Clinical data | |
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Trade names | Provigil, Alertec, Modavigil, others |
Other names | CRL-40476; Diphenylmethyl-sulfinylacetamide |
AHFS/Drugs.com | Monograph |
MedlinePlus | a602016 |
License data | |
Pregnancy category |
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Dependence liability | Relatively low |
Addiction liability | Very low to low[1] |
Routes of administration | By mouth[2] |
Drug class | CNS stimulant |
ATC code | |
Legal status | |
Legal status | |
Pharmacokinetic data | |
Protein binding | 62.3% |
Metabolism | Liver (primarily via amide hydrolysis);[7] CYP1A2, CYP2B6, CYP2C9, CYP2C19, CYP3A4, CYP3A5 involved[8] |
Elimination half-life | 12–15 h[7] (modafinil, the racemic mixture), 15 h (armodafinil, the (R)-enantiomer),[9] 4 h (esmodafinil, the (S)-enantiomer).[10] |
Excretion | Urine (80%) |
Identifiers | |
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CAS Number | |
PubChem CID | |
IUPHAR/BPS | |
DrugBank | |
ChemSpider | |
UNII | |
KEGG | |
ChEBI | |
ChEMBL | |
CompTox Dashboard (EPA) | |
ECHA InfoCard | 100.168.719 |
Chemical and physical data | |
Formula | C15H15NO2S |
Molar mass | 273.35 g·mol−1 |
3D model (JSmol) | |
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Modafinil, sold under the brand name Provigil among others, is a wakefulness-promoting medication used primarily to treat narcolepsy. It is classified as a eugeroic (a wakefulness-promoting drug) rather than a classical psychostimulant due to its lack of euphoric effects. Modafinil's unique mechanism of action sets it apart from other stimulants, making it a valuable medication for managing sleep disorders.
Narcolepsy is a neurological disorder characterized by excessive daytime sleepiness, sudden bouts of uncontrollable sleep attacks, and, in some cases, sudden muscle weakness (cataplexy). People with narcolepsy often struggle to stay awake and alert during the day, which impacts their daily activities and overall quality of life. Modafinil relieves symptoms associated with narcolepsy, allowing individuals to maintain wakefulness and reduce sleep episodes.
Beyond narcolepsy, modafinil has also proven effective in treating other conditions, such as shift work sleep disorder and excessive daytime sleepiness caused by obstructive sleep apnea, a sleep-related breathing disorder that occurs when the throat muscles relax and block the airway during sleep, that disrupts sleep and makes the person feel tired during the day. In these cases, modafinil helps individuals manage their abnormal sleeping patterns and promotes optimal wakefulness when they need to be alert for work or daily responsibilities.
While modafinil has gained popularity as a cognitive enhancer or "smart drug" among healthy individuals seeking improved focus and productivity, its use outside medical supervision raises concerns regarding potential misuse or abuse. Research on the cognitive enhancement effects of modafinil in non-sleep-deprived individuals has yielded mixed results, with some studies suggesting modest improvements in attention and executive functions while others show no significant benefits or even a decline in cognitive functions.
Usage
Medical
Sleep disorders
Modafinil, a eugeroic or wakefulness-promoting drug, is primarily used for treating narcolepsy, a sleep disorder characterized by excessive daytime sleepiness and sudden sleep attacks.[11] Being a central nervous system (CNS) stimulant (psychostimulant) itself, modafinil, unlike classical psychostimulants, does not produce euphoric effects.[12][13][14]
Narcolepsy causes a strong urge to sleep during the day and can include symptoms like cataplexy (sudden muscle weakness), sleep paralysis (inability to move or speak while falling asleep or waking up), and hallucinations. The disorder is linked to a lack of the brain chemical hypocretin (or orexin), primarily produced in the hypothalamus.[15][16]
Modafinil is also prescribed for shift work sleep disorder and excessive daytime sleepiness in obstructive sleep apnea, though it is recommended that patients use continuous positive airway pressure (CPAP) therapy before starting modafinil.[17][18][19] For obstructive sleep apnea, modafinil is advised after optimal CPAP therapy use.[20]
Modafinil's use varies by region. In the US, it's approved for adult narcolepsy, shift work sleep disorder, and obstructive sleep apnea, but not for children.[21] In the UK and EU, since 2014, it's approved solely for narcolepsy, including in children (pediatric narcolepsy), with its use for other conditions restricted by the European Medicines Agency.[22][23]
As of 2023, the French and American Academy of Sleep Medicine strongly recommend modafinil as the first-choice treatment for narcolepsy.[24]
The recommended dose of modafinil for narcolepsy is 200 mg once a day in the morning.[25][21][26]
Multiple sclerosis-related fatigue
The National Institute for Health and Care Excellence (NICE) in the UK, along with various NGOs focused on multiple sclerosis (MS), endorse the off-label use of modafinil to alleviate fatigue associated with MS.[27][28][21]
MS-related fatigue is a common and often debilitating symptom experienced by many patients. It can significantly impact their daily functioning, quality of life, and ability to perform everyday activities. When prescribed for MS-related fatigue management, modafinil works by promoting wakefulness and increasing alertness without causing drowsiness or disrupting nighttime sleep. Patients often report increased energy levels, reduced feelings of tiredness, improved cognitive function, and an overall improvement in their quality of life when taking modafinil. While modafinil can provide relief from MS-related fatigue symptoms, it does not treat the underlying cause or cure MS itself. The primary goal of using modafinil in MS is symptom management and improving daily functioning.[29][30][31] The effects of modafinil on other aspects of MS-related fatigue, such as severity and cognitive function, are less clear.[32]
