Binimetinib

Identification

Summary

Binimetinib is a medication used to treat metastatic melanoma with specific mutations.

Brand Names

Mektovi

Generic Name

Binimetinib

DrugBank Accession Number

DB11967

Background

Binimetinib, also known as Mektovi, is a potent and selective oral mitogen-activated protein kinase 1/2 (MEK 1/2) inhibitor which is combined with Encorafenib.^2,4

On June 27, 2018, the Food and Drug Administration approved the combination of Encorafenib and binimetinib (BRAFTOVI and MEKTOVI, from Array BioPharma Inc.) in combination for patients with unresectable or metastatic melanoma with the BRAF V600E or V600K mutations, as detected by an FDA-approved test.⁴

Type

Small Molecule

Groups

Approved, Investigational

Structure

3D

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MOLSDF3D-SDFPDBSMILESInChI

Similar Structures

Structure for Binimetinib (DB11967)

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Weight

Average: 441.233
Monoisotopic: 440.02956

Chemical Formula

C₁₇H₁₅BrF₂N₄O₃

Synonyms

• Binimetinib

External IDs

• ARRY-162
• ARRY-438162
• MEK-162
• MEK162
• NVP-MEK162

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Pharmacology

Indication

Binimetinib, in conjunction with encorafenib, is indicated for the treatment of unresectable or metastatic melanoma with BRAF V600E or V600K mutation and metastatic non-small cell lung cancer (NSCLC) with a BRAF V600E mutation.⁵

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Associated Conditions

Indication Type	Indication	Combined Product Details	Approval Level	Age Group	Patient Characteristics	Dose Form
Used in combination to treat	Metastatic melanoma	Regimen in combination with: Encorafenib (DB11718)	••••••••••••			••••••
Used in combination to treat	Metastatic melanoma	Regimen in combination with: Encorafenib (DB11718)	••••••••••••			••••••
Used in combination to treat	Metastatic non-small cell lung cancer	Regimen in combination with: Encorafenib (DB11718)	••••••••••••	•••••		••••••
Used in combination to treat	Unresectable melanoma	Regimen in combination with: Encorafenib (DB11718)	••••••••••••			••••••
Used in combination to treat	Unresectable melanoma	Regimen in combination with: Encorafenib (DB11718)	••••••••••••			••••••

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Pharmacodynamics

In vitro, binimetinib inhibited extracellular signal-related kinase (ERK) phosphorylation in cell-free assays as well as viability and MEK-dependent phosphorylation of BRAF-mutant human melanoma cell lines. Binimetinib also inhibited in vivo ERK phosphorylation and tumor growth in BRAF-mutant murine xenograft models.⁵ MEK is an enzyme that regulates the biosynthesis of inflammatory cytokines such as TNF, IL-6 and IL-1; therefore, binimetinib anti-tumor activity can be mediated through the interference of cytokines biosynthesis.^1,3

Binimetinib and encorafenib target two different kinases in the RAS/RAF/MEK/ERK pathway. Compared to either drug alone, coadministration of encorafenib and binimetinib resulted in greater anti-proliferative activity in vitro in BRAF mutation-positive cell lines and greater anti-tumor activity with respect to tumor growth inhibition in BRAF V600E mutant human melanoma xenograft studies in mice. Additionally, the combination of binimetinib and encorafenib delayed the emergence of resistance in BRAF V600E mutant human melanoma xenografts in mice compared to either drug alone. In a BRAF V600E mutant NSCLC patient-derived xenograft model in mice, coadministration of encorafenib and binimetinib resulted in greater anti-tumor activity compared to binimetinib alone, with respect to tumor growth inhibition. Increased tumor growth delay after dosing cessation was also observed with the coadministration compared to either drug alone.⁵

Following MEKTOVI 45 mg twice daily, no clinically meaningful QT prolongation was observed.⁵

