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Epileptiform Discharges

Febrile Seizures

First Seizure in Adulthood: Diagnosis and Treatment

First Seizure: Pediatric Perspective

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Identification of Potential Epilepsy Surgery Candidates




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Epilepsy Causes

Epilepsy Symptoms

Epilepsy Treatment


AUTHOR AND EDITOR INFORMATION

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Author: Anthony M Murro, MD, Laboratory Director, Professor, Department of Neurology, Medical College of Georgia

Anthony M Murro is a member of the following medical societies: American Academy of Neurology and American Epilepsy Society

Editors: Joseph F Hulihan, MD, Vice President, Medical Affairs, Ortho-McNeil Janssen Scientific Affairs, LLC; Francisco Talavera, PharmD, PhD, Senior Pharmacy Editor, eMedicine; Selim R Benbadis, MD, Professor, Director of Comprehensive Epilepsy Program, Departments of Neurology and Neurosurgery, University of South Florida School of Medicine, Tampa General Hospital; Matthew J Baker, MD, Consulting Staff, Collier Neurologic Specialists, Naples Community Hospital; Nicholas Y Lorenzo, MD, Chief Editor, eMedicine Neurology; Consulting Staff, Neurology Specialists and Consultants

Author and Editor Disclosure

Synonyms and related keywords: attacks, convulsions, fainting, spells, impaired consciousness, simple motor automatisms, manual automatisms, oral automatisms, perseverative automatisms, bizarre automatisms, temporal lobe complex partial seizures, parietal lobe seizures, frontal lobe seizures, extratemporal lobe seizures, occipital lobe seizures, complex partial status epilepticus, sudden unexpected death in epilepsy, SUDEP, brain trauma, encephalitis, meningitis, stroke, perinatal brain injuries, vascular malformations, cortical dysplasia, neoplasms, febrile seizures, temporal lobe epilepsy, mesial temporal sclerosis

INTRODUCTION

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Background

Complex partial seizures cause impaired consciousness and arise from a single brain region. Impaired consciousness implies decreased responsiveness and awareness of self and surroundings. During a complex partial seizure, the patient may not communicate, respond to commands, or remember events that occurred. Consciousness might not be impaired completely. During a complex partial seizure, some patients may make simple verbal responses, follow simple commands, or continue to perform simple or, less commonly, complex motor behaviors such as operating a car. Complex partial seizures typically arise from the temporal lobe but may arise from any cortical region.

Automatisms are quasi-purposeful motor or verbal behaviors that commonly accompany complex partial seizures. The behavior is called quasi-purposeful because it is repeated inappropriately or is inappropriate for the situation. Verbal automatisms range from simple vocalizations, such as moaning, to more complex, comprehensible, stereotyped speech.

Automatisms also may occur during nonepileptic states of confusion (eg, metabolic encephalopathy), after ictus, and during absence seizures. Motor automatisms are classified as simple or complex. Simple motor automatisms include oral automatisms (eg, lip smacking, chewing, swallowing) and manual automatisms (eg, picking, fumbling, patting). Unilateral manual automatisms accompanied by contralateral arm dystonia usually indicates seizure onset from the cerebral hemisphere ipsilateral to the manual automatisms.

Complex motor automatisms are more elaborate, coordinated movements involving bilateral extremities. Examples of complex motor automatisms are cycling movements of the legs and stereotyped swimming movements. De novo automatisms often begin after seizure onset. In other cases, perseverative automatisms occur as repetitions of motor activity that began before the seizure. Bizarre automatisms such as alternating limb movements, right-to-left head rolling, or sexual automatisms may occur with frontal-lobe seizures.

Seizures often begin with a brief aura (simple partial seizure) lasting seconds and then becomes a complex partial seizure. The type of aura is related to the site of cortical onset. Temporal-lobe seizures often begin with a rising abdominal sensation, fear, unreality, or déją vu. Parietal-lobe seizures may begin with an electrical sensation, tingling, or numbness. Occipital-lobe seizures may begin with visual changes, such as the perception of colored lines, spots, or shapes or even a loss of vision.

Complex partial seizures of the temporal lobe often begin with a motionless stare followed by simple oral or motor automatisms. In contrast, frontal-lobe seizures often begin with vigorous motor automatisms or stereotyped clonic or tonic activity. Extratemporal-lobe seizures may spread quickly to the frontal lobe and produce motor behaviors similar to those associated with complex partial seizures of the frontal lobe. Tonic and dystonic arm posturing may occur in the arm contralateral to the seizure focus. Sustained head or eye turning contralateral to the seizure focus may occur immediately before or simultaneously with clonic or tonic activity elsewhere.

Complex partial seizures often last 30 seconds to 2 minutes. Longer seizures may occur, particularly when the seizures become generalized convulsions. Complex partial status epilepticus may also occur with prolonged episodes of waxing and waning of consciousness.

