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AMG337

(CAS No:1173699-31-4)

AMG 337 is an oral, small molecule, ATP-competitive, highly selective inhibitor of the MET receptor.

CAS No:1173699-31-4

Molecular Weight(MW):463.46

Purity:99.00%

Specification:500MG;1G;5G;10G;50G;100G

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QC Documents

COA	MSDS	HPLC	NMR

ChemicalInfomation

CAS No:	1173699-31-4
Molecular formula(MF)	C₂₃H₂₂FN₇O₃
Molecular Weight(MW):	463.46
Alias

Solubility

In vitro	DMSO	95 mg/mL (204.97 mM)
	Ethanol	95 mg/mL (204.97 mM)
	Water	<1 mg/mL
In vivo

Biological Activity

Description

AMG 337 is an oral, small molecule, ATP-competitive, highly selective inhibitor of the MET receptor.

Targets

MET receptor ^[1]

1 nM

In vitro

AMG 337 potently inhibits the enzymatic activity of WT MET and a subset of MET mutants found in papillary renal cell carcinoma. The inability of AMG 337 to inhibit the Y1230 and D1228 mutants is likely the result of a disruption of the inactive confirmation of the activation loop in the MET kinase domain. AMG 337 also inhibits cell based HGF-induced MET phosphorylation in PC3 cells with IC50 of 5nM. AMG 337 inhibits proliferation in MET-dependent cancer cell lines. AMG 337 inhibits signaling through the PI3K and MAPK pathways in MET-amplified gastric cancer cell lines resulting in profound effects on cell proliferation and survival^[1].

In vivo

AMG 337 exhibits impressive potency with >90% inhibition of Gab-1 phosphorylation at a dose of 0.75 mg/kg (32 nmol/L free-drug concentration). AMG 337 is well tolerated at continuously administered doses that corresponded with complete MET inhibition for 24 hours, suggesting that AMG 337 has the preclinical attributes required to test the role of MET in human cancer^[1].