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Nirsevimab

Nirsevimab, sold under the brand name Beyfortus, is a humanized designed to prevent lower disease caused by () in neonates and infants entering their first season, as well as in certain high-risk children up to 24 months old entering their second season. It provides passive by to the prefusion form of the F , thereby neutralizing the and inhibiting its entry into cells, with an extended of approximately 71 days due to engineered modifications. Approved by the in October 2022 and by the U.S. in July 2023, nirsevimab represents a significant advancement in prevention, particularly for vulnerable infants born preterm or with underlying conditions that increase the risk of severe disease. In May 2025, the outlined recommendations supporting the use of long-acting monoclonal antibodies like nirsevimab for prevention in infants globally. Developed jointly by and , nirsevimab emerged from research aimed at addressing the high burden of , which is the leading cause of hospitalization among infants worldwide, affecting an estimated 3.4 million children under 5 years annually and contributing to over 100,000 deaths. Clinical trials, including the phase 3 and studies, demonstrated its efficacy: in , a single dose reduced medically attended lower respiratory tract infections by 74.5% compared to in healthy preterm and term infants, while the trial showed an 83.2% reduction in -associated hospitalizations in preterm infants across . These results highlight nirsevimab's role in reducing not only severe outcomes like hospitalization but also milder infections, with consistent protection observed in diverse populations, including those at higher risk for complications. According to current guidelines from the Centers for Disease Control and Prevention (CDC) as of 2025, nirsevimab is recommended as a single intramuscular dose for all infants younger than 8 months born during or entering their first RSV season, regardless of maternal immunization status, and for high-risk children aged 8 through 19 months entering their second season. Dosing is weight-based: 50 mg for infants weighing less than 5 kg and 100 mg for those 5 kg or more in the first season, with a 200 mg dose (two 100 mg injections) for the second season in eligible children; it can be co-administered with routine childhood vaccines without interference. Safety data from trials indicate a favorable profile, with common side effects limited to injection-site reactions and rash, though hypersensitivity reactions are possible, necessitating caution in individuals with bleeding disorders or prior allergies to monoclonal antibodies. Overall, nirsevimab's introduction has transformed RSV prophylaxis, offering a targeted, long-acting option that complements maternal vaccination strategies and reduces the healthcare burden of this seasonal pathogen.

Medical uses

Indications

Nirsevimab is indicated for the prevention of (RSV)-associated (LRTI) in neonates and infants born during or entering their first RSV season. This targets the RSV fusion (F) protein to neutralize the virus and prevent infection in this vulnerable population. In the United States, the indication extends to children up to 24 months of age who remain vulnerable to severe RSV disease through their second RSV season, particularly those at increased risk such as preterm infants, infants with chronic lung disease, or those with congenital heart disease. Efficacy data from pivotal trials support these indications, with the MELODY phase 3 trial demonstrating a 74.5% reduction (95% CI, 65.9 to 81.0) in medically attended RSV LRTI among healthy late-preterm and term infants entering their first RSV season. Similarly, the HARMONIE phase 3 trial showed an 83.2% reduction (95% CI, 67.8 to 92.0) in RSV-associated LRTI hospitalizations in infants during their first RSV season. For the 2025-2026 season, the Centers for Disease Control and Prevention (CDC) and American Academy of Pediatrics (AAP) recommend a single dose of nirsevimab for all infants younger than 8 months entering their first season, regardless of maternal vaccination status if unknown or unprotected. As of 2025, is no longer routinely recommended, with availability ending December 31, 2025, positioning nirsevimab as the primary immunoprophylaxis for eligible infants. For children aged 8 to 19 months at increased risk for severe disease entering their second season, such as those with chronic lung disease of prematurity or severe immunocompromise, nirsevimab is also recommended. European Union authorization, aligned with the (), indicates nirsevimab for the prevention of lower respiratory tract disease in neonates and infants during their first season, and in children up to 24 months of age who remain vulnerable to severe disease through their second season. National guidelines may vary.