Pathophysiology

Single photon emission CT (SPECT) ictal studies show hypoperfusion of bilateral frontal and parietal association cortex, and hyperfusion of the mediodorsal thalamus and rostral brainstem. Ictal effects on these structures by means of the spread of epileptic discharges or a transsynaptic mechanism may mediate impaired consciousness during complex partial seizures.

Frequency

United States

For people younger than 60 years, the incidence of partial seizures is 20 cases per 100,000 person-years. For people aged 60-80 years, incidence increases to 80 cases per 100,000 person-years. The prevalence of epilepsy is 0.5-1 case per 100 persons. Complex partial seizures occur in about 35% of persons with epilepsy.

International

Partial seizures are more common in countries where cysticercosis is prevalent.

Mortality/Morbidity

  • The mortality rate among individuals with epilepsy is 2-3 times that of the general population.
  • Most deaths are due to the underlying cause of epilepsy. Sudden unexpected death in epilepsy (SUDEP) occurs with no apparent cause. The incidence of SUDEP is 1 case per 370-1110 patient-years among people with epilepsy. SUDEP is most common among those with frequent, medically intractable seizures.
  • Individuals with epilepsy are at increased risk for trauma, burns, and aspiration.


CLINICAL

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History

  • Confirm that the patient does not have a nonepileptic cause for episodes of loss of consciousness. Such causes may include psychogenic nonepileptic events, syncope, transient global amnesia, migraine, or certain parasomnias.
  • A history of typical seizure auras, blank staring with the eyes open, unresponsiveness, and automatisms suggest complex partial seizures.
  • Quantify the severity of epilepsy on the basis of previous complications and seizure frequency.
  • Include the patient's responses to previous anticonvulsants or surgery.
  • Include results of previous cranial MRIs, electroencephalograms (EEGs), and EEG-video recordings.
  • Screen the patient for possible etiologies, such as brain infection, trauma, hereditary epilepsy, stroke, perinatal brain injury, cerebral palsy, cortical dysplasia, neonatal convulsions, complex febrile seizure, or vascular malformation.
  • Obtain a history from patient and from witnesses of any lateralized seizure symptoms, such as versive head or eye turning, stereotyped posturing, or postictal focal symptoms.

Physical

Physical examination is directed to elucidate focal cortical neurologic findings, such as the following:

  • Aphasia
  • Unilateral neglect
  • Apraxia
  • Unilateral limb weakness
  • Unilateral facial weakness
  • Increased muscle tone
  • Increased deep tendon reflexes
  • Pronator drift
  • Extensor plantar reflex

Causes

  • Possible causes of complex partial seizures include the following:
    • Brain trauma
    • Encephalitis
    • Meningitis
    • Stroke
    • Perinatal brain injuries
    • Vascular malformations
    • Cortical dysplasia
    • Neoplasms
  • Febrile seizures that are unusually prolonged, frequent, or associated with focal neurologic features may increase risk for later development of complex partial seizures.
  • In most patients, complex partial seizures represent a symptom of underlying temporal-lobe epilepsy, the cause of which is unknown. Characteristic pathologic changes, called mesial temporal sclerosis, are most often visible on brain MRI.


DIFFERENTIALS

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Absence Seizures
Ambulatory Electroencephalography (EEG)
Aphasia
Apraxia and Related Syndromes
Benign Childhood Epilepsy
Benign Neonatal Convulsions
Chronic Paroxysmal Hemicrania
Confusional States and Acute Memory Disorders
Early Myoclonic Encephalopathy
EEG in Common Epilepsy Syndromes
EEG in Status Epilepticus
EEG Seizure Monitoring
Epilepsia Partialis Continua
Epilepsy in Adults with Mental Retardation
Epilepsy in Children with Mental Retardation
Epilepsy, Juvenile Myoclonic
Epileptic and Epileptiform Encephalopathies
Epileptiform Discharges
Febrile Seizures
First Seizure in Adulthood: Diagnosis and Treatment
First Seizure: Pediatric Perspective
Focal EEG Waveform Abnormalities
Frontal Lobe Epilepsy
Frontal Lobe Syndromes
Identification of Potential Epilepsy Surgery Candidates

Other Problems to be Considered

Confusional arousals
Sleep walking
Sleep talking
Paroxysmal nocturnal dystonia
Night terrors
Benign epilepsy syndromes
Transient ischemic attacks
Migraines


WORKUP

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Lab Studies

  • A determination of serum anticonvulsant drug concentrations may be helpful.