Whereas modafinil has been shown to be effective in managing fatigue in patients with MS, optimal dosing and treatment schedules are not well established.[32] The usual starting dosage of modafinil for MS-related fatigue is typically 200 mg per day. However, healthcare professionals may adjust the dosage based on individual patient needs and response to treatment. Some patients may require higher doses up to 400 mg per day if necessary.[29][30][31]
Attention deficit hyperactivity disorder
Modafinil is occasionally prescribed off-label for individuals with attention deficit hyperactivity disorder (ADHD).[33][34][35] In adults, modafinil is inferior to other treatments such as lisdexamfetamine.[36][37] In children, modafinil is efficient in treating ADHD symptoms.[38][39]
Given its approved status in the US, physicians can legally prescribe modafinil for off-label uses, such as treating ADHD in both children and adults.[40][41][42]
The Canadian Network for Mood and Anxiety Treatments (CANMAT) suggests modafinil as a second-line choice for ADHD, after the first-line choices such as bupropion are exhausted.[43]
Bipolar depression
Modafinil is used off-label as an adjunctive treatment (i.e., in combination therapy) for bipolar depression, which is a depressive phase of bipolar disorder and is characterized by excessive sleepiness and fatigue. Adjunctive treatment with modafinil is an augmentation for the main treatment to increase its effect and is safe and effective especially for patients who do not respond well to standard antidepressants. Modafinil does not increase the risk of mood switches or suicide attempts in patients with bipolar depression, but common adverse effects of modafinil in bipolar depression are headache, nausea, and insomnia. Modafinil may also have cognitive benefits in patients with bipolar disorder who are in a remission phase.[44][45]
Occupational
Modafinil was utilized by the French Foreign Legion,[46] US Air Force,[47][48][49] and US Marine[50] infantry during the Gulf War to enhance "operational tempo," a term that denotes the speed and intensity at which military operations or activities are executed, aiming to optimize the overall performance and efficiency of the unit.[49][51][52]
Adrafinil, a prodrug of modafinil, was initially tested for narcolepsy in France in 1986. Modafinil, identified as more efficient, was approved by the French Ministry of Defense in 1989 for military use under the name Virgyl. Its adoption aimed to improve unit efficiency in operations, a policy implemented before modafinil's commercial release in 1994.[53] Military personnel were not informed about the nature of the product during these trials.[54] Subsequent studies did not confirm modafinil's benefits in non-sleep-deprived military contexts.[48]
Armed forces in various countries, including the US, UK, India, and France, have considered modafinil as an alternative to traditional amphetamines for managing sleep deprivation in combat or extended missions.[55] The UK's Ministry of Defence and the Indian Air Force have included modafinil in their research and contingency plans.[56][57]
The US military approved modafinil for specific Air Force missions, replacing amphetamines for fatigue management.[58][59] Modafinil is also available to astronauts on the International Space Station to manage fatigue and circadian rhythm disruptions.[60]
The use of modafinil in military contexts without sleep deprivation is not recommended due to inconclusive evidence on its cognitive enhancement benefits and potential risks.[48]
Non-medical
Modafinil has been utilized non-medically as a "smart drug"[61][62] by various groups, including students,[63][64][65] office workers, transhumanists,[66][67] and professionals in various sectors. Its use is attributed by these individuals to its potential for enhancing attention, cognitive capabilities, and alertness.[68][69]
Despite its popularity, modafinil does not significantly enhance cognitive or attentional performance in non-sleep-deprived individuals. In some cases, it has even been associated with impairments in certain cognitive functions.[70][18][71]
In this context, the term "non-sleep-deprived individual" refers to a person who is not suffering from sleep deprivation. These individuals have normal sleep patterns and are not excessively tired or sleepy during the day.[72]
Available forms
Modafinil is commercially available in 100 mg and 200 mg oral tablet forms.[17] Additionally, it is offered as the (R)-enantiomer, known as armodafinil, and as a prodrug named adrafinil.[73]
Drug tolerance
Extensive clinical research has not demonstrated drug tolerance, defined as a reduction in response, to modafinil's wakefulness-promoting and anti-fatigue properties, even with therapeutic use extending up to three years. While modafinil is generally well-tolerated, including in pediatric narcolepsy cases (sleep disorders in children), there is evidence that long-term usage can lead to tolerance in some individuals. This necessitates higher doses to maintain the same level of cognitive enhancement or relief from sleepiness. Patients with current or past substance addictions and those with a family history of addiction are particularly at risk for developing tolerance. The mechanisms driving tolerance to modafinil, which may involve its impact on dopamine and norepinephrine levels in the brain, are not fully understood. Repeated administration of modafinil for off-label use, such as increased alertness and cognitive-enhancing effects in sleep deprivation, can lead to drug tolerance, which means that the effectiveness of the drug may decrease over time. Still, modafinil therapy as a eugeroic agent to treat narcolepsy does not typically lead to drug tolerance, i.e., does not usually decrease on prolonged use, although individual responses may vary.[18][74][75]
Contraindications
Modafinil is contraindicated for individuals with known hypersensitivity to either modafinil or armodafinil.[76]
The US FDA does not endorse modafinil for children's medical conditions due to an increased risk of rare but serious dermatological toxicity.[77][78][79] However, in Europe, modafinil may be prescribed for treating narcolepsy in children.[75]
Due to the limited information available on the excretion of modafinil into breastmilk and its potential effects on infants, breastfeeding mothers using modafinil are advised to be monitored closely, or alternative drugs may be preferred until more safety data emerge.[80]
