Welcome to SuperLan Chemical Co.,Ltd.
Home > Products > Protein Tyrosine Kinase > c-Met > Crizotinib

Crizotinib

(CAS No:877399-52-5)
Crizotinib (PF-02341066) is a potent inhibitor of c-Met and ALK with IC50 of 11 nM and 24 nM in cell-based assays, respectively.
CAS No:877399-52-5
Molecular Weight(MW):450.34
Purity:99.00%
Specification:500MG;1G;5G;10G;50G;100G
Price and large packaging, please e-mail consultation:info@SuperLan-chem.com
QC Documents
 COA  MSDS  HPLC  NMR
ChemicalInfomation
CAS No: 877399-52-5
Molecular formula(MF) C21H22Cl2FN5O
Molecular Weight(MW): 450.34
Alias
Solubility
In vitro DMSO 9 mg/mL (19.98 mM)
Water <1 mg/mL
Ethanol <1 mg/mL
In vivo 5% DMSO+30% PEG 300+dd H2O 5mg/mL
Biological Activity
Description Crizotinib (PF-02341066) is a potent inhibitor of c-Met and ALK with IC50 of 11 nM and 24 nM in cell-based assays, respectively.
Targets
c-Met [1]
(A549, MDA-MB-231, GTL-16, HT29, 786-O, Colo-205, A498 cells)		 ALK [1]
(Karpas299 cells)
11 nM 24 nM
In vitro

PF-2341066 displays similar potency against c-Met phosphorylation in mIMCD3 mouse or MDCK canine epithelial cells with IC50 of 5 nM and 20 nM, respectivly. PF-2341066 shows improved or similar activity against NIH3T3 cells engineered to express c-Met ATP-binding site mutants V1092I or H1094R or the P-loop mutant M1250T with IC50 of 19 nM, 2 nM and 15 nM, respectively, compared with NIH3T3 cells expressing wild-type receptor with IC50 of 13 nM. In contrast, a marked shift in potency of PF-2341066 is observed against cells engineered to express c-Met activation loop mutants Y1230C and Y1235D with IC50 of 127 nM and 92 nM, respectively, compared with wild-type receptor. PF-2341066 also potently prevents the phosphorylation of c-Met in NCI-H69 and HOP92 cells, with IC50 of 13 nM and 16 nM, respectively, which express the endogenous c-Met variants R988C and T1010I, respectively. PF-2341066 is >1,000-fold selective for the VEGFR2 and PDGFRβ RTKs, >250-fold selective for IRK and Lck, and ∼40- to 60-fold selective for Tie2, TrkA, and TrkB, all compared with c-Met. PF-2341066 is 20- to 30-fold selective for RON and Axl RTKs. In contrast, PF-2341066 shows a near-equivalent IC50 of 24 nM against the nucleophosmin (NPM)-anaplastic lymphoma kinase (ALK) oncogenic fusion variant of the ALK RTK expressed by the KARPAS299 human anaplastic large cell lymphoma (ALCL) cell line. PF-2341066 inhibits c-Met–dependent neoplastic phenotypes of cancer cells and angiogenic phenotypes of endothelial cells. PF-2341066 suppresses human GTL-16 gastric carcinoma cell growth with IC50 of 9.7 nM. PF-2341066 induces apoptosis in GTL-16 cells with IC50 of 8.4 nM. PF-2341066 inhibits HGF-stimulated human NCI-H441 lung carcinoma cell migration and invasion with IC50 of 11 nM and 6.1 nM, respectively. PF-2341066 inhibits MDCK cell scattering with IC50 of 16 nM. PF-2341066 prevents HGF-stimulated c-Met phosphorylation, cell survival, and Matrigel invasion with IC50 of 11 nM, 14 nM and 35 nM, respectively. In addition, PF-2341066 prevents serum-stimulated HMVEC branching tubulogenesis (formation of vascular tubes) in fibrin gels. [1] PF-2341066 also potently inhibits NPM-ALK phosphorylation in Karpas299 or SU-DHL-1 ALCL cells with an IC50 of 24 nM. PF-2341066 potently prevents cell proliferation, which is associated with G(1)-S-phase cell cycle arrest and induction of apoptosis in ALK-positive ALCL cells with IC50 of 30 nM, but not ALK-negative lymphoma cells. [2] Besides, PF-2341066 prevents osteosarcoma behavior associated with primary tumor growth (i.e., proliferation and survival) as well as metastasis (eg, invasion and clonogenicity). [3]