Imaging Studies

  • Cranial MRI may be indicated to detect focal brain lesions (see Images 1-2).
    • Reduced hippocampal volume or increased signal on fluid-attenuation inversion recovery (FLAIR) T2-weighted MRI identifies sclerosis of mesial temporal lobe in 80-90% of cases.
    • Gadolinium enhancement is indicated if a neoplasm or vascular malformation is suspected.
    • Subtle cortical changes from cortical dysplasia are often overlooked.
  • During EEG-video monitoring, single-photon emission CT SPECT with the injection of radioisotope immediately at seizure onset (ictal SPECT) may reveal the seizure focus as an area of increased perfusion.
  • Subtraction of ictal SPECT scan from interictal SPECT scans enhances imaging of the seizure focus.
  • Interictal fluorine-18-deoxyglucose (FDG) positron emission tomography (PET) may show a hypometabolic zone ipsilateral to the seizure focus.
  • Specialized PET ligands, such as carbon-11 flumazenil or 11C-labeled methyl-L-tryptophan may help in identifying microdysgenesis or epileptogenic tubers of tuberous sclerosis, respectively.
  • The 3-T phased-array MRI detects lesions with greater sensitivity than the 1.5-T MRI.

Other Tests

  • EEG should be performed in every patient who has experienced a spell and therefore a possible seizure (see Image 3).
    • Epileptiform discharges may indicate the type of seizure and site of the seizure focus.
    • A negative interictal EEG does not exclude a diagnosis of epilepsy.
    • If the waking EEG is negative, a sleep-deprived EEG may demonstrate epileptiform abnormalities.
    • When the EEG and history are nondiagnostic, prolonged EEG-video monitoring is useful for differential diagnosis.
    • Ambulatory EEG may be used in some instances, although it provides less information about seizure behavior than EEG-video monitoring.
  • EEG within 24 hours is more useful in diagnosis of epileptiform abnormalities than later EEG (51 vs 34%).
  • Long-term anticonvulsant therapy with hepatic enzyme–inducing anticonvulsants increases the risk for osteoporosis. In patients receiving such therapy, periodic bone-density measurements may be useful.

Procedures

  • Lumbar puncture may be performed in patients in whom an inflammatory or infectious brain disorder (eg, encephalitis) is suspected.
  • Lumbar puncture is not necessary in every seizure evaluation.

Histologic Findings

Among patients with temporal-lobe epilepsy, the most common pathologic finding is sclerosis of the mesial temporal lobe. Mesial temporal sclerosis refers to hippocampal neuronal loss. Pyramidal cell loss is greater than granule cell loss. Relative sparing of neurons in the CA2 hippocampal area is observed.


TREATMENT

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Medical Care

  • Anticonvulsant therapy is generally indicated when patients have more than 1 seizure.
  • The goal is to make the patient seizure free.
  • Even 1 seizure per year may prevent the patient from working and/or driving.
  • Therapy with 1 agent is generally preferred to therapy with 2 or more anticonvulsants. Cognitive adverse effects are common with anticonvulsants.
  • The newer anticonvulsants gabapentin, lamotrigine, levetiracetam, oxcarbazepine, pregabalin, tiagabine, topiramate, and zonisamide have the following characteristics:
    • They are more costly than older anticonvulsants.
    • There are excellent drugs to use when treatment with 2 anticonvulsants is needed because they have minimal hepatic drug interactions.
    • They do not require serum drug-concentration monitoring.
    • They have a high therapeutic index.
    • They are well tolerated and can be used at doses greater than the maximum recommended dose.
  • Although many anticonvulsants are listed as category D (unsafe in pregnancy), the use of anticonvulsants during pregnancy is usually safer for women who require these drugs for seizure control than for others. Valproate is more likely than other anticonvulsants to cause congenital birth defects. The valproate-related congenital birth defect risk is greater at higher valproate doses.
  • Phenytoin and valproate have the following characteristics:
    • They bind strongly to serum proteins.
    • Free drug levels are required if the patient is pregnant or if the patient has abnormal serum protein levels (eg, due to hepatic and/or renal disease).
  • Phenobarbital is not a first-line anticonvulsant because of its sedative qualities.
  • Felbamate is not a first-line anticonvulsant because it has a significantly higher risk of aplastic anemia and hepatic injury than that of other agents.
  • Anticonvulsant drug-level monitoring may be needed.
    • Screening laboratory studies before the start of anticonvulsant therapy may provide information about risk factors, which may be important in selecting an anticonvulsant.
    • Subsequent, periodic blood and urine monitoring in otherwise asymptomatic patients receiving anticonvulsants does not help in identifying patients at risk for life-threatening adverse drug reactions.
    • Mild elevations in transaminase levels and mild depressions in blood cell counts often occur with anticonvulsant therapy. These mild abnormalities do not indicate pending hepatic failure or aplastic anemia, and anticonvulsant therapy is usually continued in otherwise asymptomatic patients.
    • Periodic blood and urine monitoring may be useful in select patients who are at increased risk for life-threatening adverse drug reactions.
    • Periodic blood and urine monitoring may be useful in select patients, such as those with mental disability who are unable to communicate.
  • Patients should be educated about how to recognize the signs of a severe adverse drug reaction.
  • Criteria for anticonvulsant withdrawal are as follows:
    • The patient should have been seizure free for a minimum of 2 years while taking anticonvulsants.
    • The patient has a single type of partial or generalized seizure.
    • Neurologic examination yields normal findings.
    • The patient has a normal IQ.
    • The EEG is normal.