Modafinil is also contraindicated in certain cardiac conditions, including uncontrolled moderate to severe hypertension, arrhythmia, cor pulmonale, and in cases with signs of CNS stimulant-induced mitral valve prolapse or left ventricular hypertrophy. It is further contraindicated in patients with congenital problems like galactose intolerance, lactase deficiency, or glucose-galactose malabsorption.[81][82]
Adverse effects
Modafinil is generally well-tolerated but can have potential risks and side effects. Common adverse effects of modafinil, experienced by less than 10% of users, include headaches, nausea, and reduced appetite. Anxiety, insomnia, dizziness, diarrhea, and rhinitis are also reported in 5% to 10% of users.[21] Psychiatric reactions have occurred in individuals with and without a preexisting psychiatric history.[83]
No significant changes in body weight have been observed in clinical trials, although decreased appetite and weight loss have been noted in children and adolescents.[84] Modafinil can cause a slight increase in aminotransferase enzymes, indicative of liver function, but there is no evidence of serious liver damage when levels are within reference ranges.[85]
Rare but serious adverse effects include severe skin rashes and allergy-related symptoms. Between December 1998 and January 2007, the FDA received reports of six cases of severe cutaneous adverse reactions, including erythema multiforme, Stevens–Johnson syndrome, toxic epidermal necrolysis, and DRESS syndrome. The FDA has issued alerts regarding these risks and also noted reports of angioedema and multi-organ hypersensitivity reactions in postmarketing surveillance.[86][87]
In 2007, the FDA required Cephalon to modify the Provigil leaflet to include warnings about these serious conditions. The long-term safety and effectiveness of modafinil have not been conclusively established.[88] However, a longitudinal study has shown that modafinil and armodafinil are safe and effective in children treated for narcolepsy for up to ten years, with no exacerbation of preexisting psychiatric conditions.[89]
An online survey in 2020 found higher levels of illicit drug use and psychiatric diagnoses among modafinil users compared to population-based data, with more frequent use associated with perceived benefits and a tentative link to psychiatric disorders, primarily depression and anxiety.[90]
Addiction and dependence
Whereas modafinil is a CNS stimulant, its addiction and dependence liabilities are considered very low.[1][91][14] Although modafinil shares biochemical mechanisms with stimulant drugs, it is less likely to have mood-elevating properties.[91] The similarities in effects with caffeine are not clearly established.[12][92] Unlike other stimulants, modafinil does not induce a subjective feeling of pleasure or reward, which is commonly associated with euphoria, an intense feeling of well-being. Euphoria is a potential indicator of drug abuse, which is the compulsive and excessive use of a substance despite adverse consequences. In clinical trials, modafinil has shown no evidence of abuse potential, as measured by pill return rates. Pill return rates are a method of assessing how many pills of the study medication are left over at the end of each week. If a drug is abused, patients are expected to consume more pills than prescribed and return fewer pills. However, in the case of modafinil, there was no significant difference between the number of pills returned by patients who received modafinil and those who received a placebo, suggesting that modafinil does not promote overuse or misuse, even in patients who have a history of cocaine addiction, which is a highly addictive and euphoric substance. Therefore, modafinil is considered to have a low risk of addiction and dependence.[93] However, caution is advised due to psychoactive effects similar to other CNS stimulants.[21]
The United States Drug Enforcement Administration has classified modafinil as a schedule IV controlled substance;[6] the medicine is recognized for having valid medical uses with low addiction potential.[1][40] The International Narcotics Control Board does not classify it as a narcotic or a psychotropic substance.[94][95] Studies suggest modafinil may improve abstinence in cocaine addicts, without notable adverse effects upon discontinuation.[96]
Sodium oxybate, another drug to treat narcolepsy, is a salt of gamma-hydroxybutyric acid, which is a normal metabolite of GABA that interacts with the GABAB receptor. While modafinil is a CNS stimulant, sodium oxybate is a CNS depressant. Sodium oxybate has the potential for abuse, and is classified in the US as a Schedule III controlled substance for medicinal use under the Controlled Substances Act, with illicit use subject to Schedule I penalties. It is also a controlled substance in Canada and Europe.[97][98][14]
Pitolisant, another drug to treat narcolepsy, is a histamine H3 receptor inverse agonist. It is not classified as a controlled substance, and is approved for use in Europe and the United States. Still, long-term studies comparing the effectiveness and tolerability of pitolisant with modafinil or sodium oxybate are lacking. Pitolisant, the only non-controlled anti-narcoleptic drug in the US, has shown minimal abuse risk in studies, expanding treatment options for adult narcolepsy patients, where addiction, dependence or abuse is a concern. The non-controlled status of pitolisant eliminates any potential legal penalties or restrictions, such as restrictions associated with crossing borders of countries where pitolisant is a non-controlled substance, but where certain medications, such as modafinil, may be regulated more strictly due to their controlled substance classification, meaning that patients can travel between countries where pitolisant is not a controlled substance, without worrying about obtaining special permissions or facing legal consequences related to their medication to treat narcolepsy.[99][100][101]
Overdose
