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4°C, sealed storage, away from moisture
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货期:1-2天
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MedChemExpress LLC
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10 mM * 1 mL/2 mg/5 mg/10 mg/25 mg/50 mg
| 规格: | 10 mM * 1 mL | 产品价格: | ¥1129.0 |
|---|---|---|---|
| 规格: | 2 mg | 产品价格: | ¥600.0 |
| 规格: | 5 mg | 产品价格: | ¥1000.0 |
| 规格: | 10 mg | 产品价格: | ¥1700.0 |
| 规格: | 25 mg | 产品价格: | ¥2800.0 |
| 规格: | 50 mg | 产品价格: | ¥4800.0 |
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UNC2025 hydrochloride
CAS No. : 2070015-17-5
MCE 国际站:UNC2025 hydrochloride
产品活性:UNC2025 hydrochloride 是一种强效、ATP 竞争性,高口服活性的 Mer/Flt3 抑制剂,IC50 值分别为 0.74 nM 和 0.8 nM。UNC2025 hydrochloride 对 MERTK 的选择性是 Axl 的 45 倍(IC50=122nM; Ki=13.3 nM)。UNC2025 hydrochloride 具有良好的 PK 特性,可用于急性白血病的研究。
研究领域:Protein Tyrosine Kinase/RTK
作用靶点:FLT3
In Vitro: UNC2025 is against FLT3, MER, AXL, TRKA, TRKC, QIK, TYRO3, SLK, NuaK1, KIT and Met with IC50 values of 0.35 nM, 0.46 nM, 1.65 nM, 1.67 nM, 4.38 nM, 5.75 nM, 5.83 nM, 6.14 nM, 7.97 nM , 8.18 nM and 364 nM, respectively.
UNC2025 (0-60 nM; 1 hour) mediates potent inhibition of Mer phosphorylation with an IC50 of 2.7 nM in 697 B-ALL cells.
UNC2025 (0-60 nM; 1 hour) results in decreased phosphorylation of Flt3 with an IC50 of 14 nM in Flt3-ITD positive Molm-14 acute myeloid leukemia cells.
UNC2025 (3 nM-3 μM; 1 hour) decreases p-MEK, p-AXL, p-TYRO3 expression as a concentration manner in 32D Cells.
UNC2025 (14 nM–10 μM; 48 hours) inhibits MERTK signaling and colony-forming potential in a MERTK-expressing patient sample with a 20-fold difference in sensitivity of MERTK-expressing leukemia blasts relative to normal cord or marrow blood mononuclear cells.
UNC2025 (25-300 nM; 1 hour) mediates potent and dose-dependent decreases in MERTK phosphorylation/activation in both cell lines and inhibition of MERTK correlated with decreased phosphorylation of previously reported MERTK-dependent signaling components STAT6, AKT, and ERK1/2.
In Vivo: UNC2025 (intravenous injection or oral adminstration; 3 mg/kg) exhibits an excellent PK properties: low clearance (9.2 mL/min kg), longer half-life (3.8 h), and high oral exposure (100%), it shows Tmax, Cmax, and AUClast 0.50 hour, 1.6 μM, and 9.2 h μM, respectively.
UNC2025 (orally adminstration; 50 or 75 mg/kg; 34 and 70 days) mediates a statistically significant dose-dependent reduction in tumor burden relative to vehicle. mediates dose-dependent increases in median survival from 26 days after initiation of treatment in vehicle-treated mice, to 34 and 70 days in mice treated with 50 or 75 mg/kg UNC2025, respectively.
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文献和实验knee joint. Sci Transl Med, 2025. 17(801): p. eadu9804. [4].Yang, Y.S., et al., Suppression of heterotopic ossification in fibrodysplasia ossificans progressiva using AAV gene delivery. Nat Commun, 2022. 13(1): p. 6175.
Crystallization of Kinesin Family Motor Proteins
)(Gulick et al.,1998; Yun et al.,2001)and three KAR3 mutants (Yun et al.,2001),and KCBP (Vinogradova et al.,2004); the Kinesin-3 (formerly Unc104/KIF1)motor,KIF1A bound to different nucleotides (KIF1A-ADP,KIF1A-AMPPCP,KIF1A-ADP-Vi,KIF1A-AlFx)(Kikkawa et al
"cosuppression", since the expression of both the introduced gene and the homologous endogenous gene was suppressed (1-5).First thought to be a quirk of petunias, cosuppression has since been found to occur in many species of plants. It has also been observed
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