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Mavacamten

Mavacamten, sold under the brand name Camzyos, is a first-in-class, selective, allosteric, and reversible inhibitor of cardiac approved for the treatment of symptomatic obstructive (oHCM) in adults with New York Heart Association (NYHA) class II-III to improve functional capacity and symptoms. As the first cardiac myosin inhibitor approved by the U.S. Food and Drug Administration (FDA), mavacamten targets the underlying pathophysiology of oHCM by reducing excessive actin-myosin cross-bridging in cardiac muscle cells, which decreases left ventricular outflow tract (LVOT) obstruction and improves cardiac filling pressures and exercise performance. The drug received FDA approval on April 28, 2022, based on pivotal phase 3 clinical trials such as EXPLORER-HCM, which demonstrated significant improvements in peak oxygen uptake (pVO2), NYHA class, and Kansas City Cardiomyopathy Questionnaire (KCCQ-23) scores compared to placebo, with 37% of treated patients achieving the primary composite endpoint versus 17% in the placebo group. Additional studies, including VALOR-HCM and MAVERICK-HCM, have supported its efficacy in reducing the need for septal reduction therapies and lowering markers of myocardial wall stress in obstructive HCM and, in phase 2 studies, in non-obstructive HCM, though the 2025 ODYSSEY-HCM phase 3 trial did not meet primary clinical endpoints for the latter. Mavacamten is administered orally as capsules in doses of 2.5 mg, 5 mg, 10 mg, or 15 mg, with an initial daily dose of 5 mg that is titrated every four weeks based on echocardiographic assessments and clinical response, up to a maximum of 15 mg. Due to the risk of heart failure from systolic dysfunction, it carries a boxed warning and is available only through the Camzyos Risk Evaluation and Mitigation Strategy (REMS) program, requiring echocardiographic monitoring of left ventricular ejection fraction (LVEF) before initiation and periodically during treatment, with reduced frequency (every 6 months) for stable patients in the maintenance phase as of April 2025. In April 2025, the FDA updated the label to reduce echocardiography monitoring requirements and reclassify certain contraindications. Common adverse effects include dizziness (affecting about 27% of patients) and syncope (6%), while precautions include contraindication with strong CYP2C19 inhibitors or moderate/strong CYP2C19/CYP3A4 inducers, and dose adjustments for moderate CYP2C19 or strong CYP3A4 inhibitors, as updated in April 2025, along with ensuring effective contraception due to potential embryofetal toxicity.

Pharmacology

Mechanism of action

Mavacamten is a first-in-class, selective, allosteric, and reversible inhibitor of cardiac myosin ATPase. It specifically targets the β-cardiac myosin isoform, modulating its activity to reduce sarcomere hypercontractility, a key pathological feature in conditions like hypertrophic cardiomyopathy (HCM). At the molecular level, mavacamten binds with submicromolar affinity to the S1 motor domain of cardiac myosin, particularly in the presence of ATP, where it stabilizes an autoinhibited, two-headed super-relaxed (SRX) state. This binding enhances head-head interactions within the myosin molecule, shifting the equilibrium toward an energy-sparing off-state and reducing the proportion of myosin heads available for interaction with actin filaments. By preferentially stabilizing this recruitable conformation in two-headed heavy meromyosin (HMM) over single-headed subfragment-1 (S1), mavacamten demonstrates structural selectivity that underlies its targeted action on cardiac myosin assemblies. The downstream physiological effects include inhibition of actin-activated activity, with reduced rates (e.g., kcat decreasing from 2.02 s⁻¹ to 0.48 s⁻¹) and slowed release as the rate-limiting step in the . This leads to decreased cross-bridge formation during both and , thereby alleviating dynamic left obstruction (LVOTO) and improving cardiac filling pressures without broadly compromising ventricular systolic function. Mavacamten's selectivity extends to cardiac sarcomeres, sparing skeletal and myosins due to its lower affinity for non-cardiac isoforms and minimal off-target effects on other .

