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Avapritinib
本产品不向个人销售,仅用作科学研究,不用于任何人体实验及非科研性质的动物实验。
Avapritinib图片
CAS NO:1703793-34-3
规格:≥98%
包装与价格:
包装价格(元)
5mg电议
10mg电议
25mg电议
50mg电议
100mg电议
250mg电议
500mg电议

产品介绍
Avapritinib (formerly known as BLU-285; trade name Ayvakit) is an oral, potent and selective small molecule inhibitor of PDGFRα D842V and KIT Exon 17 mutants (IC50=0.5 nM) with anticancer activity. It has been approved in 2020 for treating metastatic gastrointestinal stromal tumors (GIST). Avapritinib was being developed as a highly targeted therapy to treat SM (systemic mastocytosis), which is a disorder of the mast cells in which a KIT Exon 17 mutation is the primary driver of disease. In phase I trial for the treatment of advanced systemic mastocytosis, patients experienced rapid and durable disease control. The overall response rate was 72%, and 56% of patients experienced a complete or partial response. No patients discontinued treatment due to adverse events, most of which were mild to moderate in nature. In addition, BLU-285 may be a potential therapeutic option for KIT exon 17-mutated CBF-AMLs and t(8;21) AMLs in particular.
理化性质和储存条件
Molecular Weight (MW) 498.56
Formula C26H27FN10
CAS No. 1703793-34-3
Storage-20℃ for 3 years in powder form
-80℃ for 2 years in solvent
Solubility (In vitro)DMSO: ≥ 83.33 mg/mL
Water: <1 mg/mL
Ethanol: NA
SMILES CodeCN1N=CC(C2=CN3C(C(N4CCN(C5=NC=C([C@@](C)(N)C6=CC=C(F)C=C6)C=N5)CC4)=NC=N3)=C2)=C1
SynonymsAyvakit; BLU-285; BLU285; BLU 285
实验参考方法
In Vitro

In vitro activity: Avapritinib (formerly known as BlU-285) is a potent and selective small molecule inhibitor of PDGFRα D842V and KIT Exon 17 mutants with IC50 of 0.5 nM. It is being developed as a highly targeted therapy to treat SM (systemic mastocytosis), which is a disorder of the mast cells in which a KIT Exon 17 mutation is the primary driver of disease. In phase I trial for the treatment of advanced systemic mastocytosis, patients experienced rapid and durable disease control. The overall response rate was 72%, and 56% of patients experienced a complete or partial response. No patients discontinued treatment due to adverse events, most of which were mild to moderate in nature. In addition, BLU-285 may be a potential therapeutic option for KIT exon 17-mutated CBF-AMLs and t(8;21) AMLs in particular.


Kinase Assay: Avapritinib (BLU-285) has demonstrated biochemical in vitro activity on the KIT exon 17 mutant enzyme, KIT D816V (IC50=0.27 nM).


Cell Assay: Cellular activity of Avapritinib on KIT D816 mutants is measured by autophosphorylation in the human mast cell leukemia cell line HMC1.2, and the P815 mouse mastocytoma cell line with IC50=4 and 22 nM, respectively. In Kasumi-1 cells, a t(8;21)-positive AML cell line with a KIT exon 17 N822K mutation, Avapritinib potently inhibits KIT N822K mutant autophosphorylation (IC50=40 nM), downstream signaling, as well as cellular proliferation (IC50=75 nM).

In Vivo

(1) NMRI nu/nu mice (n = 93) were transplanted with human GIST xenografts with KIT exon 11+17 (UZLX-GIST9 KIT 11+17 ), exon 11 (UZLX-GIST3 KIT 11 ), or exon 9 (UZLX-GIST2B KIT9 ) mutations, respectively. We compared avapritinib (10 and 30 mg/kg/once daily) versus vehicle, imatinib (50 mg/kg/bid) or regorafenib (30 mg/kg/once daily; UZLX-GIST9 KIT11+17 ); avapritinib (10, 30, 100 mg/kg/once daily) versus vehicle or imatinib [UZLX-GIST3 KIT11 ]; and avapritinib (10, 30, 60 mg/kg/once daily) versus vehicle, imatinib (50, 100 mg/kg/twice daily), or sunitinib (40 mg/kg/once daily; UZLX-GIST2B KIT9 ). [1]

(2) Avapritinib (BLU-285) is well tolerated and has demonstrated dose dependent antitumor efficacy. Complete tumor growth inhibition and ≥75% KIT kinase inhibition is observed with 10 mg/kg once daily, oral dosing of Avapritinib in the aggressive KIT exon 17 mutant driven P815 mastocytoma model grown as a solid tumor allograft as well as in a disseminated model of disease. Disease burden, measured by whole body luciferase imaging (photons/second/mm2), increases 86-fold in the vehicle control animals over the 24 day dosing period with widespread disease detectable in both femurs, the pelvis and circulating in peripheral blood. Disease in the Cytarabine-treated animals advanced more slowly with a 15-fold increase in luciferase values over the course of the experiment. Strikingly, Avapritinib at both doses (10 or 30 mg/kg orally, once daily) results in a marked reduction of disease burden throughout the study as compared to both vehicle controls and animals receiving Cytarabine. Avapritinib at either 10 or 30 mg/kg results in tumor regression in all animals with disease abrogation indistinguishable from background signal measurements in several animals by the end of study. Avapritinib is also well tolerated in this in vivo model and has no adverse effects on body weight at either dose. [2]

Animal modelNMRI (nu/nu) mice [1]; Kasumi-1 luc+ AML NOG SCID mouse femoral injection model [2]
Formulation & DosageDissolved in 0.5% carbomethyl cellulose with 1% Tween 80.; 10 or 30 mg/kg; P.O.
References

[1] Clin Cancer Res. 2019 Jan 15;25(2):609-618.

[2] /23/568?sso-checked=true