N-芴甲氧羰基-1,3-二氨基丙烷 氢溴酸盐 | 352351-59-8

• 物质功能分类: 有机原料 - 氨基化合物 - 含氧基氨基化合物
• 分子结构分类: 有机化合物 - 苯类化合物 - 芴
• 中文名称: N-芴甲氧羰基-1,3-二氨基丙烷 氢溴酸盐
• 中文别名: N-芴甲氧羰基-1,3-二氨基丙烷氢溴酸盐
• 英文名称: (9H-fluoren-9-yl)methyl (3-aminopropyl)carbamate hydrobromide
• 英文别名: N-Fmoc-1,3-diaminopropane hydrobromide；N-Fmoc-1,3-propanediamine hydrobromide；9H-fluoren-9-ylmethyl N-(3-aminopropyl)carbamate;hydrobromide
• CAS: 352351-59-8
• 化学式: BrH*C₁₈H₂₀N₂O₂
• 分子量: 377.281
• InChiKey: OWAKRMILENXFGM-UHFFFAOYSA-N

物化性质

• 熔点：
  ~121℃ (dec.)

计算性质

• 辛醇/水分配系数(LogP)：
  3.45
• 重原子数：
  23
• 可旋转键数：
  6
• 环数：
  3.0
• sp3杂化的碳原子比例：
  0.28
• 拓扑面积：
  64.4
• 氢给体数：
  3
• 氢受体数：
  3

安全信息

• 危险品标志：
  Xi
• 安全说明：
  S26,S36
• 危险类别码：
  R36/37/38
• WGK Germany：
  3

反应信息

• 作为反应物：
  描述：

  4-amino-6-[[2-(4-formylphenoxymethyl)benzoyl]amino]-2-methylquinoline 、 N-芴甲氧羰基-1,3-二氨基丙烷 氢溴酸盐 在 N,N-二异丙基乙胺 作用下， 以 甲醇 为溶剂， 生成
  参考文献：
  名称：

  Synthesis and pharmacological evaluation of bivalent antagonists of the nociceptin opioid receptor

  摘要：

  Bivalent ligands constituted by two identical pharmacophores structurally related to the Nociceptin Opioid Receptor (NOPr) antagonist JTC-801 were synthesized and their binding affinities for NOPr were evaluated. The novel ligands are formed by two modified JTC-801 units linked by di-iminic and di-aminic spacers with length ranging from three to ten methylene units. Moreover, the synthesis and the pharmacological characterization were extended to the corresponding univalent ligands. The latter compounds consisted in a single modified JTC-801 unit and an alkyl or alkylamino or alkylimino tail. The purpose of this study is to feature the location and surroundings of the allosteric binding site(s) of pharmacophores containing the 4-aminoquinoline structure. Most important, the bivalent ligands were exploited to reveal the eventual occurrence of a supramolecular receptorial architecture of the NOPr.All the bivalent derivatives 4 and 5 proved to be active in the nanomolar range with no outstanding dependence on the chain length. They showed potencies from three to ten times higher than the corresponding monomers. Consequently, results clearly indicated a positive role of the second pharmacophore in the ligand-protein interaction. The pharmacological profile of I he monomers 7 and 8 clarified the contribution of the linker chain to NOP receptor affinity and suggested the presence of a lipophilic acidic site neighbouring the binding site of the JTC-like ligands.Selectivity of saturated compounds 5, 7, and 8 was tested by binding experiments on delta, kappa and mu opioid receptors. Results indicated a general loss of selectivity as compared to JTC-801. In the [(35)S]GTP gamma S binding assay, all the compounds revealed antagonistic properties at the NOP Receptor.In conclusion the present study set the basis for a systematic investigation on the structural modifications that can be introduced into novel ligands for NOPr and helped to feature the surrounds of the allosteric site of NOPr. (C) 2011 Elsevier Masson SAS. All rights reserved.

  DOI：

  10.1016/j.ejmech.2011.01.040

文献信息

• [EN] ANTIBODY DRUG CONJUGATES<br/>[FR] CONJUGUÉS DE MÉDICAMENT ANTICORPS
  申请人：PHARMA MAR SA

  公开号：WO2014191578A1

  公开（公告）日：2014-12-04

  Drug conjugates of formula [D-(X)b-(AA)w-(L)-]n-Ab wherein: D is a drug moiety having the following formula (I) or a pharmaceutically acceptable salt, ester, solvate, tautomer or stereoisomer thereof, wherein: A is selected from (II) and (III) R1, R2 and R3 is H, ORa, OCORa, OCOORa, alkyl, alkenyl, alkynyl, etc; R3' is, CORa, COORa, CONRaRb, etc; each of R4 to R10 and R12 is alkyl, alkenyl or alkynyl; R11 is H, CORa, COORa,alkyl, alkenyl or alkynyl, or R11 and R12+N+C atoms to which they are attached may form a heterocyclic group; each of R13 and R14 is H, CORa, COORa, alkyl, alkenyl or alkynyl; each Ra and Rb is H, alkyl, alkenyl, alkynyl, etc.; each dotted line represents an optional additional bond; X is an extending group; AA is an amino acid unit; L is a linker group; w is 0to 12; b is 0 or 1; A bis a moiety comprising at least one antigen binding site, and n is the ratio of the group [D-(X) b -(AA)w-(L)-] to the moiety comprising at least one antigen binding site and is in the range from 1 to 20, are useful in the treatment of cancer.

