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Vilazodone

Vilazodone, sold under the brand name Viibryd among others, is an oral antidepressant medication approved by the U.S. Food and Drug Administration (FDA) in January 2011 for the treatment of major depressive disorder (MDD) in adults.^[1]^[2] It belongs to the class of serotonin partial agonist reuptake inhibitors (SPARIs) and is currently manufactured by AbbVie, with generic versions available from multiple producers.^[3]^[4] Vilazodone exerts its therapeutic effects through a dual mechanism of action: it selectively inhibits the reuptake of serotonin (5-HT) by blocking the serotonin transporter (SERT), thereby increasing serotonin levels in the synaptic cleft, while simultaneously acting as a partial agonist at postsynaptic 5-HT_1A receptors.^[1]^[5] This combined pharmacology is intended to enhance serotonergic neurotransmission more rapidly than traditional selective serotonin reuptake inhibitors (SSRIs) alone, potentially leading to a faster onset of antidepressant action and improved efficacy in patients with MDD.^[6]^[7] The recommended dosing regimen begins with 10 mg once daily for 7 days, followed by an increase to 20 mg once daily, with a possible escalation to a maximum of 40 mg once daily after an additional 7 days, always taken with food to enhance bioavailability.^[1] Common adverse effects include diarrhea, nausea, insomnia, and vomiting, occurring at rates at least twice that of placebo, while serious risks encompass suicidal ideation (particularly in younger adults), serotonin syndrome, and activation of mania or hypomania in patients with bipolar disorder.^[1]^[8] Vilazodone is contraindicated with monoamine oxidase inhibitors (MAOIs) and carries warnings against abrupt discontinuation to avoid withdrawal symptoms.^[1]

Medical uses

Major depressive disorder

Vilazodone received approval from the U.S. Food and Drug Administration in January 2011 for the treatment of major depressive disorder (MDD) in adults.^[9] This approval was based on evidence from two pivotal phase III, randomized, double-blind, placebo-controlled trials demonstrating its efficacy in reducing depressive symptoms, with efficacy further supported by four such studies in current labeling.^[9] As a selective serotonin reuptake inhibitor (SSRI) combined with partial agonism at 5-HT_1A receptors, vilazodone modulates serotonin levels in the brain to alleviate core MDD symptoms, including persistent sadness, loss of interest in activities, and impaired concentration.^[9] This dual mechanism enhances serotonergic neurotransmission, potentially providing more targeted symptom relief compared to SSRIs alone.^[5] The recommended dosing regimen for MDD begins with 10 mg orally once daily for 7 days, followed by 20 mg once daily for an additional 7 days, and then titration to a target of 40 mg once daily, administered with food to optimize absorption.^[9] In the phase III trials, vilazodone 40 mg/day showed significant improvements in Montgomery-Åsberg Depression Rating Scale (MADRS) scores, with least squares mean differences of -3.2 and -2.5 versus placebo over 8 weeks.^[9] Pooled analyses indicated response rates of approximately 44% and remission rates of 25-28% for vilazodone compared to 30% and 18-20% for placebo, respectively, with initial benefits often emerging within 2-4 weeks.^[10] Vilazodone's 5-HT_1A partial agonism may confer advantages over traditional SSRIs, including a potentially faster onset of action by reducing the typical delay in therapeutic effects through direct receptor modulation.^[11]

Off-label and investigational uses

Vilazodone has been explored off-label for the treatment of generalized anxiety disorder (GAD), primarily due to its partial agonism at the 5-HT_1A receptor, which may confer anxiolytic effects beyond its serotonin reuptake inhibition. Small-scale clinical trials have demonstrated potential efficacy in reducing GAD symptoms, with one randomized, double-blind, placebo-controlled study involving 395 adults showing significant improvements in Hamilton Anxiety Rating Scale scores at doses of 20–40 mg/day over 8 weeks compared to placebo.^[12] However, these findings are limited by sample sizes and lack of head-to-head comparisons with established anxiolytics, and vilazodone remains unapproved for GAD by regulatory bodies like the FDA.^[13] Investigational research has examined vilazodone's role in treatment-resistant depression (TRD), including as an augmentation strategy or switch option for patients with inadequate response to prior antidepressants. Post-approval studies since 2011, such as a 2015 randomized trial of switching to vilazodone in partial responders to SSRIs or SNRIs, reported greater reductions in Montgomery-Åsberg Depression Rating Scale scores versus continued prior therapy, suggesting utility in augmentation-like scenarios. Limited small-scale studies have explored vilazodone in patients with inadequate response to prior antidepressants, showing some improvements in depressive symptoms, but comprehensive data on its efficacy in treatment-resistant depression remain lacking.^[14] As of 2025, vilazodone lacks approval for pediatric populations or other mood disorders due to insufficient large-scale evidence. Two phase 3 randomized, placebo-controlled studies in children and adolescents (ages 7–17) found no significant separation from placebo on Children's Depression Rating Scale-Revised scores after 8 weeks at 15–30 mg/day, underscoring safety concerns and limited efficacy signals.^[15] A 2025 FDA postmarketing pharmacovigilance review of serious adverse events in pediatric patients found no new safety concerns.^[16] For posttraumatic stress disorder, a preliminary trial (NCT01715519) showed no significant benefit over placebo, as published in 2017.^[17] Off-label dosing for these indications typically mirrors that for major depressive disorder, starting at 10 mg/day and titrating to 20–40 mg/day over 1–2 weeks, with adjustments based on tolerability and case reports rather than standardized guidelines.^[12] Clinicians must weigh the partial 5-HT_1A agonism's theoretical benefits against risks like serotonin syndrome in combinations.^[8]

