Details
| Stereochemistry | ABSOLUTE |
| Molecular Formula | C21H22Cl2FN5O.C2H4O2 |
| Molecular Weight | 510.389 |
| Optical Activity | UNSPECIFIED |
| Defined Stereocenters | 1 / 1 |
| E/Z Centers | 0 |
| Charge | 0 |
SHOW SMILES / InChI
SMILES
CC(O)=O.C[C@@H](OC1=CC(=CN=C1N)C2=CN(N=C2)C3CCNCC3)C4=C(Cl)C=CC(F)=C4Cl
InChI
InChIKey=LFCVDLCLKZRGFW-UTONKHPSSA-N
InChI=1S/C21H22Cl2FN5O.C2H4O2/c1-12(19-16(22)2-3-17(24)20(19)23)30-18-8-13(9-27-21(18)25)14-10-28-29(11-14)15-4-6-26-7-5-15;1-2(3)4/h2-3,8-12,15,26H,4-7H2,1H3,(H2,25,27);1H3,(H,3,4)/t12-;/m1./s1
DescriptionSources: http://www.fda.gov/Drugs/InformationOnDrugs/ApprovedDrugs/ucm376058.htm?source=govdelivery&utm_medium=email&utm_source=govdeliveryhttps://www.ncbi.nlm.nih.gov/pubmed/24695225Curator's Comment: Description was created based on several sources, including http://www.accessdata.fda.gov/drugsatfda_docs/label/2013/202570s006lbl.pdf; https://www.mskcc.org/cancer-care/clinical-trials/14-063
Sources: http://www.fda.gov/Drugs/InformationOnDrugs/ApprovedDrugs/ucm376058.htm?source=govdelivery&utm_medium=email&utm_source=govdeliveryhttps://www.ncbi.nlm.nih.gov/pubmed/24695225
Curator's Comment: Description was created based on several sources, including http://www.accessdata.fda.gov/drugsatfda_docs/label/2013/202570s006lbl.pdf; https://www.mskcc.org/cancer-care/clinical-trials/14-063
(S)-crizotinib was discovered as an attractive chemical entity for further pre-clinical evaluation, and small-molecule inhibitors of MTH1 as a promising novel class of anticancer agents.
Originator
Approval Year
Targets
| Primary Target | Pharmacology | Condition | Potency |
|---|---|---|---|
Target ID: CHEMBL4247 |
24.0 nM [IC50] | ||
Target ID: CHEMBL3717 |
11.0 nM [IC50] | ||
Target ID: P36639 Gene ID: 4521.0 Gene Symbol: NUDT1 Target Organism: Homo sapiens (Human) |
72.0 nM [IC50] |
Conditions
| Condition | Modality | Targets | Highest Phase | Product |
|---|---|---|---|---|
| Primary | XALKORI Approved UseIndicated for the treatment of patients with metastatic non-small cell lung cancer (NSCLC) whose tumors are anaplastic lymphoma kinase (ALK)-positive as detected by an FDA-approved test. Launch Date2011 |
|||
| Primary | Unknown Approved UseUnknown |
Cmax
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
475 ng/mL EXPERIMENT https://pubmed.ncbi.nlm.nih.gov/31778074 |
300 mg 2 times / day steady-state, oral dose: 300 mg route of administration: Oral experiment type: STEADY-STATE co-administered: |
CRIZOTINIB plasma | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
|
99.6 ng/mL EXPERIMENT https://www.ncbi.nlm.nih.gov/pubmed/24990113 |
250 mg single, oral dose: 250 mg route of administration: Oral experiment type: SINGLE co-administered: |
CRIZOTINIB plasma | Homo sapiens population: HEALTHY age: ADULT sex: MALE food status: FASTED |
|
328 ng/mL |
250 mg 2 times / day steady-state, oral dose: 250 mg route of administration: Oral experiment type: STEADY-STATE co-administered: |
CRIZOTINIB unknown | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
|
327 ng/mL |
250 mg 2 times / day multiple, oral dose: 250 mg route of administration: Oral experiment type: MULTIPLE co-administered: |
CRIZOTINIB unknown | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
|
87 ng/mL |
250 mg single, oral dose: 250 mg route of administration: Oral experiment type: SINGLE co-administered: |
CRIZOTINIB unknown | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
AUC
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
3240 ng × h/mL EXPERIMENT https://pubmed.ncbi.nlm.nih.gov/31778074 |
300 mg 2 times / day steady-state, oral dose: 300 mg route of administration: Oral experiment type: STEADY-STATE co-administered: |
CRIZOTINIB plasma | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
|
2321 ng × h/mL EXPERIMENT https://www.ncbi.nlm.nih.gov/pubmed/24990113 |
250 mg single, oral dose: 250 mg route of administration: Oral experiment type: SINGLE co-administered: |
