| Drug |
Dosage |
Remarks |
| Barbiturates |
| Phenobarbital (Phenobarbitone) |
30 mg PO 12 hourly or
30-350 mg/day in divided doses or
120-250 mg PO 24 hourly at night or 2-3 mg/kg PO 24 hourly at night
Management of acute seizures and status epilepticus:
10-20 mg/kg IV at a rate of ≤100 mg/min
May administer additional 5-10 mg/kg IV after 10 minutes if needed
Max dose: 1,000 mg/dose |
Adverse Reactions
- CNS effects (sedation which usually decreases after repeated administration, subtle mood changes, impairment of cognition and memory, depression)
- Rarely, hypersensitivity, rashes, Stevens-Johnson syndrome, erythema multiforme; Hepatitis and hepatic failure have occurred
- May interfere with vitamin D and folate metabolism which may lead to osteomalacia
- Prolonged administration may result in folate deficiency, rarely megaloblastic anemia
- Nystagmus, respiratory depression or ataxia may occur at high doses
- Overdose may result in severe respiratory depression, coma, CV depression, hypotension, shock and renal failure
Special Instructions
- Avoid in patients with porphyria
- Use with caution in patients with respiratory, liver or renal dysfunction
- Contraindicated if the impairment is severe
- Use with caution in patients with depression or suicidal tendencies, history of drug abuse, acute or chronic pain
- Adjust dose based on individual response to control seizures
- Clinical authorities recommend that patients taking Phenobarbital should be supplemented with folate
- Monitoring Phenobarbital plasma concentration may aid in assessing control
- Therapeutic level: 86-172 micromol/L (20-40 mcg/mL)
- Monitor CBC, liver function and mental status regularly
- Withdraw drug or transition to another anticonvulsant drug gradually to prevent increase in seizure frequency
|
| Primidone |
125 mg PO 24 hourly at bedtime
May increase dose by 125 mg every 3 days up to 500 mg/day divided 12 hourly
May further increase dose by 250 mg/day every 3 days if needed
Maintenance dose: 750-1,500 mg/day PO divided 12 hourly
Max dose: 1,500 mg/day |
Adverse Reactions
- Similar to Phenobarbital but more frequent
- Patients usually develop tolerance to CNS effects (ataxia, drowsiness, dizziness, visual disturbances)
Special Instructions
- Same as Phenobarbital
- Adjust dose based on individual response to control seizures
- Monitoring Primidone plasma concentration may aid in assessing control
- Suggested therapeutic serum concentration: 23-55 micromol/L (5-12 mcg/mL)
- Monitor CBC every 6 months
|
| Carboxamides |
| Carbamazepine1 |
Initial dose: 100-200 mg PO 12-24 hourly
May increase dose by 100-200 mg weekly
Maintenance dose: 800-1,200 mg/day divided 6-12 hourly
Max dose: 1,600 mg/day |
Adverse Reactions
- CNS effects (dizziness, drowsiness, headache, fatigue, nervousness, amnesia, insomnia, suicidal ideation); GI effects (nausea/vomiting, abdominal pain, diarrhea, dry mouth, anorexia); CV effects (hypotension, leg edema); Dermatologic effects (Stevens-Johnson syndrome, toxic epidermal necrolysis, rash which may be severe, photosensitivity reactions have been reported); Other effects (abnormal vision, nystagmus, ataxia, vertigo, abnormal gait, tremor, upper respiratory tract infection [URTI], hyponatremia, transient leukopenia)
- May decrease side effects of Carbamazepine by starting at low dose and increasing slowly
- Hypersensitivity reactions occur less frequently with Oxcarbazepine than Carbamazepine
- Potentially fatal blood cell abnormalities have been reported following treatment
Special Instructions
- Contraindicated in patients with AV block, history of bone marrow depression and acute porphyria with or within 14 days of MAO inhibitors
- Use with caution in patients with cardiac, hepatic, renal disease, history of blood disorders, glaucoma, porphyria
- Relationship between dose, serum concentration and response are variable; titrate dose according to response and side effects
- Routine Carbamazepine serum level monitoring is not indicated except to assess compliance or possible toxic symptoms
- Therapeutic serum concentration: 17-51 micromol/L (4-12 mcg/mL)
- LFT, urinalysis, BUN, CBC, serum sodium should be done prior to and periodically during treatment