Adverse effects

Common adverse effects

The most frequently reported adverse effects of vilazodone in clinical trials are gastrointestinal disturbances, which occur in a substantial proportion of patients and are often linked to its serotonergic activity. Diarrhea affects up to 28% of users, nausea up to 23%, and vomiting around 5%; these symptoms are typically mild to moderate, dose-dependent, and transient, resolving in many cases with continued treatment or dose adjustment.^[1] Taking vilazodone with food can help mitigate these gastrointestinal issues.^[8] Other common effects include insomnia (6-7%), headache (14-15%), dizziness (9%), and dry mouth (8%), which generally emerge during the initial titration phase and may improve over time. For insomnia, administering the dose in the morning is recommended to reduce interference with sleep.^[8] Insomnia and certain other effects are observed at rates at least twice that of placebo in short-term studies.^[1] Sexual dysfunction with vilazodone occurs at lower rates compared to traditional SSRIs, with specific symptoms such as decreased libido (around 4%), abnormal orgasm (3%), erectile dysfunction (2%), and delayed ejaculation (2%) reported in 4-14% of patients across various manifestations, depending on baseline function. These adverse effects often onset within the first few weeks of treatment and tend to resolve upon dose adjustment or continuation in many individuals.^[8] Patients should be monitored regularly for these common effects, particularly during the initial weeks and dose escalations, with healthcare providers advising on symptom management strategies to improve tolerability.^[1]

Serious adverse effects

Vilazodone carries a black box warning from the U.S. Food and Drug Administration (FDA) regarding an increased risk of suicidal thoughts and behaviors in children, adolescents, and young adults under 24 years of age, a class effect observed across antidepressants including selective serotonin reuptake inhibitors (SSRIs).^[9] Pooled analysis of short-term placebo-controlled trials in adults with major depressive disorder (MDD) showed no overall increase in suicidality risk with vilazodone compared to placebo, with incidences of suicidal ideation at 19.9% for vilazodone versus 24.7% for placebo; however, in young adults aged 18-24, the risk is elevated by approximately 5 additional cases per 1,000 patients treated.^[9]^[18] Close monitoring is required, particularly during the initial months of treatment and dose adjustments, as the risk may persist beyond acute phases.^[9] Serotonin syndrome, a potentially life-threatening condition, is a serious risk associated with vilazodone, especially when combined with other serotonergic agents such as monoamine oxidase inhibitors (MAOIs), which is contraindicated.^[9] Symptoms include agitation, hallucinations, coma, tachycardia, hyperthermia, muscle rigidity, and autonomic instability, with an incidence of 0.1% reported in clinical trials.^[9] Discontinuation of vilazodone and the offending agent is essential if serotonin syndrome is suspected.^[9] Other notable serious risks include hyponatremia, which can lead to seizures, coma, or death, particularly in elderly patients or those on diuretics, though specific incidence rates from vilazodone trials are not quantified beyond general SSRI warnings.^[9] Abnormal bleeding events, such as gastrointestinal hemorrhage, are heightened with concurrent use of aspirin, nonsteroidal anti-inflammatory drugs (NSAIDs), or anticoagulants.^[9] Activation of mania or hypomania occurs in approximately 0.1% of patients with undiagnosed bipolar disorder, necessitating screening prior to initiation.^[9] Postmarketing reports include cases of acute pancreatitis.^[9] Abrupt discontinuation of vilazodone may precipitate discontinuation syndrome, characterized by symptoms such as dizziness, nausea, irritability, and sensory disturbances, though these are generally milder compared to other SSRIs due to vilazodone's longer half-life and multimodal mechanism.^[9]^[8] Gradual dose tapering is recommended to minimize this risk.^[9] Long-term use of vilazodone, as with other SSRIs, has been associated with potential effects on bone mineral density and increased fracture risk based on post-marketing surveillance and class-wide data.^[3]^[19] Weight changes are minimal, with clinical trials indicating vilazodone is generally weight-neutral, showing mean increases of 0.2-0.4 kg over short-term use versus 0.1-0.4 kg with placebo.^[8]

Effects during pregnancy and breastfeeding

Vilazodone has limited data regarding its use during pregnancy, with no adequate and well-controlled studies in humans available. Animal reproduction studies have shown decreased fetal weight and delayed skeletal ossification at doses greater than 17 times the maximum recommended human dose (MRHD), but no evidence of teratogenicity in rats or rabbits. The former FDA pregnancy category for vilazodone was C, indicating that risks cannot be ruled out based on this preclinical evidence.^[1]^[20] Exposure to vilazodone during the third trimester may increase the risk of neonatal complications, similar to other serotonergic antidepressants. These include persistent pulmonary hypertension of the newborn (PPHN), with a baseline incidence of approximately 1 to 2 per 1,000 live births that may rise up to 6-fold following late-pregnancy SSRI exposure after the 20th week of gestation. Neonates may also exhibit symptoms of withdrawal or serotonergic effects, such as jitteriness, irritability, respiratory distress, or feeding difficulties, which are typically mild and resolve within days to weeks; close monitoring is recommended. Untreated maternal depression, however, carries its own risks, including preterm birth and low birth weight, necessitating a careful benefit-risk assessment.^[1]^[21]^[22] Data from pregnancy registries, including the National Pregnancy Registry for Antidepressants, remain limited for vilazodone as of 2025, with no major teratogenic effects confirmed to date, though ongoing enrollment and monitoring are advised to further evaluate long-term outcomes. Healthcare providers are encouraged to register pregnant patients exposed to vilazodone by calling 1-866-961-2388. When possible, switching to alternatives with more established safety profiles, such as sertraline, may be considered during pregnancy after consulting a specialist.^[23]^[24] Regarding breastfeeding, it is unknown whether vilazodone is excreted into human milk, though it is present in the milk of lactating rats at levels up to 13 times maternal plasma concentrations. No data exist on the effects of vilazodone on breastfed infants, but potential risks include sedation or poor feeding; monitoring the infant for such symptoms is advised if use continues. Given the lack of human lactation data, other antidepressants like sertraline or paroxetine, which have demonstrated low transfer into milk, may be preferred, particularly for newborns or preterm infants. The decision to breastfeed while taking vilazodone should weigh maternal benefits against potential infant risks, with untreated depression also posing concerns for bonding and infant development.^[1]^[25]^[25]