CRIZOTINIB plasma | Homo sapiens population: HEALTHY age: ADULT sex: MALE food status: FASTED |
|
3054 ng × h/mL |
250 mg 2 times / day steady-state, oral dose: 250 mg route of administration: Oral experiment type: STEADY-STATE co-administered: |
CRIZOTINIB unknown | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
|
3084 ng × h/mL |
250 mg 2 times / day multiple, oral dose: 250 mg route of administration: Oral experiment type: MULTIPLE co-administered: |
CRIZOTINIB unknown | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
|
1817 ng × h/mL |
250 mg single, oral dose: 250 mg route of administration: Oral experiment type: SINGLE co-administered: |
CRIZOTINIB unknown | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
T1/2
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
29 h EXPERIMENT https://www.ncbi.nlm.nih.gov/pubmed/24990113 |
250 mg single, oral dose: 250 mg route of administration: Oral experiment type: SINGLE co-administered: |
CRIZOTINIB plasma | Homo sapiens population: HEALTHY age: ADULT sex: MALE food status: FASTED |
|
47.1 h |
250 mg single, oral dose: 250 mg route of administration: Oral experiment type: SINGLE co-administered: |
CRIZOTINIB unknown | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
Funbound
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
9.3% |
CRIZOTINIB plasma | Homo sapiens population: UNKNOWN age: UNKNOWN sex: UNKNOWN food status: UNKNOWN |
Doses
| Dose | Population | Adverse events |
|---|---|---|
300 mg 2 times / day steady, oral Dose: 300 mg, 2 times / day Route: oral Route: steady Dose: 300 mg, 2 times / day Sources: |
unhealthy, 49 years n = 6 Health Status: unhealthy Age Group: 49 years Sex: M+F Population Size: 6 Sources: |
Disc. AE: Fatigue... AEs leading to discontinuation/dose reduction: Fatigue (grade 3, 1 patient) Sources: |
250 mg 2 times / day steady, oral Recommended|MTD Dose: 250 mg, 2 times / day Route: oral Route: steady Dose: 250 mg, 2 times / day Sources: |
unhealthy, 51 years (range: 21-79 years) n = 119 Health Status: unhealthy Condition: Adenocarcinoma | Squamous Cell Carcinoma |Non-small Cell Lung Cancer Age Group: 51 years (range: 21-79 years) Sex: M+F Population Size: 119 Sources: |
Disc. AE: Autoimmune thyroiditis... AEs leading to discontinuation/dose reduction: Autoimmune thyroiditis (1 patient) Sources: |
250 mg 2 times / day steady, oral Recommended|MTD Dose: 250 mg, 2 times / day Route: oral Route: steady Dose: 250 mg, 2 times / day Sources: |
unhealthy, 52 years (range: 29-82 years) n = 136 Health Status: unhealthy Condition: Adenocarcinoma | Adenosquamous Carcinoma|Non-small Cell Lung Cancer Age Group: 52 years (range: 29-82 years) Sex: M+F Population Size: 136 Sources: |
Disc. AE: ALT increased, Pneumonitis... AEs leading to discontinuation/dose reduction: ALT increased (2.2%) Sources: Pneumonitis (1.5%) |
AEs
| AE | Significance | Dose | Population |
|---|---|---|---|
| Fatigue | grade 3, 1 patient Disc. AE |
300 mg 2 times / day steady, oral Dose: 300 mg, 2 times / day Route: oral Route: steady Dose: 300 mg, 2 times / day Sources: |
unhealthy, 49 years n = 6 Health Status: unhealthy Age Group: 49 years Sex: M+F Population Size: 6 Sources: |
| Autoimmune thyroiditis | 1 patient Disc. AE |
250 mg 2 times / day steady, oral Recommended|MTD Dose: 250 mg, 2 times / day Route: oral Route: steady Dose: 250 mg, 2 times / day Sources: |
unhealthy, 51 years (range: 21-79 years) n = 119 Health Status: unhealthy Condition: Adenocarcinoma | Squamous Cell Carcinoma |Non-small Cell Lung Cancer Age Group: 51 years (range: 21-79 years) Sex: M+F Population Size: 119 Sources: |
| Pneumonitis | 1.5% Disc. AE |
250 mg 2 times / day steady, oral Recommended|MTD Dose: 250 mg, 2 times / day Route: oral Route: steady Dose: 250 mg, 2 times / day Sources: |
unhealthy, 52 years (range: 29-82 years) n = 136 Health Status: unhealthy Condition: Adenocarcinoma | Adenosquamous Carcinoma|Non-small Cell Lung Cancer Age Group: 52 years (range: 29-82 years) Sex: M+F Population Size: 136 Sources: |
