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178616-26-7

中文名稱 178616-26-7
英文名稱 1-(4'-AMINOPHENYL)-3,5-DIHYDRO-7,8-DIMETHOXY-4H-2,3-BENZODIAZEPIN-4-ONE
CAS 178616-26-7
分子式 C17H17N3O3
分子量 311.34
MOL 文件 178616-26-7.mol
更新日期 2024/12/03 15:40:31
178616-26-7 結(jié)構(gòu)式 178616-26-7 結(jié)構(gòu)式

基本信息

中文別名
化合物CFM-2
化合物 T10774
178616-26-7
英文別名
CFM-2
1-(4'-AMINOPHENYL)-3,5-DIHYDRO-7,8-DIMETHOXY-4H-2,3-BENZODIAZEPIN-4-ONE
4H-2,3-Benzodiazepin-4-one,1-(4-aminophenyl)-3,5-dihydro-7,8-dimethoxy-

物理化學性質(zhì)

密度1.32±0.1 g/cm3(Predicted)
儲存條件Store at RT
溶解度溶于二甲基亞砜
酸度系數(shù)(pKa)12.53±0.40(Predicted)
形態(tài)灰白色固體。
顏色Light yellow to khaki
178616-26-7價格(試劑級)
報價日期產(chǎn)品編號產(chǎn)品名稱CAS號包裝價格
2026/06/05HY-12503CFM-2178616-26-75 mg896元
2026/06/05HY-12503178616-26-7
CFM-2
178616-26-710mM * 1mLin DMSO985元
2026/06/05HY-12503178616-26-7
CFM-2
178616-26-710mg1352元

常見問題列表

生物活性
CFM-2 是一種有效的、選擇性的、非競爭性的 AMPAR 拮抗劑。CFM-2 在不同的驚厥動物模型中均表現(xiàn)出抗驚厥活性。
體外研究

CFM-2 inhibits the extracellular signal regulated kinase (ERK1/2) pathway, CFM-2 reduced phosphorylation of cAMP-responsive element binding protein (CREB), suppressed expression of cyclin D1, upregulated the cell cycle regulators and tumor suppressor proteins p21 and p53 and decreased number of lung adenocarcinoma cells in G2 and S phases of the cell cycle.

體內(nèi)研究

Pretreatment with CFM-2 delays the progression of seizure rank during repeated administration of pentylentetrazole. At the end of the period of repeated pentylentetrazole treatment (6 weeks) the mean seizure score was 0 in vehicle treated controls, 4.3 in animals treated with vehicle + pentylentetrazole, 2.2 in rats treated chronically with CFM-2 (20 μmol/kg; i.p.) + pentylentetrazole and 1.0 in rats treated repeatedly with CFM-2 (50 μmol/kg; i.p.) + pentylenetetrazole. CFM-2 is also able to antagonize the long-term increase in sensitivity of the convulsant effects of GABA function inhibitors in pentylentetrazole-kindled animals.Intrathecal application of two selective non-competitive AMPAR antagonists, CFM-2 (25 and 50 μg) and GYKI 52466 (50μg), significantly attenuated mechanical and thermal hypersensitivities on the ipsilateral hind paw at 2 and 24 h post-CFA injection. Neither CFM-2 nor GYKI 52466 affects the contralateral basal responses to thermal and mechanical stimuli.

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