Dosing and administration

Nirsevimab is administered as a single for the prevention of () lower respiratory tract disease in infants during their first season. For neonates and infants entering their first season who weigh less than 5 kg, the recommended dose is 50 mg (0.5 mL) administered . For those weighing 5 kg or more, the dose is 100 mg (1 mL) administered . These doses are provided via pre-filled syringes and should be inspected for particulates or discoloration prior to use. For children 8 through 19 months of age at increased risk of severe disease entering their second season, a single dose of 200 mg is recommended, administered as two separate 100 mg (1 mL) injections in the anterolateral aspect of both . The injection site for all doses is preferably the anterolateral , using a 22- to 25-gauge needle of appropriate length (e.g., ⅝ inch for newborns); the gluteal area should be avoided. Nirsevimab should not be mixed with other medications or vaccines in the same . Timing of administration aligns with the RSV season, typically from 1 through March 31 in most regions, though local may adjust this window. For infants born during the season, the dose is ideally given within the first week of life, often during birth hospitalization. Infants born outside the season should receive it prior to the start (e.g., or ). A single dose provides season-long protection without the need for boosters. Nirsevimab can be co-administered with routine infant vaccines, including DTaP, PCV13, Hib, IPV, and , as well as live vaccines such as MMR and varicella, using separate syringes and sites; no interval is required. For infants born to mothers who received an vaccine during pregnancy, nirsevimab is generally not needed if the maternal dose was administered between 32 and 36 weeks gestation and the infant is born ≥14 days after; however, it may be considered in rare cases such as maternal immunocompromise, poor transfer, or high-risk infants, particularly if birth occurs before 90 days post-maternal vaccination or during the RSV season. As of 2025, updated standing orders from Immunize.org emphasize administering one dose of nirsevimab per season for eligible infants, with compatibility confirmed for both live and non-live vaccines. These guidelines support its use in clinical settings through October 1 to March 31, unless local patterns necessitate adjustments.

Adverse effects

Common adverse reactions

The most common adverse reactions to nirsevimab are mild to moderate and typically occur shortly after administration, including injection site reactions such as , swelling, and pain, reported in 0.3% of recipients, and in 0.9%, in clinical trials. Systemic effects are less frequent but include fever, observed at rates comparable to in trials and approximately 6-7% in real-world studies, and or excessive crying post-injection in infants at around 0.4%. In pivotal clinical trials, the overall incidence of any was similar between nirsevimab and groups (e.g., 87% in both arms of the MELODY trial), with the majority of events mild, unrelated to treatment, and resolving within a few days. No routine laboratory monitoring is required following nirsevimab administration, but parents should be educated to observe for signs of or fever in the days after dosing. Post-approval data from 2025 reports, including a Canadian study showing injection-site reactions in about 9%, confirm a similar safety profile in real-world use, with no notable increase in the frequency of these common events compared to trial findings.

Serious adverse events

Serious adverse events associated with nirsevimab are rare, with clinical trials reporting no cases of or other severe reactions directly attributable to the drug. reactions occurred in less than 1% of participants, primarily manifesting as mild reactions such as or . Grade 3 or higher adverse events were observed in approximately 8% of participants in the phase 2b trial, including severe and hospitalizations for non-respiratory syncytial virus illnesses, though rates were similar to or lower than in control groups across pooled data (around 4%). Nirsevimab is contraindicated in infants and children with a history of serious reactions, including , to the drug or its excipients, such as polysorbate 80. Warnings include the potential for reactions, as observed with other immunoglobulin G1 monoclonal antibodies, though none were reported in pivotal trials; immediate support should be available during administration. A theoretical risk of of disease exists with passive strategies like nirsevimab, but no evidence of this was found in clinical studies or post-marketing surveillance. For immunocompromised infants, monitoring for infections is recommended, as nirsevimab was well-tolerated in this population with no new safety concerns identified. Discontinuation due to adverse events is uncommon, occurring in less than 1% of cases, with rare reports involving or elevated liver enzymes in high-risk groups. As of 2025, ongoing surveillance by the in high-risk groups, including preterm infants, has identified no new safety signals, underscoring the importance of to discuss these rare risks. In contrast to common adverse reactions like mild or injection-site reactions, which occur more frequently but are generally self-limited, serious events warrant prompt evaluation.