  药物偶联物公式为 [D-(X)b-(AA)w-(L)-]n-Ab，其中：D 是具有以下公式 (I) 的药物部分或其药物可接受的盐、酯、溶剂化物、互变异构体或立体异构体，其中：A 选自 (II) 和 (III)；R1、R2 和 R3 是 H、ORa、OCORa、OCOORa、烷基、烯基、炔基等；R3' 是 CORa、COORa、CONRaRb 等；R4 至 R10 和 R12 各自是烷基、烯基或炔基；R11 是 H、CORa、COORa、烷基、烯基或炔基，或者 R11 和 R12 与它们连接的 N+C 原子可以形成一个杂环组；R13 和 R14 各自是 H、CORa、COORa、烷基、烯基或炔基；Ra 和 Rb 各自是 H、烷基、烯基、炔基等；每个虚线代表一个可选的附加键；X 是一个延伸组；AA 是一个氨基酸单位；L 是一个连接组；w 是 0 到 12；b 是 0 或 1；Ab 是包含至少一个抗原结合位点的部分，n 是 [D-(X)b-(AA)w-(L)-] 组与至少含有一个抗原结合位点的部分的比例，并且范围从 1 到 20，在癌症治疗中是有用的。
• Design and Synthesis of a Highly Selective and <i>In Vivo</i>-Capable Inhibitor of the Second Bromodomain of the Bromodomain and Extra Terminal Domain Family of Proteins
  作者：Alex Preston、Stephen Atkinson、Paul Bamborough、Chun-wa Chung、Peter D. Craggs、Laurie Gordon、Paola Grandi、James R. J. Gray、Emma J. Jones、Matthew Lindon、Anne-Marie Michon、Darren J. Mitchell、Rab K. Prinjha、Francesco Rianjongdee、Inmaculada Rioja、Jonathan Seal、Simon Taylor、Ian Wall、Robert J. Watson、James Woolven、Emmanuel H Demont

  DOI：10.1021/acs.jmedchem.0c00605

  日期：2020.9.10

  better understand the contribution of each domain to their efficacy and improve their safety profile, selective inhibitors are required. This article discloses the profile of GSK046, also known as iBET-BD2, a highly selective inhibitor of the second bromodomains of the BET proteins that has undergone extensive pre-clinical in vitro and in vivo characterization.

  泛溴结构域和额外末端结构域（BET）抑制剂与BET蛋白质家族的八个溴结构域等价相互作用，并且在炎症或肿瘤学中的许多体外表型测定和体内临床前模型中显示出深远的功效。这些抑制剂中的许多已经发展到临床上，据报道药理学驱动的不良事件。为了更好地理解每个域对其功效的贡献并改善其安全性，需要选择性抑制剂。本文公开了GSK046（也称为iBET-BD2）的概况，它是BET蛋白第二个溴结构域的高度选择性抑制剂，已经在体外和体内进行了广泛的临床前研究 表征。
• HEPARAN SULFATE/HEPARIN MIMETICS WITH ANTI-CHEMOKINE AND ANTI-INFLAMMATORY ACTIVITY
  申请人：California Institute of Technology

  公开号：US20150038455A1

  公开（公告）日：2015-02-05

  The present disclosure provides for methods and compositions comprising a series of synthetic glycopolymers. The disclosure also relates to a kit which is suitable for carrying out the inventive methods.

  本公开提供了一系列合成糖聚合物的方法和组合物。该公开还涉及一种适用于执行创新方法的试剂盒。
• TAILORED GLYCOPOLYMERS AS ANTICOAGULANT HEPARIN MIMETICS
  申请人：California Institute of Technology

  公开号：US20150038436A1

  公开（公告）日：2015-02-05

  The present disclosure provides for methods and compositions comprising a series of synthetic glycopolymers. The disclosure also relates to a kit which is suitable for carrying out the inventive methods.

  本公开提供了一系列合成糖聚合物的方法和组合物。该公开还涉及一种适用于实施创新方法的试剂盒。
• [EN] AN OSTEOADSORPTIVE FLUOROGENIC SUBSTRATE OF CATHEPSIN K FOR IMAGING OSTEOCLAST ACTIVITY AND MIGRATION<br/>[FR] SUBSTRAT FLUOROGÈNE OSTÉOADSORBANT DE CATHEPSINE K POUR L'IMAGERIE DE L'ACTIVITÉ ET DE LA MIGRATION DES OSTÉOCLASTES
  申请人：UNIV CALIFORNIA

  公开号：WO2019018238A1

  公开（公告）日：2019-01-24

  In certain embodiments osteoadsorptive fluorogenic substrates of cathepsin K (or other proteases) are provided. Utilizing a bisphosphonate targeting moiety, the fluorogenic substrates provide effective bone-targeted protease sensor(s). In certain embodiments the "probes" comprise cleavable fluorophore-quencher pair linked by a cathepsin K (or other protease) peptide substrate and tethered to a bisphosphonate. Unlike existing probes that are cleared within a few days in vivo, the probes described herein (e.g., OFS-1) allow for monitoring resorption over the course of longer time periods with a single dose.

  在某些实施例中，提供了钙蛋白酶K（或其他蛋白酶）的骨吸收荧光底物。利用双磷酸盐靶向基团，荧光底物提供有效的靶向骨蛋白酶传感器。在某些实施例中，“探针”包括可切割的荧光团-猝灭剂对，由钙蛋白酶K（或其他蛋白酶）肽底物连接，并与双磷酸盐相连。与现有的在体内几天内被清除的探针不同，本文所述的探针（例如OFS-1）允许在单剂量下监测骨吸收的长时间进程。