Contraindications and precautions

Contraindications

Vilazodone should not be used in patients with a known hypersensitivity to vilazodone hydrochloride or any of its excipients, as this may precipitate severe allergic reactions such as anaphylaxis.^[26] The concurrent administration of vilazodone with monoamine oxidase inhibitors (MAOIs), including linezolid and intravenous methylene blue, or within 14 days of discontinuing an MAOI is strictly contraindicated due to the heightened risk of serotonin syndrome, a potentially life-threatening condition characterized by autonomic instability, neuromuscular abnormalities, and altered mental status.^[1] Vilazodone should be avoided in patients with untreated anatomically narrow angles due to the risk of angle-closure glaucoma, as its serotonergic activity may trigger an attack by dilating the pupil and elevating intraocular pressure.^[1] Vilazodone is not approved for use in pediatric patients under 18 years of age due to the absence of established safety and efficacy data, coupled with an elevated risk of suicidal ideation and behavior observed in short-term studies of antidepressants across this age group.^[1]

Drug interactions

Vilazodone undergoes extensive metabolism primarily via the cytochrome P450 3A4 (CYP3A4) enzyme, resulting in notable pharmacokinetic interactions with CYP3A4 modulators.^[1] Strong CYP3A4 inhibitors, such as ketoconazole, increase vilazodone's area under the curve (AUC) by approximately 50%, which can elevate exposure and risk of adverse effects; the maximum recommended dose should be limited to 20 mg daily during coadministration, with return to the original dose upon discontinuation of the inhibitor.^[27]^[1] Conversely, strong CYP3A4 inducers like rifampin decrease vilazodone exposure, potentially compromising therapeutic efficacy; clinicians may consider titrating the vilazodone dose upward by up to twofold (maximum 80 mg daily) if the inducer is used for more than 14 days, followed by gradual reduction upon its discontinuation.^[1] Coadministration with other serotonergic drugs, including triptans and tramadol, heightens the risk of serotonin syndrome through additive effects on serotonin levels; patients should be monitored closely for symptoms such as agitation, hallucinations, and hyperthermia, with discontinuation of one or both agents if the syndrome develops.^[1] Alcohol consumption during vilazodone therapy can exacerbate central nervous system depression, amplifying sedation and dizziness, which may impair cognitive and motor functions; avoidance of alcohol is advised.^[1] Similarly, concurrent use with other CNS depressants may intensify these sedative effects, necessitating caution and potential dose adjustments.^[1] Vilazodone, like other serotonin reuptake inhibitors, can increase bleeding risk when combined with warfarin due to interference with platelet serotonin uptake and aggregation; international normalized ratio (INR) monitoring is essential when initiating, titrating, or discontinuing vilazodone in patients on warfarin therapy.^[1]

Pharmacology

Pharmacodynamics

Vilazodone is a serotonin partial agonist reuptake inhibitor (SPARI) that potently inhibits the serotonin transporter (SERT), with a high binding affinity characterized by a Ki value of 0.1 nM in human membranes, thereby increasing synaptic serotonin concentrations in the central nervous system.^[28] This inhibition enhances serotonergic neurotransmission, which is central to its antidepressant effects. Additionally, vilazodone exhibits negligible affinity for other monoamine transporters, such as the norepinephrine transporter (NET; Ki = 56 nM) and dopamine transporter (DAT; Ki = 37 nM), distinguishing it from SNRIs or drugs with broader monoamine activity.^[28]^[29] Vilazodone also functions as a partial agonist at 5-HT1A receptors, with a binding affinity of approximately 0.5 nM (pKi ≥ 9.3) and intrinsic activity ranging from 43% to 98% relative to full agonist serotonin, depending on the assay; notably, it achieves about 61% efficacy in rat hippocampal tissue.^[30]^[28] This partial agonism, particularly at postsynaptic 5-HT1A receptors in regions like the prefrontal cortex, is thought to further augment serotonin transmission and contribute to faster onset of therapeutic effects compared to traditional SSRIs.^[30] The dual mechanism—SERT inhibition combined with 5-HT1A partial agonism—differentiates vilazodone from pure SSRIs, potentially conferring anxiolytic properties through enhanced serotonergic modulation.^[11] In animal models, vilazodone's pharmacodynamic actions lead to downstream effects that support neuroplasticity, including increased brain-derived neurotrophic factor (BDNF) expression; for instance, chronic administration (20 mg/kg for 14 days) in stressed rats elevated serum BDNF levels to 560.67 ± 12.10 pg/mL, significantly higher than in exercise-stressed controls (p < 0.01).^[31] This elevation of BDNF is associated with improved neuronal adaptability and resilience in stress-induced paradigms. Furthermore, the 5-HT1A partial agonism may mitigate certain SSRI-related adverse effects, such as sexual dysfunction, by balancing serotonergic signaling and reducing excessive inhibition in relevant pathways, though clinical evidence remains mixed.^[32]^[33]

Pharmacokinetics

Vilazodone exhibits dose-proportional pharmacokinetics over the range of 5 mg to 80 mg, with steady-state concentrations achieved in approximately 3 days following repeated daily dosing.^[1] The terminal elimination half-life is about 25 hours, supporting once-daily administration.^[1] Absorption of vilazodone occurs primarily in the gastrointestinal tract, with peak plasma concentrations (T_max) reached in 4 to 5 hours post-dose when taken with food.^[1] The absolute oral bioavailability is approximately 72% in the presence of food, whereas administration under fasting conditions reduces the area under the curve (AUC) by about 50% and maximum concentration (C_max) by about 60%, emphasizing the need to take the drug with meals to ensure therapeutic levels.^[1] Vilazodone is widely distributed throughout the body, with a volume of distribution of approximately 605 L following intravenous administration, indicating extensive tissue penetration.^[34] It is highly bound to plasma proteins, ranging from 96% to 99%.^[1] Metabolism of vilazodone is extensive and occurs primarily in the liver through cytochrome P450 enzymes, with CYP3A4 as the major isoform responsible, alongside minor contributions from CYP2C19 and CYP2D6, as well as non-CYP pathways; the pharmacological activity resides mainly in the parent compound, with no active metabolites identified.^[1] Elimination is predominantly fecal, with less than 1% of the dose excreted unchanged in the urine and about 2% unchanged in the feces.^[1] This hepatic metabolism via CYP3A4 contributes to potential drug interactions with strong inhibitors or inducers of this enzyme.^[1] In special populations, no clinically significant differences in vilazodone pharmacokinetics are observed based on age, gender, or the presence of mild to severe renal or hepatic impairment, and thus no dosage adjustments are recommended for these groups.^[1]

