Dimethyl Fumarate: Complete Drug Monograph

Quick Facts

Pharmacokinetic Profile (active metabolite, MMF)

Half-Life (MMF)

~1 hour (terminal)

Time to Peak (T_max)

2–2.5 hours (delayed to ~5.5 h with high-fat meal)

Metabolism

Rapid presystemic ester hydrolysis to MMF; further by TCA cycle; no CYP involvement

Protein Binding (MMF)

27–45%

Volume of Distribution (MMF)

53–73 L

Elimination

~60% as exhaled CO₂; 16% renal; 1% fecal

Clinical Information

Drug Class

Fumaric acid ester; MS disease-modifying therapy (oral)

Available Strengths

120 mg and 240 mg delayed-release capsules

Route

Oral; swallow whole (do not crush, chew, or sprinkle)

Renal Adjustment

No adjustment needed (not formally studied)

Hepatic Adjustment

No adjustment needed (not formally studied)

Pregnancy

Pregnancy registry through 2022 (n=362) showed no clear increase in major birth defects; animal data show developmental toxicity at high doses

Lactation

No human milk data; effects on infant unknown — individualized decision

Pediatric Use

Safety and effectiveness in patients <18 years not established

Generic Available

Yes

Boxed Warning

None

Major Risks

Anaphylaxis/angioedema · PML · serious opportunistic infections · lymphopenia · liver injury · serious GI reactions

Indications

Indication	Approved Population	Therapy Type	Status
Relapsing forms of multiple sclerosis — including clinically isolated syndrome, relapsing-remitting disease, and active secondary progressive disease	Adults (≥18 years)	Monotherapy	FDA Approved
Moderate-to-severe plaque psoriasis (Skilarence formulation)	Adults requiring systemic therapy	Monotherapy	EU Approved · Off-label US

Dimethyl fumarate is a fumaric acid ester originally used for decades in Germany as part of a combination product (Fumaderm) for plaque psoriasis. The delayed-release oral capsule (Tecfidera) was approved by the FDA in 2013 for relapsing forms of multiple sclerosis on the basis of the Phase III DEFINE and CONFIRM trials, both published in the New England Journal of Medicine in 2012. In 2017, a single-agent oral tablet formulation of dimethyl fumarate (Skilarence) was approved in the European Union for moderate-to-severe plaque psoriasis; this product is not available in the United States.

Dimethyl fumarate sits within the AAN treatment hierarchy as one of several oral disease-modifying therapies for relapsing MS, alongside teriflunomide, fingolimod and other sphingosine-1-phosphate receptor modulators, and the more recently approved diroximel fumarate (Vumerity, a prodrug) and monomethyl fumarate (Bafiertam, the active metabolite given directly). Across these fumarate products the underlying pharmacology is shared; the differences lie chiefly in gastrointestinal tolerability (diroximel) and pill burden (monomethyl fumarate).

Off-Label Uses

Plaque psoriasis (US): Some specialists use dimethyl fumarate off-label for moderate-to-severe psoriasis based on its EU approval and decades of European experience. Evidence: moderate quality (randomized trials with Skilarence and historical Fumaderm data).

Other uses are limited. Despite its broad anti-inflammatory and antioxidant pharmacology, dimethyl fumarate is not established for other neurological or dermatological diseases outside the indications above and should not be substituted for therapies with disease-specific evidence.

Dose

Dosing

Dimethyl fumarate has a fixed dosing schedule independent of body weight, age, and renal or hepatic function. The 7-day starter pack is designed to improve gastrointestinal and flushing tolerability during initiation; most adverse reactions emerge in month 1 and ease over time. Capsules must be swallowed whole — they are delayed-release and the enteric coating cannot be disrupted.

Standard Dosing — Adults

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Relapsing MS — initiation (days 1–7)	120 mg PO BID	—	—	Take with or without food; food may reduce flushing Swallow whole; do not crush, chew, or sprinkle on food
Relapsing MS — maintenance (day 8 onward)	—	240 mg PO BID	240 mg PO BID (= 480 mg/day)	No benefit shown for higher doses (TID was studied and showed no advantage over BID)
Tolerability issue during maintenance	—	Temporarily reduce to 120 mg PO BID	Resume 240 mg BID within 4 weeks	Discontinue if patient cannot tolerate return to maintenance dose Most flushing and GI events emerge in month 1 and improve with continued therapy
Flushing prophylaxis (optional)	—	Non-enteric-coated aspirin up to 325 mg 30 minutes before each dose	—	Aspirin does not alter MMF pharmacokinetics; weigh routine aspirin use against bleeding risk Taking with food provides similar flushing reduction (~25% in the fed state)