Pharmacokinetics

Mavacamten is administered orally and exhibits an estimated absolute of approximately 85%. It is rapidly absorbed, with a time to maximum concentration (Tmax) of 1 to 4 hours, primarily in the . Administration with a high-fat reduces the maximum concentration (Cmax) by about 56% and the area under the curve () by 12%, though these changes are not considered clinically significant. The volume of distribution at is approximately 270 L, indicating extensive distribution into tissues, including to cardiac . Mavacamten is highly bound to proteins, with approximately 97% to 98% bound to and alpha-1-acid glycoprotein. concentrations are achieved after 4 to 8 weeks of daily dosing, consistent with its elimination of 6 to 9 days in normal metabolizers. Mavacamten undergoes extensive hepatic primarily via enzymes, with responsible for about 74% of , for 18%, and for 8%; minor contributions come from CYP2D6. No active metabolites have been identified. The apparent oral clearance is approximately 0.9 L/h. This CYP-mediated contributes to potential interactions with inhibitors or inducers of these enzymes. Elimination occurs predominantly through , with approximately 85% of the dose recovered in (3% as unchanged ) and 7% in (1% as unchanged ). The terminal elimination extends to 23 days in poor metabolizers, who exhibit reduced clearance and approximately 2- to 3-fold higher systemic exposure compared to normal metabolizers.

Clinical use

Indications

Mavacamten is indicated for the treatment of adults with symptomatic obstructive (oHCM) who have Heart Association (NYHA) class II-III symptoms, specifically to improve functional capacity and alleviate symptoms. Evidence from the pivotal EXPLORER-HCM phase 3 trial supports its efficacy, demonstrating significant improvements in peak oxygen consumption (pVO2) compared to , with a greater proportion of patients achieving at least one NYHA class improvement (65% versus 31%) and enhanced health-related quality of life as measured by Kansas City Questionnaire (KCCQ) scores. These outcomes reflect mavacamten's role in enhancing exercise tolerance and symptom relief by reducing left ventricular outflow tract obstruction (LVOTO), consistent with its mechanism of action. The drug is approved for use as add-on therapy in patients already receiving beta-blockers or non-dihydropyridine such as verapamil or , or as monotherapy in those intolerant to these standard treatments. Mavacamten is not indicated for non-obstructive or asymptomatic cases, as its benefits center on improving functional capacity in symptomatic obstructive disease rather than reversing myocardial .

Dosage and administration

Mavacamten is initiated at a starting dose of 5 mg taken orally once daily, with or without food. For patients on stable therapy with a weak inhibitor or moderate inhibitor, the starting dose remains 5 mg once daily. For patients concurrently receiving a moderate inhibitor or a strong inhibitor, the starting dose should be reduced to 2.5 mg once daily to account for potential increases in mavacamten exposure. As of the April 2025 label update, mavacamten is no longer contraindicated with moderate or strong inhibitors; instead, use with dose reduction and close monitoring. Titration of the dose occurs based on assessments of left (LVEF) and Valsalva left () gradient via echocardiogram. Assess before initiation and at 4 weeks after starting or dose adjustment to guide , with the goal of achieving a post-exercise Valsalva LVOT gradient below 30 mm while maintaining LVEF at or above 50%. For stable patients in the maintenance phase who are eligible, perform echocardiographic assessments every 6 months or as clinically indicated. If LVEF remains stable at greater than 55% and the gradient is at least 30 mm , the dose may be increased in 5 mg increments to 10 mg or 15 mg once daily; however, up-titration is not recommended if LVEF is 50% to 55%. Conversely, if LVEF falls below 50%, should be interrupted, and upon recovery to at least 50%, restarted at the next lower dose (e.g., from 10 mg to 5 mg). Permanent discontinuation is required if LVEF remains below 50% after interruption while on the lowest dose of 2.5 mg or if symptoms of worsen. The maximum recommended dose is 15 mg once daily. These guidelines align with mavacamten's pharmacokinetic of approximately 7 to 9 days, allowing time to reach steady-state concentrations. Dose increases should be delayed during intercurrent illnesses such as infections or arrhythmias that could transiently affect LVEF. Due to the risk of heart failure from reduced LVEF, mavacamten is available only through the CAMZYOS Risk Evaluation and Mitigation Strategy (REMS) Program, which mandates enrollment of prescribers, patients, and pharmacies. Under this program, treatment initiation requires a negative in females of reproductive potential, with ongoing contraception recommended during and for 4 months after discontinuation to prevent fetal harm. Echocardiographic is essential before starting , during , and periodically thereafter to guide dose adjustments and ensure safety. Capsules should be swallowed whole and not opened, broken, or chewed, as splitting is unnecessary and may affect . If a dose is missed, it should be taken as soon as possible on the same day, with the next dose resuming at the regular schedule the following day; double dosing is prohibited. Consistent daily timing is advised for adherence, though exact timing within the day is flexible.