- Monitor for any emergence or worsening of depression, suicidal tendency, unusual changes in mood or behavior
- Monitor for signs of blood, liver or skin toxicity; patient should inform physician immediately if signs and symptoms of blood toxicity occur (eg lethargy, fever, sore throat, mouth ulcers, skin rash, bruising or bleeding)
- Withdraw drug or transition to another anticonvulsant drug gradually to prevent increase in seizure frequency
- Carbamazepine and Oxcarbazepine:
- HLA-B*1502 genetic testing is recommended to be done before starting therapy especially in patients of Asian descent; if positive, weigh if the benefit clearly outweighs risk of having Stevens-Johnson syndrome and toxic epidermal necrolysis
|
| Eslicarbazepine |
Monotherapy or adjunctive therapy of partial-onset seizures:
Initial dose: 400 mg PO 24 hourly
May start at 800 mg PO 24 hourly if seizure reduction outweighs risk of adverse events during initiation
Increase dose by 400-600 mg weekly based on clinical response and tolerability
Maintenance dose: 800-1,600 mg PO 24 hourly |
| Oxcarbazepine1 |
Initial dose: 300 mg PO 12 hourly or 8-10 mg/kg PO divided 12 hourly
May increase dose by 600 mg/day weekly based on clinical response
Maintenance dose: 600-2,400 mg/day PO divided 12 hourly |
| Rufinamide |
Adjunctive therapy for seizures associated with Lennox-Gastaut syndrome in patients ≥17 years old:
Initial dose: 400-800 mg PO 12 hourly
May increase dose by 400-800 mg/day every other day
Max dose: 3,200 mg/day |
| Fatty Acid Derivatives |
| Tiagabine |
Adjunctive therapy with enzyme-inducing anticonvulsants2:
Initial dose: 4 mg PO 24 hourly x 1 week
May increase dose by 4-8 mg/day at weekly intervals
Maintenance dose: 32-56 mg/day PO divided 6-12 hourly
Adjunctive therapy with non-enzyme inducing anticonvulsants:
Patients require lower dosage and slower dosage titration schedule than patients taking enzyme-inducing anticonvulsants
12 mg/day is equivalent to 32 mg/day in patients receiving enzyme-inducing anticonvulsant |
Adverse Reactions
- CNS effects (dizziness, nervousness, tiredness, somnolence, irritability, confusion, depression, difficulty in concentration, emotional lability); GI effects (diarrhea, abdominal pain, nausea); CV effects (chest pain, edema, hypertension, palpitation, tachycardia, syncope); Other effects (tremor, ataxia, nystagmus, bruising, rashes, speech difficulties, flu-like syndrome)
Special Instructions
- Take with food to avoid rapid rise in plasma concentration
- Avoid in patients with severe hepatic dysfunction
- Use with caution in patients with hepatic impairment, adjust dose accordingly
- Monitor for any emergence or worsening of depression, suicidal tendency, unusual changes in mood or behavior
- Withdraw drug or transition to another antiepileptic/anticonvulsant drug gradually (recommended over 2-3 weeks) to prevent increase in seizure frequency
|
| Valproic acid (Sodium valproate, Valproate, Valproate semisodium, Divalproex Na) |
Initial dose: 10-15 mg/kg/day PO divided 6-12 hourly
May increase dose by 5-10 mg/kg/day weekly based on clinical response
Maintenance dose: 20-30 mg/kg/day
Max dose: 60 mg/kg/day
or
Initial dose: 600 mg/day PO divided 12 hourly
May increase dose by 200 mg/day every 3 days based on clinical response
Maintenance dose: 1-2 g/day
Max dose: 2.5 g/day
For patients unable to take oral doses:
Valproic acid may be given IV to start therapy or to continue therapy previously given orally
Initial dose: 10 mg/kg IV over 3-5 minutes
Followed by IV infusion as needed
Max dose: 2.5 g/day |
Adverse Reactions
- CNS effects (headache, somnolence, behavioral changes, asthenia, dizziness, amnesia, depression); GI effects (abdominal cramps, nausea/vomiting, indigestion, anorexia, increased appetite, weight gain); Other effects (tremor, ataxia, hair loss, edema, increased bleeding time, thrombocytopenia, leukopenia, bone marrow depression, hepatic dysfunction)
Special Instructions
- GI disturbances especially at the start of therapy may be decreased by taking medication with food or large amount of water, starting with a low dosage and increasing dose gradually, and using enteric-coated forms
