7ACC-2
- CAS号:1472624-85-3
- 英文名:7ACC-2
- 中文名:7ACC-2
- CBNumber:CB22729349
- 分子式:C18H15NO4
- 分子量:309.32
- MOL File:1472624-85-3.mol
- 沸点 :548.9±50.0 °C(Predicted)
- 密度 :1.368±0.06 g/cm3(Predicted)
- 储存条件 :2-8°C
- 溶解度 :insoluble in EtOH; insoluble in H2O; ≥47.5 mg/mL in DMSO
- 形态 :Powder
- 酸度系数(pKa) :-98.37±0.20(Predicted)
- 颜色 :Light yellow to yellow
- 海关编码 :2932990090
7ACC-2性质、用途与生产工艺
- 生物活性 7ACC2是一种有效的MCT1抑制剂,在SiHa人源宫颈细胞癌中抑制乳酸吸收,IC50为10 nM。
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靶点
Target Value MCT1
() -
体外研究
7ACC2 (compound 19; 72 hours) inhibits SiHa cells proliferation in lactate-containing medium with an EC50 of 0.22 μM. In SiHa cells, lactate uptake primarily depends on the high affinity MCT1 transporter.
7ACC2 (compound 19) shows an excellent chemical stability in simulated gastric (SGF) and intestinal (SIF) fluids, a good apparent permeability coefficient (Papp) through Caco-2 monolayer and a high metabolic stability on mouse (MLM) and human liver microsomes (HLM) as well as on human hepatocytes.
7ACC2 is a potent inhibitor of mitochondrial pyruvate transport which consecutively blocks extracellular lactate uptake by promoting intracellular pyruvate accumulation. -
体内研究
7ACC2 (3 mg/kg; intraperitoneal administration; daily; for 5 days or 10days) treatment significantly inhibits tumor growth in mice. 7ACC2 radiosensitizes tumor cells by reducing hypoxia in vivo.
The intraperitoneal administration of 7ACC2 (compound 19; 3 mg/kg) to mice leads to a C max of 1246 ng/ml (4 μM) in a very short time (T max =10 min) associated with a plasma half-life of 4.5 h.Animal Model: 7-week-old female NMRI nude mice with radiotherapy administered Dosage: 3 mg/kg Administration: Intraperitoneal administration; daily; for 5 days or 10days Result: A significant increase in tumor growth delay was observed.
- 更新日期:2024/11/08
- 产品编号:HY-D0713
- 产品名称:7ACC-2 7ACC2
- CAS编号:1472624-85-3
- 包装:2mg
- 价格:600元
- 更新日期:2024/11/08
- 产品编号:HY-D0713
- 产品名称:7ACC-2 7ACC2
- CAS编号:1472624-85-3
- 包装:5mg
- 价格:900元
- 公司名称:Alsachim SAS
- 联系电话:--
- 电子邮件:sales@alsachim.com
- 国家:法国
- 产品数:424
- 优势度:0