1619994-68-1

中文名稱 GSK2801

英文名稱 GSK 2801

CAS 1619994-68-1

分子式 C20H21NO4S

分子量 371.45

MOL 文件 1619994-68-1.mol

更新日期 2024/07/24 18:26:22

1619994-68-1 結(jié)構(gòu)式

基本信息物理化學(xué)性質(zhì) 安全數(shù)據(jù) 圖譜信息 GSK2801價格(試劑級) 常見問題列表

基本信息

中文別名

BAZ2A和BAZ2B抑制劑(GSK2801)
1-(1-(2-(甲磺酰)苯基)-7-丙氧基吲哚嗪-3-基)乙酮
1-[1-[2-(甲基磺酰基)苯基]-7-丙氧基-3-吲哚嗪基]乙酮

英文別名

CS-1607
GSK2801
GSK 280
GSK 2801
GSK-2801
GSK2801, >98%
GSK-2801
GSK 280
GSK2801 GSK-2801
GSK2801
GSK-2801
GSK 2801
1-[1-[2-(Methylsulfonyl)phenyl]-7-propoxy-3-indolizinyl]ethanone

所屬類別

生物化工：激動劑抑制劑

物理化學(xué)性質(zhì)

密度1.23±0.1 g/cm3(Predicted)

儲存條件-20°C

溶解度insoluble in H2O; ≥18.55 mg/mL in DMSO; ≥2.82 mg/mL in EtOH with gentle warming and ultrasonic

形態(tài)固體

顏色Light yellow to khaki

InChI1S/C20H21NO4S/c1-4-11-25-15-9-10-21-18(14(2)22)13-17(19(21)12-15)16-7-5-6-8-20(16)26(3,23)24/h5-10,12-13H,4,11H2,1-3H3

InChIKeyKHWCPNJRJCNVRI-UHFFFAOYSA-N

SMILESCCCOC1=CC2=C(C3=CC=CC=C3S(=O)(C)=O)C=C(C(C)=O)N2C=C1

安全數(shù)據(jù)

危險性符號(GHS) 有害 (GHS07)

GHS07

警示詞警告

危險性描述H302

防范說明P280-P305+P351+P338

危險品標(biāo)志Xn

危險類別碼22

WGK GermanyWGK 3

存儲類別11 - Combustible Solids

危險性類別Acute Tox. 4 Oral

圖譜信息

GSK2801(1619994-68-1)核磁圖(¹HNMR)

GSK2801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
2026/03/03	46803	GSK2801, 95% GSK2801, 95%	1619994-68-1	100mg	6997元
2025/12/22	HY-15658	GSK2801 GSK2801	1619994-68-1	5mg	623元
2025/12/22	HY-15658	GSK2801 GSK2801	1619994-68-1	10mM * 1mLin DMSO	715元

常見問題列表

生物活性

GSK2801 是一種有效的，選擇性的，口服活性的和細胞活性的乙酰賴氨酸競爭性 BAZ2A 和 BAZ2B 溴結(jié)構(gòu)域抑制劑，Kd 值分別為 136 nM 和 257 nM。GSK2801 對 BAZ2A/B 的選擇性是 BRD4 的 50 倍以上。

靶點

Kd: 136 nM (BAZ2A) and 257 nM (BAZ2B)

體外研究

GSK2801 binds TAF1L(2) with an affinity K _B of 0.31μM (K _D : 3.2 μM) and a binding enthalpy change ΔH of ?8.6 kcal/mol. ITC experiments using the bromodomain of BRD9 results in the determination of an affinity K _B of 0.826 μM (K _D : 1.1 μM) and ΔH of ?9.8 kcal/mol.
GSK2801 or RNAi knockdown of BAZ2A/B with JQ1 selectively displaced BRD2 at promoters/enhancers of ETS-regulated genes. In 2D cultures, enhances displacement of BRD2 from chromatin by combination drug treatment induced senescence. In spheroid cultures, combination treatment induces cleaved caspase-3 and cleaved PARP characteristic of apoptosis in tumor cells. Thus, GSK2801 blocks BRD2-driven transcription in combination with BET inhibitor and induces apoptosis of TNBC.

體內(nèi)研究

In order to determine the suitability of GSK2801 for in vivo experiments, pharmacokinetic parameters after intraperitoneal and oral dosing to male CD1 mice is measured. GSK2801 has reasonable in vivo exposure after oral dosing, modest clearance, and reasonable plasma stability.