- Contraindicated in patients with significant hepatic impairment and urea cycle disorders
- Increased risk of hyperammonemic encephalopathy in patients with urea cycle disorders
- Avoid in females of childbearing age
- Use lowest effective dose when the potential benefit of administration outweighs the potential risk
- Use with caution in patients with congenital metabolic disorders, organic brain disease, severe seizure disorder, HIV and renal dysfunction
- Routine Valproic acid serum level monitoring is not indicated except to assess compliance or assess possible toxic symptoms
- Therapeutic serum concentration: 350-690 micromol/L (50-100 mcg/mL) at baseline and during the first 6 months of therapy, increased liver enzymes may respond to lower dose
- Monitor CBC, PT/PTT especially prior to surgery, serum ammonia
- Monitor for any emergence or worsening of depression, suicidal tendency, unusual changes in mood or behavior
- Watch out for signs of pancreatitis, blood and liver toxicity
- Withdraw drug or transition to another anticonvulsant drug gradually to prevent increase in seizure frequency
|
| Gamma-aminobutyric acid (GABA)-Analogues |
| Gabapentin |
Monotherapy or adjunctive therapy:
Day 1: 300 mg PO 24 hourly
Day 2: 300 mg PO 12 hourly
Day 3: 300 mg PO 8 hourly
May increase dose by 300 mg/day every 2-3 days if required until effective epileptic control is achieved
Usual dose: 900-3,600 mg/day PO divided 8 hourly
Max dose: 3,600 mg/day |
Adverse Reactions
- CNS effects (somnolence, dizziness, fatigue, anxiety, amnesia, headache, ataxia, tremor); GI effects (weight gain, dyspepsia, nausea/vomiting); Other effects (nystagmus, diplopia, pharyngitis, arthralgia, purpura, weakness)
- Rarely pancreatitis, altered LFT, erythema multiforme, Stevens-Johnson syndrome, rhinitis, nervousness, myalgia and blood glucose fluctuations in DM
Special Instructions
- Gabapentin: Use with caution in patients with severe renal impairment, history of psychotic illness
- Pregabalin: Use with caution in patients with CHF, hypertension, DM, renal impairment
- Monitor for any emergence or worsening of depression, suicidal tendency, unusual changes in mood or behavior
- Withdraw drug or transition to another anticonvulsant drug gradually (recommended ≥7 days) to prevent increase in seizure frequency
|
| Pregabalin |
Initial dose: 150 mg/day PO divided 8-12 hourly
May increase dose by 300 mg/day PO after 3-7 days
Max dose: 600 mg/day after additional 7 days |
| Vigabatrin |
Adjunctive therapy for refractory focal-onset seizures:
Initial dose: 500 mg PO 12 hourly
May increase dose by 500 mg/day weekly based on clinical response and patient tolerance
Usual dose: 1,500 mg PO 12 hourly
Max dose: 3,000 mg/day |
Adverse Reactions
- CNS effects (drowsiness, fatigue, dizziness, headache, paresthesia, impaired concentration, confusion, memory disturbances, ataxia, tremor); GI effects (weight gain, GI disturbances); Other effects (alopecia, rashes, urticaria, decrease in hemoglobin and liver enzymes, irreversible visual field defects ranging from mild-moderate and usually occurring after months or years of therapy)
- May exacerbate myoclonic and absence seizures
Special Instructions
- Avoid in patients with visual field defects
- Use with caution in patient with history of psychosis or behavioral problems, renal impairment and in the elderly
- Assess visual field functions before and during treatment regularly every 6 months
- Withdraw drug or transition to another anticonvulsant drug gradually (recommended over 2-4 weeks) to prevent increase in seizure frequency
|
| Hydantoins |
| Fosphenytoin |
Dose is expressed as Phenytoin equivalent (PE)
Status epilepticus:
Loading dose: 15-20 PE mg/kg IV given at a rate of 100-150 PE mg/min
Followed by maintenance dose of parenteral Fosphenytoin or oral/parenteral Phenytoin
Maintenance dose: 4-6 PE mg/kg/day IV/IM in divided doses
Non-emergent treatment of tonic-clonic or focal-onset seizures:
Loading dose: 10-20 PE mg/kg IV/IM
Maintenance dose: 4-6 PE mg/kg/day IV/IM in divided doses |
Adverse Reactions