Surgical Care

  • Epilepsy surgery is indicated for patients who have frequent, disabling seizures despite adequate trials of 2 or more anticonvulsants.
  • Surgical procedures include temporal lobectomy, extratemporal resections, corpus callosotomy, placement of a vagus-nerve stimulator, hemispherectomy, and multiple subpial transection.

Consultations

  • Refer the patient to an epilepsy specialist for EEG-video monitoring if his or her history and previous EEGs have been nondiagnostic, refer for EEG-video monitoring.
  • Refer the patient to an epilepsy specialist if the patient has seizures despite previous trials with multiple anticonvulsants.
  • Refer the patient to an epilepsy specialist if the patient is a possible candidate for epilepsy surgery.

Activity

  • All persons with uncontrolled seizures must be advised to refrain from high-risk activities that put themselves and/or others in danger in the event of a seizure. These activities include, but are not limited to the following:
    • Operating a motor vehicle
    • Operating a stove or other dangerous machinery
    • Working at heights
  • Persons with uncontrolled epilepsy should be advised to contact the appropriate state agency regarding driving regulations. Some states require physician reporting of drivers who experience seizures.
  • These activity restrictions should be reviewed in detail (and documented in the medical record) with the patient, family, and/or caregivers.


MEDICATION

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The goals of pharmacotherapy are to reduce morbidity and prevent complications.

Drug Category: Anticonvulsants

These agents are used to terminate clinical and electrical seizure activity as rapidly as possible and to prevent seizure recurrence.

Drug NameCarbamazepine (Carbamazepine, Tegretol, Tegretol XR)
DescriptionEffective for treatment of complex partial seizures. Appears to act by reducing polysynaptic responses and blocking posttetanic potentiation. Major mechanism of action is reducing sustained, high-frequency, repetitive neural firing.
Adult Dose200 mg PO bid (100 mg qid of suspension); increase qwk by no more than 200 mg/d tid/qid (bid with extended release) until best response; generally not to exceed 1600 mg/d
Pediatric Dose<6 years: 10-20 mg/kg/d PO bid/tid (qid with suspension); increase qwk to achieve optimal clinical response with tid/qid
6-12 years: 100 mg bid (50 mg qid of suspension); gradually increase qwk by 100 mg/d tid/qid (bid with extended release) until best response; generally not to exceed 1000 mg/d
>12 years: Administer as in adults; generally not to exceed 1000 mg/d in children 12-15 y or 1200 mg/d in adolescents >15 y
ContraindicationsDocumented hypersensitivity; history of bone-marrow depression
InteractionsDo not use concomitantly with MAOIs; discontinue MAOIs at least 14 d before initiating carbamazepine; may decrease serum concentrations of primidone or phenobarbital, which may increase serum concentration of carbamazepine, possibly because of altered hepatic metabolism; cimetidine may increase plasma levels and toxicity; interaction appears to be most important when cimetidine added during first 4 wk of therapy; use of danazol within 30 d may increase levels 38-123% (avoid concomitant administration if possible)
PregnancyD - Unsafe in pregnancy
PrecautionsNot simple analgesic; do not use for relief of minor aches or pains; caution in increased intraocular pressure; manufacturer recommends pretreatment CBC count, including platelets and possibly reticulocytes, and serum iron level; CBC count, platelets, and differential should be performed monthly in first 2 mo and then yearly or every other year; patients should observe caution while driving or performing other tasks requiring alertness, coordination, or physical dexterity (may produce drowsiness, dizziness, or blurred vision); hyponatremia