Mechanism of action

Binimetinib, noncompetitive with ATP, binds reversibly to and inhibits the activity of mitogen-activated extracellular signal-regulated kinase (MEK) 1 and 2. The inhibition of MEK1/2 prevents the activation of MEK1/2-dependent effector proteins and transcription factors, resulting in the inhibition of growth factor-mediated cell signaling such as the downstream extracellular signal-related kinase (ERK) pathway. This may lead to the inhibition of tumor cell proliferation and an inhibition in the production of various inflammatory cytokines including interleukin-1, -6, and tumor necrosis factor. MEK1/2 are themselves threonine and tyrosine kinases that possess a dual specificity. They subsequently contribute critically to the activation of the RAS/RAF/MEK/ERK pathway and are typically upregulated in a number of different tumor cell types.^3,5

Target	Actions	Organism
ADual specificity mitogen-activated protein kinase kinase 2	inhibitor	Humans
ADual specificity mitogen-activated protein kinase kinase 1	inhibitor	Humans

Absorption

The pharmacokinetics of binimetinib was studied in healthy subjects and patients with solid tumors. After twice-daily dosing, the accumulation is 1.5-fold and the coefficient of variation (CV%) of the area under the concentration-time curve (AUC) is <40% at steady state. The systemic exposure of binimetinib is approximately dose proportional.⁵

After oral administration, at least 50% of the binimetinib dose was absorbed with a median time to maximum concentration (T_max) of 1.6 hours.⁵

The administration of a single dose of binimetinib 45 mg with a high-fat, high-calorie meal (consisting of approximately 150 calories from protein, 350 calories from carbohydrate, and 500 calories from fat) in healthy subjects had no effect on binimetinib exposure.⁵

Volume of distribution

The geometric mean (CV%) of the apparent volume of distribution of binimetinib is 92 L (45%).⁵

Protein binding

Binimetinib is 97% bound to human plasma proteins and the blood-to-plasma ratio is 0.72.⁵

Metabolism

The primary metabolic pathway is glucuronidation with UGT1A1 contributing up to 61% of the binimetinib metabolism. Other pathways of binimetinib metabolism include N-dealkylation, amide hydrolysis, and loss of ethane-diol from the side chain. The active metabolite M3 produced by CYP1A2 and CYP2C19 represents 8.6% of the binimetinib exposure. Following a single oral dose of 45 mg radiolabeled binimetinib, approximately 60% of the circulating radioactivity AUC in plasma was attributable to binimetinib.⁵

Route of elimination

Following a single oral dose of 45 mg radiolabeled binimetinib in healthy subjects, 62% (32% unchanged) of the administered dose was recovered in the feces while 31% (6.5% unchanged) was recovered in the urine.⁵

Half-life

The mean (CV%) terminal half-life (t1/2) of binimetinib is 3.5 hours (28.5%).⁵

Clearance

The apparent clearance (CL/F) of binimetinib is is 20.2 L/h (24%).⁵

Adverse Effects

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Toxicity

Based on findings from animal reproduction studies and its mechanism of action, binimetinib can cause fetal harm when administered to a pregnant woman. There are no available clinical data on the use of binimetinib during pregnancy. In animal reproduction studies, oral administration of binimetinib during the period of organogenesis was embryotoxic and an abortifacient in rabbits at doses greater than or equal to those resulting in exposures approximately 5 times the human exposure at the clinical dose of 45 mg twice daily. Advise pregnant women and females of reproductive potential of the potential risk to a fetus.⁵

No overall differences in the safety or effectiveness of MEKTOVI plus encorafenib were observed in older patients as compared to younger patients.⁵

Since binimetinib is 97% bound to plasma proteins, hemodialysis is likely to be ineffective in the treatment of overdose with binimetinib.⁵

Carcinogenicity studies with binimetinib have not been conducted. Binimetinib was not genotoxic in studies evaluating reverse mutations in bacteria, chromosomal aberrations in mammalian cells, or micronuclei in the bone marrow of rats.⁵

Pathways

Not Available

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Not Available

Interactions

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This information should not be interpreted without the help of a healthcare provider. If you believe you are experiencing an interaction, contact a healthcare provider immediately. The absence of an interaction does not necessarily mean no interactions exist.

• Approved
• Vet approved
• Nutraceutical
• Illicit
• Withdrawn
• Investigational
• Experimental
• All Drugs

Drug	Interaction
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Abametapir	The serum concentration of Binimetinib can be increased when it is combined with Abametapir.
Abatacept	The metabolism of Binimetinib can be increased when combined with Abatacept.
Abemaciclib	Abemaciclib may decrease the excretion rate of Binimetinib which could result in a higher serum level.
Abiraterone	The serum concentration of Binimetinib can be increased when it is combined with Abiraterone.
Abrocitinib	The serum concentration of Binimetinib can be increased when it is combined with Abrocitinib.