| ALT increased | 2.2% Disc. AE |
250 mg 2 times / day steady, oral Recommended|MTD Dose: 250 mg, 2 times / day Route: oral Route: steady Dose: 250 mg, 2 times / day Sources: |
unhealthy, 52 years (range: 29-82 years) n = 136 Health Status: unhealthy Condition: Adenocarcinoma | Adenosquamous Carcinoma|Non-small Cell Lung Cancer Age Group: 52 years (range: 29-82 years) Sex: M+F Population Size: 136 Sources: |
Overview
| CYP3A4 | CYP2C9 | CYP2D6 | hERG |
|---|---|---|---|
OverviewOther
Drug as perpetrator
| Target | Modality | Activity | Metabolite | Clinical evidence |
|---|---|---|---|---|
| no | ||||
| no | ||||
| weak [IC50 44 uM] | ||||
| weak [IC50 48 uM] | ||||
| weak [Inhibition 30 uM] | ||||
| yes [IC50 0.83 uM] | ||||
| yes [IC50 14.6 uM] | ||||
| yes [IC50 22 uM] | ||||
| yes [IC50 23 uM] | ||||
| yes [IC50 5.79 uM] | ||||
| yes [IC50 7.3 uM] | yes (co-administration study) Comment: crizotinib increased AUC of midazolam by 3.7x |
|||
| yes [IC50 >30 uM] | ||||
| yes [IC50 >30 uM] | ||||
| yes [IC50 >30 uM] | ||||
| yes [IC50 >30 uM] | ||||
| yes | no (co-administration study) Comment: effect is masked by inhibition |
Drug as victim
| Target | Modality | Activity | Metabolite | Clinical evidence |
|---|---|---|---|---|
| major | yes (co-administration study) Comment: ketoconazole increased cmax of crizotinib by 44%, auc by 216% |
|||
| major | yes (co-administration study) Comment: ketoconazole increased cmax of crizotinib by 44%, auc by 216% |
|||
| minor | ||||
| minor | ||||
| no | ||||
| no | ||||
| no | ||||
| yes |
Tox targets
| Target | Modality | Activity | Metabolite | Clinical evidence |
|---|---|---|---|---|
PubMed
| Title | Date | PubMed |
|---|---|---|
| Crizotinib, a small-molecule dual inhibitor of the c-Met and ALK receptor tyrosine kinases. | 2010 Dec |
|
| Trial watch: success for crizotinib in ALK-driven cancer. | 2010 Dec |
|
| New drugs in advanced non-small-cell lung cancer: searching for the correct clinical development. | 2010 Dec |
|
| ALK inhibition for non-small cell lung cancer: from discovery to therapy in record time. | 2010 Dec 14 |
|
| The neuroblastoma-associated F1174L ALK mutation causes resistance to an ALK kinase inhibitor in ALK-translocated cancers. | 2010 Dec 15 |
|
| Exciting new targets in lung cancer therapy: ALK, IGF-1R, HDAC, and Hh. | 2010 Jun |
|
| Gender specific drug metabolism of PF-02341066 in rats--role of sulfoconjugation. | 2010 May |
|
| EML4-ALK mutations in lung cancer that confer resistance to ALK inhibitors. | 2010 Oct 28 |
|
| Synthesis and c-Met kinase inhibition of 3,5-disubstituted and 3,5,7-trisubstituted quinolines: identification of 3-(4-acetylpiperazin-1-yl)-5-(3-nitrobenzylamino)-7- (trifluoromethyl)quinoline as a novel anticancer agent. | 2011 Apr 14 |
|
| Favorable response to crizotinib in three patients with echinoderm microtubule-associated protein-like 4-anaplastic lymphoma kinase fusion-type oncogene-positive non-small cell lung cancer. | 2011 Aug |
|
| ALK mutations conferring differential resistance to structurally diverse ALK inhibitors. | 2011 Dec 1 |
|
| Genotype-driven therapies for non-small cell lung cancer: focus on EGFR, KRAS and ALK gene abnormalities. | 2011 May |
|
| Therapeutic strategies to overcome crizotinib resistance in non-small cell lung cancers harboring the fusion oncogene EML4-ALK. | 2011 May 3 |
|
| Effect of crizotinib on overall survival in patients with advanced non-small-cell lung cancer harbouring ALK gene rearrangement: a retrospective analysis. | 2011 Oct |
|
| Adenocarcinoma of the lung with miliary brain and pulmonary metastases with echinoderm microtubule-associated protein like 4-anaplastic lymphoma kinase translocation treated with crizotinib: a case report. | 2012 Dec |
|
| Isolated central nervous system progression on Crizotinib: an Achilles heel of non-small cell lung cancer with EML4-ALK translocation? | 2012 Dec |
|