Chemistry

Chemical structure and properties

Vilazodone is chemically described by the molecular formula C₂₆H₂₇N₅O₂, with a molecular weight of 441.5 g/mol for the free base.^[35] It is typically employed as the hydrochloride salt, which has a molecular weight of 478.0 g/mol.^[36] The compound belongs to the class of indolealkylamines and features a core structure incorporating an indole ring connected via a butyl chain to a piperazine moiety, which is further linked to a benzofuran-2-carboxamide group.^[37] The IUPAC name for vilazodone is 5-[4-[4-(5-cyano-1H-indol-3-yl)butyl]piperazin-1-yl]benzofuran-2-carboxamide.^[35] Physically, it appears as a white to off-white crystalline powder.^[36] Vilazodone is sparingly soluble in water, with a solubility of approximately 0.32 mg/mL, and exhibits a pKa of 7.1, indicating moderate basicity.^[36] Regarding stability, vilazodone hydrochloride is slightly hygroscopic and sensitive to light and moisture, necessitating protection during storage to maintain integrity.^[36] It is recommended to store the compound at controlled room temperature (15–30°C), often with desiccants to mitigate moisture effects.^[38]

Synthesis and formulation

Vilazodone is synthesized through a multi-step process starting from 5-cyanoindole as the key starting material. The initial step involves Friedel-Crafts acylation of 5-cyanoindole with 4-chlorobutyryl chloride under Lewis acid catalysis to form the intermediate 1-(5-cyano-1H-indol-3-yl)-4-chlorobutan-1-one.^[39] This ketone intermediate is then reduced using sodium bis(2-methoxyethoxy)aluminum hydride to yield 3-(4-chlorobutyl)-5-cyanoindole.^[39] The piperazine moiety is introduced via nucleophilic substitution (alkylation) of the chlorobutyl intermediate with 1-(2-ethoxycarbonylbenzofuran-5-yl)piperazine in acetonitrile under basic conditions, forming the coupled product.^[39] Subsequent hydrolysis of the ester group followed by amidation with ammonium hydroxide completes the synthesis of vilazodone base, which is then converted to the hydrochloride salt. Alternative routes may incorporate reductive amination of a butanone precursor with a piperazine derivative to achieve the side chain linkage, improving yield in scale-up processes.^[40] Vilazodone hydrochloride is formulated as immediate-release, film-coated tablets available in 10 mg (pink), 20 mg (orange), and 40 mg (blue) strengths for oral administration.^[41] The inactive excipients include lactose monohydrate, microcrystalline cellulose, colloidal silicon dioxide, magnesium stearate, and a film coating composed of polyethylene glycol, polyvinyl alcohol, talc, titanium dioxide, and appropriate colorants (FD&C Red #40 for 10 mg, FD&C Yellow #6 for 20 mg, FD&C Blue #1 for 40 mg); the formulation contains no gluten or preservatives.^[42] To optimize bioavailability, the absolute bioavailability of vilazodone is approximately 72% when taken with food; in the fasted state, exposure (AUC) and peak concentration (Cmax) are decreased by approximately 50% and 60%, respectively, compared to the fed state, so vilazodone tablets must be administered once daily with a meal.^[41] The original U.S. patent for vilazodone (US 5,532,241) expired in June 2022, enabling the development and market entry of generic formulations.^[43]

Society and culture

Brand names and availability

Vilazodone is primarily marketed under the brand name Viibryd in the United States by AbbVie, following its acquisition of Allergan and the original developer Forest Laboratories.^[1] This brand formulation is available as oral tablets in strengths of 10 mg, 20 mg, and 40 mg, supplied in bottles of 30 tablets or patient starter kits for dose titration, which include 7 tablets of 10 mg and 23 tablets of 20 mg to facilitate the recommended initiation schedule.^[1]^[44] In Canada, Viibryd is also available as a prescription medication for adults, distributed by AbbVie Canada with similar tablet formulations and packaging in blister packs or bottles of 30 units.^[3] Generic versions, such as Apo-Vilazodone, were approved in Canada on September 17, 2024, by Apotex Inc.^[45] However, vilazodone has not received marketing authorization in the European Union, limiting its availability there despite clinical interest.^[46] Globally, access remains restricted in many developing countries, where it is not widely approved or distributed as of 2025.^[47] Generic versions of vilazodone hydrochloride became available in the United States following the expiration of key patents in June 2022, with pediatric exclusivity ending on July 31, 2023. Note that vilazodone is not approved for pediatric use. The FDA approved the first generic version on September 30, 2019 (ANDA to Teva Pharmaceuticals), with additional generics approved in subsequent years, including in 2023.^[48]^[49]^[4] These generics are offered in equivalent strengths and packaging, typically 30-tablet bottles, and are prescription-only. No other international brand names beyond Viibryd have been established in approved markets. In the US, the brand-name Viibryd without insurance coverage costs approximately $240–$400 for a 30-day supply of 40 mg tablets, depending on the pharmacy and dosage, while generic equivalents reduce this to $30–$100 per month, enhancing accessibility for patients.^[50]^[51] In Canada, similar pricing dynamics apply, with generics expected to lower costs further as uptake increases.^[3]