Cell Data
Cell Lines Assay Type Concentration Incubation Time Formulation Activity Description PMID
BAF3 Cytotoxic Assay 48 h DMSO Cytotoxicity against mouse BAF3 cells expressing ALK F1174L mutant coexpressing EML4 with IC50 of 0.62 μM 21572589
BAF3 Cytotoxic Assay 48 h DMSO Cytotoxicity against mouse BAF3 cells expressing ALK L1196M mutant coexpressing EML4 with IC50 of 2.2 μM 21572589
BAF3 Cytotoxic Assay 48 h DMSO Cytotoxicity against mouse BAF3 cells expressing EML4-ALK with IC50 of 0.28 μM 21572589
Kelly Cytotoxic Assay DMSO Cytotoxicity against human Kelly cells expressing ALK F1174L mutant with IC50 of 0.42 μM 21572589
SH-SY5Y Cytotoxic Assay DMSO Cytotoxicity against human SH-SY5Y cells expressing ALK F1174L mutant with IC50 of 0.53 μM 21572589
SMS-KCN Cytotoxic Assay DMSO Cytotoxicity against human SMS-KCN cells expressing ALK R1275Q mutant with IC50 of 0.91 μM 21572589
BAF3 Cytotoxic Assay 48 h DMSO Cytotoxicity against mouse BAF3 cells expressing Tel-ALK with IC50 of 0.19 μM 21572589
3T3 Function Assay 1 h DMSO Inhibition of RON assessed as growth factor-induced autophosphorylation with IC50 of 0.08 μM 21812414
3T3-E Function Assay 1 h DMSO Inhibition of TIE2 assessed growth factor-induced autophosphorylation with IC50 of 0.448 μM 21812414
A549 Kinase Assay 1 h DMSO Inhibition of human recombinant c-MET kinase expressed assessed as inhibition of HGF-induced autophosphorylation with IC50 of 0.008 μM 21812414
BAF3-BCL Function Assay 1 h DMSO Inhibition of ABL assessed as growth factor-induced autophosphorylation with IC50 of 1.159 μM 21812414
HEK293 Function Assay 1 h DMSO Inhibition of AXL assessed as growth factor-induced autophosphorylation with IC50 of 0.294 μM 21812414
HEK293 Function Assay 1 h DMSO Inhibition of IR assessed as growth factor-induced autophosphorylation with IC50 of 2.887 μM 21812414
Jurkat Function Assay 1 h DMSO Inhibition of LCK assessed as growth factor-induced autophosphorylation with IC50 of 2.741 μM 21812414
KARPAS299 Kinase Assay 1 h DMSO Inhibition of ALK assessed as growth factor-induced autophosphorylation with IC50 of 0.02 μM 21812414
PAE Function Assay 1 h DMSO Inhibition of TRKB assessed as growth factor-induced autophosphorylation with IC50 of 0.399 μM 21812414
BAF3 Function Assay 2-3 d DMSO Inhibition of TEL-fused insulin receptor expressed with IC50 of 1.643 μM 23742252
KARPAS299 Cytotoxic Assay 2-3 d DMSO IC50=0.0642 μM 23742252
EBC1 Growth Inhibition Assay 72 h DMSO IC50=0.023 μM 23993328
HCT116 Growth Inhibition Assay 72 h DMSO IC50=14.82 μM 23993328
MCF7 Growth Inhibition Assay 72 h DMSO IC50=9.58 μM 23993328
MDA-MB-231 Growth Inhibition Assay 72 h DMSO IC50=10.8 μM 23993328