- Side effects may decrease with dose reduction or continued administration
- GI effects (nausea/vomiting, abdominal pain, lack of appetite, gum tenderness, gingival hyperplasia); CNS effects (headache, dizziness, insomnia); Other effects (hirsutism, coarsening of facial features, mild hypersensitivity with skin rash)
- Rarely, Stevens-Johnson syndrome, SLE or erythema multiforme, blood disorders (eg thrombocytopenia, leukopenia)
- Prolonged administration may result in subtle changes in mental function and cognition
- Rickets and osteomalacia have occurred and may be caused by interference of vitamin D and folate metabolism
- Phenytoin toxicity may result in nystagmus, diplopia, slurred speech, ataxia, confusion and hyperglycemia
- Severe CV reactions that are sometimes fatal have occurred with IV infusion of Fosphenytoin
- Fosphenytoin: Burning, itching and paresthesia especially in groin area may occur; reducing the rate of infusion or temporarily stopping administration may relieve discomfort
Special Instructions
- IV administration should be given slowly
- Hypotension may occur with rapid administration
- Adjust dose based on individual response to control seizures
- Avoid IV administration in patients with sinus bradycardia, heart block and Stokes-Adams syndrome
- Clinical authorities recommend that patients taking Phenytoin should be supplemented with Folate
- Use with caution in patients with liver dysfunction, DM, CV disease, hypoalbuminemia and porphyria; IV should be used with caution in patients with heart failure, hypotension or MI
- Routine Phenytoin serum level monitoring is not indicated except during dose adjustment and to assess compliance or possible toxicity
- Therapeutic serum concentration: 40-80 micromol/L (10-20 mcg/mL)
- Monitor ECG, BP and respiratory function during IV administration
- Observe patient for 10-20 minutes after IV administration
- Monitor for signs of blood or skin toxicity; patient should inform physician immediately if signs of blood toxicity occur (eg fever, sore throat, bruising, skin rash etc)
- Withdraw drug or transition to another anticonvulsant drug gradually to prevent increase in seizure frequency
|
| Phenytoin (Phenytoin Na) |
Management of acute seizures:
Initial dose: 100-300 mg PO as single dose or in divided doses or 3-4 mg/kg PO as single dose or in divided doses
May increase dose by 100 mg every 2-4 weeks until desired response is obtained
Maintenance dose: 300-400 mg/day PO divided 6-8 hourly
Max dose: 600 mg/day
Status epilepticus:
Loading dose: 10-20mg/kg slow IV at a rate of ≤50 mg/min
May administer additional 5-10 mg/kg IV as single dose after 10 minutes if needed
Maintenance dose: 100 mg PO/IV 6-8 hourly |
| Succinimides |
| Ethosuximide |
Initial dose: 500 mg/day PO as single dose or divided 12 hourly
May increase dose by 250 mg/day every 4-7 days based on clinical response
Usual dose: 1-1.5 g/day PO divided 12 hourly
Max dose: 1.5 g/day |
Adverse Reactions
- GI effects (nausea/vomiting, abdominal pain, anorexia, weight loss); CNS effects (headache, fatigue, lethargy, drowsiness, dizziness, ataxia, mild euphoria, depression); Other effect (hiccups)
- Rarely, personality changes, dyskinesia, rashes, SLE, photophobia, Stevens-Johnson syndrome, erythema multiforme, abnormal renal function and LFT, hematologic effects (thrombocytopenia, leukopenia, aplastic anemia)
- Mesuximide: Adverse reactions other than above are CNS effects (confusion, aggressiveness, hypochondrial behavior, emotional lability, insomnia, nervousness); Hematologic effects (eosinophilia, leukopenia, monocytosis, pancytopenia)
Special Instructions
- Use with caution in patients with liver or renal dysfunction and porphyria
- Monitoring Ethosuximide plasma concentration may aid in assessing control
- Therapeutic serum concentration: 300-700 micromol/L (40-100 mcg/mL)
- Monitor hepatic and renal function, CBC and urinalysis regularly
- Monitor for any emergence or worsening of depression, suicidal tendency, unusual changes in mood or behavior
- Patient should inform physician immediately if signs of blood toxicity occur (eg fever, sore throat, bruising, skin rash, etc)
