Efgartigimod (Vyvgart): Complete Drug Monograph

Pharmacokinetic Profile

Terminal Half-Life

80–120 hours (3–5 days)

Volume of Distribution

15–20 L

Pharmacokinetics

Linear up to 50 mg/kg IV (5× recommended) and up to 1,750 mg SC (1.75×)

Catabolism

Proteolytic degradation to peptides and amino acids

Renal Excretion

< 0.1% of IV dose recovered in urine

CYP450 Metabolism

None — no expected CYP-mediated drug interactions

Clinical Information

Drug Class

First-in-class neonatal Fc receptor (FcRn) antagonist; human IgG1 Fc fragment, ~ 54 kDa, produced in CHO cells

Available Doses

Vyvgart IV: 400 mg / 20 mL (20 mg/mL) single-dose vial · Vyvgart Hytrulo SC: 1,008 mg / 11,200 U per 5.6 mL vial (180 mg/mL) or 200 mg/mL prefilled syringe

Route

Vyvgart: IV infusion over 1 hour · Vyvgart Hytrulo: SC injection over 30–90 seconds

Renal Adjustment

No adjustment in mild impairment (mild CKD ↑ exposure ~ 11–22%); insufficient data for moderate or severe impairment

Hepatic Adjustment

No adjustment expected — no PK study performed

Pregnancy

No human data; pregnancy registry available (1-855-272-6524 / Vyvgartpregnancy.com)

Lactation

No human data on milk presence; consider benefits vs maternal need

Schedule / Legal Status

Rx only, non-controlled biologic

Generic / Biosimilar

No biosimilar available

Black Box Warning

None

Indications

Indication	Approved Population	Therapy Type	Status
Generalized myasthenia gravis (gMG) — Vyvgart IV	Adults who are anti-acetylcholine receptor (AChR) antibody positive	Add-on to standard background therapy (acetylcholinesterase inhibitors, corticosteroids, and/or non-steroidal immunosuppressants)	FDA Approved (Dec 2021)
Generalized myasthenia gravis (gMG) — Vyvgart Hytrulo SC	Adults who are anti-AChR antibody positive	Add-on to standard background therapy; same indication as Vyvgart IV with subcutaneous administration	FDA Approved (Jun 2023)
Chronic inflammatory demyelinating polyneuropathy (CIDP) — Vyvgart Hytrulo SC	Adults with definite or probable CIDP (EFNS/PNS criteria); progressing or relapsing forms	Maintenance therapy as continuous once-weekly subcutaneous injections (no cycling)	FDA Approved (Jun 2024)

Efgartigimod is the first commercially available agent that selectively blocks the neonatal Fc receptor (FcRn). FcRn is expressed on endothelial cells, monocytes, and other antigen-presenting cells, where it normally rescues internalised IgG molecules from lysosomal degradation and recycles them back into the circulation. By occupying FcRn with an engineered, high-affinity IgG1 Fc fragment, efgartigimod accelerates the catabolism of all IgG subclasses — including pathogenic autoantibodies — without depleting B cells, complement components, IgM, IgA, IgE, or albumin. The clinical effect is a rapid, reversible, dose-related reduction in total IgG (and consequently autoantibody) levels that begins within days, peaks around weeks 3–4 of a treatment cycle, and recovers over the following weeks. Vyvgart (intravenous) was the first FcRn antagonist approved in the United States (December 2021) for adults with anti-AChR-positive generalized myasthenia gravis. Vyvgart Hytrulo (June 2023) is a subcutaneous co-formulation with recombinant human hyaluronidase that allows the same efgartigimod alfa molecule to be delivered by a brief subcutaneous injection rather than a one-hour intravenous infusion. In June 2024 the SC formulation also became the first FcRn antagonist approved for CIDP, based on the ADHERE trial.

Place in Therapy

Generalized MG: Efgartigimod is positioned as add-on therapy for adults with anti-AChR-antibody-positive disease who remain symptomatic despite standard care (pyridostigmine, corticosteroids, and/or steroid-sparing immunosuppressants). It is given in cycles of four weekly doses, with subsequent cycles individualised to clinical response — distinct from the chronic continuous dosing of complement inhibitors (eculizumab, ravulizumab, zilucoplan) and the FcRn-pathway alternative rozanolixizumab.

CIDP: Efgartigimod (SC only) is given as continuous once-weekly maintenance therapy for adults with definite or probable CIDP, joining intravenous immunoglobulin (IVIG), subcutaneous immunoglobulin (SCIG), corticosteroids, and plasma exchange in the available chronic-care options.

Investigational and Off-Label Considerations

Efgartigimod is being studied across a range of IgG-mediated autoimmune disorders — including pemphigus vulgaris, primary immune thrombocytopenia (ITP), idiopathic inflammatory myopathy, bullous pemphigoid, post-COVID and idiopathic autoimmune encephalitides, lupus nephritis, and Sjögren disease — but at the time of this monograph, only the gMG and CIDP indications listed above are FDA-approved. Off-label use should be approached with the same caution that applies to all biologics: with documented patient consent, specialist supervision, and recognition that the efficacy and safety profile in non-approved indications has not been characterised in registrational trials. Evidence quality outside approved indications: low to moderate (mainly phase 2 / early-phase data).