Special Populations

Population	Recommendation	Rationale
Renal impairment (any severity)	No dose adjustment required	Renal elimination accounts for only ~16% of the dose; not formally studied but adjustment is not expected to be needed
Hepatic impairment (any severity)	No dose adjustment required	Not formally studied; predominant elimination is via CO₂ exhalation and no CYP metabolism is involved
Body weight, age, sex, race	No dose adjustment required	Population PK analyses found no clinically relevant effect on MMF exposure
Geriatric patients (≥65 years)	No specific adjustment; clinical experience limited	Pivotal trials enrolled few patients ≥65 years
Pediatric patients (<18 years)	Not recommended	Safety and effectiveness not established
Pre-existing low lymphocyte count	Not studied; obtain baseline CBC and weigh risk individually	Lymphopenia is a known adverse effect; pre-existing low ALC is a relative contraindication in clinical practice

Clinical Pearl — Why a 7-Day Titration Matters

Approximately 40% of patients experience flushing on dimethyl fumarate, and around 18% report abdominal pain. Both classes of reactions emerge primarily in the first month, are usually mild to moderate, and improve with continued therapy. The 7-day 120 mg BID starter dose, taking the medication with food, and using non-enteric-coated aspirin 30 minutes before dosing are the three evidence-based interventions that allow most patients to reach and stay on the 240 mg BID maintenance dose. Discontinuation rates for flushing (~3%) and GI events (~4%) in the placebo-controlled trials remain modest when these strategies are applied.

Pharmacology

Mechanism of Action

The mechanism by which dimethyl fumarate exerts its therapeutic effect in multiple sclerosis is not fully established. Both dimethyl fumarate and its active metabolite monomethyl fumarate (MMF) activate the nuclear factor (erythroid-derived 2)-like 2 (Nrf2) pathway, which is involved in the cellular response to oxidative stress and induces a battery of cytoprotective and anti-inflammatory gene products. MMF also acts as an agonist at the hydroxycarboxylic acid receptor 2 (HCA2, also known as the nicotinic acid receptor or GPR109A) in vitro; this activity is thought to contribute to flushing and may contribute to anti-inflammatory effects on macrophages and dendritic cells.

Clinically, dimethyl fumarate produces a modest dose-related decrease in absolute lymphocyte count, with selective reductions in CD8+ T cells more pronounced than reductions in CD4+ T cells in many patients. This shift in lymphocyte subsets, together with effects on immune-cell trafficking and oxidative defence, is believed to underlie its therapeutic activity in relapsing MS — but it is also the basis for the risk of severe lymphopenia and progressive multifocal leukoencephalopathy (PML) that accompanies long-term therapy.

ADME Profile

Because dimethyl fumarate undergoes rapid presystemic hydrolysis by ubiquitous esterases in the gut, blood, and tissues, parent drug is not quantifiable in plasma after oral administration. All pharmacokinetic parameters refer to the active metabolite monomethyl fumarate (MMF).

Parameter	Value	Clinical Implication
Absorption	Rapid presystemic ester hydrolysis to MMF; T_max 2–2.5 h. Mean steady-state C_max 1.87 mg/L and AUC 8.21 mg·h/L on 240 mg BID with food. C_max and AUC increase approximately dose-proportionally over 120–360 mg	A high-fat, high-calorie meal does not change AUC but reduces C_max by ~40% and delays T_max to ~5.5 h, with ~25% lower flushing incidence — a useful tolerability strategy
Distribution	Apparent V_d of MMF 53–73 L; plasma protein binding 27–45% and concentration-independent	Low-to-moderate protein binding makes displacement interactions clinically unimportant
Metabolism	Esterase-mediated conversion of dimethyl fumarate to MMF; further breakdown of MMF through the tricarboxylic acid (TCA) cycle to fumaric acid, citric acid, and glucose; no CYP P450 involvement	No clinically significant CYP-mediated drug interactions; no dose adjustments for CYP inducers or inhibitors
Elimination	~60% of an administered dose is eliminated as exhaled CO₂; ~16% renal and ~1% fecal. Mean terminal t½ of MMF ~1 hour. No accumulation with multiple BID dosing	Short half-life means BID dosing is required; the lack of accumulation simplifies titration and limits residual exposure after discontinuation

Dimethyl fumarate is not a substrate, inhibitor, or inducer of P-glycoprotein in vitro at clinically relevant concentrations, and no interaction has been demonstrated with single doses of interferon beta-1a, glatiramer acetate, or with combined oral contraceptives (norelgestromin/ethinyl estradiol). Therapeutic drug monitoring is not used.

