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1140525-25-2

中文名称 1140525-25-2
英文名称 SB 290157 trifluoroacetate salt
CAS 1140525-25-2
分子式 C22H28N4O4?CF3COOH
分子量 526.51
MOL 文件 1140525-25-2.mol
更新日期 2024/08/14 15:30:12
1140525-25-2 结构式 1140525-25-2 结构式

基本信息

中文别名
化合物SB290157 TRIFLUOROACETATE
N2-[2-(2,2-二苯基乙氧基)乙酰基]-L-精氨酸三氟乙酸盐
英文别名
SB290157 (trifluoroacetate)
SB 290157 trifluoroacetate salt
SB 290157 - CAS 1140525-25-2 - Calbiochem
SB 290157 TRIFLUOROACETATE
SB-290157 TRIFLUOROACETATE
N2-(2-(2,2-diphenylethoxy)acetyl)-L-arginine, 2,2,2-trifluor
(2S)-5-(diaminomethylideneamino)-2-[[2-(2,2-diphenylethoxy)acetyl]amino]pentanoic acid

物理化学性质

熔点>43°C (dec.)
储存条件-20°C
溶解度可溶于乙醇(轻微,超声),甲醇(轻微),水(轻微)
形态粉末
颜色白色至米色
旋光性 (optical activity)[α]/D +1.5 to +5°, c = 1.0 in DMSO
稳定性吸湿性

安全数据

危险性符号(GHS)
GHS07
警示词警告
危险性描述H302-H315-H319-H335

常见问题列表

生物活性
SB290157 trifluoroacetate (SB 290157 TFA) 是一种有效的 C3a receptor (C3aR) 的竞争性、选择性的拮抗剂,对RBL-C3aR的IC50值为200 nM。
靶点
TargetValue
RBL-C3aR
(Cell-free assay)
200 nM
体外研究

SB 290157, functions as a competitive antagonist of 125 I-C3a radioligand binding to rat basophilic leukemia-2H3 cells expressing the human C3aR (RBL-C3aR), with an IC 50 of 200 nM. SB 290157 blocks C3a-induced C3aR internalization in a concentration-dependent manner and C3a-induced Ca 2+ mobilization in RBL-C3aR cells and human neutrophils with IC 50 s f 27.7 and 28 nM, respectively. SB 290157 is selective for the C3aR in that it does not antagonize the C5aR or six other chemotactic G protein-coupled receptors. SB 290157 also inhibits C3a-induced Ca 2+ mobilization of RBL-2H3 cells expressing the mouse and guinea pig C3aRs. It potently inhibits C3a-mediated ATP release from guinea pig platelets and inhibits C3a-induced potentiation of the contractile response to field stimulation of perfused rat caudal artery.

体内研究

SB 290157, inhibits neutrophil recruitment in a guinea pig LPS-induced airway neutrophilia model and decreases paw edema in a rat adjuvant-induced arthritis model. The antagonist is able to reduce joint swelling only at 3 h, and about 50% inhibition of joint swelling is observed with the concentration of 30 mg/kg. The C3 level is significantly decreased at 3 h compared with naive mice showing complement consumption. Furthermore, the C3 activation is observed and increased corresponding to the graded concentration of anti-OVA pAb.

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