Dose

Dosing

Dosing depends on both the formulation (Vyvgart IV or Vyvgart Hytrulo SC) and the indication (gMG vs CIDP). For gMG, both formulations are given in cycles of four weekly doses, with subsequent cycles initiated based on clinical response. For CIDP, only the SC formulation is approved, and it is given as continuous once-weekly maintenance dosing without a planned cycle break. Verify the product, indication, and dosing schedule on every order. Live vaccines should be given before, not during, treatment.

Vyvgart (Intravenous) — Generalized Myasthenia Gravis

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Adult, anti-AChR-positive gMG, < 120 kg	10 mg/kg IV over 1 hour	10 mg/kg IV once weekly × 4 weeks per cycle	Capped at 1,200 mg per infusion	Dilute the calculated dose in 0.9% sodium chloride to a total volume of 125 mL; infuse via 0.2-micron in-line filter; flush line with 0.9% NaCl after infusion Each vial = 400 mg / 20 mL (20 mg/mL); use aseptic technique; single-dose vial
Adult, anti-AChR-positive gMG, ≥ 120 kg	1,200 mg IV over 1 hour	1,200 mg IV once weekly × 4 weeks per cycle	1,200 mg per infusion (3 vials)	Fixed dose for patients ≥ 120 kg replaces the per-kg calculation Three 400 mg vials per infusion
Subsequent treatment cycles	Same dose as cycle 1	Cycle of 4 weekly doses	—	Time subsequent cycles by clinical evaluation. Per the FDA prescribing information, the safety of initiating a new cycle sooner than 50 days from the start of the previous cycle has not been established. In ADAPT, the median time to second cycle in efgartigimod-treated patients was 72 days from cycle 1 Reassess MG-ADL / QMG at the end of each cycle to plan timing of the next
Missed dose	—	Administer up to 3 days late, then resume original schedule	—	Do not double up; if delay exceeds 3 days, contact the prescribing centre to plan whether to reset the cycle

Vyvgart Hytrulo (Subcutaneous) — Generalized Myasthenia Gravis

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Adult, anti-AChR-positive gMG (any body weight)	1,008 mg / 11,200 U SC	1,008 mg / 11,200 U SC once weekly × 4 weeks per cycle	Fixed dose; no per-kg adjustment	Inject over 30–90 seconds via a 25G winged infusion set (12-inch tubing, max prime 0.4 mL); abdominal injection ≥ 2–3 inches from the navel; rotate sites; do not dilute Co-formulated with recombinant human hyaluronidase (PH20) — transiently increases SC tissue permeability for ~24–48 h
Subsequent treatment cycles	—	Cycle of 4 weekly SC injections	—	As with Vyvgart IV, safety of initiating a new cycle sooner than 50 days from the start of the previous cycle has not been established

Vyvgart Hytrulo (Subcutaneous) — Chronic Inflammatory Demyelinating Polyneuropathy

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Duration	Notes
Adult with definite or probable CIDP	1,008 mg / 11,200 U SC once weekly	1,008 mg / 11,200 U SC continuous once-weekly dosing	No defined maximum; reassess response periodically	CIDP dosing is continuous — there is no 4-week cycle and no 50-day cycle restriction. In the ADHERE trial, mean treatment duration in stage B was 25 weeks, with placebo-controlled follow-up extending up to 48 weeks Reassess CIDP disability (e.g., aINCAT, I-RODS) at periodic intervals; consider tapering only if sustained remission is documented
Missed dose (gMG or CIDP)	—	Administer up to 3 days late, then resume schedule	—	Do not double up

Population-Specific Considerations

Population	Adjustment	Rationale
Mild renal impairment (eGFR 60–89 mL/min/1.73 m²)	No dose adjustment	Population PK analyses showed a 22% increase in IV exposure and an 11–20% increase in SC exposure relative to normal renal function; not considered clinically significant
Moderate (eGFR 30–59) or severe (eGFR < 30 mL/min/1.73 m²) renal impairment	Insufficient data — use with caution	No dedicated PK study; safety not established
Hepatic impairment	No dedicated guidance	Hepatic impairment is not expected to affect pharmacokinetics — efgartigimod is catabolised proteolytically rather than by the liver
Geriatric (≥ 65 years)	No specific adjustment	Clinical studies did not enrol sufficient older patients to determine differential response, but population PK suggests no clinically meaningful effect of age
Pediatric (< 18 years)	Not established	Safety and effectiveness in pediatric patients have not been established for any indication
Pregnancy	Individualised — enrol in pregnancy registry	No human data; transplacental IgG transfer increases through pregnancy and reduction in maternal IgG is expected to reduce passive immunity to the newborn — defer live or live-attenuated vaccines in exposed infants until safe

Clinical Pearl — Cycle Timing in gMG vs Continuous Dosing in CIDP

In gMG, efgartigimod is given as cycles of four weekly doses, after which the patient is observed for clinical and serological response. The next cycle is timed by symptom recurrence — typically 4 to 12+ weeks later — but cannot start sooner than 50 days from the start of the previous cycle (FDA PI). Many patients re-treat at intervals approximating their individual IgG re-accumulation time; the median time to a second cycle in ADAPT was 72 days. In contrast, CIDP dosing is continuous once-weekly with no cycle break — interruption risks relapse, as demonstrated by the ADHERE stage B placebo-withdrawal data (hazard ratio for clinical deterioration 0.394 favouring efgartigimod). Confirm the indication on every order before scheduling subsequent doses.