Legal and regulatory status

Vilazodone hydrochloride, marketed under the brand name Viibryd, received approval from the U.S. Food and Drug Administration (FDA) on January 21, 2011, for the treatment of major depressive disorder (MDD) in adults.^[52] This approval was based on clinical trials demonstrating its efficacy as a selective serotonin reuptake inhibitor (SSRI) and 5-HT1A receptor partial agonist.^[2] In Canada, Health Canada approved vilazodone for MDD on July 16, 2015, with market entry on January 31, 2018.^[53] Vilazodone is not classified as a controlled substance under the U.S. Controlled Substances Act, as it has not demonstrated potential for abuse or dependence in preclinical or clinical studies.^[1] The FDA prescribing information explicitly states that vilazodone hydrochloride is not a scheduled drug, reflecting its low risk profile for misuse compared to substances with higher abuse potential.^[54] As part of the FDA approval, the sponsor was required to conduct several post-marketing commitments, including studies to evaluate the minimum effective dose, long-term safety, and potential effects on suicidality, particularly in younger populations.^[55] One such commitment was fulfilled in 2015 with the approval of the 20 mg dose based on a phase IV trial confirming its efficacy.^[56] As of 2025, ongoing pharmacovigilance efforts continue to monitor adverse events, including risks of suicidality and withdrawal effects, in line with class-wide requirements for antidepressants.^[1] The FDA approved the first generic version of vilazodone hydrochloride tablets (10 mg, 20 mg, and 40 mg) on September 30, 2019, with the ANDA granted to Teva Pharmaceuticals. Additional generics were approved in subsequent years, including in 2023, enhancing accessibility and reducing costs for patients.^[49]^[57] This followed the expiration of key patents in June 2022, allowing generic entry into the U.S. market.^[48] Internationally, vilazodone's regulatory status varies significantly. It has not received marketing authorization from the European Medicines Agency (EMA) and is not approved for use in the European Union.^[46] Similarly, it lacks approval from the Therapeutic Goods Administration (TGA) in Australia or the Pharmaceuticals and Medical Devices Agency (PMDA) in Japan, limiting its availability outside North America.^[58] Vilazodone is not included on the World Health Organization's Model List of Essential Medicines.

History

Development

Vilazodone was discovered in the late 1990s by researchers at Merck KGaA in Darmstadt, Germany, as part of efforts to develop a novel antidepressant combining selective serotonin reuptake inhibition with partial agonism at the 5-HT_1A receptor to potentially improve efficacy and onset of action over existing SSRIs.^[59]^[60] The compound advanced through early pre-clinical stages under Merck, focusing on its dual mechanism to target both serotonin reuptake and receptor modulation for enhanced therapeutic potential in major depressive disorder.^[30] Merck KGaA licensed vilazodone to GlaxoSmithKline in February 2001 for global development and commercialization, but GSK returned the rights in April 2003 after Phase II trials failed to meet efficacy endpoints for progression.^[61]^[62] In September 2004, Merck licensed the compound exclusively to Clinical Data, Inc., through its subsidiary Trovis Pharmaceuticals LLC (formerly PGxHealth), which assumed responsibility for further non-clinical and clinical advancement.^[59]^[28] Pre-clinical studies from the 1990s through the early 2000s, primarily conducted by Merck KGaA, evaluated vilazodone in established animal models of depression, including the forced swim test and tail suspension test in rodents, where it demonstrated robust antidepressant-like effects by reducing immobility time indicative of behavioral despair.^[63] These models also revealed minimal induction of sedation or motor impairment at therapeutically relevant doses, attributed to vilazodone's selective serotonergic profile avoiding substantial interactions with histaminergic or adrenergic systems.^[64]^[65] Additional rodent assays confirmed efficacy in depression-predictive paradigms without the sedative liabilities observed in some comparator agents.^[66] Early research emphasized indole-based scaffolds, as vilazodone's core structure incorporates a 5-cyanoindole moiety linked to a piperazine and benzofurancarboxylic acid, which provided high selectivity for the serotonin transporter (SERT) and 5-HT_1A receptor while minimizing off-target binding to other neurotransmitter systems.^[67] This structural design, refined during Merck's discovery phase, aimed to optimize dual pharmacodynamics for improved tolerability and reduced side effects like sexual dysfunction or weight gain common in SSRIs.^[68]^[30] Following the 2004 licensing, Clinical Data funded vilazodone's advancement with internal resources and milestone payments to Merck, including a €9.5 million payment in December 2007 upon completion of Phase II and entry into Phase III.^[69] Early Phase I trials assessing safety, tolerability, and pharmacokinetics in healthy volunteers were conducted in the late 1990s under Merck KGaA and subsequent licensees, with further studies supporting later development phases under Clinical Data, prioritizing the compound's favorable side effect profile to differentiate it in the antidepressant market.^[70]^[28]