Food Interactions

• Take with or without food.

Products

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Brand Name Prescription Products

Name	Dosage	Strength	Route	Labeller	Marketing Start	Marketing End	Region	Image
Mektovi	Tablet	15 mg	Oral	Pfizer Canada Ulc	2021-07-05	Not applicable
Mektovi	Tablet, film coated	15 mg/1	Oral	Array BioPharma Inc.	2018-06-27	Not applicable
Mektovi	Tablet, film coated	15 mg	Oral	Pierre Fabre Médicament	2020-12-16	Not applicable
Mektovi	Tablet, film coated	15 mg	Oral	Pierre Fabre Médicament	2020-12-16	Not applicable

Categories

ATC Codes

L01EE03 — Binimetinib

• L01EE — Mitogen-activated protein kinase (MEK) inhibitors
• L01E — PROTEIN KINASE INHIBITORS
• L01 — ANTINEOPLASTIC AGENTS
• L — ANTINEOPLASTIC AND IMMUNOMODULATING AGENTS

Drug Categories

• Antineoplastic Agents
• Antineoplastic and Immunomodulating Agents
• BCRP/ABCG2 Substrates
• Cytochrome P-450 CYP1A2 Substrates
• Cytochrome P-450 CYP1A2 Substrates with a Narrow Therapeutic Index
• Cytochrome P-450 CYP2C19 Substrates
• Cytochrome P-450 CYP2C19 Substrates with a Narrow Therapeutic Index
• Cytochrome P-450 Substrates
• Heterocyclic Compounds, Fused-Ring
• Kinase Inhibitor
• MAP Kinase Kinase 1, antagonists & inhibitors
• MAP Kinase Kinase 2, antagonists & inhibitors
• Mitogen-activated protein kinase (MEK) inhibitors
• Narrow Therapeutic Index Drugs
• P-glycoprotein substrates
• P-glycoprotein substrates with a Narrow Therapeutic Index
• Protein Kinase Inhibitors
• UGT1A1 Substrates
• UGT1A1 Substrates with a Narrow Therapeutic Index

Chemical TaxonomyProvided by Classyfire

Description

This compound belongs to the class of organic compounds known as 3-halobenzoic acids and derivatives. These are benzoic acids or derivatives carrying a halogen atom at the 3-position of the benzene ring.

Kingdom

Organic compounds

Super Class

Benzenoids

Class

Benzene and substituted derivatives

Sub Class

Benzoic acids and derivatives

Direct Parent

3-halobenzoic acids and derivatives

Alternative Parents

Benzimidazoles / Aniline and substituted anilines / Fluorobenzenes / Bromobenzenes / Primary aromatic amines / Aryl bromides / Aryl fluorides / N-substituted imidazoles / Vinylogous amides / Heteroaromatic compounds / Amino acids and derivatives / Secondary amines / Azacyclic compounds / Hydrocarbon derivatives / Organic oxides / Organobromides / Organofluorides / Primary alcohols

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Substituents

3-halobenzoic acid or derivatives / Alcohol / Amine / Amino acid or derivatives / Aniline or substituted anilines / Aromatic heteropolycyclic compound / Aryl bromide / Aryl fluoride / Aryl halide / Azacycle / Azole / Benzimidazole / Bromobenzene / Carboxylic acid derivative / Fluorobenzene / Halobenzene / Heteroaromatic compound / Hydrocarbon derivative / Imidazole / N-substituted imidazole / Organic nitrogen compound / Organic oxide / Organic oxygen compound / Organobromide / Organofluoride / Organohalogen compound / Organoheterocyclic compound / Organonitrogen compound / Organooxygen compound / Primary alcohol / Primary aromatic amine / Secondary amine / Vinylogous amide

