CKI-7 DIHYDROCHLORIDE
CKI-7 DIHYDROCHLORIDE 用途与合成方法
CK1 6 μM (IC 50 ) |
CK1 8.5 μM (Ki) |
Cdc7
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SGK
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S6K1
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MSK1
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CKI-7 (0.1-10 μM; 5 days; ES cells) treatment significantly increases the expression of the early neuroectodermal marker Sox1 and the number of cells positive for the neural markers nestin and βIII-tubulin, in a concentration-dependent manner.
CKI-7 (5 μM; 5 days; ES cells) treatment suppresses SFEB-induced β-catenin stabilization on day 5, indicating that CKI-7 inhibits Wnt signaling.
RT-PCR
Cell Line: | Mouse ES cells |
Concentration: | 0.1-10 μM |
Incubation Time: | 5 days |
Result: | Significantly increased the expression of the early neuroectodermal marker Sox1 and the number of cells positive for the neural markers nestin and βIII-tubulin, in a concentration-dependent manner. |
Western Blot Analysis
Cell Line: | Mouse ES cells |
Concentration: | 5 μM |
Incubation Time: | 5 days |
Result: | Suppressed SFEB-induced β-catenin stabilization on day 5. |
In vivo dose-dependent anti-tumor activity of CKI-7 is demonstrated in a SCID-Beige mouse systemic tumor model utilzing a recently isolated Philadelphia chromosome positive acute lymphoblastic leukemia cell line. Standard cell cycle synchronization studies established that exposure to CKI-7 results in cell cycle dependent caspase 3 activation and apoptotic cell death.