Clinical trials and approval

The pivotal efficacy of vilazodone for major depressive disorder (MDD) was established through two phase III, randomized, double-blind, placebo-controlled trials conducted between 2008 and 2010, involving a combined total of over 1,000 adult patients aged 18-70 years.^[71] In these 8-week studies (GNSC-04-DP-02 and CLDA-07-DP-02), patients received vilazodone at a target dose of 40 mg/day following a 2-week titration, with primary efficacy assessed via change in Montgomery-Åsberg Depression Rating Scale (MADRS) total scores from baseline.^[71] The first trial (n=410 randomized) showed least-squares mean MADRS reductions of -12.9 points for vilazodone versus -9.7 points for placebo (difference -3.2, p=0.001), while the second (n=481 randomized) demonstrated -13.3 versus -10.8 points (difference -2.5, p=0.009), confirming statistical superiority over placebo in both.^[71] Secondary outcomes, including MADRS response rates (≥50% reduction) and remission rates (<10 score), further supported efficacy, with vilazodone achieving 43.7% response versus 30.3% for placebo in the second trial (p=0.0024).^[71] A meta-analysis of these and additional phase III/IV trials corroborated the findings, reporting a mean difference in MADRS change of -3.73 points at week 8 favoring vilazodone (95% CI -4.74 to -2.72, p<0.001) and a relative risk of response of 1.42 (95% CI 1.28-1.56, p<0.001).^[72] Long-term safety and tolerability were evaluated in a 52-week, open-label extension study (CLDA-07-DP-04) involving 599 patients who had completed prior acute trials, with a total exposure of 348 patient-years.^[71] Vilazodone 40 mg/day was generally well tolerated, with mean MADRS reductions reaching -22.8 points by week 52 on an observed-case basis, and discontinuation due to treatment-emergent adverse events occurring in 21% of participants.^[71] Common adverse events included nausea (1.3 per patient-year), diarrhea (1.2), and insomnia (1.0), with no clinically significant changes in vital signs, weight, or ECG parameters such as QTc intervals at therapeutic doses.^[71] Serious adverse events were rare (4% of patients), primarily infections or respiratory issues, supporting the drug's long-term profile without new safety signals.^[71] The New Drug Application (NDA 22-567) for vilazodone was submitted to the U.S. Food and Drug Administration (FDA) on March 22, 2010, by PGxHealth (formerly Clinical Data, Inc.), based on data from the two pivotal phase III trials and supporting safety studies.^[34] The review process addressed concerns regarding potential QT prolongation, with a dedicated thorough QT study (PGX-08-P1-06) at supratherapeutic doses (80 mg) showing tachycardia in 18% of subjects versus 5% on placebo but no significant QTc changes at the approved 40 mg dose.^[71] Following label revisions to include warnings for cardiac events and dry eye, the FDA approved vilazodone (as Viibryd) on January 21, 2011, for the treatment of MDD in adults, with a recommended starting dose of 10 mg/day titrated to 40 mg/day taken with food.^[52]^[71] Following FDA approval, Clinical Data was acquired by Forest Laboratories in April 2011 for $1.2 billion, which assumed responsibility for the commercialization of Viibryd.^[73] Post-approval, pediatric development was pursued under FDA requirements, with studies initiated for children and adolescents aged 7-17 years with MDD.^[52] A phase III trial (NCT02372799) evaluated vilazodone 15-30 mg/day versus placebo over 8 weeks but found no significant differences in Children's Depression Rating Scale-Revised (CDRS-R) scores or response rates, failing to support efficacy.^[74] Similar negative results were reported in another randomized trial, with no new safety concerns but insufficient evidence for approval.^[75] As of 2025, vilazodone remains unapproved for pediatric use.^[76] Globally, vilazodone received approval in the United States in 2011 and in Canada in 2018, primarily based on the U.S. clinical data, with limited availability elsewhere due to lack of broader regulatory endorsements.