MKN45 Growth Inhibition Assay 72 h DMSO IC50=0.013 μM 23993328
NCI-H441 Growth Inhibition Assay 72 h DMSO IC50=17.25 μM 23993328
NCI-H661 Growth Inhibition Assay 72 h DMSO IC50=11.47 μM 23993328
SK-MEL-28 Growth Inhibition Assay 72 h DMSO IC50=10.97 μM 23993328
SKOV3 Growth Inhibition Assay 72 h DMSO IC50=12.85 μM 23993328
SNU5 Growth Inhibition Assay 72 h DMSO IC50=0.016 μM 23993328
NCI-H2228 Growth Inhibition Assay 72 h DMSO Inhibition of ALK-fusion driven cell proliferation with IC50 of 0.118 μM 24432909
NCI-H3122 Growth Inhibition Assay 72 h DMSO Inhibition of ALK-fusion driven cell proliferation with IC50 of 0.108 μM 24432909
NCI-H3122 Growth Inhibition Assay 72 h DMSO Inhibition of ALK-fusion driven cell proliferation in human NCI-H3122 cells harboring ALK G1269A mutant with IC50 of 0.623 μM 24432909
NCI-H3122 Growth Inhibition Assay 72 h DMSO Inhibition of ALK-fusion driven cell proliferation in human NCI-H3122 cells harboring ALK L1196M mutant with IC50 of 0.838 μM 24432909
NIH-3T3 Kinase Assay 1 h DMSO Inhibition of human wild type EML4-fused ALK expressed assessed as phosphorylated ALK level with IC50 of 0.08 μM 24432909
NIH-3T3 Kinase Assay 1 h DMSO Inhibition of human EML4-fused ALK G1269A mutant expressed assessed as phospho-ALK level with IC50 of 0.605 μM 24432909
NIH-3T3 Kinase Assay 1 h DMSO Inhibition of human EML4-fused ALK S1206Y mutant expressed assessed as phospho-ALK level with IC50 of 0.626 μM 24432909
NIH-3T3 Kinase Assay 1 h DMSO Inhibition of human EML4-fused ALK L1196M mutant expressed assessed as phospho-ALK level with IC50 of 0.843 μM 24432909
NIH-3T3 Kinase Assay 1 h DMSO Inhibition of human EML4-fused ALK L1152R mutant expressed assessed as phospho-ALK level with IC50 of 1.026 μM 24432909
BAF3 Function Assay 72 h DMSO Inhibition of NPM/ALK transfected assessed as cell growth inhibition with IC50 of 0.051 μM 24468632
BAF3 Cytotoxic Assay 72 h DMSO IC50=0.98 μM 24468632
NIH-3T3 Kinase Assay 1 h Inhibition of human EML4-fused ALK F1174L mutant expressed assessed as phospho-ALK level with IC50 of 0.165 μM 24819116
NIH-3T3 Kinase Assay 1 h Inhibition of human EML4-fused ALK C1156Y mutant expressed assessed as phospho-ALK level with IC50 of 0.478 μM 24819116
NIH-3T3 Kinase Assay 1 h Inhibition of human EML4-fused ALK G1202R mutant expressed assessed as phospho-ALK level with IC50 of 1.148 μM 24819116
NIH-3T3 Kinase Assay 1 h Inhibition of human EML4-fused ALK 1151Tins mutant expressed assessed as phospho-ALK level with IC50 of 3.039 μM 24819116
KARPAS299 Kinase Assay 90 min DMSO Inhibition of NPM-fused ALK phosphorylation expressed with IC50 of 0.11 μM 24900750
MKN 45 Kinase Assay 1 h DMSO Inhibition of c-Met phosphorylation with IC50 of 0.02 μM 24900750
A549 Cytotoxic Assay 48 h DMSO IC50 of 4.084 μM 24900830
NCI-H1975 Cytotoxic Assay 48 h DMSO IC50 of 7.551 μM 24900830
NCI-H1993 Cytotoxic Assay 48 h DMSO IC50 of 0.061 μM 24900830
NCI-H1993 Apotosis Assay 1 μM 24 h DMSO does not induce apoptosis 24900830
NIH-3T3 Cytotoxic Assay 48 h DMSO IC50 of 0.364 μM 24900830
EBC1 Growth Inhibition Assay 72 h DMSO IC50 of 0.0069 μM 24900831
KARPAS299 Growth Inhibition Assay 72 h DMSO IC50 of 0.2 μM 24900831