Drug NamePhenytoin (Dilantin, Phenytek)
DescriptionPrimary site of action of hydantoins, appears to be motor cortex, where it may inhibit spread of seizure activity. May reduce maximal activity of brainstem, centers responsible for tonic phase of grand mal seizures. Individualize dose. If daily dosage cannot be divided equally, large dose should be taken at bedtime. Phosphorylated formulation (fosphenytoin) available for parenteral use and may be given IM or IV.
Adult DoseInitial dose: 100 mg (125 mg suspension) PO/IV tid
Maintenance: 300-400 mg/d PO/IV divided tid, or qd/bid if using extended release; increase to 600 mg/d (625 mg/d suspension) may be necessary; not to exceed 1500 mg/24h
Pediatric DoseInitial dose: 5 mg/kg/d PO/IV divided bid/tid
Maintenance: 4-8 mg/kg PO/IV divided bid/tid
>6 years: May require minimum adult dose (300 mg/d); not to exceed 300 mg/d
ContraindicationsDocumented hypersensitivity; because of effect on ventricular automaticity, do not use in sinoatrial block, sinus bradycardia, second- or third-degree AV block, or Adams-Stokes syndrome
InteractionsAmiodarone, benzodiazepines, chloramphenicol, cimetidine, disulfiram, ethanol (acute ingestion), fluconazole, isoniazid, metronidazole, miconazole, omeprazole, phenacemide, phenylbutazone, succinimides, sulfonamides, trimethoprim, and valproic acid may increase toxicity; barbiturates, carbamazepine, diazoxide, ethanol (chronic ingestion), rifampin, theophylline, antacids, charcoal, and sucralfate may decrease effects; may decrease effects of acetaminophen, amiodarone, carbamazepine, cardiac glycosides, corticosteroids, dicumarol, disopyramide, doxycycline, estrogens, haloperidol, methadone, metyrapone, mexiletine, oral contraceptives, quinidine, theophylline, and valproic acid
PregnancyD - Unsafe in pregnancy
PrecautionsDeath from cardiac arrest has occurred after too-rapid IV administration, sometimes preceded by marked QRS widening; blood dyscrasias have occurred (manufacturer recommends CBC counts and urinalyses at start and monthly intervals for several months thereafter); discontinue if skin rash appears, and do not resume if rash is exfoliative, bullous, or purpuric; caution in acute intermittent porphyria or diabetes (may raise blood glucose levels); discontinue if hepatic dysfunction occurs

Drug NameValproic acid (Depakote, Depakene, Depacon)
DescriptionChemically unrelated to other drugs used to treat seizure disorders. Mechanism of action not established, but activity may be related to increased brain levels of GABA or enhanced GABA action. May also potentiate postsynaptic GABA responses, affect potassium channel, or have direct membrane-stabilizing effect.
For conversion to monotherapy, concomitant AED dosage ordinarily reduced by approximately 25% q2wk. Reduction may be started at beginning of therapy or delayed 1-2 wk if seizures likely to occur with reduction. Monitor patients closely during this period for increased seizure frequency.
As adjunctive therapy, divalproex sodium 10-15 mg/kg/d may be added to regimen; dosage may be increased 5-10 mg/kg/d qwk to optimal clinical response (usually with <60 mg/kg/d).
Adult DoseMonotherapy: 10-15 mg/kg/d PO in 1-3 divided doses; increase by 5-10 mg/kg/wk until seizures controlled or adverse effects prevent further increases; not to exceed 60 mg/kg/d; if total daily dose >250 mg, give in divided doses
Pediatric DoseAdminister as in adults
ContraindicationsDocumented hypersensitivity; hepatic disease/dysfunction
InteractionsCimetidine may slightly but significantly decrease clearance and increase half-life; erythromycin may increase serum concentrations, producing toxicity; felbamate may increase mean peak levels by 35%; rifampin may increase oral clearance by 40%; in children, salicylates decrease protein binding and metabolism
May cause variable changes in carbamazepine concentration with increased levels of active metabolite; carbamazepine may decrease levels, with possible loss of seizure control; displaces diazepam from plasma albumin-binding sites and inhibits metabolism, increasing toxicity; inhibits ethosuximide metabolism, and thus serum levels of both drugs should be monitored, especially in presence of other anticonvulsants; inhibits phenobarbital metabolism; phenobarbital can increase clearance; may increase action of phenytoin, even at therapeutic levels; phenytoin may increase metabolism, with decreased pharmacologic effects; may displace warfarin from protein binding sites (monitor coagulation); may decrease zidovudine clearance in HIV-seropositive patients
PregnancyD - Unsafe in pregnancy
PrecautionsThrombocytopenia and abnormal coagulation parameters have occurred; probability of thrombocytopenia increases significantly at total trough valproate plasma concentrations >110 mcg/mL in females and 135 mcg/mL in males; manufacturer recommends determining platelet counts and bleeding time before therapy, at periodic intervals, and before surgery; hemorrhage, bruising, or hemostasis/coagulation disorder indication for dosage reduction or withdrawal; hyperammonemia may occur if patient has increased renal ammonium production and inhibited urea synthesis (combined effect may contribute to hepatotoxicity; pancreatitis possible; closely monitor patients for malaise, weakness, facial edema, anorexia, jaundice, and vomiting; patients should use caution while driving or performing other tasks requiring alertness, coordination, or physical dexterity

Drug NameGabapentin (Neurontin)
DescriptionHas properties in common with other anticonvulsants but exact mechanism of action unknown. Structurally related to GABA but does not interact with GABA receptors.
Adult DoseDay 1: 100 mg PO tid or 300 mg hs
Day 2: Increase dose to 400 mg PO tid over 3 d and titrate dose prn
Increases in daily dose best tolerated when done slowly; not to exceed 1200 mg qid
Pediatric Dose<12 years: Not established
>12 years: Administer as in adults
ContraindicationsDocumented hypersensitivity
InteractionsAntacids may reduce bioavailability by about 20% and should be administered at least 2 h before; cimetidine may reduce clearance but may not be of clinical significance; may increase norethindrone levels by 13%
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsCaution in severe renal disease