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Vilazodone blocks the serotonin reuptake pump (serotonin transporter or SERT), desensitizes serotonin receptors (especially 5HT1A autoreceptors), and therefore ...
[7]
A Review of Vilazodone, Serotonin, and Major Depressive Disorder
Jan 9, 2014 · Vilazodone was specifically designed to function both as an SSRI and a partial agonist at 5-HT1A receptors. This combined mechanism is proposed ...
[8]
Vilazodone: Pharmacology, Indications, Dosing Guidelines and ...
Oct 10, 2025 · Vilazodone is a selective serotonin reuptake inhibitor and a 5-HT1A receptor partial agonist · This dual mechanism is often termed Serotonin ...
[9]
[PDF] Reference ID: 2894777 1 - accessdata.fda.gov
VIIBRYD is not approved for use in pediatric patients (8.4). INDICATIONS AND USAGE. VIIBRYD is indicated for the treatment of major ...
[10]
Evaluating the efficacy of vilazodone in achieving remission in ... - NIH
Previous pooled analyses of the data from the two pivotal phase III trials showed that vilazodone-treated patients had significantly higher rates of remission, ...
[11]
A Review of Vilazodone, Serotonin, and Major Depressive Disorder
Vilazodone was specifically designed to function both as an SSRI and a partial agonist at 5-HT1A receptors. This combined mechanism is proposed to decrease time ...
[12]
Vilazodone in patients with generalized anxiety disorder - NIH
This was a positive clinical trial of 20–40 mg/day vilazodone versus placebo in the treatment of GAD.
[13]
Efficacy and tolerability of vilazodone for the acute treatment of ...
Vilazodone is an effective treatment for generalized anxiety disorder, though further trials are required for a more adequate comparison with established ...
[14]
An 8-Week Randomized, Double-Blind Trial Comparing Efficacy ...
Aug 6, 2015 · The present study indicates the potential benefit of switching to vilazodone in patients with MDD who are inadequate responders to SSRIs or SNRIs.Missing: post- | Show results with:post-
[15]
Vilazodone for Major Depression in Adults: Pharmacological Profile ...
Jun 14, 2022 · In a more rigorous randomized relapse prevention trial, 1204 adults with MDD received 20 weeks of open treatment with vilazodone 40 mg/day. Of ...
[16]
Vilazodone no better than placebo or fluoxetine in multisite RCT
Jul 24, 2020 · Vilazodone was found not effective for pediatric patients with major depressive disorder (MDD) in a recent study comparing it with placebo ...
[17]
Study Details | NCT01715519 | Vilazodone for the Treatment of Posttraumatic Stress Disorder | ClinicalTrials.gov
- **Status**: Completed
[18]
[PDF] This label may not be the latest approved by FDA. For current ...
INDICATIONS AND USAGE. VIIBRYD is indicated for the treatment of major depressive disorder (MDD) in adults (1). DOSAGE AND ADMINISTRATION.
[19]
Effects of vilazodone on suicidal ideation and behavior in adults with ...
Incidences of C-SSRS suicidal ideation were as follows: MDD (vilazodone=19.9%, placebo=24.7%); GAD (vilazodone=7.7%, placebo=9.4%).Missing: clinical | Show results with:clinical
[20]
Vilazodone (Viibryd) | National Alliance on Mental Illness (NAMI)
Vilazodone is an antidepressant medication that works in the brain. It is approved for the treatment of major depressive disorder (MDD).What Is Vilazodone And What... · What Is The Most Important... · What Should I Discuss With...Missing: investigational | Show results with:investigational<|control11|><|separator|>
[21]
[PDF] Page 1 of 14 - accessdata.fda.gov
Signs and symptoms associated with more severe and/or acute cases have included hallucination, syncope, seizure, coma, respiratory arrest, and death. 6. ADVERSE ...
[22]
Vilazodone (Viibryd®) - MotherToBaby | Fact Sheets - NCBI Bookshelf
Studies have not been done to see if vilazodone use in pregnancy can cause behavior or learning issues for the child. Breastfeeding while taking vilazodone: It ...
[23]
SSRI antidepressant use during pregnancy and reports of a ... - FDA
Feb 13, 2018 · Untreated depression during pregnancy may lead to poor birth outcomes, including low birth weight, preterm delivery, lower Apgar Scores, poor ...<|control11|><|separator|>
[24]
https://pmc.ncbi.nlm.nih.gov/articles/PMC10696173/
[25]
Concepts for selection and utilization of psychiatric medications in ...
Dec 1, 2023 · Sertraline is currently considered the most preferred agent during pregnancy. Citalopram is considered a preferred agent, and fluoxetine is ...
[26]
Vilazodone - Drugs and Lactation Database (LactMed®) - NCBI - NIH
Apr 18, 2022 · Mothers who took an antidepressant only during the third trimester were 75% less likely to be breastfeeding at discharge. Those who took an ...<|control11|><|separator|>
[27]
Viibryd (vilazodone) dosing, indications, interactions, adverse effects ...
... FDA recommendation: FDA advises health-care professionals not to alter their current clinical practice of treating depression during pregnancy and to report ...
[28]
Influence of CYP3A4 induction/inhibition on the pharmacokinetics of ...
Nov 1, 2014 · Findings: In study 1/parts 1 and 2 (n = 15 and 22 enrolled, respectively), mean vilazodone AUC increased 42% and 51%, respectively, in the ...
[29]
[PDF] 022567Orig1s000 - accessdata.fda.gov
Jan 14, 2011 · Vilazodone is a new molecular entity submitted under the current NDA for treatment of major depressive disorder. The pharmacology/toxicology ...
[30]
Vilazodone for the Treatment of Major Depressive Disorder
As noted above, insomnia is one of the important adverse effects caused by vilazodone. Its effect on sleep was specifically investigated via analyzing and ...
[31]
Vilazodone: A 5‐HT1A Receptor Agonist/Serotonin Transporter ...
Vilazodone is a combined 5-HT reuptake inhibitor and 5-HT 1A receptor partial agonist, which has been developed to presumably produce a more rapid and specific ...Missing: advantages | Show results with:advantages
[32]
[PDF] BASIC SCIENCES 73 VILAZODONE ENHANCES THE ...
The treatment with VLZ improved the physical performances and the endurance capacity in this experimentally-induced stress model in rats. The use of this antide ...Missing: neuroplasticity | Show results with:neuroplasticity
[33]
Differential effects of vilazodone versus citalopram and paroxetine ...
Jan 13, 2016 · The current studies showed that chronic treatment with vilazodone, in contrast to citalopram and paroxetine, was not associated with diminished sexual ...
[34]
Vilazodone for the treatment of major depressive disorder - NIH
Vilazodone is excreted into the milk of lactating rats (Forest Pharmaceuticals). The effect of vilazodone on lactation and nursing in humans is unknown.Missing: breastfeeding | Show results with:breastfeeding
[35]
[PDF] 022567Orig1s000 - accessdata.fda.gov
Dec 10, 2010 · Vilazodone is extensively metabolized through CYP and non-CYP pathways, and mainly excreted through feces.
[36]
Vilazodone | C26H27N5O2 | CID 6918314 - PubChem - NIH
It is not known if vilazodone gets into breast milk or causes side effects for a baby who receives the milk. The benefit of continuing vilazodone while ...
[37]
[PDF] 022567Orig1s000 - accessdata.fda.gov
Jan 7, 2011 · The solubility in water is 0.32mg/mL. The partition coefficient between n-octanol and water is The pKa is 7.1. The melting point and ...Missing: IUPAC | Show results with:IUPAC
[38]
[PDF] 022567Orig1s000 - accessdata.fda.gov
Jan 5, 2011 · As illustrated in the table below, the most common adverse reactions were diarrhea, nausea, vomiting, dry mouth, dizziness, insomnia ...
[39]
[PDF] Vilazodone Hydrochloride Tablets
Sep 17, 2024 · excluded from clinical trials with vilazodone hydrochloride tablets. Caution should be exercised in treating patients with uncontrolled ...
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https://www.semanticscholar.org/paper/Scale-Up-Synthesis-of-Antidepressant-Drug-Hu-Song/b4f33d0af8c46be0820b062af61fcc61d4541a1f
