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ETC159(ETC192215)
本产品不向个人销售,仅用作科学研究,不用于任何人体实验及非科研性质的动物实验。
ETC159(ETC192215)图片
CAS NO:1638250-96-0
规格:≥98%
包装与价格:
包装价格(元)
5mg电议
10mg电议
25mg电议
50mg电议
100mg电议
250mg电议
500mg电议
1g电议

产品介绍
理化性质和储存条件
Molecular Weight (MW) 391.38
Formula C19H17N7O3
CAS No. 1638250-96-0
Storage-20℃ for 3 years in powder form
-80℃ for 2 years in solvent
Solubility (In vitro)DMSO: ≥ 34 mg/mL
Water: <1 mg/mL
Ethanol: <1 mg/mL
SMILES O=C1C2C(N=CN2C(CNC3=CC=C(C4=CC=CC=C4)N=N3)=O)N(C)C(N1C)=O
Synonyms ETC-1922159; ETC 1922159; ETC1922159; ETC-159; ETC159; ETC 159
实验参考方法
In Vitro

In vitro activity: ETC-159 (also known as ETC-192215) is a novel, potent and orally bioavailable PORCN inhibitor. It inhibits β-catenin reporter activity with an IC50 of 2.9 nM and blocks the secretion and activity of all Wnts. ETC-159 has robust activity in multiple cancer models driven by high Wnt signaling. ETC-159 is highly efficacious in molecularly defined colorectal cancers (CRCs) with R-spondin translocations.


Kinase Assay: ETC-159 inhibits mouse PORCN with an IC50 of 18.1 nM, whereas the IC50 for Xenopus Porcn is approximately four fold higher (70 nM).


Cell Assay: HEK293 cells stably transfected with STF reporter and pPGK-WNT3A plasmid (STF3A cells) are treated with varying concentrations of compounds. For Wnt secretion, STF3A cells are treated with ETC-159 diluted in 1% fetal bovine serum-containing media

In VivoETC-159 is remarkably effective in treating RSPO-translocation bearing colorectal cancer (CRC) patient-derived xenografts. ETC-159 is remarkably effective in treating RSPO-translocation bearing colorectal cancer (CRC) patient-derived xenografts. ETC-159 exhibits good oral pharmacokinetics in mice allowing preclinical evaluation via oral administration. After a single oral dose of 5 mg/kg, ETC-159 is rapidly absorbed into the blood with a Tmax of ~0.5 h and oral bioavailability of 100%
Animal modelMice bearing colorectal cancer (CRC) patient-derived xenografts
Formulation & DosageFormulated in 50% PEG400 (vol/vol) in water
References Oncogene. 2016 Apr 28;35(17):2197-207.