Side Effects

Adverse-event data below are drawn from the integrated safety analysis of the two placebo-controlled Phase III studies (DEFINE and CONFIRM), in which 769 patients received dimethyl fumarate 240 mg twice daily and 771 received placebo. Frequencies shown are the dimethyl fumarate rate followed by the placebo rate. Only events that occurred at ≥2% higher incidence than placebo are listed in the PI’s primary table.

≥10% Very Common (DEFINE/CONFIRM, ≥2% above placebo)

Adverse Effect	Incidence (DMF vs Placebo)	Clinical Note
Flushing (warmth, redness, pruritus, burning)	40% vs 6%	Most common adverse reaction; emerges soon after initiation, usually mild–moderate, improves over time. ~3% discontinue; <1% have severe flushing requiring hospitalization
Abdominal pain	18% vs 10%	Part of the GI symptom cluster that peaks in month 1
Diarrhea	14% vs 11%	Modest absolute increase over placebo
Nausea	12% vs 9%	Taking with food may help

1–10% Common (DEFINE/CONFIRM, ≥2% above placebo)

Adverse Effect	Incidence (DMF vs Placebo)	Clinical Note
Vomiting	9% vs 5%	Usually transient
Pruritus	8% vs 4%	May occur with or independent of flushing
Rash	8% vs 3%	Most are mild; evaluate any new rash for hypersensitivity
Albumin in urine	6% vs 4%	Usually transient and clinically silent; persistent proteinuria warrants further workup
Erythema	5% vs 1%	Often part of the flushing complex
Dyspepsia	5% vs 3%	Component of the early GI symptom cluster
Aspartate aminotransferase (AST) increased	4% vs 2%	Most elevations are <3× ULN and occur in the first 6 months
Lymphopenia (laboratory)	2% vs <1%	Refers to the lymphopenia adverse-event term; the proportion with lymphocyte counts <0.5 × 10⁹/L during therapy is approximately 6%

Serious Serious — Regardless of Frequency

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Anaphylaxis and angioedema	Postmarketing — frequency not established	After first dose or any time during therapy	Discontinue and do not restart; treat as for any anaphylactic reaction; seek emergency care
Progressive multifocal leukoencephalopathy (PML)	Rare (postmarketing); has occurred predominantly in patients with prolonged lymphopenia, but reported with lymphocyte counts <0.9 × 10⁹/L	Months to years	Withhold at first sign or symptom suggestive of PML (progressive hemiparesis, visual disturbance, cognitive or personality change); obtain MRI and CSF JCV PCR
Severe persistent lymphopenia	~6% of treated patients had ALC <0.5 × 10⁹/L; ~2% had prolonged severe lymphopenia for ≥6 months	First year of treatment	Consider interruption if ALC persistently <0.5 × 10⁹/L for >6 months; recovery can take many months
Herpes zoster, including disseminated zoster, zoster ophthalmicus, and CNS zoster	Postmarketing — frequency not established	Any time during therapy	Treat zoster promptly; consider withholding dimethyl fumarate until infection resolves
Other serious opportunistic infections (HSV, CMV, West Nile virus, Candida, Aspergillus, Nocardia, Listeria monocytogenes, Mycobacterium tuberculosis)	Postmarketing — frequency not established; reported with both reduced and normal ALC	Variable	Prompt diagnostic evaluation and pathogen-directed treatment; consider withholding dimethyl fumarate
Liver injury (clinically significant)	Postmarketing; transaminase elevations >5× ULN with bilirubin >2× ULN reported, none progressing to liver failure or death in published cases	Days to several months	Discontinue if clinically significant liver injury suspected; check ALT, AST, ALP, total bilirubin at baseline and as clinically indicated
Serious gastrointestinal reactions (perforation, ulceration, hemorrhage, obstruction) — Warning added 12/2023	Postmarketing reports across fumaric acid esters, some fatal; in clinical trials serious GI events occurred in 1% (vomiting 0.3%, abdominal pain 0.3%, none fatal)	Majority within 6 months of fumarate initiation	Promptly evaluate new or worsening severe abdominal pain, hematemesis, melena, or rectal bleeding; discontinue dimethyl fumarate
Acute pancreatitis	Postmarketing — frequency not established	Variable	Discontinue and evaluate any patient with new severe upper abdominal pain
Persistent transaminase elevation ≥3× ULN with bilirubin >2× ULN (Hy’s law pattern)	Postmarketing	Variable	Discontinue; investigate for drug-induced liver injury
Alopecia	Postmarketing — usually mild and reversible	Months	Reassure; usually does not require discontinuation