| Mechanisms of acquired crizotinib resistance in ALK-rearranged lung Cancers. | 2012 Feb 8 |
|
| Antitumor action of the MET tyrosine kinase inhibitor crizotinib (PF-02341066) in gastric cancer positive for MET amplification. | 2012 Jul |
|
| Paracrine receptor activation by microenvironment triggers bypass survival signals and ALK inhibitor resistance in EML4-ALK lung cancer cells. | 2012 Jul 1 |
|
| The ALK(F1174L) mutation potentiates the oncogenic activity of MYCN in neuroblastoma. | 2012 Jul 10 |
|
| [Management of crizotinib, a new individualized treatment]. | 2012 Jul-Aug |
|
| Crizotinib in the treatment of non-small-cell lung cancer. | 2012 Jun |
|
| Development of treatment strategies for advanced neuroblastoma. | 2012 Jun |
|
| Pharmacokinetic/pharmacodynamic modeling of crizotinib for anaplastic lymphoma kinase inhibition and antitumor efficacy in human tumor xenograft mouse models. | 2012 Mar |
|
| Targeted therapy for lung cancer. | 2012 Nov |
|
| Treatment of ALK-positive non-small cell lung cancer. | 2012 Oct |
|
| [Cavitating nodules in a 40-year-old non-smoking woman: a very particular tumour]. | 2012 Sep |
|
| Targeting ALK: a promising strategy for the treatment of non-small cell lung cancer, non-Hodgkin's lymphoma, and neuroblastoma. | 2012 Sep |
|
| Correlations between the percentage of tumor cells showing an anaplastic lymphoma kinase (ALK) gene rearrangement, ALK signal copy number, and response to crizotinib therapy in ALK fluorescence in situ hybridization-positive nonsmall cell lung cancer. | 2012 Sep 15 |
|
| Enhancement of the antiproliferative activity of gemcitabine by modulation of c-Met pathway in pancreatic cancer. | 2013 |
|
| Development and validation of a high-throughput intrinsic ATPase activity assay for the discovery of MEKK2 inhibitors. | 2013 Apr |
|
| Prediction of crizotinib-midazolam interaction using the Simcyp population-based simulator: comparison of CYP3A time-dependent inhibition between human liver microsomes versus hepatocytes. | 2013 Feb |
|
| Overcoming erlotinib resistance with tailored treatment regimen in patient-derived xenografts from naïve Asian NSCLC patients. | 2013 Jan 15 |
|
| Crizotinib for the treatment of non-small-cell lung cancer. | 2013 Jun 1 |
|
| Cell culture and Drosophila model systems define three classes of anaplastic lymphoma kinase mutations in neuroblastoma. | 2013 Mar |
|
| Targeted agents in the third-/fourth-line treatment of patients with advanced (stage III/IV) non-small cell lung cancer (NSCLC). | 2013 May |
|
| Multi-parameter in vitro toxicity testing of crizotinib, sunitinib, erlotinib, and nilotinib in human cardiomyocytes. | 2013 Oct 1 |
|
| Stereospecific targeting of MTH1 by (S)-crizotinib as an anticancer strategy. | 2014 Apr 10 |
|
| Elucidating mechanisms of toxicity using phenotypic data from primary human cell systems--a chemical biology approach for thrombosis-related side effects. | 2015 Jan 5 |
Sample Use Guides
The recommended dose and schedule for crizotinib is 250 mg orally, twice daily, with or without food.
Route of Administration:
fVal
PF-2341066 potently inhibited NPM-ALK phosphorylation in Karpas299 or SU-DHL-1 ALCL cells (mean IC50 value of 24 nmol/L). In biochemical and cellular screens, PF-2341066 was shown to be selective for c-Met and ALK at pharmacologically relevant concentrations across a panel of >120 diverse kinases. PF-2341066 potently inhibited cell proliferation, which was associated with G(1)-S-phase cell cycle arrest and induction of apoptosis in ALK-positive ALCL cells at IC50 values of approximately 30 nmol/L but not ALK-negative lymphoma cells.
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67175389
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FB99MH8KWZ
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877399-53-6
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DTXSID00236600
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ACTIVE MOIETY
SUBSTANCE RECORD
