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AD57 (hydrochloride)

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产品名称: AD57 (hydrochloride)
产品型号: GOY-Y1834
产品展商: 谷研
产品文档: 无相关文档
发布时间:2023-04-25

简单介绍

AD57 (hydrochloride)≤5mg/ml in ethanol;10mg/ml in DMSO;14mg/ml in dimethyl formamide


AD57 (hydrochloride)  的详细介绍

性能参数

产品名称

AD57 (hydrochloride)

规格

mg 5mg 10mg

货号

GOY-Y1834

 含量

>98.00%

CAS

Cas No.

别名

 

 

 

化学名

N-[4-[4-amino-1-(1-methylethyl)-1H-pyrazolo[3,4-d]pyrimidin-3-yl]phenyl]-N'-[3-(trifluoromethyl)phenyl]-urea, monohydrochloride

分子式

C22H20F3N7O ? HCl

分子量

分子 491.9

溶解度

≤5mg/ml in ethanol;10mg/ml in DMSO;14mg/ml in dimethyl formamide

储存条件

Store at -20°C

General tips

 

用途

仅供科研

价格

电询

详细内容

IC50: 2 nM: blocks the receptor tyrosine kinase RET in Drosophila.

AD57, as a polypharmacological cancer therapeutic, is designed to regulate multiple targets related to cancer. AD57 effectively suppresses tyrosine kinase RET, weakens the activity of numerous other kinases, and interferes with kinases downstream of RET, including Raf, Src, and S6K, providing further efficacy in preventing signaling leading to invasion, proliferation, and metabolism related to cancer. Tyrosine kinase RET is probably sufficient to initiate a series of transformation events including medullary thyroid carcinoma, multiple endocrine neoplasias type 2A (MEN2A) and 2B (MEN2B).

In vitro: AD57 was demonstrated to be able to inhibit tyrosine kinase RET. But the efficacy of AD57 did not correlate solely with the blockade of RET, suggesting that the targeting of additional kinases is necessary for its biological efficacy. AD57 potently dampened the pathway-related human kinases B-Raf, mTOR, S6K, and Src [1].

In vivo: Male nu nu mice, injected subcutaneously with MEN2A cell lines, were administered AD57 (20 mg/kg) by oral gavage (per os) once daily, five times a week. AD57 inhibited the activity of relevant target kinases at 1 μM compared with the vehicle-treated nude mice transplanted with MEN2A cells [1].

Reference:

[1].  Dar, A., Das, T., Shokat, K., & Cagan, R. Chemical genetic discovery of targets and anti-targets for cancer polypharmacology. Nature. 2012; 486(7401): 80-84.

 

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