Drug NameLamotrigine (Lamictal)
DescriptionTriazine derivative useful in treatment of seizures and neuralgic pain. Inhibits release of glutamate and inhibits voltage-sensitive sodium channels, which stabilizes neuronal membrane. Follow manufacturer's recommendations for dose adjustments.
Adult DoseAdjunctive therapy with enzyme-inducing anticonvulsant
Weeks 1-2: 50 mg/d PO
Weeks 3-4: 100 mg/d in 2 divided doses
Maintenance: 300-500 mg/d (in 2 divided doses); to achieve maintenance, increase by 100 mg/d q1-2wk
Adjunctive therapy with anticonvulsant regimen containing valproate
Weeks 1-2: 25 mg PO qod
Weeks 3-4: 25 mg/d
Maintenance: 100-200 mg/d PO qd/bid; to achieve maintenance, increase by 25-50 mg/d PO q1-2wk
Conversion from single enzyme-inducing anticonvulsant to lamotrigine monotherapy
Weeks 1-2: 50 mg/d
Weeks 3-4: 100 mg/d in 2 divided doses
Maintenance: 300-500 mg/d (in 2 divided doses); to achieve maintenance, increase by 100 mg/d PO q1-2wk; enzyme-inducing anticonvulsant gradually withdrawn over 4 wk by 20% decrements q1wk
Pediatric Dose2-12 years

Adjunctive therapy with enzyme-inducing anticonvulsant
Weeks 1-2: 0.6 mg/kg/d PO in 2 divided doses, rounded down to nearest 5 mg
Weeks 3-4: 1.2 mg/kg/d PO in 2 divided doses, rounded down to nearest 5 mg
Maintenance: 5-15 mg/kg/d; not to exceed 400 mg/d divided bid; to achieve usual maintenance dose, increase subsequent doses q1-2wk as follows: Calculate 1.2 mg/kg/d, round down to nearest 5 mg, and add amount to previous daily dose
As concomitant therapy with valproic acid
Weeks 1-2: 0.15 mg/kg/d PO qd or divided bid, rounded down to nearest 5 mg; if initially calculated daily dose is 2.5-5 mg, then 5 mg PO qod for first 2 wk
Weeks 3-4: 0.3 mg/kg/d PO qd or divided bid, rounded down to nearest 5 mg
Maintenance: 1-5 mg/kg/d PO; not to exceed 200 mg/d qd or divided bid; to achieve usual maintenance dose, increase subsequent doses q1-2wk as follows: Calculate 0.3 mg/kg/d, round down to nearest 5 mg, and add amount to previous qd dose

>12 years

As adjunctive therapy with enzyme-inducing anticonvulsant
Weeks 1-2: 50 mg/d
Weeks 3-4: 100 mg/d PO divided bid
Maintenance: 300-500 mg/d PO divided bid; to achieve maintenance, increase by 100 mg/d q1-2wk
As concomitant therapy with valproic acid
Weeks 1-2: 25 mg PO qod
Weeks 3-4: 25 mg PO qd
Maintenance: 100-400 mg/d PO qd or divided bid; to achieve maintenance, increase by 25-50 mg/d PO q1-2wk

ContraindicationsDocumented hypersensitivity
InteractionsAcetaminophen increases renal clearance, decreasing effects; phenobarbital and phenytoin increase metabolism, decreasing levels; valproic acid increases half-life
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsCaution in impaired renal or hepatic function; rash in 5% of patients; children who take with valproate have significantly increased risk of severe allergic drug reactions

Drug NameTopiramate (Topamax)
DescriptionSulfamate-substituted monosaccharide with broad spectrum of antiepileptic activity; may have state-dependent sodium channel blocking action; potentiates inhibitory activity of neurotransmitter GABA. May block glutamate activity. Monitoring plasma concentrations not necessary to optimize therapy. If added to phenytoin, may need to adjust phenytoin dose to achieve optimal clinical outcome.
Adult Dose50 mg/d PO; titrate by 50 mg/d qwk to target dose of 200 mg PO bid; not to exceed 1600 mg/d
Pediatric DoseNot established
ContraindicationsDocumented hypersensitivity
InteractionsPhenytoin can decrease levels by as much as 48%; carbamazepine and valproic acid reduce levels by 40% and 14%, respectively; reduces digoxin and norethindrone levels; carbonic anhydrase inhibitors may increase risk of renal stone formation and should be avoided; may have additive effect with CNS depressants in CNS depression and other cognitive or neuropsychiatric adverse effects
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsIncreases risk of kidney stone by 2-4 times that of untreated population (1.5%); increasing fluid intake may reduce this risk; caution in renal or hepatic impairment