Pharmacology

Mechanism of action

Nirsevimab is a recombinant human immunoglobulin G1 kappa (IgG1κ) that provides against () by targeting the viral fusion (F) glycoprotein. It specifically binds to a highly conserved in antigenic site Ø on the prefusion conformation of the RSV F protein, with dissociation constants of 0.12 nM for RSV subtype A and 1.22 nM for RSV subtype B. This binding stabilizes the prefusion state and inhibits the conformational changes required for the F protein to mediate fusion between the viral envelope and host , thereby preventing viral entry into host cells. By blocking this essential membrane fusion step, nirsevimab neutralizes and inhibits formation, the process by which infected cells fuse to spread the virus to adjacent cells. Unlike some antibodies, it does not recognize or affect the post-fusion conformation of the F protein, ensuring targeted action at the pre-entry stage of infection. Nirsevimab demonstrates broad neutralizing activity against both RSV subtypes A and B, including diverse clinical isolates. As a , nirsevimab delivers immediate protection to infants without stimulating an active immune response from the host. To enhance its duration of action, the antibody incorporates YTE mutations (M252Y/S254T/T256E) in the Fc region, which increase binding affinity to the neonatal (FcRn) and thereby extend . This supports sustained passive with a single dose, aligning with the that enable season-long protection.

Pharmacokinetics

Nirsevimab is administered via and exhibits nearly complete absorption, with an absolute of approximately 84-85% in infants. Following a single dose, the median time to reach maximum concentration (T_max) is 6 days, with a range of 1 to 28 days. Pharmacokinetics are dose-proportional across clinically relevant doses of 25 to 300 mg in pediatric populations. The drug distributes primarily within the serum compartment, with a central volume of distribution of approximately 216-249 mL and a peripheral volume of 241-261 mL in a typical 5 kg infant; these volumes increase with body weight according to an allometric scaling exponent of 0.84. Nirsevimab, as a monoclonal antibody, shows minimal placental transfer due to its large molecular size, but neonatal protection is achieved through direct infant administration rather than maternal dosing. Metabolism occurs via proteolytic degradation into small peptides through intracellular catabolic pathways, similar to endogenous IgG antibodies, without involvement of hepatic enzymes or specific renal clearance mechanisms. Elimination is characterized by a low clearance rate of approximately 3.4 mL/day in a 5 kg , which scales with body weight (allometric exponent of 0.589); there is no evidence of target-mediated drug disposition at clinical concentrations. The terminal is extended to about 69-71 days in infants during their first () season, owing to a modified Fc region that enhances neonatal binding and reduces compared to unmodified antibodies (which have of 20-25 days). This prolonged exposure supports a single-dose regimen covering an entire RSV season. In preterm infants, the is slightly shorter, averaging 59 days, compared to 69 days in term infants, primarily due to differences in postmenstrual age and body weight influencing clearance; however, serum concentrations remain above protective thresholds for the season even in infants weighing less than 5 kg. No clinically significant pharmacokinetic differences are observed based on , gestational age-related comorbidities like , or antidrug antibody development.