- Withdraw drug or transition to another anticonvulsant drug gradually to prevent increase in seizure frequency
|
Mesuximide
(Methsuximide, Methosuximide) |
Initial dose: 300 mg PO 24 hourly for the first week
May increase dose by 300 mg/day weekly
Max dose: 1-2 g/day PO in 3-4 divided doses |
| Other Anticonvulsants |
| Brivaracetam |
Initial dose: 50 or 100 mg/day PO/IV divided 12 hourly
May adjust dose between 50-200 mg/day PO/IV divided 12 hourly if needed
Max dose: 200 mg/day PO/IV
Max dose in patients with hepatic impairment: 150 mg/day PO/IV |
Adverse Reactions
- CNS effects (somnolence, dizziness, convulsion, depression, anxiety, irritability, insomnia, vertigo); Respiratory effects (URTI, flu, cough); GI effects (nausea/vomiting, constipation); Other effects (decreased appetite, fatigue)
Special Instructions
- Contraindicated in patients with end-stage renal disease or undergoing dialysis
- Use with caution in patients with hepatic impairment, adjust dose accordingly
- Monitor for suicidal ideation and behaviors
|
| Cenobamate |
Week 1 and 2: 12.5 mg PO 24 hourly
Week 3 and 4: 25 mg PO 24 hourly
Week 5 and 6: 50 mg PO 24 hourly
Week 7 and 8: 100 mg PO 24 hourly
Week 9 and 10: 150 mg PO 24 hourly
Week 11 and onwards: 200 mg PO 24 hourly
May further increase dose by 50 mg/day PO every 2 weeks based on response
Max dose: 400 mg/day |
Adverse Reactions
- CNS effects (cognitive dysfunction, drowsiness, fatigue, dizziness, visual changes, coordination abnormalities, aggressive behavior, psychosis, suicidal ideation); Other effects (QT prolongation, delayed hypersensitivity reaction)
Special Instructions
- Avoid in patients with familial short QT syndrome
- Use with caution in patients on drugs known to shorten QT interval
- Use with caution in patients with renal and hepatic impairment
- When discontinuing, gradually reduce the dose over ≥2 weeks
|
| Felbamate |
Monotherapy for refractory focal-onset seizures:
Initial dose: 1,200 mg/day PO divided 6-8 hourly
May increase dose by 600 mg every 2 weeks based on clinical response up to 2,400 mg/day divided 6-8 hourly
Max dose: 3,600 mg/day
Adjunctive therapy for refractory focal-onset seizures:
Reduce dose of concomitant anticonvulsants by 20-33%
Initial dose: 1,200 mg/day PO divided 6-8 hourly
May increase dose by 1,200 mg/day weekly based on clinical response
Max dose: 3,600 mg/day |
Adverse Reactions
- CNS effects (somnolence, headache, dizziness, insomnia, fatigue, nervousness); GI effects (anorexia, nausea/vomiting, weight loss, constipation, dyspepsia); Other effects (diplopia, photosensitivity, rashes, URTI, abnormal gait, tremor)
Special Instructions
- Use only in severe epilepsy refractory to other treatments when advantages outweigh the risks
- Patient should use protective measures to avoid UV radiation
- Contraindicated in patients with hepatic impairment or history of blood disorders
- Use with caution in patients with renal impairment
- Monitor for any emergence or worsening of depression, suicidal tendency, unusual changes in mood or behavior
- Monitor CBC and LFT before and regularly during therapy
- Continue to monitor CBC after discontinuation
- Withdraw drug or transition to another anticonvulsant drug gradually to prevent increase in seizure frequency
|
| Fenfluramine |
Management of seizures associated with Dravet syndrome and Lennox-Gastaut syndrome:
Initial dose: 0.1 mg/kg PO 12 hourly
May increase dose by 0.2 mg/kg PO 12 hourly after 1 week then by 0.35 mg/kg PO 12 hourly after another week based on tolerability
Max dose: 26 mg/day |
Adverse Reactions
- Dravet Syndrome: GI effects (diarrhea, vomiting, constipation, drooling, salivary hypersecretion); CNS effects (somnolence, sedation, lethargy, ataxia, balance disorder, gait disturbance, status epilepticus); CV effect (increased BP); Other effects (decreased appetite, fatigue, pyrexia, upper respiratory tract infection, decreased weight, fall)
- Lennox-Gastaut syndrome: GI effects (diarrhea, vomiting); CNS effect (somnolence); CV effect (abnormal echocardiogram); Other effects (decreased appetite, fatigue, malaise, asthenia)
Special Instructions
- Use with caution in patients taking serotonergic drugs
