化合物信息

ID:73304

基本信息

化学结构

分子式

C₂₇H₂₅N₅O₂

分子量

451.5197

精确质量

451.20082507

电荷

InChI

InChI=1S/C27H25N5O2/c1-17-8-9-21(31-25(33)18-6-5-7-19(12-18)27(2,3)15-28)14-24(17)30-20-10-11-23-22(13-20)26(34)32(4)16-29-23/h5-14,16,30H,1-4H3,(H,31,33)

InChIKey

ZGBGPEDJXCYQPH-UHFFFAOYSA-N

Canonic Smiles

N#CC(c1cccc(c1)C(=O)Nc1ccc(c(c1)Nc1ccc2c(c1)c(=O)n(cn2)C)C)(C)C

Isomeric Smiles

c1(cccc(c1)C(=O)Nc1ccc(c(c1)Nc1cc2c(cc1)ncn(c2=O)C)C)C(C#N)(C)C

计算属性

JChem

Acid pKa

12.707882

质子受体

质子供体

LogD (pH = 5.5)

4.694179

LogD (pH = 7.4)

4.7870164

Log P

4.7883477

摩尔折射率

136.2194

极化性

49.125027

极化表面积

97.59

可自由旋转的化学键

里宾斯基五规则

true

数据来源

产品目录

学术数据

数据来源

名称和标识

IUPAC传统名

3-(1-cyano-1-methylethyl)-N-{4-methyl-3-[(3-methyl-4-oxoquinazolin-6-yl)amino]phenyl}benzamide

别名

AZ628

IUPAC标准名

3-(1-cyano-1-methylethyl)-N-{4-methyl-3-[(3-methyl-4-oxo-3,4-dihydroquinazolin-6-yl)amino]phenyl}benzamide

名称和标识

数据登录号

CAS号

878739-06-1

PubChem CID

11676786

PubChem SID

162038224

数据登录号

化合物性质

安全信息

保存条件

-20°C

产品相关信息

成盐信息

Free Base

药理学性质

作用靶点

B-Raf

化合物性质

分子相关蛋白质

暂无数据

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分子图谱

暂无数据

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描述信息

Selleck Chemicals

S2746

Research Area

Description

Cancer

Biological Activity

Description

AZ628 is a potent inhibitor for wild-type CRAF and BRAF^V600E with IC50 of 29 nM and 34 nM, respectively.

Targets

wild-type CRAF

IC₅₀

29 nM

In Vitro

AZ628 prevents activation of number of tyrosine protein kinases including VEGFR2, DDR2, Lyn, Flt1, FMS and others. AZ628 suppresses anchorage-dependent and -independent growth, gives rise to cell cycle arrest, and induces apoptosis in colon and melanoma cell lines harboring B-RafV600E mutation. The profile of AZ628 cross-reactivity suggests that similar to sorafenib, AZ628 may be antiangiogenic based on prevention of VEGFR2. ^[1] AZ628-resistant clones are approximately 100-fold more resistant to AZ628 than the parental cell line, exhibiting IC50 of approximately 10 μM, compared with 0.1 μM for the parental cell line. Effective suppression of p-ERK1/2 levels is observed in the M14 parental cell line following treatment with increasing concentrations of AZ628. AZ628-resistant clones express elevated CRAF. Elevated CRAF expression is a potential mechanism of acquired resistance to continuous AZ628 exposure, resulting in sustained activation of ERK1/2. p-ERK1/2 activity is not significantly inhibited by exposure to AZ628 in one of these three AZ628-insensitive cell lines (Wm1552C). Unlike in the AZ628-resistant M14 cells in which AZ628 fails to suppress the activation of ERK, AZ628 treatment efficiently attenuates ERK activation in the NRAS mutant melanoma cells.^[2]

In Vivo

Clinical Trials

Features

Protocol

Kinase Assay ^[]

Cell Assay ^[1]

Cell Lines

M14 expressing the V600E BRAF mutation

Concentrations

0.01-10 μM

Incubation Time

Overnight

Methods

Approximately 0.5-2.5 × 10⁵ M14 cells are seeded in 12 or 24 - well plates, respectively, in medium supplemented with 5% FBS. After overnight incubation, the cells are treated with various concentrations of AZ628. Fresh medium and drug is replaced every 2 days until the untreated control wells reached confluence. At this time-point, the media is removed and the cells are fixed in 4% formaldehyde in PBS for 20 minutes at room temperature. Cells are then washed twice with PBS and stained with a 1:5000 solution of the fluorescent nucleic acid stain Syto60. Quantitation of fluorescent signal intensity is carried out at 700 nm, using an Odyssey Infrared Imager. Each experiment is performed in quadruplicate and the results shown represent the average of the four values compared to untreated wells. Error bars represent standard deviation of the 4 values from the mean. High-throughput cell growth/viability assays are performed.