Safety and monitoring

Adverse effects

Mavacamten's most frequent adverse effects include (reported in 27% of patients in clinical trials) and syncope (6%), often resulting from the drug's negative inotropic effects that reduce . Serious risks associated with mavacamten therapy involve reversible reductions in left ventricular (LVEF) below 50% (observed in 6% of patients in EXPLORER-HCM), events (approximately 1.3% across phase III trials), new-onset (5-10% incidence in various studies), and ventricular arrhythmias, though the latter are uncommon and may even decrease with treatment in some patients. In the phase 3 EXPLORER-HCM , s led to permanent discontinuation in 1.6% of mavacamten-treated patients, with overall rates similar to (88% vs. 81%). To mitigate cardiac risks, echocardiographic of LVEF is required before initiation, during (every 4-12 weeks as needed), and every 6 months in the for stable patients (LVEF ≥55% and Valsalva LVOT gradient <30 mmHg, or ≥30 mmHg without need for up-titration), per the April 2025 FDA label update; is also required 8 weeks after discontinuation, with immediate interruption if LVEF falls below 50% or symptoms worsen.

Contraindications and drug interactions

Mavacamten is contraindicated in patients with concomitant use of strong , as these increase mavacamten exposure and may elevate the risk of heart failure due to systolic dysfunction. It is also contraindicated with moderate to strong or moderate to strong , such as or , which can decrease mavacamten exposure and potentially reduce its therapeutic effect. Following the April 2025 label update, it is no longer contraindicated with moderate or strong (e.g., ), but requires dose adjustments and close monitoring instead. Initiation of mavacamten is not recommended in patients with left ventricular ejection fraction () less than 55% prior to starting therapy, due to the risk of exacerbating systolic dysfunction. Drug interactions with moderate CYP3A4 inhibitors, such as fluconazole, or weak CYP2C19 inhibitors, like omeprazole, may increase mavacamten plasma concentrations, necessitating dose reductions to mitigate heart failure risk; for example, the starting dose should be reduced from 5 mg to 2.5 mg when coadministered with these agents. Concomitant use with negative inotropes, including verapamil (especially with beta-blockers), disopyramide, ranolazine, or diltiazem with beta-blockers, should be avoided due to additive effects that may further impair cardiac contractility and increase heart failure potential; if unavoidable, close LVEF monitoring is essential. Mavacamten is not recommended during pregnancy, as animal studies have demonstrated embryotoxicity, including fetal malformations and increased post-implantation loss at exposures comparable to the human maximum recommended dose, though no human data are available; effective contraception is advised during treatment and for 4 months after discontinuation. For patients with severe hepatic impairment (Child-Pugh C), use of mavacamten should be avoided due to unknown pharmacokinetic effects, while no dose adjustment is needed for mild to moderate impairment despite up to a 220% increase in exposure. Genotyping for is recommended prior to initiation, particularly in poor metabolizers (e.g., *2/*2 genotype), who exhibit approximately 241% higher area under the curve and 47% higher maximum concentration compared to normal metabolizers, requiring dose adjustments to prevent excessive exposure.