History

Development

Nirsevimab, known during development as MEDI8897, was developed by MedImmune, a biologics arm of , leveraging the company's established platform for (RSV) monoclonal antibodies. It represents a third-generation RSV neutralizing antibody, engineered from the first-generation palivizumab (Synagis) by incorporating YTE substitutions in the Fc region to extend its serum half-life from approximately 20 days to over 60 days. This modification enables a single intramuscular dose to provide season-long protection against RSV in infants. The antibody specifically targets the prefusion conformation of the RSV fusion (F) protein, enhancing its neutralizing potency against diverse RSV strains. In March 2017, and announced a global collaboration to co-develop and commercialize nirsevimab, with retaining responsibility for manufacturing and initial development activities while Sanofi focused on commercialization efforts outside certain regions. The partnership built on MedImmune's preclinical advancements and aimed to accelerate progression to later-stage trials for broader populations. Funding for the program was jointly supported through this , which also facilitated resource sharing for clinical evaluation. Preclinical evaluation confirmed nirsevimab's potential in relevant animal models of infection. In cotton rats, a susceptible to RSV replication in the lower , prophylactic administration of nirsevimab demonstrated dose-dependent reduction in viral lung titers and protection from weight loss following intranasal RSV challenge, outperforming at equivalent doses due to its prolonged exposure. These studies, conducted prior to 2017, established the antibody's efficacy across RSV A and B subtypes and supported dose selection for trials. Key development milestones included the U.S. FDA's Fast Track designation for nirsevimab in March 2015, recognizing its potential to address an unmet need in prevention. The first-in-human 1 trial, evaluating and in healthy adults, initiated in 2014 and completed in 2015, reported no serious adverse events and confirmed the extended . Subsequent 1b/2a studies from 2016 to 2020 in healthy preterm infants ( 32-35 weeks) further validated tolerability, with a mean of 67 to 93 days and no clinically significant immunogenicity, paving the way for efficacy-focused trials.

Regulatory approvals

Nirsevimab received its first regulatory approvals in and the in late 2022, following successful early clinical trials that demonstrated its efficacy in preventing (RSV) lower respiratory tract disease. The (EMA) granted a positive opinion in September 2022 and the approved nirsevimab (branded as Beyfortus) on October 31, 2022, for active immunization to prevent RSV lower respiratory tract disease in neonates and infants during their first RSV season. This approval was facilitated by the EMA's PRIME designation in 2019, which provided enhanced support for development addressing an unmet need in RSV prevention, and an accelerated assessment procedure initiated in February 2022 due to the product's major public health interest in protecting all infants from severe RSV. In the , the Medicines and Healthcare products Regulatory Agency (MHRA) authorized nirsevimab on November 9, 2022, under the same indications for the first RSV season, marking it as the first long-acting for this purpose in the region. In North America, issued a Notice of Compliance on April 24, 2023, approving nirsevimab for the prevention of lower disease in neonates and infants born during or entering their first season, as well as in infants up to 24 months at increased risk entering their second season. The U.S. (FDA) followed with approval on July 17, 2023, for the same indications: prevention in neonates and infants entering or during their first season, and in children aged 8 to 19 months at increased risk entering their second season. This FDA approval was supported by a granted in January 2023, which shortened the review timeline to address the urgent need for prevention options. Further approvals expanded access in other regions during 2023 and 2024. Swissmedic approved nirsevimab on December 22, 2023, for the prevention of lower respiratory tract disease in neonates and infants. The Australian (TGA) registered nirsevimab on November 22, 2023, for prevention of lower respiratory tract disease in neonates, infants, and children up to 24 months at increased risk. In , the approved nirsevimab on January 2, 2024, for the prevention of lower respiratory tract disease in infants during their first season. Japan's Ministry of Health, Labour and Welfare approved nirsevimab on March 27, 2024, for prophylaxis of lower respiratory tract disease in infants during their first season, with additional authorizations in several Latin American nations during 2024. In the United States, the FDA updated the nirsevimab label in 2024 to include detailed guidance on dosing for children entering a second season, specifying a 200 mg dose for those aged 8 to 19 months at increased risk if more than 90 days have passed since the initial dose, reinforcing its role in extended protection for vulnerable populations. By 2025, the U.S. Centers for Disease Control and Prevention's Advisory Committee on Practices (ACIP) maintained its recommendation for with nirsevimab (or the alternative clesrovimab) as a single intramuscular dose for all infants younger than 8 months born during or entering their first season, regardless of maternal status (unless protected by maternal ), and for high-risk children aged 8 through 19 months entering their second season.