Important — Vyvgart IV ≠ Vyvgart Hytrulo SC; Doses Are Not Interchangeable

Vyvgart (efgartigimod alfa-fcab) is a 10 mg/kg intravenous dose (or 1,200 mg fixed dose at ≥ 120 kg) delivered over one hour. Vyvgart Hytrulo (efgartigimod alfa and hyaluronidase-qvfc) is a fixed 1,008 mg / 11,200 U subcutaneous dose delivered over 30–90 seconds; it contains co-formulated recombinant human hyaluronidase that the IV product does not. Patients with a history of serious hypersensitivity to hyaluronidase cannot receive Vyvgart Hytrulo even if they previously tolerated Vyvgart IV. Verify product, route, and indication on every order; use distinct order sets if your institution allows both formulations.

Pharmacology

Mechanism of Action

Efgartigimod alfa is an Fc fragment derived from human IgG1 (the za allotype) and engineered for high-affinity, pH-dependent binding to the neonatal Fc receptor (FcRn). FcRn does not recognise IgG at neutral plasma pH, but in the acidic environment of endosomes inside endothelial and antigen-presenting cells it captures internalised IgG and recycles it back to the cell surface, releasing it into the circulation. This recycling mechanism is the reason endogenous IgG has an unusually long half-life of approximately three weeks. By saturating FcRn with a competitive Fc fragment that does not have an antigen-binding (Fab) region, efgartigimod prevents this recycling: internalised endogenous IgG, including pathogenic autoantibodies against the acetylcholine receptor (in gMG) or against peripheral nerve antigens (in CIDP), is shunted to the lysosome and degraded. The result is a rapid, reversible, dose-dependent reduction in total IgG of approximately 60–70% by week 4 of a treatment cycle, with proportional reductions in IgG-subtype autoantibodies. Importantly, efgartigimod does not bind antigen, does not deplete B cells or plasma cells, and does not reduce IgM, IgA, IgE, complement components, or albumin — distinguishing it pharmacologically from broad immunosuppressants and from complement inhibitors. The hyaluronidase component of Vyvgart Hytrulo is unrelated to the IgG-lowering effect: it transiently depolymerises hyaluronan in the subcutaneous interstitium to permit dispersion of the larger SC injection volume; the effect resolves within 24–48 hours.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	IV: 100% bioavailable (intravenous administration). SC: bioavailability not separately reported in the FDA PI; pharmacodynamic noninferiority to IV demonstrated in ADAPT-SC (mean total IgG reduction at day 29: 66.4% SC vs 62.2% IV)	Both formulations achieve clinically equivalent IgG-lowering at the recommended doses; SC offers reduced chair time and the option of administration outside a dedicated infusion suite
Distribution	Volume of distribution 15–20 L; consistent with predominantly vascular and interstitial-fluid distribution typical of a 54 kDa Fc fragment; no information on placental or breast-milk transfer in humans, but transplacental IgG transfer increases through pregnancy	Reduction in maternal IgG during pregnancy is expected to reduce passive immunity to the newborn — defer live or live-attenuated vaccines in exposed infants and individualise risk-benefit
Metabolism	Catabolism by widespread proteolytic enzymes to small peptides and amino acids; not metabolised by cytochrome P450 enzymes	Negligible CYP-mediated drug interactions; no specific hepatic-impairment dose adjustment
Elimination	Terminal half-life 80–120 hours (3–5 days); < 0.1% of an IV dose recovered in urine; PK is approximately linear up to 50 mg/kg IV (5× the recommended dose) and up to 1,750 mg SC (1.75× the recommended dose)	The relatively short half-life (compared with intact IgG, which is ~ 21 days) is intentional: it mediates rapid IgG turnover during dosing, then rapid recovery between cycles, allowing intermittent re-treatment in gMG. Renal impairment has minimal effect; hepatic impairment is not expected to be relevant

How efgartigimod differs from other gMG biologics

Efgartigimod is mechanistically distinct from the other targeted therapies approved for AChR-positive gMG. Complement inhibitors (eculizumab, ravulizumab, zilucoplan) block terminal complement activity at C5, preventing membrane attack complex formation at the neuromuscular junction. FcRn antagonists (efgartigimod, rozanolixizumab) lower circulating IgG, reducing the supply of pathogenic AChR autoantibodies. The two strategies have complementary biology, different infection-risk profiles (meningococcal precautions are essential for complement inhibitors but not FcRn antagonists), and different administration logistics (continuous chronic dosing for complement inhibitors vs cyclical or weekly dosing for FcRn antagonists).

Side Effects

The overall safety profile of efgartigimod has been characterised primarily in three pivotal trials: ADAPT (Vyvgart IV in gMG, n = 84 vs 83 placebo), ADAPT-SC (Vyvgart Hytrulo SC vs Vyvgart IV in gMG, n = 55 vs 55), and ADHERE stage B (Vyvgart Hytrulo SC vs placebo in CIDP, n = 111 vs 110). Most adverse reactions are mild to moderate, related either to the route of administration (infusion-related reactions for IV; injection site reactions for SC) or to the predictable consequences of lowering total IgG (mild increase in infections, especially upper respiratory and urinary tract). Serious infections, hypersensitivity reactions, and infusion-related reactions are uncommon but clinically important and are highlighted in the FDA prescribing information.