Drug NameTiagabine (Gabitril)
DescriptionMechanism of action in antiseizure effect unknown but thought related to its ability to enhance activity of GABA, major inhibitory neurotransmitter in CNS. May block GABA uptake into presynaptic neurons, increasing GABA for receptor binding on surfaces of postsynaptic cells and possibly preventing propagation of neural impulses that contribute to seizures by GABAergic action. Modification of concomitant AED doses not necessary unless clinically indicated.
Adult Dose4 mg PO qd in 2 or 4 divided doses; increase 4-8 mg/wk until clinical response achieved or total daily dose of 56 mg/d; Doses >56 mg/d not systematically evaluated in well-controlled trials
Pediatric Dose<12 years: Not established
12-18 years: 4 mg PO qd; increase by 4 mg at beginning of wk 2; thereafter, may increase total daily dose by 4-8 mg/wk until clinical response achieved or 32 mg/d administered
Doses >32 mg/d tolerated in small number of adolescent patients for relatively short duration
ContraindicationsDocumented hypersensitivity
InteractionsHastened clearance in patients treated with carbamazepine, phenytoin, primidone, or phenobarbital
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsPatients receiving valproate monotherapy may require low doses or slow dose titration for clinical response; moderately severe to incapacitating generalized weakness reported in as many as 1% of patients with epilepsy; weakness may resolve after dose reduction or discontinuation; withdraw slowly to reduce potential for increased seizure frequency

Drug NameFelbamate (Felbatol)
DescriptionOral AED with weak inhibitory effects on GABA receptor binding and benzodiazepine receptor binding but interacts as antagonist at strychnine-insensitive glycine recognition site of NMDA receptor-ionophore complex. Not indicated as first-line antiepileptic treatment. Recommended only in those patients whose epilepsy is so severe that benefits outweigh risks of aplastic anemia or liver failure.
Adult DoseMonotherapy
Initial dose: 1200 mg/d PO divided tid/qid; titrate to 2400 mg/d by 600-mg q2wk and to 3600 mg/d if clinically indicated
Conversion to monotherapy
Initial dose: 1200 mg/d PO divided tid/qid
Week 1: Reduce dose of concomitant AEDs by one third at start
Week 2: Increase dosage to 2400 mg/d while reducing dosage of other AEDs by additional one third of original dosage
Week 3: Increase dosage up to 3600 mg/d and continue to reduce dosage of other AEDs prn
Adjunctive therapy
Week 1: 1200 mg/d PO and reduce dose of concomitant AEDs
Week 2: 2400 mg/d PO and reduce original AED doses by 33%
Week 3: 3600 mg/d PO and reduce AED doses as clinically indicated
Pediatric Dose<14 years: Not established
Adjunctive therapy
2-14 years: 15 mg/kg/d PO divided tid/qid while reducing AED doses by 20% to control plasma levels of concurrent phenytoin, valproic acid, phenobarbital, and carbamazepine (and metabolites)
Increase felbamate dosage by 15 mg/kg/d PO qwk to 45 mg/kg/d; most adverse effects during adjunctive therapy resolve as dosage of concomitant AEDs decreased
>14 years: Administer as in adults
ContraindicationsDocumented hypersensitivity; history of any blood dyscrasia or hepatic dysfunction
InteractionsMay increase steady-state phenytoin levels (reduction of phenytoin dose by as much as 40% may be necessary); phenytoin may double felbamate clearance, resulting in >45% decrease in steady-state levels; may increase phenobarbital plasma concentrations; phenobarbital may reduce plasma levels; may decrease steady-state carbamazepine levels and increase steady-state carbamazepine metabolite levels; may increase steady-state valproic acid levels
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsAssociated with marked increase in incidence of aplastic anemia (risk may be greatest during first year of therapy); manufacturer recommends periodic CBC count monitoring; increases risk of hepatic failure resulting in death; manufacturer recommends liver function testing (ALT, AST, bilirubin) before start and then q1-2wk during therapy; immediately discontinue if any liver abnormalities detected during treatment