NB1 Growth Inhibition Assay IC50=91.98 nM SANGER
NCI-SNU-5 Growth Inhibition Assay IC50=105.75 nM SANGER
SR Growth Inhibition Assay IC50=126.31 nM SANGER
SF539 Growth Inhibition Assay IC50=204.24 nM SANGER
SU-DHL-1 Growth Inhibition Assay IC50=336.82 nM SANGER
SCC-3 Growth Inhibition Assay IC50=356.76 nM SANGER
DEL Growth Inhibition Assay IC50=369.9 nM SANGER
CTV-1 Growth Inhibition Assay IC50=596.48 nM SANGER
EM-2 Growth Inhibition Assay IC50=601.34 nM SANGER
MHH-CALL-2 Growth Inhibition Assay IC50=682.57 nM SANGER
KM12 Growth Inhibition Assay IC50=706.9 nM SANGER
KINGS-1 Growth Inhibition Assay IC50=749.75 nM SANGER
MEG-01 Growth Inhibition Assay IC50=857.66 nM SANGER
BV-173 Growth Inhibition Assay IC50=1.05997 μM SANGER
LAMA-84 Growth Inhibition Assay IC50=1.38282 μM SANGER
KARPAS-299 Growth Inhibition Assay IC50=1.40861 μM SANGER
K-562 Growth Inhibition Assay IC50=1.72269 μM SANGER
SK-LMS-1 Growth Inhibition Assay IC50=1.76867 μM SANGER
MOLT-16 Growth Inhibition Assay IC50=1.95575 μM SANGER
CMK Growth Inhibition Assay IC50=1.96159 μM SANGER
ST486 Growth Inhibition Assay IC50=2.43073 μM SANGER
CI-1 Growth Inhibition Assay IC50=2.49659 μM SANGER
KP-N-RT-BM-1 Growth Inhibition Assay IC50=2.70122 μM SANGER
ALL-PO Growth Inhibition Assay IC50=3.18207 μM SANGER
KS-1 Growth Inhibition Assay IC50=3.21225 μM SANGER
Becker Growth Inhibition Assay IC50=4.2393 μM SANGER
GDM-1 Growth Inhibition Assay IC50=4.24617 μM SANGER
BC-1 Growth Inhibition Assay IC50=4.49277 μM SANGER
NB14 Growth Inhibition Assay IC50=4.83524 μM SANGER
NOS-1 Growth Inhibition Assay IC50=5.33874 μM SANGER
MZ1-PC Growth Inhibition Assay IC50=5.82151 μM SANGER
A498 Growth Inhibition Assay IC50=6.08473 μM SANGER
EW-16 Growth Inhibition Assay IC50=6.37773 μM SANGER
NALM-6 Growth Inhibition Assay IC50=6.68387 μM SANGER
EB-3 Growth Inhibition Assay IC50=7.07233 μM SANGER
697 Growth Inhibition Assay IC50=9.24329 μM SANGER
Ramos-2G6-4C10 Growth Inhibition Assay IC50=9.59842 μM SANGER
KNS-81-FD Growth Inhibition Assay IC50=9.69653 μM SANGER
HUTU-80 Growth Inhibition Assay IC50=9.74642 μM SANGER
LS-411N Growth Inhibition Assay IC50=10.0567 μM SANGER
RPMI-8402 Growth Inhibition Assay IC50=10.116 μM SANGER
KU812 Growth Inhibition Assay IC50=10.2991 μM SANGER
EW-1 Growth Inhibition Assay IC50=10.4425 μM SANGER
HC-1 Growth Inhibition Assay IC50=10.4844 μM SANGER
NB69 Growth Inhibition Assay IC50=10.5043 μM SANGER
MFH-ino Growth Inhibition Assay IC50=10.8303 μM SANGER
CCRF-CEM Growth Inhibition Assay IC50=11.597 μM SANGER
SK-N-DZ Growth Inhibition Assay IC50=12.0436 μM SANGER
NCI-H720 Growth Inhibition Assay IC50=12.1705 μM SANGER
HCC1187 Growth Inhibition Assay IC50=12.2041 μM SANGER
IST-SL2 Growth Inhibition Assay IC50=12.4872 μM SANGER
KE-37 Growth Inhibition Assay IC50=12.7966 μM SANGER
HCC1599 Growth Inhibition Assay IC50=12.9069 μM SANGER
A4-Fuk Growth Inhibition Assay IC50=12.9586 μM SANGER
NKM-1 Growth Inhibition Assay IC50=13.2925 μM SANGER
BE-13 Growth Inhibition Assay IC50=13.7989 μM SANGER
MV-4-11 Growth Inhibition Assay IC50=14.0324 μM SANGER
OPM-2 Growth Inhibition Assay IC50=14.4085 μM SANGER
KARPAS-422 Growth Inhibition Assay IC50=14.5126 μM SANGER
RPMI-8226 Growth Inhibition Assay IC50=14.8915 μM SANGER
