Edaravone

Edaravone, sold under the brand name Radicava among others, is a medication used to treat stroke and amyotrophic lateral sclerosis (ALS).^[4][5] It is given by intravenous infusion^[4] and by mouth.^[4][6]

Edaravone

Clinical data
Trade names	Radicava, others
Other names	MCI-186
AHFS/Drugs.com	Monograph
MedlinePlus	a617027
License data	US DailyMed: Edaravone
Pregnancy category	AU: B3[1]
Routes of administration	Intravenous, by mouth
ATC code	N07XX14 (WHO)
Legal status
Legal status	AU: S4 (Prescription only)[1][2] CA: ℞-only[3] US: ℞-only[4] In general: ℞ (Prescription only)
Identifiers
IUPAC name 5-methyl-2-phenyl-4H-pyrazol-3-one
CAS Number	89-25-8 Y
PubChem CID	4021
DrugBank	DB12243 Y
ChemSpider	3881 Y
UNII	S798V6YJRP
KEGG	D01552 Y
ChEBI	CHEBI:31530 Y
ChEMBL	ChEMBL290916 Y
PDB ligand	W1P (PDBe, RCSB PDB)
CompTox Dashboard (EPA)	DTXSID9021130
ECHA InfoCard	100.001.719
Chemical and physical data
Formula	C10H10N2O
Molar mass	174.203 g·mol−1
3D model (JSmol)	Interactive image
SMILES O=C1N(/N=C(\C1)C)c2ccccc2
InChI InChI=1S/C10H10N2O/c1-8-7-10(13)12(11-8)9-5-3-2-4-6-9/h2-6H,7H2,1H3 Y Key:QELUYTUMUWHWMC-UHFFFAOYSA-N Y
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The mechanism by which edaravone might be effective is unknown.^[4] The medication is known to be an antioxidant, and oxidative stress has been hypothesized to be part of the process that kills neurons in people with ALS and in stroke victims.^[7]

The most common side effects include bruising (contusions), problems walking (gait disturbances), and headaches.^[6]

The U.S. Food and Drug Administration (FDA) considers it to be a first-in-class medication.^[8]

Medical uses

Edaravone is used to help people recover from stroke in Japan,^[9] and is used to treat ALS in the US and Japan.^[4][7]

Adverse effects

The label carries a warning about the potential for hypersensitivity reactions to edaravone, and adverse effects include bruising, gait disturbances, headache, skin inflammation, eczema, problems breathing, excess sugar in urine, and fungal skin infections.^[4]

The following adverse effects in at least 2% more people given the medication than were given placebo: bruising, gait disturbances, headache, skin inflammation, eczema, problems breathing, excess sugar in urine, and fungal skin infections.^[4]

There is no data on whether it is safe for pregnant women to take, and it is unknown if edaravone is secreted in breast milk.^[4]

Pharmacology

The mechanism by which edaravone might be effective is unknown.^[4] The medication is known to be an antioxidant, and oxidative stress has been hypothesized to be part of the process of neurodegeneration.^[7]

The half-life of edaravone is 4.5 to 6 hours and the half-lives of its metabolites are 2 to 3 hours. It is metabolized to a sulfate conjugate and a glucuronide conjugate, neither of which are active. It is primarily excreted in urine as the glucuronide conjugate form.^[4]

It suppresses reperfusion injury in animal models of stroke and improves stroke recovery after reperfusion therapy in humans.^[10]

History

Researchers first developed the free radical scavenger edaravone in the late 1980s as a treatment for stroke. The approach, introduced by Koji Abe, at Okayama University Hospital ("University Hospital" in the late 1980s)^[11] in Japan, aimed to prevent the brain swelling that sometimes follows stroke.^[12] It has been marketed in Japan by Mitsubishi Pharma for stroke since 2001 and is now generic.^[9][13]

Mitsubishi Pharma started a phase III clinical trial in ALS in 2011, in Japan, and by June 2015, it had been approved for that use in Japan. The company had received orphan drug designation for edaravone from the FDA and the EU by 2016.^[14]

It was approved for ALS in the US in 2017, based on a small randomized-controlled trial with people who had early-stage ALS in Japan, who were administered the medication for 6 months; it had failed two earlier trials in people with all stages of ALS.^[4][7]

In May 2017, I.V. edaravone was approved by the FDA to treat people with amyotrophic lateral sclerosis (ALS) in the United States.^[15] The FDA approval was conditioned on Mitsubishi Tanabe completing several additional studies to clarify the risks of cancer and liver disease, among other effects of the medication.^[16][17]

Re-analyses of efficacy

The efficacy of edaravone for the treatment of ALS was previously demonstrated in a six-month clinical trial that served as the basis for approval in 2017.^[6] In that trial, 137 participants were randomized to receive edaravone or placebo. At week 24, individuals receiving edaravone declined less on a clinical assessment of daily functioning than those receiving placebo.^[6] An analysis of real-world data from 194 patients from 12 ALS clinics of the intravenous formulation failed to reproduce the effect.^[18]

Efficacy of edaravone for stroke as an adjunct to regular reperfusion therapy has been reproduced in two retrospective studies of Japanese medical records.^[10][9]

New formulations

A formulation of edaravone by mouth, which is a mixture of edaravone and hydroxypropyl-sulfobutyl ether β-cyclodextrin (SBE-HP-βCD),^[19] has been under development by Ferrer (called FAB122) and licensed by Treeway (called TW001) for ALS. As of 2015, the drug had successfully completed a phase I trial and received orphan status in the US and the European Union.^[20] Ferrer reported on 10 January 2024 that the phase III ADORE clinical trial (EudraCT 2020-003376-40/NCT05178810) of FAB122/TW001 fo4 ALS did not meet the primary or key secondary study endpoints.^[21]

A different oral formulation of edaravone from Mitsubishi Tanabe Pharma America (MT1186/MT-1186) was approved for medical use in the United States in May 2022.^[4][6][22] The estimated effectiveness of oral edaravone is based on a study that showed comparable levels of oral edaravone in the bloodstream to the levels from the IV formulation of edaravone.^[6] A global phase 3b study of MT1186 was halted in 2023 due to failure.^[23]

Combination formulations

Edaravone is combined with dextro-borneol (dexborneol) in edaravone/dexborneol, a drug approved in China for stroke. It is approved in intravenous (2021) and sublingual (2025) forms. The intravenous combination was approved on the basis of trials showing it to be superior to edavarone alone.^[24][25]

Society and culture

Economics

The price for the medication when it launched in Japan for stroke in 2001, was set by the Japanese government at 9,931 yen/ampule.^[26]

When the medication launched in Japan for ALS in 2001, the price was $35,000; the price in Japan in 2017 was $5,000, the US price at launch was around $145,000.^[13] In the US the medication was approved for all people with ALS but it was unclear at approval whether insurers would agree to pay for the medication for all people with ALS, or only people in the early stages of the disease.^[13][27]

Brand names

Brand names include Radicut, Radicava, Xavron.^[28]