳季立构中心的对映体富集 2,3'-双(吲哚基)甲烷。该反应具有条件温和、催化剂负载量低、效率高和对映选择性高的特点。所得产物显示出有前途的抗癌活性。
    DOI:
    10.1021/acs.orglett.2c04109
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文献信息

  • [EN] ANTI-BACTERIAL PYRUVATE KINASE MODULATOR COMPOUNDS, COMPOSITIONS, USES, AND METHODS<br/>[FR] COMPOSÉS ANTIBACTÉRIENS MODULATEURS DE LA PYRUVATE KINASE, COMPOSITIONS, UTILISATIONS ET MÉTHODES ASSOCIÉES
    申请人:UNIV BRITISH COLUMBIA
    公开号:WO2012051708A1
    公开(公告)日:2012-04-26
    Compounds having a structure of Formulas A-C are provided. Uses of such compounds as an antibiotic, including both gram-negative and gram-positive micro-organisms, as well as methods of treatment and uses involving such compounds are provided.
    提供了具有A-C式结构的化合物。提供了这些化合物作为抗生素的用途,包括革兰氏阴性和革兰氏阳性微生物,以及涉及这些化合物的治疗方法和用途。
  • Fragment-Based Discovery of Indole Inhibitors of Matrix Metalloproteinase-13
    作者:Steven J. Taylor、Asitha Abeywardane、Shuang Liang、Ingo Muegge、Anil K. Padyana、Zhaoming Xiong、Melissa Hill-Drzewi、Bennett Farmer、Xiang Li、Brandon Collins、John Xiang Li、Alexander Heim-Riether、John Proudfoot、Qiang Zhang、Daniel Goldberg、Ljiljana Zuvela-Jelaska、Hani Zaher、Jun Li、Neil A. Farrow
    DOI:10.1021/jm201129m
    日期:2011.12.8
    Matrix metalloproteases (MMPs) play an important role in cartilage homeostasis under both normal and inflamed disease states and, thus, have become attractive targets for the treatment of arthritic diseases. Herein, we describe the identification of a potent, selective MMP-13 inhibitor, developed using fragment-based structure-guided lead identification and optimization techniques. Virtual screening
    基质蛋白酶(MMP)在正常和发炎疾病状态下的软骨稳态中都起着重要作用,因此已成为治疗关节炎疾病的诱人靶标。在这里,我们描述了一种有效的,选择性的MMP-13抑制剂的鉴定,该抑制剂是使用基于片段的结构指导的鉴定和优化技术开发的。虚拟筛选方法确定了一种新型的基于吲哚的MMP-13抑制剂,该抑制剂结合到蛋白质的S1'口袋中,展现出迄今为止在MMP-13抑制剂中未观察到的新型相互作用模式。X射线晶体学结构用于指导片段的加工,最终导致一种强效抑制剂的选择性是所测试的其他九种MMP同工型的100倍以上。
  • Novel MreB inhibitors with antibacterial activity against Gram (-) bacteria
    作者:Hye Yeon Sagong、Jesus D. Rosado-Lugo、Eric J. Bryan、Edgar Ferrer-González、Yiling Wang、Yanlu Cao、Ajit K. Parhi、Daniel S. Pilch、Edmond J. LaVoie
    DOI:10.1007/s00044-022-02967-y
    日期:2022.10
    these compounds has hindered efforts to assess the in vivo efficacy of these MreB inhibitors. The present study further examines the structure-activity of analogs related to CBR-4830 as it relates to relative antibiotic activity and improved drug properties. These data reveal that certain analogs have enhanced antibiotic activity. In addition, we evaluated several representative analogs (9, 10, 14, 26
    MreB 是一种存在于杆状细菌中的细胞骨架蛋白,对细菌细胞分裂至关重要且高度保守。由于大多数革兰氏 (-) 细菌需要 MreB 来进行细胞分裂、染色体分离、细胞壁形态发生和细胞极性,因此它是抗菌药物发现的一个有吸引力的目标。由于 MreB 调节与临床使用中的抗生素活性无关,因此对 MreB 抑制剂的获得性耐药性也不太可能。A22 和 CBR-4830 等化合物已知会通过抑制 ATP 酶活性来破坏 MreB 功能。然而,这些化合物的毒性阻碍了评估这些 MreB 抑制剂体内功效的努力。本研究进一步检查了与 CBR-4830 相关的类似物的结构活性,因为它与相对抗生素活性和改进的药物特性有关。这些数据表明某些类似物具有增强的抗生素活性。此外,我们评估了几个有代表性的类似物(9、10、14、26和31 ) 靶向纯化的大肠杆菌MreB ( EcMreB )并抑制其 ATP 酶活性的能力。除14外,所有这些类似物作为
  • Optimization and structure–activity relationships of a series of potent inhibitors of methicillin-resistant Staphylococcus aureus (MRSA) pyruvate kinase as novel antimicrobial agents
    作者:Nag S. Kumar、Emily A. Amandoron、Artem Cherkasov、B. Brett Finlay、Huansheng Gong、Linda Jackson、Sukhbir Kaur、Tian Lian、Anne Moreau、Christophe Labrière、Neil E. Reiner、Raymond H. See、Natalie C. Strynadka、Lisa Thorson、Edwin W.Y. Wong、Liam Worrall、Roya Zoraghi、Robert N. Young
    DOI:10.1016/j.bmc.2012.10.002
    日期:2012.12
    A novel series of hydrazones were synthesized and evaluated as inhibitors of methicillin-resistant Staphylococcus aureus (MRSA) pyruvate kinase (PK). PK has been identified as one of the most highly connected 'hub proteins' in MRSA. PK has been shown to be critical for bacterial survival which makes it a potential target for development of novel antibiotics and the high degree of connectivity implies it should be very sensitive to mutations and thus less able to develop resistance. PK is not unique to bacteria and thus a critical requirement for such a PK inhibitor would be that it does not inhibit the homologous human enzyme(s) at therapeutic concentrations. Several MRSA PK inhibitors (including 8d) were identified using in silico screening combined with enzyme assays and were found to be selective for bacterial enzyme compared to four human PK isoforms (M1, M2, R and L). However these lead compounds did not show significant inhibitory activity for MRSA growth presumably due to poor bacterial cell penetration. Structure-activity relationship (SAR) studies were carried out on 8d and led us to discover more potent compounds with enzyme inhibiting activities in the low nanomolar range and some were found to effectively inhibit bacteria growth in culture with minimum inhibitory concentrations (MIC) as low as 1 mu g/mL. These inhibitors bind in two elongated flat clefts found at the minor interfaces in the homo-tetrameric enzyme complex and the observed SAR is in keeping with the size and electronic constraints of these binding sites. Access to the corresponding sites in the human enzyme is blocked. (C) 2012 Elsevier Ltd. All rights reserved.
  • THERAPEUTIC COMPOUNDS AND METHODS TO TREAT INFECTION
    申请人:RUTGERS, THE STATE UNIVERSITY OF NEW JERSEY
    公开号:US20200325124A1
    公开(公告)日:2020-10-15
    Disclosed herein are compounds of formula (I), or a salt thereof and compositions comprising compounds of formula I that exhibit antibacterial activities, when tested alone and/or in combination with a bacterial efflux pump inhibitor. Also disclosed are methods of treating or preventing a bacterial infection in an animal comprising administering to the animal a compound of formula I alone or in combination with the administration of a bacterial efflux pump inhibitor.
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