Society and culture

Brand names and availability

Nirsevimab is marketed under the brand name Beyfortus globally, while it is specifically designated as nirsevimab-alip under the same brand. The product is formulated as a preservative-free solution for in single-use prefilled syringes, available in two strengths: 50 mg/0.5 mL (100 mg/mL concentration) for infants weighing less than 5 kg, and 100 mg/1 mL (100 mg/mL concentration) for those weighing 5 kg or more. Beyfortus was first launched in the in late 2022 following marketing authorization, with availability in the beginning in November 2022; in the United States, rollout commenced after FDA approval in July 2023, with broader distribution during the 2023-2024 () season. However, high demand led to shortages in the US during the 2023-2024 season, prompting temporary prioritization guidance from health authorities for high-risk infants. Distribution of nirsevimab occurs primarily through specialty pharmacies and vaccine programs such as the Vaccines for Children (VFC) program, ensuring targeted access for eligible infants and young children. In 2025, expansions aim to improve availability in low- and middle-income countries through partnerships, including shipments facilitated by manufacturers and organizations like , the Vaccine Alliance, to address global disparities in prevention access ahead of the 2025-2026 season. The list price for a dose of nirsevimab in the was approximately $495 in 2023, with variations by region and payer; for instance, the VFC program price was lower at $395 per dose, while private market costs averaged around $445 when accounting for mixed insurance coverage. Pricing in other markets, such as , is negotiated through national health systems and tends to be lower due to public procurement frameworks.

Legal status

Nirsevimab is classified as a prescription-only biologic in major regulatory jurisdictions, functioning as a long-acting for intramuscular administration by healthcare providers. It is not subject to controlled substance scheduling, as it lacks abuse potential and is intended solely for preventive use in infants against (). In the United States, nirsevimab qualifies for coverage without cost-sharing under the (ACA) for infants, as it aligns with Advisory Committee on Immunization Practices (ACIP) recommendations for routine . Eligibility for nirsevimab may be impacted by maternal RSV during pregnancy; according to CDC guidelines, infants born to vaccinated mothers ≥14 days prior to delivery generally do not require nirsevimab, except in rare clinical circumstances determined by a healthcare provider. Globally, the (WHO) recommends nirsevimab as a passive option for infants in settings where maternal is unavailable, supporting its use in low- and middle-income countries to address RSV burden. Off-label use of nirsevimab is not recommended, with administration restricted to FDA- and EMA-approved indications for RSV lower disease prevention in neonates and infants entering their first RSV season. During the 2023–2024 RSV season, initial supply constraints in the prompted CDC-issued prioritization guidelines, directing limited nirsevimab doses to high-risk infants, such as preterm or those with underlying , to mitigate impacts. These measures addressed shortages affecting both commercial and Vaccines for Children program supplies, ensuring equitable access amid heightened RSV activity.

Research

Pivotal clinical trials

The pivotal clinical trials establishing nirsevimab's efficacy and safety were two phase 3 studies: the MELODY trial in healthy late-preterm and term infants and the HARMONIE trial in a broader population of infants. The MELODY trial, conducted from 2019 to 2020, was a randomized, double-blind, placebo-controlled study involving 1,490 healthy infants born at 35 weeks gestation or later and entering their first RSV season. Participants received a single intramuscular dose of nirsevimab (50 mg for those <5 kg or 100 mg for those ≥5 kg) or placebo in a 2:1 ratio. The primary endpoint was the incidence of medically attended RSV-associated lower respiratory tract infection (LRTI) through 150 days post-dose, which occurred in 1.2% of nirsevimab recipients versus 5.0% of placebo recipients, yielding a relative risk reduction of 74.5% (95% CI, 49.6–87.1). A time-to-event analysis showed a hazard ratio of 0.22 (95% CI, 0.12–0.42) for this endpoint. The trial was powered to detect at least 70% relative efficacy against the primary endpoint, assuming an 11% event rate in the placebo group. Secondary endpoints included hospitalization for RSV LRTI (relative reduction 62.1%, 95% CI −8.6 to 86.8) and very severe RSV LRTI requiring medical attention (relative reduction 79%, 95% CI 58–89). Subgroup analyses demonstrated consistent efficacy across preterm (35 to <37 weeks gestation) and term (≥37 weeks) infants, with relative risk reductions of 70.3% and 77.3%, respectively, for the primary endpoint. Safety profiles were similar between groups, with serious adverse events in 6.8% of nirsevimab recipients versus 7.3% of placebo recipients and no treatment-related deaths. The trial, conducted from 2022 to 2023, was an open-label, randomized phase 3b study comparing nirsevimab to standard care in 8,058 high-risk infants, including preterm infants and those with chronic lung disease or congenital heart disease. Participants received a single dose of nirsevimab or up to five monthly doses of as part of standard care. The primary endpoint was -associated hospitalization due to LRTI, which showed an 83.2% relative reduction in the nirsevimab group (0.3% incidence versus 1.5% in the control group; 95% CI, 67.8–92.0). Efficacy was consistent across subgroups, including preterm infants (relative reduction 75.4%) and those with underlying conditions (relative reduction 80.1%). Secondary endpoints, such as very severe LRTI requiring oxygen support, demonstrated an 87.5% reduction. The trial used a Cox proportional hazards model for time-to-event analyses, confirming sustained protection through the season. Safety was comparable to controls, with adverse events primarily mild and no new safety signals. Both trials supported nirsevimab's label claims for prevention of LRTI in infants. However, limitations include their conduct primarily before shifts in circulating strains, potentially affecting generalizability to current variants, and a lack of long-term data beyond 150–180 days post-dose.

