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1094067-13-6

中文名稱 1094067-13-6
英文名稱 SCH1473759 (HCl salt)
CAS 1094067-13-6
更新日期 2023/03/20 15:41:27
分子式 C20H27ClN8OS
分子量 463
MOL 文件 1094067-13-6.mol
1094067-13-6 結構式 1094067-13-6 結構式

基本信息

中文別名
AURORA A和AURORA B抑制劑(SCH-1473759 HYDROCHLORIDE)
英文別名
SCH-1473759 HCl
SCH1473759 (HCl salt)
SCH-1473759 hydrochloride

物理化學性質

儲存條件-20°C儲存
溶解度DMSO: 70 mg/mL (151.19 mM)
形態(tài)Solid
顏色White to yellow
1094067-13-6價格(試劑級)
報價日期產品編號產品名稱CAS號包裝價格
2024/11/08HY-104831094067-13-6
SCH-1473759 hydrochloride
1094067-13-62mg1800元
2024/11/08HY-104831094067-13-6
SCH-1473759 hydrochloride
1094067-13-65mg2800元
2024/11/08HY-104831094067-13-6
SCH-1473759 hydrochloride
1094067-13-610mM * 1mLin DMSO2852元

常見問題列表

生物活性
SCH-1473759 hydrochloride是多靶點的的極光激酶 (aurora) 抑制劑,對極光激酶A和B的IC50 值分別為4 和13 nM。
靶點

Aurora A

4 nM (IC 50 )

Aurora B

13 nM (IC 50 )

體外研究

SCH-1473759 directly binds to aurora A and B with K d s of 20 and 30 nM, respectively. SCH-1473759 also inhibits the Src family of kinases (IC 50 <10 nM), Chk1 (IC 50 =13 nM), VEGFR2 (IC 50 =1 nM), and IRAK4 (IC 50 =37 nM). It does not have significant activity (IC 50 >1000 nM) against 34 other kinases representing different families of the kinome. SCH-1473759 inhibits HCT116 cells proliferation with an IC 50 of 6 nM. SCH 1473759 inhibits tumor cell lines from different tissues (breast, ovarian, prostate, lung, colon, brain, gastric, renal, skin, and leukemia). The most sensitive cell lines includ A2780, LNCap, N87, Molt4, K562, and CCRF-CEM with IC 50 values <5 nM.

體內研究

SCH-1473759 at a low dose of 5 mg/kg (ip, bid) is well-tolerated in a continuous dosing schedule and shows 50% tumor growth inhibition(TGI) on day 16. A higher dose of 10mg/kg(ip, bid) is well-tolerated in an intermittent schedule (5 days on, 5 days off) and gave 69% TGI on day 16. SCH-1473759 shows good exposure in all species with the clearance being high in rodents and moderate in dog and monkey. The half-life is also moderate, but the tissue distribution is high. SCH 1473759 dose- and schedule-dependent anti-tumor activity in four human tumor xenograft models. Further, the efficacy is enhanced in combination with taxanes and found to be most efficacious when SCH 1473759 is dosed 12-h post-taxane treatment.

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