An overdose of modafinil can lead to a range of symptoms and complications. Psychiatric symptoms may include psychosis, mania, hallucinations, and suicidal ideation, which can occur even in individuals without a history of mental illness and may persist after discontinuation of the drug.[102] Neurological complications, such as seizures, tremors, dystonia, and dyskinesia, may arise from modafinil's interaction with various neurotransmitter systems.[102]
Allergic reactions such as rash, angioedema, anaphylaxis, and Stevens–Johnson syndrome may be triggered by an immunological response to modafinil or its metabolites.[103][104] Cardiovascular complications like hypertension, tachycardia, chest pain, and arrhythmias may also be observed due to modafinil's sympathomimetic action.[102]
In animal studies, the median lethal dose (LD50) of modafinil is approximately 1 mg/kg in mice and rats, and higher in other species. Human clinical trials have involved doses up to 1200 mg/d for 7–21 days. Acute one-time overdoses up to 4500 mg have not been life-threatening but resulted in symptoms like agitation, insomnia, tremor, palpitations, and gastrointestinal disturbances.[17]
The management of modafinil overdose involves supportive care, monitoring of vital signs, and treatment of specific complications. In cases of recent consumption, activated charcoal, gastric lavage, or hemodialysis may be used. There is no specific antidote for modafinil overdose.[102][105][106]
Interactions
As of 2024, modafinil is known to interact with 463 drugs. These interactions can be classified as major (71), moderate (211), and minor (181).[107]
Some of the drugs that frequently interact with modafinil include aripiprazole (an antipsychotic), amphetamine (including its enantiomers and salts; stimulants), aspirin, diphenhydramine (an antihistamine), and others.[107]
Modafinil is a weak to moderate inducer of CYP3A4[108][109] and a weak inhibitor of CYP2C19, enzymes of the cytochrome P450 group of enzymes.[21] Modafinil also induces or inhibits other cytochrome P450 enzymes. One in vitro study predicts that modafinil may induce the cytochrome P450 enzymes CYP1A2, CYP3A4, and CYP2B6, as well as may inhibit CYP2C9 and CYP2C19.[8] However, other in-vitro studies find no significant inhibition of CYP2C9.[7][110] Modafinil may induce P-glycoprotein, which may affect drugs transported by P-glycoprotein, such as digoxin.[111] Therefore, modafinil affects pharmacodynamics of drugs which are metabolized by CYP3A4 and other enzymes of the cytochrome P450 family.[108]
For instance, induction of CYP3A4 by modafinil affects metabolism of the following medications and endogenous substances:[112]
- opioids, such as methadone, hydrocodone, oxycodone, or fentanyl – modafinil may result in a drop in opioid plasma concentrations because of faster clearance by CYP3A4. If the patient is not monitored closely, reduced efficacy or withdrawal symptoms can occur.[112]
- steroid hormones, such as estradiol, progesterone or cortisol. Modafinil may have an adverse effect on hormonal contraceptives for up to a month after discontinuation.[113] In a 2006 study, a single dose of modafinil 200 mg caused a decrease in blood prolactin levels, although it did not affect human growth hormone or thyroid-stimulating hormone.[114][115] Since modafinil induces the activity of the CYP3A4 enzyme involved in cortisol clearance,[116] modafinil may reduce the bioavailability of hydrocortisone. Therefore, it may be necessary to adjust the steroid substitution dose in subjects receiving CYP3A4-metabolism-inducing drugs such as modafinil.[117]
Pharmacology
Pharmacodynamics
Site | Potency | Type | Species | Refs |
---|---|---|---|---|
DAT | 1.8–2.6 μM 4.8 μM 6.4 μM 4.0 μM | Ki Ki IC50a IC50a | Human Rat Human Rat | [118][119] [118] [120][121] [118] |
NET | >10 μM >92 μM 35.6 μM 136 μM | Ki Ki IC50a IC50a | Human Rat Human Rat | [118][119] [118] [120][121] [118] |
SERT | >10 μM 46.6 μM >500 μM >50 μM | Ki Ki IC50a IC50a | Human Rat Human Rat | [118][119] [118] [120][121] [118] |
D2 | >10 μM 16 μMb 120 μMb | Ki Ki EC50a | Human Rat Rat | [118] [122] [122] |
Footnotes: a = Functional activity, not binding inhibition. b = Armodafinil at D2High. Notes: No activity at a variety of other assessed targets.[118] |
The precise mechanism of action of modafinil for narcolepsy and other sleep disorders remains unknown.[2][123][124][125]
Modafinil's mechanism of action involves various interactions with neurotransmitter systems in the brain. While its exact mode of action is not fully understood, several mechanisms have been proposed.[126][123]
One of the mechanisms is the binding of modafinil to the dopamine transporter and inhibiting dopamine reuptake.[123] One significant aspect of modafinil's mechanism is its ability to inhibit the reuptake of dopamine, a neurotransmitter involved in motivation, reward, and wakefulness. Modafinil acts as a weak inhibitor of the dopamine transporter (DAT), which prevents the reabsorption of dopamine into presynaptic neurons. By blocking this reuptake process, modafinil increases extracellular dopamine levels in certain brain regions. Modafinil acts as an atypical, selective, and weak dopamine reuptake inhibitor and indirectly activates the release of orexin neuropeptides and histamine from the lateral hypothalamus and tuberomammillary nucleus, all of which may contribute to heightened arousal.[124][125][127][128] Modafinil has little to no affinity for serotonin or norepinephrine transporters and does not directly interact with these systems. However, studies have shown that elevated concentrations of norepinephrine and serotonin can occur as an indirect effect following modafinil administration due to increased extracellular dopamine activity. Unlike traditional psychostimulant drugs like cocaine or amphetamine, which often induce euphoric effects by directly binding to DATs or increasing synaptic dopamine levels significantly more than modafinil does, modafinil shows low potential for causing euphoria due to differences in how it interacts with DAT at a molecular level.[126][123]