≥10% Very Common — Vyvgart IV in gMG (Study 1 / ADAPT)

Adverse Effect	Vyvgart IV (n = 84)	Placebo (n = 83)	Clinical Note
Respiratory tract infection	33%	29%	Includes upper and lower RTI; majority mild to moderate
Headache (incl. migraine, procedural headache)	32%	29%	Not consistently dose-related; usually responsive to standard analgesia
Urinary tract infection	10%	5%	Approximately twice the placebo rate; counsel patients on prompt reporting of urinary symptoms

For Vyvgart Hytrulo SC in gMG (Study 2 / ADAPT-SC): the most common adverse reactions reported in ≥ 10% of patients were injection site reactions and headache. Injection site reactions occurred in 38% of patients receiving SC efgartigimod (Study 2 and its open-label extension, n = 168); all were mild to moderate, none led to treatment discontinuation, and incidence decreased with each subsequent cycle.

5–10% Common (gMG, IV; reported in ≥ 5% and more frequently than placebo)

Adverse Effect	Vyvgart IV	Placebo	Clinical Note
Paraesthesia (incl. oral hypoaesthesia, hypoaesthesia, hyperaesthesia)	7%	5%	Mostly mild and transient
Myalgia	6%	1%	Important to distinguish from MG-related muscle weakness or worsening

CIDP-specific adverse reactions (Study 3 / ADHERE stage B, n = 111): injection site reactions occurred in 15% of Vyvgart Hytrulo-treated patients vs 6% with placebo; the most common were injection site bruising and erythema. All injection site reactions were mild to moderate; most occurred during the first 3 months of treatment.

Serious Serious Adverse Reactions

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Anaphylaxis / serious hypersensitivity reactions	Postmarketing reports — frequency not quantified	During administration or within 1 hour; some hypersensitivity (rash, angioedema, dyspnoea) reported up to 3 weeks post-dose	Discontinue the infusion/injection; institute appropriate supportive measures; consider permanent discontinuation if severe; future doses are contraindicated after a serious hypersensitivity reaction
Hypotension leading to syncope	Postmarketing reports — frequency not quantified	During or within 1 hour of administration	Discontinue the dose; supportive care including IV fluids and supine positioning; contraindicated for further use after a serious episode
Infusion-related reactions (Vyvgart IV) — hypertension, chills, shivering, thoracic / abdominal / back pain	Postmarketing reports — frequency not quantified	During or within 1 hour of infusion	Severe: discontinue; weigh risks/benefits of re-administration. Mild–moderate: rechallenge with close clinical observation, slower infusion rate, and pre-medications
Serious infection	Uncommon at recommended dosing; frequency not separately quantified in PI	Any time during therapy	Delay efgartigimod administration if active infection; treat infection appropriately; consider withholding until resolved
Below-normal hematology values (WBC, lymphocyte, neutrophil counts)	In Study 1: WBC < LLN 12% (vs 5% placebo); lymphocyte < LLN 28% (vs 19%); neutrophil < LLN 13% (vs 6%)	During cycles	Most are mild to moderate; periodic CBC monitoring is reasonable, particularly in patients on concomitant immunosuppression
Reduced response to vaccinations / loss of passive immunity in pregnancy	Expected pharmacological consequence of IgG reduction	During treatment cycles; for neonates of treated mothers, throughout exposure period	Update age-appropriate vaccinations before each treatment cycle; do not give live vaccines during therapy; defer live or live-attenuated vaccines in infants exposed in utero until safe

Discontinuation & Immunogenicity Treatment Discontinuation, Anti-Drug Antibodies

Vyvgart IV in gMG (Study 1)

20% ADA over 26 wk

Anti-drug antibodies: 17/83 (20%) developed antibodies; 6/83 (7%) developed neutralizing antibodies. Hypersensitivity reactions in clinical trials were mild to moderate and did not lead to discontinuation.

Vyvgart Hytrulo SC vs IV (Study 2)

35% / 20% ADA SC / IV at ~10 wk

Anti-drug antibodies: 19/55 (35%) SC vs 11/55 (20%) IV. Neutralizing antibodies: 2/55 (4%) in each arm. Available data are too limited to draw firm conclusions about clinical impact.