Discontinuation Treatment Discontinuation Due to Adverse Reactions

Discontinuation due to gastrointestinal events

4% vs <1% placebo

Most discontinuations occurred during the first month of therapy. Combining a 7-day starter dose with food and pre-dose aspirin substantially reduces this rate in clinical practice.

Discontinuation due to flushing

3% vs minimal placebo

In the majority of patients flushing was mild or moderate; serious flushing events leading to hospitalization occurred in <1%.

Management Pearl — Approach to Lymphopenia

Mean lymphocyte counts fall by approximately 30% during the first year of dimethyl fumarate therapy and then plateau. About 6% of patients drop below 0.5 × 10⁹/L at some point, and 2% develop prolonged severe lymphopenia (≥6 months <0.5 × 10⁹/L). PML in trials and postmarketing experience has occurred almost exclusively in patients with sustained lymphopenia, especially <0.5 × 10⁹/L for prolonged periods, although postmarketing cases at counts <0.9 × 10⁹/L are described. Per the PI, consider interrupting therapy when ALC persists below 0.5 × 10⁹/L for more than six months and continue to monitor counts after stopping — recovery to normal can take many months (median 96 weeks for prolonged severe lymphopenia).

Int

Drug Interactions

Dimethyl fumarate has an unusually clean drug-interaction profile. Because metabolism proceeds via ubiquitous esterases and the tricarboxylic acid cycle rather than cytochrome P450 enzymes, it is neither a substrate, inhibitor, nor inducer of clinically relevant CYPs in vivo. The interactions below reflect overlapping pharmacodynamics with immune-modulating therapies and one mitigation strategy (aspirin) for flushing.

Major Other immunosuppressants and immunomodulators (natalizumab, fingolimod and other S1P modulators, anti-CD20 agents, cladribine, alemtuzumab, mitoxantrone, methotrexate, azathioprine)

MechanismAdditive immunosuppression and additive risk of opportunistic infection (including PML) and lymphopenia

EffectIncreased infection risk; potential for compounded haematologic effects when switching between MS disease-modifying therapies

ManagementCoadministration is generally not recommended; observe a washout period when switching from one disease-modifying therapy to another, guided by MS specialist input. After natalizumab, enhanced pharmacovigilance with brain MRI is advised by AAN

Class effect · AAN Guideline

Major Live and live-attenuated vaccines (e.g., MMR, varicella, zoster live, yellow fever, intranasal influenza)

MechanismTheoretical risk of disseminated infection in patients with treatment-induced lymphopenia; safety not assessed in clinical studies

EffectPossible vaccine-strain disease in immunocompromised hosts

ManagementAvoid live vaccines during dimethyl fumarate therapy; complete recommended live vaccinations before initiation. Inactivated vaccines (tetanus, pneumococcal, meningococcal) generated normal antibody responses in a comparator study

FDA PI

Moderate Aspirin (non-enteric-coated, up to 325 mg)

MechanismUsed 30 minutes before dosing to blunt the prostaglandin-mediated flushing response (HCA2-mediated)

EffectReduced incidence and severity of flushing without altering MMF pharmacokinetics

ManagementReasonable in selected patients during the first weeks of therapy; weigh routine aspirin use against bleeding risk and history of GI ulceration, particularly given the warning for serious GI reactions on dimethyl fumarate

FDA PI

Moderate Other fumaric acid esters (diroximel fumarate, monomethyl fumarate, Fumaderm)

MechanismAll deliver MMF as the systemically active species; combining them is duplicative and increases systemic exposure

EffectCompounded toxicity (lymphopenia, GI events, flushing, liver injury)

ManagementDo not combine; switching between fumarates is done as direct substitution rather than overlap

Class effect

Moderate Hepatotoxic medications (e.g., methotrexate, isoniazid, valproate, alcohol)

MechanismPharmacodynamic — additive risk of hepatic injury given postmarketing reports of clinically significant liver injury on dimethyl fumarate