History and development

Discovery and preclinical studies

Mavacamten, formerly known as MYK-461, was discovered by MyoKardia Inc. in 2012 through a high-throughput screening campaign targeting sarcomere dysfunction in hypertrophic cardiomyopathy (HCM). The company, founded that year by researchers including James Spudich, licensed a compound library from Cytokinetics and employed structure-activity relationship (SAR) studies to identify small molecules that modulate cardiac myosin ATPase activity. This effort addressed longstanding gaps in HCM treatment, where sarcomeric mutations lead to hypercontractility without effective disease-modifying options. Preclinical investigations began with in vitro binding assays using purified cardiac myosin from bovine, , and other species, revealing mavacamten's selective allosteric inhibition of actin-activated ATPase activity. The compound exhibited an IC50 of approximately 500 nM for bovine and human cardiac , with greater than 100-fold selectivity over non-cardiac myosins such as and non-muscle types, minimizing off-target effects like broad . This selectivity was attributed to mavacamten's stabilization of myosin in an energy-sparing, autoinhibited super-relaxed state, reducing cross-bridge formation without impairing overall . In vivo studies utilized models, including mice harboring heterozygous HCM-causing mutations in α-myosin heavy chain, where mavacamten administration prevented development, reversed established myocardial thickening, and reduced in a dose-dependent manner. models, such as naïve dogs, demonstrated improved left ventricular compliance and , with no of toxicity across tested doses. These preclinical models also showed mavacamten's ability to alleviate left obstruction (LVOTO) under stress conditions, supporting its potential as a . The promising preclinical profile, emphasizing allosteric modulation for cardiac specificity, paved the way for an (IND) application filed by MyoKardia in 2014, which became effective in November of that year.

Clinical trials and approval

The development of mavacamten advanced through key clinical trials evaluating its efficacy in patients with symptomatic obstructive (oHCM). The phase 2 PIONEER-HCM trial, an open-label proof-of-concept study conducted in 2018, enrolled 21 adults with oHCM and Heart Association (NYHA) class II-III symptoms. In this trial, mavacamten significantly reduced the mean post-exercise left (LVOT) gradient from 103 mm Hg at baseline to 19 mm Hg after 12 weeks of treatment in the primary cohort, while also improving exercise capacity and symptoms as measured by NYHA class and Kansas City Cardiomyopathy Questionnaire scores. These results provided initial evidence of mavacamten's potential to address the underlying of oHCM without invasive procedures. The phase 2 MAVERICK-HCM trial, conducted from 2018 to 2019, evaluated mavacamten in 59 patients with symptomatic non-obstructive HCM (n=28) and oHCM (n=31) over 16 weeks. It demonstrated reductions in cardiac biomarkers of wall stress (e.g., NT-proBNP and cTnI) and improvements in symptoms and functional capacity, supporting efficacy in both HCM subtypes. Building on these findings, the phase 3 EXPLORER-HCM trial, a randomized, double-blind, -controlled study with 251 participants, reported results in that supported regulatory submission. Patients received mavacamten or for 30 weeks alongside standard care, with the primary composite endpoint defined as an improvement of at least 1.5 mL/kg/min in peak oxygen consumption (pVO2) and a reduction of at least 30 mm Hg in post-exercise LVOT gradient. This endpoint was achieved by 37% of mavacamten-treated patients compared to 17% in the placebo group (p=0.0005), alongside secondary improvements in NYHA class (65% vs 32% achieving at least one-class reduction) and health-related . The trial demonstrated mavacamten's ability to enhance functional capacity and alleviate symptoms in a broader oHCM population. The phase 3 VALOR-HCM trial, reported in 2022, further evaluated mavacamten in 112 patients with oHCM eligible for septal reduction therapy (SRT), randomizing them to mavacamten or for weeks. The primary , the proportion of patients no longer meeting guideline criteria for SRT at week , was met by 82% in the mavacamten group versus 18% in placebo (difference 64%, p<0.0001), supporting the potential to defer invasive SRT in high-risk patients. Long-term extension data through week 128 showed sustained benefits, with approximately 83% of patients avoiding SRT as of 2024. Development accelerated following Bristol Myers Squibb's acquisition of MyoKardia in October 2020 for $13.1 billion in cash, which integrated mavacamten into a broader cardiovascular portfolio and facilitated late-stage trials and submissions. The U.S. (FDA) granted accelerated approval for mavacamten (as Camzyos) on April 28, 2022, under priority review for adults with NYHA class II-III oHCM to improve functional capacity and symptoms, with a Risk Evaluation and Mitigation Strategy (REMS) program due to risks of from reduced left ventricular . The approved it on June 26, 2023, for the same indication in adults. As of November 2025, the phase 3 SCOUT-HCM (NCT06253221) is ongoing and recruiting, evaluating the , , and of mavacamten versus in adolescents (aged 12-17 years) with symptomatic oHCM (NYHA class II-III) over 40 weeks, with primary endpoints including change in peak oxygen uptake and LVOT gradient.