Reason for Treatment Modification	Frequency / Context	Action
Active infection	Per protocol	Delay administration until the infection has resolved; treat appropriately; consider withholding subsequent doses for serious infection
Serious hypersensitivity reaction (anaphylaxis, hypotensive syncope)	Per FDA PI	Permanent discontinuation; future use of efgartigimod alfa products (and, for Vyvgart Hytrulo, hyaluronidase products) is contraindicated
Severe infusion-related reaction (Vyvgart IV)	Per FDA PI	Discontinue the infusion; consider risks and benefits of readministration. Mild-moderate reactions may be rechallenged with slower rate and pre-medication
Loss of clinical response in gMG	Per clinical evaluation	Reassess timing of next cycle; consider switching mechanism (e.g., complement inhibitor) if multi-cycle response wanes
Loss of efficacy or relapse in CIDP	Per clinical evaluation	Confirm the diagnosis (consider chronic immune-mediated alternatives); review whether dose interruptions occurred; coordinate with neuromuscular specialist for next-line therapy (IVIG, SCIG, corticosteroids, or plasma exchange)

Management Pearl — Vaccination Planning Is Time-Sensitive

Because efgartigimod transiently lowers total IgG (including vaccine-specific antibodies), vaccination should be planned before, not during, treatment cycles. The FDA prescribing information directs clinicians to evaluate the need for age-appropriate vaccines according to immunization guidelines before initiating each new cycle, and explicitly recommends against live-attenuated vaccines during therapy. Practical strategy: at the time of gMG diagnosis or before the first cycle, update inactivated vaccines (annual influenza, COVID-19 boosters, pneumococcal series, recombinant zoster, hepatitis B if applicable) and bring live vaccines (MMR, varicella, yellow fever) up to date if needed. For CIDP — where dosing is continuous — vaccinations should be updated before initiation; live vaccines are generally avoided thereafter, with timing of any necessary live vaccine considered in collaboration with infectious-disease and neurology teams.

Int

Drug Interactions

Efgartigimod has a relatively narrow drug-interaction profile: it is not metabolised by cytochrome P450 enzymes, no clinical drug-interaction studies have been conducted, and standard small-molecule pharmacokinetic interactions are not expected. The clinically meaningful interactions are pharmacodynamic and arise from two mechanisms — (1) competition with co-administered IgG-based or IgG-Fc-containing therapies for FcRn binding, and (2) the immune effects of lowering circulating IgG. The interactions below are drawn from the FDA prescribing information (Section 7) and from the established pharmacology of FcRn antagonism.

Major Immunoglobulin products (IVIG / SCIG)

MechanismBoth compete for FcRn binding; efgartigimod accelerates clearance of all IgG, including therapeutic IgG

EffectReduced effectiveness of IVIG/SCIG replacement or immunomodulation

ManagementAvoid concomitant chronic use; if both are essential, consider discontinuing efgartigimod and using alternative therapy. In CIDP transitions, plan a deliberate hand-off rather than overlap

FDA PI 7.1

Major Therapeutic monoclonal antibodies (Fc-containing IgG mAbs)

MechanismEfgartigimod accelerates clearance of any agent that uses an IgG Fc domain to bind FcRn

EffectLower systemic exposure and potentially reduced effectiveness of co-administered mAbs (e.g., rituximab, infliximab, eculizumab, ravulizumab, anti-PD-1 agents)

ManagementClosely monitor for reduced effectiveness of the co-administered mAb. When concomitant long-term use is essential for patient care, consider discontinuing efgartigimod and using an alternative therapy

FDA PI 7.1

Major Live or live-attenuated vaccines

MechanismReduced IgG impairs the natural antibody response that limits replication of attenuated organisms

EffectTheoretical risk of vaccine-related illness; immune response to vaccination during treatment is unknown

ManagementVaccination with live vaccines is not recommended during treatment with efgartigimod. Update live vaccinations (MMR, varicella, yellow fever) before initiating therapy where feasible

FDA PI 5.1, 2.1

Moderate Concomitant immunosuppressants (corticosteroids, azathioprine, mycophenolate)

MechanismAdditive effects on innate / adaptive immunity

EffectTheoretical increase in serious-infection risk; in pivotal trials > 70% of patients received concomitant steroids and ~ 60% non-steroidal immunosuppressants without reported additive serious-infection signals

ManagementCombination is permitted by the FDA PI and was the rule rather than the exception in ADAPT and ADHERE; monitor clinically for infection and consider periodic CBC if infection-risk concern is high

Based on ADAPT / ADHERE trial design

Moderate Other FcRn antagonists (rozanolixizumab, nipocalimab)

MechanismBoth target FcRn; combined use has not been studied

EffectExcessive IgG reduction with possible additive infection risk

ManagementAvoid simultaneous use; if switching between FcRn antagonists, allow appropriate washout and re-baseline IgG-mediated immunity expectations

Class-effect / clinical practice

Minor Small-molecule drugs metabolised by CYP450 enzymes

MechanismEfgartigimod is not metabolised by CYP450 and does not modulate CYP activity

EffectClassical pharmacokinetic interactions are unlikely

ManagementNo specific dose adjustment for routine small-molecule co-medications

FDA PI 12.3

Mon

Monitoring

Monitoring of efgartigimod therapy is largely clinical — symptom response, infection surveillance, and watchfulness for infusion-related and hypersensitivity reactions. Routine measurement of total IgG levels is not required by the FDA prescribing information for clinical decision-making, although some specialty centres track total IgG to characterise pharmacodynamic response or to time subsequent gMG cycles. The most consistent monitoring requirement is a structured pre-cycle vaccination check.