EffectIncreased risk of transaminase elevation and hepatotoxicity

ManagementMonitor LFTs more vigilantly; counsel on alcohol moderation

Clinical extrapolation

Minor Interferon beta-1a, glatiramer acetate

MechanismSingle doses of either agent did not alter MMF pharmacokinetics in PK studies

EffectNo PK interaction

ManagementRoutine concomitant use is not common practice; switching follows standard MS DMT transition principles

FDA PI

Minor Combined oral contraceptives (norelgestromin/ethinyl estradiol)

MechanismNo relevant change in oral contraceptive exposure when coadministered with dimethyl fumarate

EffectNo PK interaction documented; data limited to one progestin

ManagementRoutine contraceptive use is not expected to be compromised; data are limited for other progestins

FDA PI

Minor CYP substrates, inhibitors, and inducers; P-glycoprotein substrates

MechanismDimethyl fumarate and MMF were not identified as CYP or P-gp substrates, inhibitors, or inducers in in-vitro studies

EffectNo clinically relevant interactions expected

ManagementNo dose adjustments based on CYP/P-gp interactions

FDA PI

Mon

Monitoring

Routine monitoring on dimethyl fumarate centres on the absolute lymphocyte count, hepatic biochemistry, and a high index of suspicion for opportunistic infection — particularly herpes zoster and PML — and for serious gastrointestinal reactions. Monitoring intervals below combine PI requirements and standard MS practice.

Complete blood count with lymphocyte differential Baseline; 6 months after start; then every 6–12 months and as clinically indicated
Routine Consider interruption of therapy when ALC persists below 0.5 × 10⁹/L for more than six months. If discontinuing for lymphopenia, continue measuring ALC until recovery — median time to normalization is 4.3 weeks (mild lymphopenia at d/c), 10.0 weeks (moderate), 16.7 weeks (severe), and 96 weeks for prolonged severe lymphopenia.
Liver function (ALT, AST, ALP, total bilirubin) Baseline before initiation; then as clinically indicated during therapy
Routine Most enzyme elevations are <3× ULN and occur in the first 6 months. Discontinue if clinically significant liver injury is suspected (e.g., new transaminase rise >5× ULN with bilirubin >2× ULN, jaundice, dark urine, RUQ pain).
Symptoms of PML At each contact; heightened vigilance with prolonged lymphopenia
Routine Withhold therapy at the first sign of progressive hemiparesis, ataxia, visual disturbance, cognitive or personality change, and arrange MRI plus CSF JCV PCR. Patterns may be apparent on MRI before clinical symptoms.
Signs of herpes zoster and other opportunistic infections At each contact
Routine Counsel on dermatomal rash, neuralgia, and red-flag symptoms (visual change with vesicles, encephalitis features). Consider withholding dimethyl fumarate during treatment of zoster or other serious infection.
Anaphylaxis / angioedema awareness Especially after first dose and during early therapy
Routine Counsel patients to discontinue immediately and seek emergency care for swelling of the face, lips, mouth, or throat, urticaria, or shortness of breath. Do not rechallenge.
GI symptoms (severe abdominal pain, hematemesis, melena, severe vomiting, severe diarrhea) At each contact, especially in the first 6 months
Routine Warning added 12/2023 for serious GI reactions (perforation, ulceration, hemorrhage, obstruction), some fatal across fumaric acid esters. Promptly evaluate and discontinue dimethyl fumarate for new or worsening severe GI symptoms.
Flushing tolerance During first month and at each visit
Routine Most flushing improves over time. Reinforce administration with food and consider non-enteric-coated aspirin pre-dose for persistent symptoms.
MRI of brain Per MS practice (commonly baseline and at intervals to monitor disease activity); additional MRI if PML suspected
Trigger-based Routine MRI is part of MS care rather than dimethyl fumarate-specific monitoring. Any new neurological symptom while on dimethyl fumarate should prompt urgent imaging to differentiate MS relapse from PML.
Renal function (urinalysis for proteinuria) Routine clinical follow-up
Trigger-based Asymptomatic albuminuria (~6%) is usually transient and clinically silent; persistent or progressive proteinuria should prompt further evaluation.
Vaccinations Before initiation; routine inactivated vaccines during therapy
Trigger-based Complete live and live-attenuated vaccinations (e.g., MMR, varicella) before starting therapy. Inactivated vaccines (tetanus, pneumococcal, meningococcal) elicited normal antibody responses on dimethyl fumarate. Recombinant zoster vaccine is generally preferred over live zoster vaccine in MS DMT-treated patients per AAN.