KARPAS-45 Growth Inhibition Assay IC50=15.7716 μM SANGER
SK-PN-DW Growth Inhibition Assay IC50=15.8631 μM SANGER
LC-2 Growth Inhibition Assay IC50=16.1506 μM SANGER
NCI-H1648 Growth Inhibition Assay IC50=16.254 μM SANGER
RL95-2 Growth Inhibition Assay IC50=16.3978 μM SANGER
KNS-42 Growth Inhibition Assay IC50=16.7274 μM SANGER
RPMI-6666 Growth Inhibition Assay IC50=16.9211 μM SANGER
SIG-M5 Growth Inhibition Assay IC50=17.1903 μM SANGER
VA-ES-BJ Growth Inhibition Assay IC50=17.7451 μM SANGER
MONO-MAC-6 Growth Inhibition Assay IC50=17.9312 μM SANGER
LAN-6 Growth Inhibition Assay IC50=18.7557 μM SANGER
A388 Growth Inhibition Assay IC50=19.3059 μM SANGER
SK-NEP-1 Growth Inhibition Assay IC50=20.2132 μM SANGER
TE-10 Growth Inhibition Assay IC50=20.5221 μM SANGER
HL-60 Growth Inhibition Assay IC50=20.9099 μM SANGER
MC116 Growth Inhibition Assay IC50=21.7221 μM SANGER
SW962 Growth Inhibition Assay IC50=21.7915 μM SANGER
NOMO-1 Growth Inhibition Assay IC50=22.6564 μM SANGER
CTB-1 Growth Inhibition Assay IC50=22.8671 μM SANGER
MRK-nu-1 Growth Inhibition Assay IC50=22.9074 μM SANGER
GR-ST Growth Inhibition Assay IC50=23.76 μM SANGER
HH Growth Inhibition Assay IC50=24.003 μM SANGER
NCI-H1963 Growth Inhibition Assay IC50=24.0782 μM SANGER
QIMR-WIL Growth Inhibition Assay IC50=24.8772 μM SANGER
CGTH-W-1 Growth Inhibition Assay IC50=25.0723 μM SANGER
LP-1 Growth Inhibition Assay IC50=25.6551 μM SANGER
NCI-H748 Growth Inhibition Assay IC50=26.5137 μM SANGER
PF-382 Growth Inhibition Assay IC50=27.2223 μM SANGER
ATN-1 Growth Inhibition Assay IC50=27.3732 μM SANGER
L-540 Growth Inhibition Assay IC50=27.6459 μM SANGER
LXF-289 Growth Inhibition Assay IC50=27.7519 μM SANGER
LS-513 Growth Inhibition Assay IC50=28.1807 μM SANGER
NCI-H1581 Growth Inhibition Assay IC50=30.3976 μM SANGER
ES6 Growth Inhibition Assay IC50=30.6899 μM SANGER
SW982 Growth Inhibition Assay IC50=30.8566 μM SANGER
DOHH-2 Growth Inhibition Assay IC50=31.5893 μM SANGER
DB Growth Inhibition Assay IC50=33.9431 μM SANGER
MPP-89 Growth Inhibition Assay IC50=34.1756 μM SANGER
LB831-BLC Growth Inhibition Assay IC50=34.5184 μM SANGER
NB5 Growth Inhibition Assay IC50=34.8535 μM SANGER
GB-1 Growth Inhibition Assay IC50=35.0469 μM SANGER
TE-15 Growth Inhibition Assay IC50=35.2238 μM SANGER
LC4-1 Growth Inhibition Assay IC50=35.3847 μM SANGER
NCI-H747 Growth Inhibition Assay IC50=36.1369 μM SANGER
NTERA-S-cl-D1 Growth Inhibition Assay IC50=38.7347 μM SANGER
SK-MM-2 Growth Inhibition Assay IC50=40.1146 μM SANGER
TGW Growth Inhibition Assay IC50=41.0563 μM SANGER
ONS-76 Growth Inhibition Assay IC50=42.4883 μM SANGER
CPC-N Growth Inhibition Assay IC50=42.9971 μM SANGER
ES4 Growth Inhibition Assay IC50=44.4153 μM SANGER
Daudi Growth Inhibition Assay IC50=45.0827 μM SANGER
MOLT-4 Growth Inhibition Assay IC50=45.0853 μM SANGER
HT-144 Growth Inhibition Assay IC50=46.726 μM SANGER
SW872 Growth Inhibition Assay IC50=48.1933 μM SANGER
D-283MED Growth Inhibition Assay IC50=48.3542 μM SANGER
NCI-H2126 Growth Inhibition Assay IC50=48.8476 μM SANGER
NCI-SNU-16 Growth Inhibition Assay IC50=49.2143 μM SANGER
CESS Growth Inhibition Assay IC50=49.5088 μM SANGER