Vaccination Status Before initiation; before each new gMG cycle
Routine Per FDA PI: evaluate need to administer age-appropriate vaccines according to immunization guidelines before initiation of a new treatment cycle. Do not give live vaccines during therapy. Coordinate with primary care to update inactivated vaccines (influenza, COVID-19, pneumococcal, zoster, hepatitis B as indicated).
Active Infection Screen Before each dose
Routine Ask specifically about urinary, respiratory, and skin/soft-tissue symptoms. Defer the dose if active infection is present; treat first and reassess.
Symptom Response (gMG) End of each cycle and 4 weeks later
Routine Use a structured tool — MG-ADL is the validated instrument from the ADAPT trial (≥ 2-point reduction at 4+ consecutive weeks defined a responder). QMG is the secondary assessment. The pattern of response and recurrence informs the timing of the next cycle.
Symptom Response (CIDP) Periodic during continuous weekly therapy
Routine Use aINCAT (adjusted Inflammatory Neuropathy Cause and Treatment disability score), I-RODS, and grip strength as in the ADHERE trial. A ≥ 1-point increase in aINCAT (with confirmation) defined clinical deterioration.
Infusion-Related / Hypersensitivity Surveillance During and after each dose
Routine For Vyvgart IV: monitor during infusion and for 1 hour thereafter for signs and symptoms of hypersensitivity. For Vyvgart Hytrulo SC: monitor for at least 30 minutes after administration. Train staff to recognise anaphylaxis, angioedema, hypotension, dyspnoea, and severe infusion-related reactions.
Complete Blood Count Before initiation; periodically during therapy
Trigger-based Below-normal WBC, lymphocyte, and neutrophil counts are more common with efgartigimod than placebo (12% vs 5%, 28% vs 19%, 13% vs 6%, respectively, in Study 1). Most are mild to moderate, but periodic CBC is reasonable in patients on concomitant immunosuppression or those with recurrent infections.
Total IgG (Optional) Per institutional protocol
Trigger-based Not required by the FDA PI. Some centres measure total IgG at baseline and at end of cycle to characterise individual response or to inform cycle timing in gMG. Mean reduction at week 4 was approximately 60–70% in pivotal trials.
Pregnancy and Breastfeeding At initiation; if pregnancy planned/discovered
Trigger-based Discuss the pregnancy registry (1-855-272-6524 / Vyvgartpregnancy.com). Plan delivery and neonatal care with an awareness that maternal IgG reduction may reduce passive immunity and that live vaccines should be deferred in exposed infants.

Contraindications & Cautions

Absolute Contraindications

Vyvgart IV: Serious hypersensitivity to efgartigimod alfa products or to any of the excipients of Vyvgart. Reactions in the FDA PI include anaphylaxis and hypotension leading to syncope.
Vyvgart Hytrulo SC: Serious hypersensitivity to efgartigimod alfa products, to hyaluronidase, or to any of the excipients of Vyvgart Hytrulo. The hyaluronidase contraindication applies even if the patient previously tolerated Vyvgart IV.

Relative Contraindications (Specialist Input Recommended)

Active serious infection — defer initiation or subsequent doses until the infection is resolved (FDA PI Section 5.1).
Recent live or live-attenuated vaccine — schedule live vaccines before initiation where feasible; live vaccines are not recommended during therapy.
Concomitant chronic IVIG, SCIG, or other Fc-containing biologic therapy — efficacy of either agent may be reduced. If both are clinically needed, consider an alternative for one, with neuromuscular-specialist input.
Hypogammaglobulinaemia at baseline — although the PI does not specify a contraindication, profound baseline IgG depletion (e.g., from prior rituximab plus IVIG) may amplify infection risk; specialist immunology input is appropriate.

Use with Caution

Pregnancy — no human data; maternal IgG reduction reduces passive immunity to the newborn. Enrol in the pregnancy registry; defer live vaccines in exposed infants until safe (FDA PI Section 8.1).
Lactation — no data on breast-milk presence; weigh maternal need against potential infant exposure (FDA PI Section 8.2).
Pediatric patients — safety and effectiveness not established (FDA PI Section 8.4).
Geriatric patients (≥ 65 years) — clinical trials enrolled limited numbers; population PK suggests no clinically meaningful effect of age, but individual evaluation is appropriate.
Moderate (eGFR 30–59) or severe (eGFR < 30 mL/min/1.73 m²) renal impairment — insufficient data; use with caution.
History of recurrent UTI or other infections — UTI was approximately twice as common in efgartigimod-treated patients as placebo in Study 1; counsel patients to report symptoms early.

No FDA Boxed Warning

At the time of this monograph, neither Vyvgart nor Vyvgart Hytrulo carries an FDA boxed warning. The FDA prescribing information’s most prominent safety messages are the warnings and precautions for infections, hypersensitivity reactions (including postmarketing anaphylaxis and hypotension), and infusion-related reactions, plus the recommendation to optimise vaccination status before each new cycle.

Patient Counselling

Purpose of Therapy

Explain in plain language that efgartigimod works by lowering the level of certain antibodies (called immunoglobulin G, or IgG) in the blood. In myasthenia gravis and CIDP, some of these antibodies attack the body’s own nerves and muscles; lowering them improves nerve-to-muscle communication (in MG) or nerve function (in CIDP). The medicine is not a cure, but it can substantially reduce symptoms while it is being given. The effect builds up over the four weekly doses of a cycle and then gradually wears off — which is why the next gMG cycle is timed by the return of symptoms, and why CIDP treatment is continued every week without breaks.