Practical Pearl — When to Suspect PML

PML on dimethyl fumarate is rare but devastating. The dominant risk factor is prolonged severe lymphopenia, but cases have occurred at counts <0.9 × 10⁹/L. Any patient with new neurological symptoms — particularly subacute cognitive change, hemiparesis, ataxia, or visual disturbance — should have therapy withheld and undergo urgent MRI plus CSF JCV PCR before treatment is resumed. Differentiating PML from a new MS relapse based on clinical features alone is unreliable.

Contraindications & Cautions

Absolute Contraindications

Known hypersensitivity to dimethyl fumarate or any excipient. Reactions reported include anaphylaxis and angioedema; patients with such reactions must not be rechallenged.

Note: hypersensitivity to dimethyl fumarate or excipients is the only formal contraindication listed in the Tecfidera prescribing information. The cautions below reflect class- and pharmacology-based clinical practice.

Relative Contraindications — Specialist Input Recommended

Active serious infection, including herpes zoster, opportunistic viral, fungal, or bacterial infection — withhold dimethyl fumarate until the infection is treated and resolved.
Pre-existing severe lymphopenia (ALC <0.5 × 10⁹/L) — not formally studied; the additive lymphopenia risk argues against initiation.
Pre-existing moderate lymphopenia (0.5–0.8 × 10⁹/L) — initiate only if benefit clearly outweighs risk; monitor more frequently.
Active or suspected progressive multifocal leukoencephalopathy.
Severe active hepatic disease, including drug-induced liver injury attributable to fumarates.
Recent or planned use of other immunosuppressive disease-modifying therapy without an appropriate washout — risk of cumulative immune compromise.
Recent or planned live or live-attenuated vaccination.
Pregnancy planning — discuss benefits and risks; pregnancy registry data through 2022 are reassuring but limited, and animal data show developmental toxicity at clinically relevant doses.

Use With Caution

Patients with peptic ulcer disease, inflammatory bowel disease, or recent GI bleeding — given the warning for serious GI reactions including perforation, ulceration, and hemorrhage.
Patients with chronic respiratory disease, JC virus seropositivity, or other PML risk factors — these increase the importance of strict ALC monitoring.
Concomitant hepatotoxic medications — increased vigilance for liver injury.
Pregnancy and lactation — see Use in Specific Populations; benefit-risk discussion essential.
Pediatric patients (<18 years) — safety and effectiveness not established.

Important Safety Signals (No Boxed Warning) Dimethyl fumarate does not carry a boxed warning, but the following warnings and precautions in the prescribing information must be discussed before initiation:

Anaphylaxis and angioedema — discontinue and do not restart.

PML — withhold at the first sign or symptom suggestive of PML; the risk is greatest with prolonged severe lymphopenia.

Herpes zoster and other serious opportunistic infections.

Lymphopenia — monitor CBC at baseline, 6 months, then every 6–12 months.

Liver injury — clinically significant hepatic injury reported postmarketing.

Flushing — common at initiation; usually self-limited.

Serious gastrointestinal reactions — perforation, ulceration, hemorrhage, obstruction (warning added 12/2023).

Patient Counselling

Purpose of Therapy

Explain that dimethyl fumarate is a long-term oral medication used to reduce relapses, brain MRI lesions, and the progression of disability in relapsing forms of multiple sclerosis. It does not cure MS, but pivotal trials and long-term extension data show sustained reductions in relapse rate compared with placebo. The capsules contain a delayed-release coating, so they must be swallowed whole — they cannot be opened, crushed, chewed, or sprinkled on food.

How to Take

Begin with one 120 mg capsule by mouth twice daily for the first 7 days, then increase to one 240 mg capsule by mouth twice daily from day 8 onward. The medication can be taken with or without food, but taking it with food often reduces flushing. If flushing remains bothersome, ask the prescriber whether non-enteric-coated aspirin (up to 325 mg) taken about 30 minutes before each dose may help — this is an evidence-based option for short-term use. Store the capsules in their original container, protected from light.

Flushing

Tell patient Flushing — a feeling of warmth, redness, itching, or tingling — affects about 4 in 10 patients. It usually starts soon after the first doses, lasts only minutes to a couple of hours, and improves over the following weeks. Taking dimethyl fumarate with a meal helps; aspirin 30 minutes before may help further if your prescriber agrees.