In addition to its influence on dopaminergic pathways, modafinil may impact other neurotransmitter systems such as orexin/hypocretin and histamine. Orexin neurons play a crucial role in promoting wakefulness and regulating arousal states. Modafinil has been presumed to increase signaling within hypothalamic orexin pathways, potentially contributing to its wake-promoting effects. Histamine is another neurotransmitter associated with arousal regulation. Animal studies suggest that modafinil may affect histamine release or receptor activity in specific brain regions involved in sleep-wake control. Furthermore, there are indications that modafinil might have glutamatergic effects based on animal research findings.[21]
Another mechanism is modulating the function of astroglial connexins, specifically connexin 30,[123] which are proteins that facilitate intercellular communication and play a role in sleep-wake regulation.[129][130][131] Connexins form channels that allow the exchange of ions and signaling molecules between cells. In the brain, they are mainly expressed by astrocytes, which help regulate neuronal activity.[132] Modafinil increases the levels of connexin 30 in the cortex, enhancing communication between astrocytes and promoting wakefulness. Conversely, during sleep, connexin 30 levels decrease, contributing to the transition from wakefulness to sleep. Flecainide, a drug that blocks astroglial connexins, can enhance the effects of modafinil on wakefulness and cognition, and reduce narcoleptic episodes in animal models. These findings suggest that modafinil may exert its therapeutic effects by modulating astroglial connexins.[132][123][126]
Modafinil dampens amygdala activity by enhancing the availability and regulation of norepinephrine (NE) in the locus coeruleus (LC). The loss or reduction of hypocretin/orexin neurons in narcolepsy leads to LC dysregulation, which contributes to excessive daytime sleepiness and cataplexy symptoms. Modafinil increases catecholamines like NE, which helps regulate GABAergic inputs from the amygdala. This increased NE activation of GABA receptors reduces overall excitatory input to the LC, resulting in a decrease in amygdala activity. Consequently, modafinil dampens amygdala activity through its effects on NE neurotransmission within these neural circuits involved in regulating wakefulness and muscle tone during sleep/wake cycles.[133]
Pharmacokinetics
Cmax (peak levels) occurs approximately 2 to 3 hours after modafinil administration. Food slows absorption of modafanil, but does not affect the total AUC. In vitro measurements indicate that 60% of modafinil is bound to plasma proteins at clinical concentrations of the drug. This percentage changes very little when the concentration of modafinil is varied.[134]
Renal excretion of unchanged modafinil usually accounts for less than 10% of an oral dose. This means that when modafinil is taken by mouth, less than 10% of the drug is eliminated from the body through the urine without being metabolized (broken down) by the liver or other organs. The rest of the drug is either metabolized or excreted through other routes, such as feces or bile.[7] The two major circulating metabolites of modafinil are modafinil acid (CRL-40467) and modafinil sulfone (CRL-41056). Both of these metabolites have been described as inactive, and neither appears to contribute to the wakefulness-promoting effects of modafinil.[78][135] However, modafinil sulfone does appear to possess anticonvulsant effects, a property that it shares with modafinil.[78][136] Elimination half-life is in the range of 10 to 12 hours, subject to differences in cytochrome P450 genotypes, liver function, and renal function. Modafinil is metabolized mainly in the liver,[7] and its inactive metabolite is excreted in the urine. Urinary excretion of the unchanged drug is usually less than 10%, but can range from 0% to as high as 18.7%, depending on the factors mentioned.[134]
Chemistry
Enantiomers
Modafinil is a racemic mixture of two enantiomers, armodafinil ((R)-modafinil) and esmodafinil ((S)-modafinil).[137]
Detection in body fluids
Modafinil and/or its major metabolite, modafinil acid, may be quantified in plasma, serum, or urine to monitor dosage in those receiving the drug therapeutically, to confirm a diagnosis of poisoning in hospitalized patients, or to assist in the forensic investigation of a vehicular traffic violation. Instrumental techniques involving gas or liquid chromatography are usually employed for these purposes.[138][139] In 2011, modafinil was not tested for by common drug screens (except for anti-doping screens) and is unlikely to cause false positives for other chemically unrelated drugs such as substituted amphetamines.[121][137]
Reagent testing can screen for the presence of modafinil in samples.[140][141]
RC | Marquis Reagent | Liebermann | Froehde |
---|---|---|---|
Modafinil | Yellow/Orange > Brown[140][141] | Darkening Orange[140] | Deep orange/red[141] |
Structural analogues
Many derivatives and structural analogues of modafinil have been synthesized.[13][142][143] Examples include adrafinil, CE-123, fladrafinil (CRL-40941; fluorafinil), flmodafinil (CRL-40940; bisfluoromodafinil, lauflumide), and modafinil sulfone (CRL-41056).[144][13]
History
Modafinil was developed in France by neurophysiology professor Michel Jouvet and Lafon Laboratories. It is part of a series of benzhydryl sulfinyl compounds, including adrafinil, initially used as a treatment for narcolepsy in France in 1986.[53] Modafinil, the primary metabolite of adrafinil,[145] has been prescribed in France since 1994 under the name Modiodal,[53] and in the United States since 1998 as Provigil.[146] Unlike modafinil, adrafinil does not have FDA approval and was withdrawn from the French market in 2011.[147]
The US Food and Drug Administration approved modafinil in 1998 for narcolepsy treatment, and later for shift work sleep disorder and obstructive sleep apnea/hypopnea in 2003.[6][148] It was approved in the UK in December 2002. In the United States, modafinil is marketed by Cephalon,[149] who acquired the rights from Lafon and purchased the company in 2001.[149]
Cephalon introduced armodafinil, the (R)-enantiomer of modafinil, in the United States in 2007. Generic versions of modafinil became available in the US in 2012 after extensive patent litigation.[150][151]
Society and culture
Legal status
Australia
In Australia, modafinil is considered to be a Schedule 4 prescription-only medicine or prescription animal remedy.[152]
Canada