How to Take

Vyvgart (the IV form) is given as a one-hour infusion in an infusion clinic; expect to stay for an additional hour of monitoring afterwards. Vyvgart Hytrulo (the SC form) is given as a brief injection (30–90 seconds) into the abdominal skin by a healthcare professional, with at least 30 minutes of post-injection monitoring. Plan to remain reachable for the day after each dose so that any delayed reactions can be reported. Mark the date of every dose on a calendar, and bring an updated medication and vaccine list to every clinic visit.

Infections — Especially Urinary and Respiratory

Tell patient Lowering IgG modestly increases the risk of common infections, especially urinary tract infections and upper respiratory infections. Most are mild and respond to standard antibiotics, but they should be treated promptly.

Call prescriber Burning or pain on urination, fever, cough with phlegm, breathing difficulty, severe sore throat, or any infection that is not improving in a few days. If you are due for a dose and are unwell, contact the centre before attending.

Allergic and Infusion Reactions

Tell patient Some patients experience reactions during or shortly after a dose — typically a rash, swelling, dizziness, or pain in the chest, abdomen, or back. Most are mild and treatable on the spot. Rarely, severe allergic reactions (anaphylaxis) can occur during or within an hour of a dose.

Call prescriber Difficulty breathing, swelling of the lips or throat, severe dizziness or fainting, widespread rash or hives — call emergency services first. Tell the team about any rash, itching, or feeling unwell after a dose, even if it resolves.

Vaccinations

Tell patient Stay up to date on age-appropriate inactivated vaccines (annual flu, COVID-19 boosters, pneumococcal, shingles, hepatitis B if indicated). Live vaccines (such as MMR, varicella, and yellow fever) should usually be given before starting therapy, and should not be given during therapy without specialist advice. Tell your doctor about any planned travel that might require live vaccines.

Call prescriber Before any vaccination — including travel vaccines — and before any planned pregnancy, so that vaccinations and treatment can be sequenced safely.

Surgery, Other Biologic Therapies, and IVIG

Tell patient Always tell surgeons, anaesthetists, and other specialists that you are receiving efgartigimod. If another biologic medicine (such as IVIG, SCIG, rituximab, eculizumab, or another monoclonal antibody) is recommended for any condition, your treatment teams need to coordinate — efgartigimod can reduce the effectiveness of these other therapies.

Call prescriber If a new biologic is being prescribed, before starting; if elective surgery is planned, to discuss timing of doses around the procedure.

Pregnancy, Breastfeeding, and Family Planning

Tell patient There is no human safety data for efgartigimod in pregnancy. If you become pregnant or are planning a pregnancy, your team will help weigh the benefits and risks. There is a confidential pregnancy registry (1-855-272-6524 / Vyvgartpregnancy.com) — participation helps generate safety information for future patients. Babies born to mothers on efgartigimod may temporarily have lower antibody levels, so live vaccines for the infant may need to be delayed.

Call prescriber If you become pregnant, are planning pregnancy, or are breastfeeding while on efgartigimod.

Disease Flare or Worsening (gMG)

Tell patient The benefit of each gMG cycle wears off gradually. Many patients notice symptoms returning before the next cycle is due — this is expected. Do not adjust other myasthenia medicines on your own; coordinate the timing of the next cycle with your neurology team based on how you are feeling.

Call prescriber Sudden severe weakness, swallowing difficulty, slurred speech, or breathing difficulty — these can signal myasthenic crisis and need urgent assessment, regardless of the timing in the cycle.

Ref

Sources

Regulatory (PI / SmPC)

VYVGART® (efgartigimod alfa-fcab) injection, for intravenous use, and VYVGART® HYTRULO (efgartigimod alfa and hyaluronidase-qvfc) injection, for subcutaneous use — Combined US Prescribing Information. argenx US, Inc. Revised August 2024 (Reference ID 5427102). accessdata.fda.gov Primary FDA label combining both formulations and all approved indications (gMG for IV and SC; CIDP for SC only). Source for all dosing, contraindications, warnings, adverse-event frequencies, pharmacokinetics, immunogenicity figures, and clinical-trial summaries cited in this monograph.
FDA News Release: FDA Approves New Treatment for Myasthenia Gravis. U.S. Food and Drug Administration. December 17, 2021. fda.gov FDA announcement of the initial approval of Vyvgart (efgartigimod alfa-fcab) — the first FcRn antagonist for any disease and the first new gMG mechanism since the approval of complement inhibition.