Call prescriber If flushing is severe, persistent, or accompanied by chest tightness, difficulty breathing, or swelling of the face, lips, tongue, or throat — these may signal an allergic reaction.

Stomach & Bowel Symptoms

Tell patient Abdominal pain, nausea, vomiting, indigestion, and diarrhoea are common in the first month and usually improve. Taking the medicine with food and staying well hydrated helps. Do not crush or open the capsule — the coating protects your stomach.

Call prescriber Urgently for severe stomach pain, vomiting blood or material that looks like coffee grounds, bright-red blood in the stool, black tarry stools, severe ongoing diarrhoea, or any rapidly worsening abdominal symptoms — these can rarely indicate serious gastrointestinal complications and the medicine may need to be stopped.

Allergic Reactions

Tell patient Serious allergic reactions can occur with the first dose or at any time during therapy. Symptoms include hives, swelling of the face, lips, mouth or tongue, and difficulty breathing.

Call prescriber Stop the medicine immediately and seek emergency care for any of these symptoms. Do not restart dimethyl fumarate after a serious allergic reaction.

Infections, Including PML

Tell patient Dimethyl fumarate can lower lymphocyte (a type of white blood cell) counts, especially with long-term use. This may slightly increase the risk of infections, including shingles (herpes zoster) and a very rare but serious brain infection called PML. Routine blood tests will be checked at baseline, after 6 months, and then every 6–12 months.

Call prescriber For any new fever, painful blistering rash (especially on one side of the body), persistent cough, unexplained weakness on one side, problems with vision or speech, confusion, or personality change. Keep all blood-test appointments — these are essential for safe long-term use.

Liver

Tell patient Dimethyl fumarate can occasionally affect the liver. Your healthcare provider will check liver enzymes before starting and during treatment as needed.

Call prescriber For unusual fatigue, loss of appetite, pain in the right upper part of the abdomen, dark or tea-coloured urine, or yellowing of the skin or eyes.

Vaccines

Tell patient Routine inactivated vaccines (tetanus, flu, pneumococcal, meningococcal, COVID-19) generally work normally on dimethyl fumarate and are recommended. Live vaccines (such as MMR, varicella, yellow fever, intranasal flu, live shingles) should be completed before starting therapy and avoided during treatment.

Call prescriber Before any planned vaccination, especially live vaccines or international travel vaccines, and before being exposed to chickenpox or measles if you have not had them before.

Pregnancy & Contraception

Tell patient Information from the manufacturer’s pregnancy registry through 2022 (more than 360 pregnancies) has not shown a clear increase in birth defects. However, animal studies show effects on developing offspring at high doses, and human data remain limited. Hormonal contraception is not affected by dimethyl fumarate based on the available study, but additional methods may be appropriate; discuss family planning before starting and during therapy.

Call prescriber If pregnancy occurs or is being planned. Do not stop the medicine on your own — your team can advise on whether and how to switch or pause therapy. Consider enrolling in the Tecfidera Pregnancy Registry if you become pregnant while on therapy.

Breastfeeding

Tell patient It is not known whether dimethyl fumarate passes into human milk or how much would reach a breastfed infant. Decisions about breastfeeding should weigh the developmental and health benefits of breastfeeding, the mother’s clinical need for therapy, and any potential effects on the infant.

Call prescriber Before breastfeeding while on therapy or before stopping the medicine to breastfeed.

Ref

Sources

Regulatory (PI / SmPC)

Biogen. Tecfidera (dimethyl fumarate) delayed-release capsules — full prescribing information. Revised March 2024. Available at: https://www.accessdata.fda.gov/drugsatfda_docs/label/2024/204063s031lbl.pdf Authoritative source for indication, dosing, warnings and precautions (including the December 2023 addition of serious gastrointestinal reactions), pharmacokinetics, adverse-reaction tables, and pregnancy registry data through 2022.
U.S. Food and Drug Administration. DailyMed: Tecfidera (dimethyl fumarate) labelling. Available at: https://dailymed.nlm.nih.gov/ Maintained repository of current FDA-approved labelling for branded and generic dimethyl fumarate products.
U.S. Food and Drug Administration. Tecfidera (dimethyl fumarate) Information. Available at: https://www.fda.gov/drugs/postmarket-drug-safety-information-patients-and-providers/tecfidera-dimethyl-fumarate-information Postmarket safety updates and communications from the FDA, including the original PML safety communication.