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Scale-Up Synthesis of Antidepressant Drug Vilazodone
Sep 13, 2012 · A scale-up synthesis of antidepressant drug vilazodone was accomplished in five steps. Friedel–Crafts acylation of ...
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See full prescribing information for - VILAZODONE - DailyMed
VILAZODONE tablets for oral administration contain polymorph Form IV vilazodone hydrochloride (HCl), a selective serotonin reuptake inhibitor and a 5HT1A ...
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Clinical Data's anti-depressant gets US patent | Reuters
Nov 16, 2010 · The patent will expire in June 2022, the company said in a statement. A similar patent has also been granted in Europe till May 2022, it said.
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VILAZODONE HYDROCHLORIDE tablet, film coated - DailyMed - NIH
Store at 20° to 25°C (68° to 77°F) [See USP Controlled Room Temperature]. Dispense in a tight, light-resistant container as defined in the USP, with a child- ...
[46]
Vilazodone for major depressive disorder in adults - PMC
Vilazodone is an antidepressant that is at present only approved in the USA for the treatment of MDD (Kalia 2011).
[47]
Vilazodone - an overview | ScienceDirect Topics
(Viibryd). International Brand Names. Drug Class, Antidepressant, SSRI. Indications, Depression. Mechanism, Inhibits serotonin reuptake; 5-HT1 ...
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Generic Viibryd Availability - Drugs.com
Oct 8, 2025 · Yes, the FDA has approved a generic version of Viibryd. However, FDA approval doesn't guarantee the generic will be available in pharmacies.Missing: current | Show results with:current
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https://www.fda.gov/drugs/first-generic-drug-approvals/2019-first-generic-drug-approvals
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Viibryd cost 2025: Savings tips and more - MedicalNewsToday
Dec 17, 2024 · The active ingredient of Viibryd is vilazodone. It's available in a generic version. A generic drug is considered to be as safe and effective as ...
[51]
[PDF] 022567Orig1s000 | FDA
Jan 21, 2011 · This new drug application provides for the use of Viibryd (vilazodone hydrochloride) for the treatment of Major Depressive Disorder. We have ...
[52]
Summary Basis of Decision for Viibryd
Requirements for post-market commitments are outlined in the Food and Drugs Act and Regulations. 5 What post-authorization activity has taken place for Viibryd?
[53]
Vilazodone: Package Insert / Prescribing Information - Drugs.com
Vilazodone hydrochloride tablets are not approved for use in pediatric patients (8.4). Indications and Usage for Vilazodone. Vilazodone hydrochloride tablets ...Missing: hypersensitivity | Show results with:hypersensitivity
[54]
[PDF] 022567Orig1s000 - accessdata.fda.gov
Jan 24, 2011 · 22567 Vilazodone- Requested Postmarketing Requirements and Commitments. Required Pediatric Assessments. We are waiving the pediatric study ...
[55]
Actavis Receives FDA Approval for VIIBRYD® (vilazodone HCl ...
Mar 16, 2015 · VIIBRYD was approved in January 2011 as the first and only selective serotonin reuptake inhibitor (SSRI) and 5HT1a receptor partial agonist for ...
[56]
ANDA Approvals of Q3 - Fall 2023 | Hatch-Waxman
A quarter 3 list of generic drug ANDA approvals in GENERICally Speaking Hatch-Waxman Litigation Bulletin by Robins Kaplan LLP.
[57]
KEGG DRUG: Vilazodone hydrochloride
New drug approvals in the USA, Europe and Japan [br08328.html] Approval dates by FDA, EMA and PMDA D09699 Drug metabolizing enzymes and transporters ...
[58]
Vilazodone - SEC.gov
Vilazodone was discovered by Merck KGaA (a €7.2B global pharmaceutical and chemical company) as a candidate for the treatment of depression. It was found to ...Missing: Trovir | Show results with:Trovir
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[PDF] Vilazodone for major depressive disorder
Remission rates (MADRS <10) were not re- ported in this study, but the ... Efficacy of vilazodone in phase III clinical trials. Table 2 continued on ...
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Merck KGaA licenses antidepressant to GlaxoSmithKline - BioWorld
Feb 15, 2001 · GlaxoSmithKline and Merck KGaA have signed a worldwide development and commercialization agreement for the antidepressant vilazodone ...
[61]
GSK returns vilazodone rights to Merck KGaA
Apr 21, 2003 · GlaxoSmithKline is returning rights to investigational antidepressant vilazodone to Merck KgaA following failed Phase II studies.
[62]
[PDF] 022567Orig1s000 - accessdata.fda.gov
Jan 7, 2011 · Vilazodone produces antidepressant-like behavioral effects in preclinical models of depression. 4. Animal self-administration studies ...
[63]
Vilazodone: A 5-HT 1A Receptor Agonist/Serotonin Transporter ...
May 6, 2009 · Three separate studies have evaluated the efficacy of vilazodone in various rodent models thought to be predictive of anxiolytic activity. In ...
[64]
Vilazodone - an overview | ScienceDirect Topics
Vilazodone's mechanism of antidepressive action involves serotonin reuptake inhibition and agonist activity to the 5-HT1A receptor [92].
[65]
Vilazodone HCl (Viibryd): A Serotonin Partial Agonist and Reuptake ...
Vilazodone was approved by the FDA for the treatment of MDD in January 2011. DOSAGE AND ADMINISTRATION. Vilazodone tablets are available in 10-mg, 20-mg, and 40 ...
[66]
Structural basis of vilazodone dual binding mode to the serotonin ...
The antidepressant vilazodone has been shown to inhibit SERT by binding to an allosteric site. Here, we present the cryo-EM structure of SERT with vilazodone ...
[67]
The antidepressant drug vilazodone is an allosteric inhibitor ... - Nature
Aug 20, 2021 · Its action on the 5-HT1A receptor is thought to provide for its faster onset of action relative to the classical SSRIs47, as has been observed ...
[68]
Clinical Data Delivers Vilazodone Milestone Payment to Merck KGaA
Dec 10, 2007 · Clinical Data's PGxHealth Division acquired the rights to develop and commercialize Vilazodone from Merck in September 2004. Under the terms ...
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Viibryd - Treatment for Major Depressive Disorder
Feb 21, 2011 · Viibryd (Vilazodone) is an antidepressant manufactured for the treatment of adults with major depressive disorder (MDD).
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[PDF] 022567Orig1s000 - accessdata.fda.gov
Jan 21, 2011 · 1.2 Risk Benefit Assessment. The efficacy of vilazodone was demonstrated in two (2) of seven (7) controlled trials.
[71]
Efficacy and tolerability of vilazodone for major depressive disorder
Nov 25, 2016 · 40 mg/day of vilazodone had a rapid onset of response and showed good improvement in anxiety symptoms as well as good tolerability during short-term treatment ...
[72]
A Randomized, Double-Blind, Placebo-Controlled Trial of ... - NIH
This study does not support the efficacy of vilazodone 15 or 30 mg/day for pediatric patients with MDD. No new or unexpected safety concerns were detected.Missing: post- | Show results with:post-
[73]
A Phase 3, Double-Blind, Randomized, Placebo-Controlled Study of ...
Apr 9, 2018 · In this double-blind randomized clinical trial of adolescents with MDD, no significant differences between vilazodone and placebo were observed ...
[74]
[PDF] Viibryd - VHB-master-uspi-vilazodone - 20084716 10-2023 and 4 ...
INDICATIONS AND USAGE. VIIBRYD is indicated for the treatment of major depressive disorder (MDD) in adults (1). DOSAGE AND ADMINISTRATION.
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Vilazodone - Wikipedia
Pharmacology. edit. Pharmacodynamics. edit. Vilazodone acts as a serotonin reuptake inhibitor (IC50 = 2.1 nM; Ki = 0.1 nM) and 5-HT1A receptor partial agonist ...