- Monitor BP and for presence of somnolence, sedation, suicidal behavior and thoughts, visual acuity changes and ocular pain during treatment
|
| Lacosamide |
IV dose should only be used temporarily when oral dose is not feasible
Monotherapy for focal-onset and tonic-clonic seizures:
Initial dose: 50-100 mg PO/IV 12 hourly or 200 mg PO/IV as single dose followed by 100 mg PO/IV 12 hourly after 12 hours
May increase dose by 50 mg PO 12 hourly weekly
Maintenance dose: 300-400 mg/day
Max dose: 600 mg/day
Adjunctive therapy for focal-onset and tonic-clonic seizures:
Initial dose: 50 mg PO/IV 12 hourly
May increase dose by 50 mg PO 12 hourly weekly
Maintenance dose: 200-400 mg/day
Max dose: 400 mg/day |
Adverse Reactions
- CNS effects (dizziness, headache, fatigue, ataxia, somnolence, impaired coordination, vertigo); Ophthalmologic effects (diplopia, blurring of vision, nystagmus); GI effects (nausea/vomiting, diarrhea); Local effects (contusion, pain/discomfort at injection site, irritation); Other effects (pruritus, syncope for dose >400 mg/day)
Special Instructions
- Switching from IV to oral formulations makes use of the same total daily dose and frequency
- IV Lacosamide is only used as a short-term alternative to oral therapy (eg in patients with GI disorders, difficulty swallowing, undergoing surgical procedures)
- Use with caution in patients with conduction problems as Lacosamide may prolong PR interval
- Use with caution in patients performing tasks which require alertness (eg driving, operating machineries) as ataxia and dizziness may occur during therapy
- Lacosamide should be withdrawn gradually (by discontinuing over ≥1 week and/or tapering daily dosage by 200 mg/wk) to lessen risk for increased seizure frequency
|
| Lamotrigine |
Monotherapy:
Initial dose: 25 mg PO 24 hourly x 2 weeks followed by 50 mg PO 24 hourly x 2 weeks
May increase dose by 50-100 mg every 1-2 weeks based on clinical response
Maintenance dose: 100-200 mg/day PO 24 hourly or divided 12 hourly
Max dose: 500 mg/day
Adjunctive therapy with enzyme-inducing anticonvulsants2:
Initial dose: 50 mg PO 24 hourly x 2 weeks followed by 50 mg PO 12 hourly x 2 weeks
May increase dose by 100 mg every 1-2 weeks based on clinical response
Maintenance dose: 200-400 mg/day PO divided 12 hourly
Max dose: 700 mg/day
Adjunctive therapy with Valproic acid:
Initial dose: 25 mg PO every other day x 2 weeks followed by 25 mg PO 24 hourly x 2 weeks
May increase dose by 25-50 mg every 1-2 weeks based on clinical response
Maintenance dose: 100-200 mg/day PO 24 hourly or divided 12 hourly |
Adverse Reactions
- CV effects (chest pain, edema); CNS effects (dizziness, drowsiness, insomnia, headache, confusion, agitation); GI effects (nausea/vomiting); Other effects (photosensitivity, angioedema, blurred vision, tremor); Hypersensitivity effects (fever, malaise, flu-like symptoms, drowsiness, lymphadenopathy, facial edema, rarely hepatic dysfunction)
- Skin rashes, including Stevens-Johnson syndrome and toxic epidermal necrolysis
- Usually occur within 8 weeks of starting therapy
- Symptoms associated with aseptic meningitis typically occur 1-42 days after starting of therapy and resolve upon discontinuation
Special Instructions
- Use with caution in patients with impaired cardiac function, hepatic or renal impairment
- Patient should inform doctor immediately if signs of rash, flu-like hypersensitivity symptoms, or signs and symptoms associated with aseptic meningitis develop
- Monitor for any emergence or worsening of depression, suicidal tendency, unusual changes in mood or behavior
- Withdraw drug or transition to another anticonvulsant drug gradually by decreasing the dose to ~50%/week, over at least 2 weeks to prevent increase in seizure frequency
|
| Levetiracetam |
Initial dose: 250-500 mg PO 12 hourly
May increase dose by 250-500 mg PO 12 hourly every 2-4 weeks
Max dose: 3 g/day |
Adverse Reactions
- CNS effects (somnolence, dizziness, ataxia, headache, amnesia, depression, emotional lability, insomnia, aggression, nervousness, vertigo); GI effects (nausea/vomiting, anorexia); Other effects (weakness, tremor, diplopia)
Special Instructions