Pivotal Clinical Trials

Gold R, Kappos L, Arnold DL, Bar-Or A, Giovannoni G, Selmaj K, Tornatore C, Sweetser MT, Yang M, Sheikh SI, Dawson KT; DEFINE Study Investigators. Placebo-controlled phase 3 study of oral BG-12 for relapsing multiple sclerosis. N Engl J Med. 2012;367(12):1098–1107. doi: 10.1056/NEJMoa1114287 (PMID: 22992073) Pivotal Phase III DEFINE trial in relapsing-remitting MS demonstrating dose-dependent reductions in relapse rate and disability progression versus placebo; basis for FDA approval.
Fox RJ, Miller DH, Phillips JT, Hutchinson M, Havrdova E, Kita M, Yang M, Raghupathi K, Novas M, Sweetser MT, Viglietta V, Dawson KT; CONFIRM Study Investigators. Placebo-controlled phase 3 study of oral BG-12 or glatiramer in multiple sclerosis. N Engl J Med. 2012;367(12):1087–1097. doi: 10.1056/NEJMoa1206328 (PMID: 22992072) Pivotal Phase III CONFIRM trial including a glatiramer acetate reference arm; supported the BID 240 mg dose and the favourable benefit-risk profile reflected in the Tecfidera label.
Gold R, Arnold DL, Bar-Or A, Fox RJ, Kappos L, Mokliatchouk O, Jiang X, Lyons J, Kapadia S, Miller C. Long-term safety and efficacy of dimethyl fumarate for up to 13 years in patients with relapsing-remitting multiple sclerosis: Final ENDORSE study results. Mult Scler. 2022;28(5):801–816. doi: 10.1177/13524585211037909 (PMID: 34465252) Final results of the long-term ENDORSE extension showing sustained efficacy and a stable safety profile through up to 13 years of dimethyl fumarate therapy.

Guidelines

Rae-Grant A, Day GS, Marrie RA, Rabinstein A, Cree BAC, Gronseth GS, Haboubi M, Halper J, Hosey JP, Jones DE, Lisak R, Pelletier D, Potrebic S, Sitcov C, Sommers R, Stachowiak J, Getchius TSD, Merillat SA, Pringsheim T. Practice guideline recommendations summary: Disease-modifying therapies for adults with multiple sclerosis: Report of the Guideline Development, Dissemination, and Implementation Subcommittee of the American Academy of Neurology. Neurology. 2018;90(17):777–788. doi: 10.1212/WNL.0000000000005347 (Reaffirmed October 2024) AAN consensus practice guideline on starting, switching, and stopping disease-modifying therapies in MS; positions dimethyl fumarate among first-line oral options for relapsing forms.
Rae-Grant A, Day GS, Marrie RA, et al. Comprehensive systematic review summary: Disease-modifying therapies for adults with multiple sclerosis: Report of the Guideline Development, Dissemination, and Implementation Subcommittee of the American Academy of Neurology. Neurology. 2018;90(17):789–800. doi: 10.1212/WNL.0000000000005345 Companion systematic review providing the evidence base for the AAN recommendations.
Montalban X, Gold R, Thompson AJ, et al. ECTRIMS/EAN guideline on the pharmacological treatment of people with multiple sclerosis. Mult Scler. 2018;24(2):96–120. doi: 10.1177/1352458517751049 Joint European guideline that places dimethyl fumarate among approved DMTs for active relapsing MS, with monitoring guidance for lymphocyte counts and PML risk.

Pharmacology & Mechanism

Linker RA, Lee DH, Ryan S, et al. Fumaric acid esters exert neuroprotective effects in neuroinflammation via activation of the Nrf2 antioxidant pathway. Brain. 2011;134(Pt 3):678–692. doi: 10.1093/brain/awq386 Foundational mechanistic study describing Nrf2-mediated antioxidant and neuroprotective effects of fumarates in models of inflammatory CNS disease.
European Medicines Agency. Skilarence (dimethyl fumarate) — Summary of Product Characteristics. Almirall. Available via the EMA website. EU label for the dimethyl fumarate monoproduct approved for moderate-to-severe plaque psoriasis (not available in the US); useful comparator for off-label dermatologic use.
Greenwich Biosciences. Vumerity (diroximel fumarate) — full prescribing information; Banner Life Sciences. Bafiertam (monomethyl fumarate) — full prescribing information. Available at: https://www.accessdata.fda.gov/scripts/cder/daf/ FDA labelling for the related fumarate products in the US, sharing the same active species (MMF) but differing in formulation and tolerability profile.