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Molecular Framework

Aromatic heteropolycyclic compounds

External Descriptors

Not Available

Affected organisms

• Humans and other mammals

Chemical Identifiers

UNII

181R97MR71

CAS number

606143-89-9

InChI Key

ACWZRVQXLIRSDF-UHFFFAOYSA-N

InChI

InChI=1S/C17H15BrF2N4O3/c1-24-8-21-16-13(24)7-10(17(26)23-27-5-4-25)15(14(16)20)22-12-3-2-9(18)6-11(12)19/h2-3,6-8,22,25H,4-5H2,1H3,(H,23,26)

IUPAC Name

5-[(4-bromo-2-fluorophenyl)amino]-4-fluoro-N-(2-hydroxyethoxy)-1-methyl-1H-1,3-benzodiazole-6-carboxamide

SMILES

CN1C=NC2=C(F)C(NC3=CC=C(Br)C=C3F)=C(C=C12)C(=O)NOCCO

References

General References

1. Koelblinger P, Dornbierer J, Dummer R: A review of binimetinib for the treatment of mutant cutaneous melanoma. Future Oncol. 2017 Aug;13(20):1755-1766. doi: 10.2217/fon-2017-0170. Epub 2017 Jun 7. [Article]
2. Bendell JC, Javle M, Bekaii-Saab TS, Finn RS, Wainberg ZA, Laheru DA, Weekes CD, Tan BR, Khan GN, Zalupski MM, Infante JR, Jones S, Papadopoulos KP, Tolcher AW, Chavira RE, Christy-Bittel JL, Barrett E, Patnaik A: A phase 1 dose-escalation and expansion study of binimetinib (MEK162), a potent and selective oral MEK1/2 inhibitor. Br J Cancer. 2017 Feb 28;116(5):575-583. doi: 10.1038/bjc.2017.10. Epub 2017 Feb 2. [Article]
3. Cancer.gov link [Link]
4. FDA approves encorafenib and binimetinib in combination for unresectable or metastatic melanoma with BRAF mutations [Link]
5. FDA Approved Drug Products: MEKTOVI® (binimetinib) tablets, for oral use [Link]
6. Binimetinib [File]
7. EMA assessment [File]

External Links

Human Metabolome Database

HMDB0304890

PubChem Compound

10288191

PubChem Substance

347828291

ChemSpider

8463660

ChEBI

145371

ChEMBL

CHEMBL3187723

ZINC

ZINC000038460704

PharmGKB

PA166179867

PDBe Ligand

QO7

Wikipedia

Binimetinib

PDB Entries

7m0u

Clinical Trials

Clinical Trials Learn More" title="About Clinical Trials" id="clinical-trials-info" class="drug-info-popup" href="javascript:void(0);">

Phase	Status	Purpose	Conditions	Count
4	Recruiting	Treatment	Solid Tumors	1
3	Active Not Recruiting	Treatment	Melanoma	3
3	Completed	Treatment	BRAF V600E-mutant Metastatic Colorectal Cancer	1
3	Completed	Treatment	Metastatic or Unresectable Cutaneous Melanoma	1
3	Not Yet Recruiting	Treatment	Biliary Tract Neoplasms	1

Pharmacoeconomics

Manufacturers

Not Available

Packagers

Not Available

Dosage Forms

Form	Route	Strength
Tablet	Oral	15 mg
Tablet	Oral	15.000 mg
Tablet, film coated	Oral	15 mg/1
Tablet, film coated	Oral	15 MG

Prices

Not Available

Patents

Patent Number	Pediatric Extension	Approved	Expires (estimated)	Region
US9314464	No	2016-04-19	2031-07-04
US9850229	No	2017-12-26	2030-08-27
US10005761	No	2018-06-26	2030-08-27
US9593100	No	2017-03-14	2030-08-27
US9980944	No	2018-05-29	2033-10-18
US9598376	No	2017-03-21	2033-10-18
US8193229	No	2012-06-05	2023-03-13
US8513293	No	2013-08-20	2023-03-13
US7777050	No	2010-08-17	2023-03-13
US8178693	No	2012-05-15	2023-03-13
US9562016	No	2017-02-07	2033-10-18