- Use with caution in patients with renal impairment and/or severe hepatic impairment, adjust dose accordingly
- Monitor for any emergence or worsening of depression, suicidal tendency, unusual changes in mood or behavior
- Withdraw drug or transition to another anticonvulsant drug gradually to prevent increase in seizure frequency
|
| Perampanel |
Initial dose: 2 mg PO 24 hourly
May increase dose by 2 mg/day every 1-2 weeks
Maintenance dose: 4-8 mg/day
May further increase dose by 2 mg/day
Max dose: 12 mg/day |
Adverse Reactions
- CNS effects (dizziness, somnolence; aggression, anger, anxiety, confusional state, ataxia, dysarthria, balance disorder, irritability, diplopia, blurred vision, vertigo, gait disturbance); Other effects (decreased/increased appetite, fatigue, weight gain, fall, nausea, back pain)
Special Instructions
- Contraindicated in patients with moderate to severe renal impairment and/or severe hepatic impairment
- Use with caution in patients with rare hereditary problems of galactose intolerance, Lapp-lactase deficiency or glucose-galactose malabsorption
- Monitor for signs of suicidal ideation and behaviors
- Avoid abrupt discontinuation of treatment
|
| Topiramate |
Monotherapy:
Initial dose: 25 mg PO 24 hourly at night x 1 week
May increase dose by 25-50 mg/day divided 12 hourly every 1-2 weeks
Usual dose: 100 mg/day
Max dose: 500 mg/day
Adjunctive therapy:
Initial dose: 25-50 mg/day PO 24 hourly at night x 1 week
May increase dose by 25-100 mg/day PO in divided 12 hourly every 1-2 weeks
Usual dose: 200-400 mg/day PO divided 12 hourly |
Adverse Reaction
- CNS effects (fatigue, confusion, paresthesia, somnolence, difficulty with concentration, mood changes); GI effects (weight loss, nausea, anorexia, diarrhea, taste perversion); Other effects (ataxia, abnormal vision, hyperthermia, risk of stone formation, metabolic acidosis)
- Rare cases of acute myopia with or without secondary angle-closure glaucoma have been reported
Special Instructions
- Maintain adequate hydration to reduce the risk of renal calculi
- Use with caution in patients with hepatic or renal impairment
- Monitor for any emergence or worsening of depression, suicidal tendency, unusual changes in mood or behavior
- Discontinue use in patients with acute onset of decreased visual acuity or ocular pain
- Withdraw drug or transition to another anticonvulsant drug gradually to prevent increase in seizure frequency
|
| Zonisamide |
Monotherapy:
Week 1 and 2: 100 mg PO 24 hourly
Week 3 and 4: 200 mg PO 24 hourly
Week 5 and 6: 300 mg PO 24 hourly
Maintenance dose: 300 mg PO 24 hourly
May further increase dose by 100 mg/day every 2 weeks
Max dose: 500 mg/day
Adjunctive therapy:
Initial dose: 100-200 mg/day PO divided 8-24 hourly
May gradually increase dose by 200-400 mg/day divided 8-24 hourly every 1-2 weeks
Max dose: 600 mg/day |
Adverse Reactions
- CNS effects (somnolence, dizziness, headache, confusion, irritability, depression, psychosis, reduced concentration); GI effects (anorexia, nausea/vomiting, abdominal pain, weight loss); Other effects (nystagmus, paresthesia, renal calculi, psychomotor slowing, language or speech difficulties, pancreatitis, rhabdomyolysis, metabolic acidosis)
- Isolated cases of aplastic anemia and agranulocytosis; Rarely severe skin reactions (Stevens-Johnson syndrome, toxic epidermal necrolysis)
Special Instructions
- Maintain adequate hydration to reduce the risk of renal calculi
- Contraindicated in patients with hypersensitivity to sulfonamide and women who are lactating
- Use with caution in patients with hepatic or renal impairment
- Monitor BUN, serum creatinine, serum bicarbonate
- Monitor for any emergence or worsening of depression, suicidal tendency, unusual changes in mood or behavior
- If patient has unexplained rashes, withdraw drug
- Withdraw drug or transition to another antiepileptic/anticonvulsant drug gradually to prevent increase in seizure frequency
|
1Extended-release preparations are available. Please see the latest MIMS for specific formulations and prescribing information.
2Enzyme-inducing antiepileptic drugs include Carbamazepine, Phenytoin, Primidone and Phenobarbital. |