Society and culture

Legal status

Mavacamten, marketed as Camzyos, received approval from the U.S. (FDA) on April 28, 2022, for the treatment of adults with symptomatic New York Heart Association (NYHA) class II-III obstructive (oHCM) to improve functional capacity and symptoms. Due to the risk of from reduced left ventricular ejection fraction (LVEF), its use requires enrollment in the Camzyos Risk Evaluation and Mitigation Strategy (REMS) program, which mandates prescribers to assess LVEF before initiation and periodically thereafter, while patients must avoid and use contraception. Internationally, the granted marketing authorization for mavacamten on June 26, 2023, for symptomatic oHCM in adults. approved it on November 11, 2022, for the same indication in adults. Australia's (TGA) authorized it on October 13, 2022, for symptomatic NYHA class II-III oHCM in adults. Japan's Ministry of Health, Labour and Welfare approved it on March 27, 2025, for hypertrophic obstructive cardiomyopathy. As of 2025, mavacamten has received regulatory approvals in more than 50 countries and regions across five continents. Mavacamten is not a under international scheduling conventions, but its distribution is restricted worldwide due to potential cardiac risks. In the United States, it is available only through certified specialty pharmacies enrolled in the REMS program, which limits dispensing to no more than a 35-day supply in the first year and requires verification of prescriber and . Similar restricted applies in other approved regions to ensure monitoring compliance. As of November 2025, mavacamten remains under investigation for pediatric use through the ongoing phase 3 SCOUT-HCM trial evaluating its and safety in adolescents with symptomatic oHCM, with no approval yet for patients under 18 years old. The phase 3 ODYSSEY-HCM trial for expanded indications in symptomatic non-obstructive (nHCM) did not meet its primary endpoint of improved peak oxygen uptake in September 2025, and no regulatory submission for this use has been pursued. No versions of mavacamten are available in any approved market. Access to mavacamten is limited by its high cost, with the U.S. of approximately $89,500 annually before discounts or , though assistance programs like MyCamzyos provide co-pay reducing out-of-pocket expenses to as low as $10 per month for eligible commercially insured and free trials or bridging for uninsured individuals.

Names

Mavacamten is the (INN) for this medication, as established by the and adopted by regulatory bodies such as the . The primary brand name is Camzyos, marketed by in the United States, , and most international markets. As of 2025, no alternative brands or versions are available. During its development, the drug was coded as MYK-461 by the original developer, MyoKardia. The pronunciation of mavacamten is /məˈvækəmˌtɛn/, commonly rendered as ma-VAK-a-ten.

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