4-((dibenzylamino)methyl)benzoic acid | 271243-24-4

分子结构分类

有机化合物 - 苯类化合物 - 苯和取代衍生物

中文名称

——

中文别名

——

英文名称

4-((dibenzylamino)methyl)benzoic acid

英文别名

4-[(Dibenzylazaniumyl)methyl]benzoate

4-((dibenzylamino)methyl)benzoic acid化学式

CAS

271243-24-4

化学式

C₂₂H₂₁NO₂

mdl

MFCD09722714

分子量

331.414

InChiKey

LVLFRFFNPLOMON-UHFFFAOYSA-N

BEILSTEIN

——

EINECS

——

物化性质

沸点：

477.5±33.0 °C(Predicted)
密度：

1.183±0.06 g/cm3(Predicted)

计算性质

辛醇/水分配系数(LogP)：

2
重原子数：

25
可旋转键数：

7
环数：

3.0
sp3杂化的碳原子比例：

0.136
拓扑面积：

40.5
氢给体数：

1
氢受体数：

3

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
对醛基苯甲酸	4-Carboxybenzaldehyde	619-66-9	C₈H₆O₃	150.134

反应信息

作为反应物：

描述：

4-((dibenzylamino)methyl)benzoic acid 在草酰氯、 N,N-二甲基甲酰胺作用下，以二氯甲烷为溶剂，生成 C₂₂H₂₀ClNO

参考文献：

名称：

Discovery of novel PTP1B inhibitors via pharmacophore-oriented scaffold hopping from Ertiprotafib

摘要：

An integrated molecular design strategy combining pharmacophore recognition and scaffold hopping was exploited to discover novel PTP1B inhibitors based on the known PTP1B inhibitor Ertiprotafib. A composite pharmacophore model was proposed from the interaction mode of Ertiprotafib, and 21 diverse molecules from five distinct structural classes were designed and synthesized accordingly. New compounds with considerable inhibition against PTP1B were identified from each series, and the most active compound 3a showed IC50 value of 1.3 mu mol L-1 against human recombinant PTP1B. Docking study indicated that the new inhibitors assumed binding modes similar to that of Ertiprotafib. (C) 2013 Elsevier Ltd. All rights reserved.

DOI：

10.1016/j.bmcl.2013.10.002
作为产物：

描述：

methyl 4-[(dibenzylamino)methyl]benzoate 在水、 potassium hydroxide 作用下，以乙醇为溶剂，生成 4-((dibenzylamino)methyl)benzoic acid

参考文献：

名称：

Discovery of novel PTP1B inhibitors via pharmacophore-oriented scaffold hopping from Ertiprotafib

摘要：

An integrated molecular design strategy combining pharmacophore recognition and scaffold hopping was exploited to discover novel PTP1B inhibitors based on the known PTP1B inhibitor Ertiprotafib. A composite pharmacophore model was proposed from the interaction mode of Ertiprotafib, and 21 diverse molecules from five distinct structural classes were designed and synthesized accordingly. New compounds with considerable inhibition against PTP1B were identified from each series, and the most active compound 3a showed IC50 value of 1.3 mu mol L-1 against human recombinant PTP1B. Docking study indicated that the new inhibitors assumed binding modes similar to that of Ertiprotafib. (C) 2013 Elsevier Ltd. All rights reserved.

DOI：

10.1016/j.bmcl.2013.10.002

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文献信息

Chemokine receptor modulators

申请人：Clark Michael P.

公开号：US20080261978A1

公开（公告）日：2008-10-23

The invention provides compounds of Formula (I) and pharmaceutical compositions comprising compounds of Formula (I). These compounds are useful treating or preventing HIV infections, and in treating proliferative disorders such as inhibiting the metastasis of various cancers

该发明提供了式（I）的化合物及包含该化合物的药物组合物。这些化合物可用于治疗或预防HIV感染，并用于治疗增殖性疾病，如抑制各种癌症的转移。
WO2008/109154

申请人：——

公开号：——

公开（公告）日：——
Synthesis and pharmacological characterization of benzenesulfonamides as dual species inhibitors of human and murine mPGES-1

作者：Thomas Hanke、Florian Rörsch、Theresa M. Thieme、Nerea Ferreiros、Gisbert Schneider、Gerd Geisslinger、Ewgenij Proschak、Sabine Grösch、Manfred Schubert-Zsilavecz

DOI：10.1016/j.bmc.2013.10.006

日期：2013.12

The microsomal prostaglandin E-2 synthase 1 (mPGES-1) became a desirable target in recent years for the research of new anti-inflammatory drugs. Even though many potent inhibitors of human mPGES-1, tested in vitro assay systems, have been synthesized, they all failed in preclinical trials in rodent models of inflammation, due to the lack of activity on rodent enzyme. Within this work we want to present a new class of mPGES-1 inhibitors derived from a benzenesulfonamide scaffold with inhibitory potency on human and murine mPGES-1. Starting point with an IC50 of 13.8 mu M on human mPGES-1 was compound 1 (4-benzyl[(4-methoxyphenyl) methyl] sulfamoyl} benzoic acid; FR4), which was discovered by a virtual screening approach. Optimization during a structure-activity relationship (SAR) process leads to compound 28 (4-[(cyclohexylmethyl)[(4-phenylphenyl) methyl] sulfamoyl] benzoic acid) with an improved IC50 of 0.8 mu M on human mPGES-1. For the most promising compounds a broad pharmacological characterization has been carried out to estimate their anti-inflammatory potential. (C) 2013 Elsevier Ltd. All rights reserved.
[EN] CHEMOKINE RECEPTOR MODULATORS<br/>[FR] MODULATEURS DE RÉCEPTEUR DE CHIMIOKINE

申请人：METASTATIX INC

公开号：WO2008109154A1

公开（公告）日：2008-09-12

[EN] The invention provides compounds of Formula (I) and pharmaceutical composi tions comprising compounds of Formula (I). These compounds are useful treating or preventing HIV infections, and in treating proliferative disorders such as inhibiting the metastasis of various cancers
[FR] L'invention concerne des composés de la formule (I) et des compositions pharmaceutiques comprenant des composés de la formule (I). Ces composés sont utiles pour traiter ou prévenir des infections par le VIH, et pour traiter des troubles prolifératifs par l'inhibition de la métastase de divers cancers, par exemple.
Discovery of novel PTP1B inhibitors via pharmacophore-oriented scaffold hopping from Ertiprotafib

作者：Jun-Zheng Liu、Shu-En Zhang、Feilin Nie、Ying Yang、Yan-Bo Tang、Wenwen Yin、Jin-Ying Tian、Fei Ye、Zhiyan Xiao

DOI：10.1016/j.bmcl.2013.10.002

日期：2013.12

An integrated molecular design strategy combining pharmacophore recognition and scaffold hopping was exploited to discover novel PTP1B inhibitors based on the known PTP1B inhibitor Ertiprotafib. A composite pharmacophore model was proposed from the interaction mode of Ertiprotafib, and 21 diverse molecules from five distinct structural classes were designed and synthesized accordingly. New compounds with considerable inhibition against PTP1B were identified from each series, and the most active compound 3a showed IC50 value of 1.3 mu mol L-1 against human recombinant PTP1B. Docking study indicated that the new inhibitors assumed binding modes similar to that of Ertiprotafib. (C) 2013 Elsevier Ltd. All rights reserved.

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