Key Clinical Trials

Howard JF Jr, Bril V, Vu T, et al. Safety, efficacy, and tolerability of efgartigimod in patients with generalised myasthenia gravis (ADAPT): a multicentre, randomised, placebo-controlled, phase 3 trial. Lancet Neurol. 2021 Jul;20(7):526-536. doi: 10.1016/S1474-4422(21)00159-9. PMID: 34146511. pubmed.ncbi.nlm.nih.gov/34146511 Pivotal phase 3 ADAPT trial that established the efficacy of intravenous efgartigimod in adults with gMG. Source for the MG-ADL responder rate (67.7% vs 29.7% placebo) and QMG responder rate (63.1% vs 14.1% placebo) in the AChR-Ab-positive subgroup that supported FDA approval.
Howard JF Jr, Vu T, Li G, et al. Subcutaneous efgartigimod PH20 in generalized myasthenia gravis: A phase 3 randomized noninferiority study (ADAPT-SC) and interim analyses of a long-term open-label extension study (ADAPT-SC+). Neurotherapeutics. 2024 Sep 2;e00378. doi: 10.1016/j.neurot.2024.e00378. PMID: 39227284. pubmed.ncbi.nlm.nih.gov/39227284 Pharmacodynamic noninferiority study comparing the SC and IV formulations in gMG; supported the 2023 FDA approval of Vyvgart Hytrulo. Source for the day-29 IgG reduction comparison (66.4% SC vs 62.2% IV) and the SC immunogenicity figures.
Allen JA, Lin J, Basta I, et al. Safety, tolerability, and efficacy of subcutaneous efgartigimod in patients with chronic inflammatory demyelinating polyradiculoneuropathy (ADHERE): a multicentre, randomised-withdrawal, double-blind, placebo-controlled, phase 2 trial. Lancet Neurol. 2024. doi: 10.1016/S1474-4422(24)00309-0. PMID: 39304241. pubmed.ncbi.nlm.nih.gov/39304241 Pivotal ADHERE trial that supported the June 2024 FDA approval of Vyvgart Hytrulo for CIDP. Source for the stage-A response rate, the stage-B hazard ratio for clinical deterioration (HR 0.394, 95% CI 0.253-0.614, p < 0.0001), and the CIDP-specific safety profile.
Howard JF Jr, Bril V, Burns TM, et al; Efgartigimod MG Study Group. Randomized phase 2 study of FcRn antagonist efgartigimod in generalized myasthenia gravis. Neurology. 2019 Jun 4;92(23):e2661-e2673. doi: 10.1212/WNL.0000000000007600. PMID: 31118245. pubmed.ncbi.nlm.nih.gov/31118245 Foundational phase 2 study that established proof of concept for FcRn antagonism in autoimmune disease and provided the rationale for the ADAPT trial design.

Guidelines

Narayanaswami P, Sanders DB, Wolfe G, et al. International Consensus Guidance for Management of Myasthenia Gravis: 2020 Update. Neurology. 2021 Jan 19;96(3):114-122. doi: 10.1212/WNL.0000000000011124. PMID: 33144515. doi.org/10.1212/WNL.0000000000011124 International consensus guidance for the management of myasthenia gravis. Verify the current edition at time of publication — the consensus is updated periodically and a new revision may incorporate FcRn antagonists more explicitly.
Van den Bergh PYK, van Doorn PA, Hadden RDM, et al. European Academy of Neurology/Peripheral Nerve Society Guideline on diagnosis and treatment of chronic inflammatory demyelinating polyradiculoneuropathy: Report of a joint Task Force — Second revision. J Peripher Nerv Syst. 2021 Sep;26(3):242-268. doi: 10.1111/jns.12455. PMID: 34085743. doi.org/10.1111/jns.12455 EAN/PNS 2021 second-revision guideline on the diagnosis and management of CIDP — provides the EFNS/PNS diagnostic criteria used to enrol the ADHERE trial. Verify the most recent version at time of publication.

Mechanistic / Basic Science

Roopenian DC, Akilesh S. FcRn: the neonatal Fc receptor comes of age. Nat Rev Immunol. 2007 Sep;7(9):715-725. doi: 10.1038/nri2155. PMID: 17703228. pubmed.ncbi.nlm.nih.gov/17703228 Foundational review of neonatal Fc receptor biology that underpins the rationale for FcRn antagonism as a therapeutic strategy in IgG-mediated autoimmune disease.
Ulrichts P, Guglietta A, Dreier T, et al. Neonatal Fc receptor antagonist efgartigimod safely and sustainably reduces IgGs in humans. J Clin Invest. 2018 Oct 1;128(10):4372-4386. doi: 10.1172/JCI97911. PMID: 30040076. pubmed.ncbi.nlm.nih.gov/30040076 First-in-human study characterising the IgG-lowering pharmacodynamics of efgartigimod, including dose-response, selectivity for IgG over other immunoglobulin classes, and tolerability — the basis for the dose selection used in the phase 2 and phase 3 programmes.

Pharmacokinetics / Special Populations

VYVGART / VYVGART HYTRULO Section 12.3 — Pharmacokinetics. argenx US, Inc. Revised August 2024 (Reference ID 5427102). accessdata.fda.gov Primary source for the volume of distribution (15–20 L), terminal half-life (80–120 h), linear PK boundaries, urinary recovery (< 0.1%), absence of CYP metabolism, and renal-impairment population PK figures (mild renal impairment increases exposure ~ 11–22%).
Heo YA. Efgartigimod: First Approval. Drugs. 2022 Mar;82(3):341-348. doi: 10.1007/s40265-022-01678-3. PMID: 35179720. pubmed.ncbi.nlm.nih.gov/35179720 Approval-summary review of efgartigimod’s pharmacology, clinical development, and place in therapy at the time of initial FDA approval — a useful single-source summary of the early evidence package.

Vyvgart / Vyvgart Hytrulo (Efgartigimod)