In Canada, modafinil is not listed in the Controlled Drugs and Substances Act, but it is a Schedule F prescription drug.[153]
China
In mainland China, modafinil is strictly controlled like other stimulants such as amphetamines and methylphenidate. It is classified as Class I psychotropic drug, requiring prescription.[154][155]
Moldova
In the Republic of Moldova, modafinil is classified as a psychotropic drug and is available by prescription.[156] Importation of modafinil may be considered illegal and subject to severe penalties.[157] In Transnistria, modafinil is completely prohibited, with possession potentially leading to imprisonment.[158]
Japan
In Japan, modafinil is Schedule I psychotropic drug.[159][160] Cephalon licensed Alfresa Corporation to produce, and Mitsubishi Tanabe Pharma to sell modafinil products under the trade name Modiodal in Japan.[161] There have been arrests of people who imported modafinil for personal use.[162][163]
Romania
In Romania, modafinil is classified as a stimulant doping agent and is prohibited in sports competitions.[164] In 2022, laws were passed making its importation or sale a felony, punishable by three to seven years in jail.[165] Simple possession for personal use may result in a fine and confiscation.[165]
Russia
In Russia, starting from May 18, 2012, modafinil is Schedule II controlled substance like cocaine and morphine. Possession of a few modafinil pills can lead to three to ten years imprisonment.[158][166] There are multiple cases of criminal proceedings initiated against Russian residents who tried to import modafinil by mail from abroad.[167][168]
Sweden
In Sweden, modafinil is classified as a schedule IV substance; possession is illegal without prescription.[169]
United States
In the United States, modafinil is classified as a schedule IV controlled substance under US federal law.[6][170] It is illegal to import it without a DEA-registered importer and a prescription.[171] Individuals may legally bring modafinil into the US from a foreign country for personal use, limited to 50 dosage units, with a prescription and proper declaration at the border.[172] Under the Pure Food and Drug Act, marketing drugs for off-label uses is prohibited.[173] Cephalon, the manufacturer of Modafinil, faced legal issues for promoting off-label uses and paid significant fines in 2008.[174]
Other countries
The following countries do not classify modafinil as a controlled substance:
- In Finland, modafinil is a prescription drug but not listed as a controlled substance.[175]
- In Denmark, modafinil is a prescription drug but not listed as a controlled substance.[176]
- In Mexico, modafinil is not listed as a controlled substance, in the National Health Law, and can be purchased in pharmacies without prescription.[177]
- In South Africa, it is Schedule V substance.[178]
- In the United Kingdom, it is not listed in Misuse of Drugs Act, so possession is not illegal, but a prescription is required.[179]
Brand names
Modafinil is sold under a variety of brand names worldwide, including Alertec, Alertex, Altasomil, Aspendos, Bravamax, Forcilin, Intensit, Mentix, Modafinil, Modafinilo, Modalert, Modanil, Modasomil, Modvigil, Modiodal, Modiwake, Movigil, Provigil, Resotyl, Stavigile, Vigia, Vigicer, Vigil, Vigimax, Waklert, and Zalux.[180]
Economics
Originally developed in the 1970s by French neuroscientist Michel Jouvet and Lafon Laboratories, Modafinil has been prescribed in France since 1994,[53] and was approved for medical use in the United States in 1998.[17]
Concerns have been raised about the growing use of modafinil as a "smart drug" or cognitive enhancer among healthy individuals who use it to improve concentration and memory.[181][182] In 2003, modafinil sales were skyrocketing, with some experts concerned that it had become a tempting pick-me-up for people looking for an extra edge in a productivity-obsessed society.[181] The cost of modafinil varied depending on factors such as location and insurance coverage,[181][182][183] still, in 2004, the price of Modafinil in the US was around $120 or more per monthly supply.[181] However, the availability of generic versions has increased since then and may have driven down prices.[181][182][183]
In 2020, modafinil was the 302nd most commonly prescribed medication in the United States, with just over 1000000 prescriptions.[184]
As of 2024," the global sales figures for modafinil are not known. Still, modafinil sold under the brand name Provigil accounted for over 40% of Cephalon's global turnover for several years, according to the information published in 2020.[185]
Patent protection and litigation
Modafinil's patent history involves several key developments. The original patent, U.S. Patent 4,927,855, was granted to Laboratoire L. Lafon in 1990, covering the chemical compound of modafinil. This patent expired in 2010.[186] In 1994, Cephalon filed a patent for modafinil in the form of particles of a defined size, represented by U.S. Patent 5,618,845, which expired in 2015.[187]
Following the nearing expiration of marketing rights in 2002, generic manufacturers, including Mylan and Teva, applied for FDA approval to market a generic form of modafinil, leading to legal challenges by Cephalon regarding the particle size patent.[188] The patent RE 37,516 was declared invalid and unenforceable in 2011.[189]
In addition, Cephalon entered agreements with several generic drug manufacturers to delay the sale of generic modafinil in the US. These agreements were subject to legal scrutiny and antitrust investigations, culminating in a ruling by the Court of Appeals in 2016, which found that the settlements did not violate antitrust laws.[190]
Sports
The regulation of modafinil as a doping agent has been controversial in the sporting world, with high-profile cases attracting press coverage since several prominent American athletes tested positive for the substance. Some athletes who used modafinil protested that the drug was not on the prohibited list at the time of their offenses.[191] However, the World Anti-Doping Agency (WADA) maintains that modafinil was related to already-banned substances. The Agency added modafinil to its list of prohibited substances on August 3, 2004, ten days before the start of the 2004 Summer Olympics.