Post-approval studies

Post-approval studies of nirsevimab have focused on real-world , , and extensions of clinical evaluations to confirm and expand upon its protective benefits against () lower respiratory tract disease (LRTD) in infants. An observational from seven U.S. pediatric medical centers involving over 31,900 healthy term infants demonstrated high , with 98.0% (95% , 85.1–99.7%) against hospitalized LRTI during the 2023–2024 season. Similarly, a test-negative case-control study from the 2023–2024 season reported nirsevimab at 80.5% (95% , 52.0–93.5%) against RSV-associated hospitalizations and 84.6% (95% , 58.7–95.6%) against severe disease among infants, based on data from a U.S. health system covering more than 10,000 immunized infants. These findings indicate substantial protection in diverse populations, including preterm and term infants. Real-world data from the 2024–2025 season, as of September 2025, show nirsevimab 77% effective against -associated hospitalizations in infants from the VISION network. Ongoing trials are investigating extended protection and dosing strategies beyond the first RSV season. The HARMONIE trial extension has evaluated 180-day efficacy, showing sustained reduction in RSV hospitalizations (0.3% vs. 1.7%), and is assessing second-season dosing with an additional 100 mg intramuscular dose for infants aged 9–24 months at continued risk, demonstrating feasibility without new safety concerns. Comparative evaluations with clesrovimab, a newly approved long-acting , are in early phases through 2026, though direct head-to-head trials are limited; Advisory Committee on Immunization Practices (ACIP) reviews note similar endpoints but highlight differences in trial definitions, positioning clesrovimab as an alternative without established superiority. Surveillance efforts, including the CDC's network, have monitored nirsevimab use from 2023 to 2025 across multiple U.S. sites, reporting no new safety signals such as increased adverse events or beyond those identified pre-approval. Effectiveness data from this network confirmed 77% protection against visits and 98% against hospitalizations for RSV-LRTD, including against common variants, supporting broad implementation. In settings, such as Spain's post-marketing involving over 5,000 infants, nirsevimab maintained a favorable safety profile with low rates of serious adverse events (1.2%), reinforcing its role in universal programs. Comparative real-world data underscore nirsevimab's advantages over , the prior standard for high-risk , primarily due to its single-dose regimen improving adherence rates from palivizumab's reported 50–70% completion in multi-dose schedules. Combination strategies with maternal have shown additive benefits, with interrupted time-series analyses indicating up to 90% reduction in infant hospitalizations when both are used, though uptake varies by . Future directions include long-term follow-up studies for neurodevelopmental outcomes, as preventing severe may mitigate risks like recurrent wheezing observed in infected infants, with planned cohorts tracking immunized children through age 5. Global equity trials from 2025–2027 aim to evaluate access and effectiveness in low-resource settings, addressing implementation barriers identified in initial rollouts.

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