Properties

State

Solid

Experimental Properties

Not Available

Predicted Properties

Property	Value	Source
Water Solubility	0.0499 mg/mL	ALOGPS
logP	3	ALOGPS
logP	3.81	Chemaxon
logS	-4	ALOGPS
pKa (Strongest Acidic)	10.26	Chemaxon
pKa (Strongest Basic)	5.3	Chemaxon
Physiological Charge	0	Chemaxon
Hydrogen Acceptor Count	5	Chemaxon
Hydrogen Donor Count	3	Chemaxon
Polar Surface Area	88.41 Å2	Chemaxon
Rotatable Bond Count	6	Chemaxon
Refractivity	98.02 m3·mol-1	Chemaxon
Polarizability	38.55 Å3	Chemaxon
Number of Rings	3	Chemaxon
Bioavailability	1	Chemaxon
Rule of Five	Yes	Chemaxon
Ghose Filter	Yes	Chemaxon
Veber's Rule	No	Chemaxon
MDDR-like Rule	Yes	Chemaxon

Predicted ADMET Features

Not Available

Spectra

Mass Spec (NIST)

Not Available

Spectra

Spectrum	Spectrum Type	Splash Key
Predicted MS/MS Spectrum - 10V, Positive (Annotated)	Predicted LC-MS/MS	splash10-0006-0000900000-611f9ca261be4b64ea83
Predicted MS/MS Spectrum - 10V, Negative (Annotated)	Predicted LC-MS/MS	splash10-01dr-0009800000-49b4276f279db04bc60b
Predicted MS/MS Spectrum - 20V, Positive (Annotated)	Predicted LC-MS/MS	splash10-014l-0009400000-c0ead1fc64a3cdaebd2d
Predicted MS/MS Spectrum - 20V, Negative (Annotated)	Predicted LC-MS/MS	splash10-004i-5009300000-944283b5294b7bcd2110
Predicted MS/MS Spectrum - 40V, Positive (Annotated)	Predicted LC-MS/MS	splash10-06ri-0049100000-04fe4b0a75a92e3ebe86
Predicted MS/MS Spectrum - 40V, Negative (Annotated)	Predicted LC-MS/MS	splash10-004i-9000000000-308ba3122a7cc4b1a574
Predicted 1H NMR Spectrum	1D NMR	Not Applicable
Predicted 13C NMR Spectrum	1D NMR	Not Applicable

Chromatographic Properties

Collision Cross Sections (CCS)

Adduct	CCS Value (Å2)	Source type	Source
[M-H]-	184.66072	predicted	DeepCCS 1.0 (2019)
[M+H]+	187.01872	predicted	DeepCCS 1.0 (2019)
[M+Na]+	194.30202	predicted	DeepCCS 1.0 (2019)

Targets

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Details1. Dual specificity mitogen-activated protein kinase kinase 2

Kind

Protein

Organism

Humans

Pharmacological action

Yes

Actions

Inhibitor

General Function

Scaffold protein binding

Specific Function

Catalyzes the concomitant phosphorylation of a threonine and a tyrosine residue in a Thr-Glu-Tyr sequence located in MAP kinases. Activates the ERK1 and ERK2 MAP kinases (By similarity).

Gene Name

MAP2K2

Uniprot ID

P36507

Uniprot Name

Dual specificity mitogen-activated protein kinase kinase 2

Molecular Weight

44423.735 Da

References

1. Koelblinger P, Dornbierer J, Dummer R: A review of binimetinib for the treatment of mutant cutaneous melanoma. Future Oncol. 2017 Aug;13(20):1755-1766. doi: 10.2217/fon-2017-0170. Epub 2017 Jun 7. [Article]
2. FDA Approved Drug Products: MEKTOVI® (binimetinib) tablets, for oral use [Link]

Details2. Dual specificity mitogen-activated protein kinase kinase 1

Kind

Protein

Organism

Humans

Pharmacological action

Yes

Actions

Inhibitor

General Function

Receptor signaling protein tyrosine phosphatase activity

Specific Function

Dual specificity protein kinase which acts as an essential component of the MAP kinase signal transduction pathway. Binding of extracellular ligands such as growth factors, cytokines and hormones t...

Gene Name

MAP2K1

Uniprot ID

Q02750

Uniprot Name

Dual specificity mitogen-activated protein kinase kinase 1

Molecular Weight

43438.65 Da

References

1. FDA Approved Drug Products: MEKTOVI® (binimetinib) tablets, for oral use [Link]

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Drug created at October 20, 2016 21:06 / Updated at November 24, 2023 04:34