Several athletes (such as sprinter Kelli White in 2003,[192] cyclist David Clinger[193] and basketball player Diana Taurasi[194] in 2010, and rower Timothy Grant in 2015[195]) were accused of using modafinil as a performance-enhancing doping agent. Taurasi and another player—Monique Coker, tested at the same lab—were later cleared.[196] Kelli White, who tested positive after her 100m victory at the 2003 World Championships in Paris, was stripped of her gold medals.[197] She claimed that she used modafinil to treat narcolepsy, but the International Association of Athletics Federations (IAAF) ruled that modafinil was a performance-enhancing drug.[197]
The BALCO scandal brought to light an unsubstantiated (but widely published) account of Major League Baseball's all-time leading home-run hitter Barry Bonds' supplemental chemical regimen that included modafinil in addition to anabolic steroids and human growth hormone.[198]
In a study on 15 healthy male subjects, published in Medicine & Science in Sports & Exercise, an academic journal, acute ingestion of modafinil of 4 mg·kg−1 (at a dose of 4 mg per kilogram of body weight), prolonged exercise time to exhaustion while performing at 85% of VO2max threshold, and also reduced the perception of effort required to maintain this threshold,[199] i.e., the control subjects were able to perform at 85% of their maximum oxygen consumption without feeling as much effort as without modafinil (with placebo).[199]
Social views
The use of modafinil as a supposed cognitive enhancer is viewed differently among various groups.[200] Some groups consider such use as cheating, unnatural, or risky.[201] For instance, some academic institutions such as University of Sussex in the UK have explored this question raised by the students, although the university do not have a strong, official stance on its use, explaining that it is a prescription drug and the decision should be made by the doctor on whether to prescribe modafinil to a student.[202] In the realm of bioethics, the President's Council on Bioethics in the US, chaired by Leon Kass, argued that excellence achieved through the use of drugs like modafinil is "cheap" as it obviates the need for hard work and study, and is not fully authentic because the excellence is partly attributable to the drug, not the individual.[203] On the other hand, some people, particularly those in high-pressure environments like Wall Street traders, do not view the use of modafinil as cheating. They argue that if modafinil can give them an edge and they are aware of the risks involved, it should not be considered as cheating.[204] Due to such varying views, modafinil users for narcolepsy may cope with stigma by hiding, denying, or justifying their use, or by seeking support from others who share their views or experiences.[90][205]
Research
Psychiatric conditions
Major depression
Modafinil has been studied in the treatment of major depressive disorder.[206][207][208] In a 2021 systematic review and meta-analysis of randomized controlled trials of psychostimulants for depression, modafinil and other stimulants such as methylphenidate and amphetamines improved depression in traditional meta-analysis.[208] However, when subjected to network meta-analysis, modafinil and most other stimulants did not significantly improve depression, with only methylphenidate remaining effective.[208] Modafinil and other stimulants likewise did not improve quality of life in the meta-analysis, although there was evidence for reduced fatigue and sleepiness with modafinil and other stimulants.[208] While significant effectiveness of modafinil for depression has been reported,[209][210][207] reviews and meta-analyses note that the effectiveness of modafinil for depression is limited, the quality of available evidence is low, and the results are inconclusive.[211][208][212]
Bipolar depression
Modafinil and armodafinil have been repurposed as adjunctive treatments for acute depression in people with bipolar disorder.[213] A 2021 meta-analysis concluded that add-on modafinil and armodafinil were more effective than placebo on response to treatment, clinical remission, and reduction in depressive symptoms, with only minor side effects, but the effect sizes are small and the quality of evidence is therefore low, limiting the clinical relevance of the evidence.[213] Very low rates of mood switch (a change in mood from one extreme to another)[214] have been observed with modafinil and armodafinil in bipolar disorder.[210][215]
Attention deficit hyperactivity disorder (research)
Modafinil was considered for the treatment of attention deficit hyperactivity disorder (ADHD) because of its lower abuse potential than conventional psychostimulants like methylphenidate and amphetamines.[41][216] In 2008, an application to market modafinil for pediatric ADHD was submitted to the Food and Drug Administration in the USA.[217]
However, evidence of modafinil for treatment of adult ADHD is mixed, and a 2016 systematic review of alternative drug therapies for adult ADHD did not recommend its use in this context.[37] In a later large phase 3 clinical trial of modafinil for adult ADHD, modafinil was not effective in improving symptoms, and there was a high rate of side effects (86%) and discontinuation (47%).[218] The poor tolerability of modafinil in this study was possibly due to the use of excessively high doses (210–500 mg).[218] Another reason for the denial of the approval was due to concerns about rare but serious dermatological toxicity (Stevens–Johnson syndrome).[217]
Substance dependence
Modafinil was studied for the treatment of stimulant dependence, but the results are mixed and inconclusive.[13][219]