A101D Growth Inhibition Assay IC50=49.9736 μM SANGER

... Click to View More Cell Line Experimental Data
In vivo In the GTL-16 model, PF-2341066 reveals the ability to cause marked regression of large established tumors (>600 mm3) in both the 50 mg/kg/day and 75 mg/kg/day treatment cohorts, with a 60% decrease in mean tumor volume over the 43-day administration schedule. In an another study, PF-2341066 displays the ability to completely inhibits GTL-16 tumor growth for >3 months, with only 1 of 12 mice exhibiting a significant increase in tumor growth over the 3-month treatment schedule at 50 mg/kg/day. In the NCI-H441 NSCLC model, a 43% decrease in mean tumor volume is observed at 50 mg/kg/day during the 38-day PF-2341066 administration cycle. In the Caki-1 RCC model, a 53% decrease in mean tumor volume is observed to be associated with decreased volume of each tumor by at least 30% at 50 mg/kg/day during the 33-day PF-2341066 administration cycle. PF-2341066 also reveals near-complete prevention of the growth of established tumors at 50 mg/kg/day in the U87MG glioblastoma or PC-3 prostate carcinoma xenograft models, with 97% or 84% inhibition on the final study day, respectively. In contrast, PF-2341066 p.o. given at 50 mg/kg/day does not significantly inhibit tumor growth in the MDA-MB-231 breast carcinoma model, or the DLD-1 colon carcinoma model. A significant dose-dependent reduction of CD31–positive endothelial cells is observed at 12.5 mg/kg/day, 25 mg/kg/day, and 50 mg/kg/day in GTL-16 tumors, indicating that inhibition of MVD shows a dose-dependent correlation to antitumor efficacy. PF-2341066 displays a significant dose-dependent reduction of human VEGFA and IL-8 plasma levels in both the GTL-16 and U87MG models. Marked inhibition of phosphorylated c-Met, Akt, Erk, PLCλ1, and STAT5 levels is observed in GTL-16 tumors following p.o. administration of PF-2341066.[1] P.o. administration of PF-2341066 to severe combined immunodeficient-Beige mice bearing Karpas299 ALCL tumor xenografts leads to dose-dependent antitumor efficacy with complete regression of all tumors at the 100 mg/kg/d dose within 15 days of initial compound administration. In addition, inhibition of key NPM-ALK signaling mediators, including phospholipase C-gamma, signal transducers and activators of transcription 3, extracellular signal-regulated kinases, and Akt by PF-2341066 are observed at concentrations or dose levels, which correlated with inhibition of NPM-ALK phosphorylation and function.[2] PF-2341066 prevents osteosarcoma behavior associated with primary tumor growth (eg, proliferation and survival) as well as metastasis (eg, invasion and clonogenicity). In nude mice treated with PF-2341066 via oral gavage, the growth and associated osteolysis and extracortical bone matrix formation of osteosarcoma xenografts are prevented by PF-2341066.[3] Treatment of c-MET-amplified GTL-16 xenografts with 50 mg/kg PF-2341066 elicits tumor regression that is associated with a slow reduction in 18F-FDG uptake and decreases expression of the glucose transporter 1, GLUT-1.[4]
Copyright 2016 Shanghai Superlan Chemcial Technology Centre
Technical Support:chem960