Modafinil has been investigated as a possible pharmacotherapy for substance abuse, especially stimulant abuse, because of its effects on the dopaminergic system. Modafinil binds to the dopamine transporter and inhibits its reuptake, increasing extracellular dopamine levels in the brain. The affinity and occupancy of modafinil at the dopamine transporter are comparable to those of low doses of methylphenidate, a widely used stimulant with high abuse potential. Modafinil also shares behavioral effects with psychostimulants, such as enhancing arousal, attention, and cognitive performance. However, unlike most psychostimulants, modafinil has a low potential for misuse and abuse, as evidenced by its low self-administration rates in animals and humans and its lack of euphoric or reinforcing effects in clinical studies. This combination of pharmacological and behavioral properties makes modafinil a promising candidate for replacement therapy for stimulant abuse, as it could provide some of the therapeutic benefits of stimulants without their adverse consequences, still, modafinil is not a controlled substance in most countries, unlike other medications that have similar effects on the dopaminergic system, such as bupropion, which has a lower affinity and occupancy at the dopamine transporter than modafinil or methylphenidate and is also used to treat depression and nicotine dependence.[220]
Despite these theoretical advantages, the empirical evidence for the efficacy of modafinil in treating substance abuse has been inconsistent. Several randomized controlled trials have evaluated the effects of modafinil on cocaine and amphetamine dependence, but the results have been mostly negative or inconclusive. Neither modafinil nor methylphenidate were effective in promoting sustained abstinence from cocaine or amphetamine use, compared to placebo or other active treatments. The lack of efficacy of modafinil might be due to its relatively weak effects on the dopaminergic system, which might not be sufficient to counteract the solid reinforcing effects of stimulants. Still, the doses of modafinil used in the trials (ranging 100–400 mg/d) might have been too low to produce optimal effects, and higher doses (up to 800 mg/d) might be more effective, but also more likely to cause adverse effects and abuse liability.[220]
The clinical trials that have tested modafinil as a treatment for stimulant abuse have failed to demonstrate its efficacy and the optimal dose and duration of modafinil treatment remain unclear, and modafinil is not a recommended pharmacotherapy for stimulant abuse.[220]
Treatment of cocaine addiction
Modafinil has been studied for the treatment of cocaine addiction.[21] Modafinil binds to the dopamine transporter (DAT) in an open-to-out conformation, differently than cocaine and methylphenidate.[221][222][223] Subjects pretreated with modafinil report experiencing less euphoria from cocaine administration.[222] Modafinil does not potentiate self-administration of cocaine in pretreated rats.[224]
The mechanism by which modafinil inhibits cocaine self-administration is likely more complex than the simple observation that modafinil occupies the DAT, as drugs like methylphenidate (another dopamine reuptake inhibitor (DRI) fail to reduce cocaine self-administration.[221][225] Atypical DRIs like modafinil that bind to the DAT in an open-to-out conformation often lack abuse potential relative to cocaine-like DAT ligands.[226]
Schizophrenia
Modafinil and armodafinil were studied as a complement to antipsychotic medications in the treatment of schizophrenia. They showed no effect on positive symptoms or cognitive performance.[227][228] A 2015 meta-analysis found that modafinil and armodafinil may slightly reduce negative symptoms in people with acute schizophrenia, though they do not appear useful for people with the condition who are stable, with high negative symptom scores.[228] Among medications demonstrated to be effective for reducing negative symptoms in combination with antipsychotics, modafinil and armodafinil are among the smallest effect sizes.[229]
Cognitive enhancement
A 2015 review of clinical studies of possible nootropic effects in healthy people found: "...whilst most studies employing basic testing paradigms show that modafinil intake enhances executive function, only half show improvements in attention and learning and memory, and a few even report impairments in divergent creative thinking. In contrast, when more complex assessments are used, modafinil appears to consistently engender enhancement of attention, executive functions, and learning. Importantly, we did not observe any preponderances for side effects or mood changes."[18] A 2019 review of studies of a single dose of modafinil on mental function in healthy, non-sleep-deprived people found a statistically significant but small effect and concluded that the drug has limited usefulness as a cognitive enhancer in non-sleep-deprived persons.[72][230] A 2020 review of the cognitive enhancing potential of methylphenidate, d-amphetamine, and modafinil in healthy individuals across various domains found that modafinil has a small, positive effect on memory updating.[231]
Modafinil has been used off-label in trials with people with post-chemotherapy cognitive impairment, also known as "chemobrain", but a 2011 review found that it was no better than a placebo.[232]
Post-anesthesia sedation
General anesthesia is required for many surgeries, but may cause lingering fatigue, sedation, and/or drowsiness after surgery that lasts for hours to days. In outpatient settings in which patients are discharged home after surgery, this sedation, fatigue, and occasional dizziness is problematic, but it was only tested in one small study, and the results are inconclusive.[40]
Postural orthostatic tachycardia syndrome
Caution should be exercised in patients who have narcolepsy in comorbidity with postural orthostatic tachycardia syndrome (POTS). Modafinil, like other centrally acting stimulants prescribed for patients with narcolepsy, increases POTS-related autonomic dysfunction and results in tachycardia/arrhythmia side effects in patients with cardiovascular risk factors. Sodium oxybate, a metabolite of GABA, is an alternative drug for stimulant-intolerant patients with POTS.[233][234]
Inflammation
There is limited research on the potential use of modafinil as an anti-inflammatory agent,[235][236] even though some studies predict that modafinil may have anti-inflammatory effects.[237][238] The results of studies on the potential anti-inflammatory properties of modafinil still need to be more conclusive.[236][239][235]
Modafinil is hypothesized to possess neuroprotective effects due to its antioxidant properties.[14]
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