Drug NamePhenobarbital (Luminal)
DescriptionAnticonvulsant activity at anesthetic doses and can be administered orally. If IM chosen, should be injected into large muscle, eg, gluteus maximus, vastus lateralis, or other areas with little risk of encountering nerve trunk or major artery. Injection into or near peripheral nerves may result in permanent neurologic deficit.
Restrict IV use to conditions in which other routes not feasible because patient unconscious (eg, cerebral hemorrhage, eclampsia, status epilepticus) or when prompt action imperative
Adult DosePO: 60-100 mg/d
IV or IM: 200-320 mg q6h prn
Pediatric DosePO: 3-6 mg/kg/d
IV or IM: 4-6 mg/kg/d for 7-10 d to blood level of 10-15 mcg/mL, or 10-15 mg/kg/d
ContraindicationsDocumented hypersensitivity; marked impairment of liver function; severe respiratory disease; nephritis
InteractionsAlcohol may produce additive CNS effects and death; chloramphenicol may inhibit metabolism (phenobarbital may enhance chloramphenicol metabolism); MAOIs may enhance sedative effects; rifampin induces hepatic microsomal enzymes and may decrease effectiveness; valproic acid may decrease metabolism and increase toxicity; can decrease effects of anticoagulants (patients whose PT/aPTT stabilized with anticoagulants may require dosage adjustments if phenobarbital added to or withdrawn from regimen); may decrease serum carbamazepine levels
May decrease contraceptive effects because of induction of microsomal enzymes; menstrual irregularities and pregnancy may occur (alternate birth control suggested); may enhance corticosteroid metabolism by inducing hepatic microsomal enzymes; may increase digitoxin metabolism; may decrease antimicrobial effectiveness of metronidazole; decreases theophylline levels, possibly decreasing effects; may increase clearance and decrease bioavailability of verapamil
PregnancyB - Usually safe but benefits must outweigh the risks.
PrecautionsIn select patients receiving prolonged therapy, periodic laboratory evaluation of organ (eg, hematopoietic, renal, hepatic systems) may be useful; caution in fever, hyperthyroidism, diabetes mellitus, or severe anemia (adverse reactions possible); caution in myasthenia gravis or myxedema

Drug NameOxcarbazepine (Trileptal)
DescriptionPharmacologic activity primarily by 10-monohydroxy metabolite (MHD). May block voltage-sensitive sodium channels, inhibit repetitive neuronal firing, and impair synaptic impulse propagation. Anticonvulsant effect may occur by affecting potassium conductance and high-voltage activated calcium channels. Pharmacokinetics similar in children > 8 y and adults. Children <8 y have 30-40% increased clearance. Use in children <2 y not studied in controlled clinical trials.
Adult DoseAdjunctive therapy
Initial dose: 600 mg/d PO divided bid; may increase by maximum of 600 mg/d qwk; recommended daily dose is 1200 mg/d PO; monitor for adverse effects
Conversion to monotherapy
Initial dose: 600 mg/d PO divided bid; gradually reduce dose of concomitant anticonvulsants over about 3-6 wk, and gradually increase oxcarbazepine dose over 2-4 wk; may increase dose as needed by maximum 600 mg/d PO qwk; closely monitor during transition adverse effects
Initiation of monotherapy
Initial dose: 600 mg/d PO divided bid; increase by 300 mg/d PO q3d to 1200 mg/d; monitor patients for adverse effects
Pediatric DoseAdjunctive therapy
4-16 years: 8-10 mg/kg/d PO divided bid; not to exceed 600 mg/d; gradually increase to target dose over 2 wk
Target dose based on body weight as follows:
20-29 kg: 900 mg/d PO
29.1-39 kg: 1200 mg/d PO
>39 kg: 1800 mg/d PO
ContraindicationsDocumented hypersensitivity
InteractionsMay inhibit CYP2C19 and induce CYP3A4/5; CYPP450 inducers can decrease plasma concentrations of oxcarbazepine and MHD; may decrease levels of dihydropyridine calcium antagonists and oral contraceptives; significant drug interactions related to protein binding unlikely because MHD plasma protein binding low (40%); can reduce serum concentrations of carbamazepine, phenobarbital, phenytoin, and valproic acid; doses >1200 mg/d may increase phenytoin serum concentration by as much as 40% and phenobarbital concentrations by as much as 15%; drugs metabolized by CYP450 enzymes (eg, carbamazepine, phenytoin, phenobarbital) can decrease MHD serum concentration by about 29-40%; can reduce serum concentrations of oral contraceptives and make them ineffective; can increase clearance of felodipine; verapamil may reduce serum MHD levels
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsAdverse cognitive effects (eg, psychomotor slowing, impaired concentration, impaired speech, impaired language); in impaired renal function (CrCl <30 mL/min), begin at half usual starting dose and increase increments slowly; can cause hyponatremia ( <125 mmol/L); 25-30% of people with hypersensitivity to carbamazepine hypersensitive to oxcarbazepine; rapid withdrawal can exacerbate seizures (closely observe patient for drug adverse effects, and monitor plasma levels of concomitant anticonvulsants during titration)

Drug NameLevetiracetam (Keppra)
DescriptionFor adjunctive treatment of partial seizures. Binds to presynaptic vesicle protein (SV2A). Blocks high-voltage calcium currents. Suppresses several negative modulators of GABA and glycine-gated currents.
Adult Dose500 mg PO bid initially; may increase by 1000 mg/d q2wk; not to exceed 3000 mg/d; reduce dose in reduced renal clearance
Pediatric Dose<4 years: Not established
4-15 years: 20 mg/kg/d PO divided bid; may increase by 20-mg/kg/d q2wk; not to exceed 60 mg/kg/d; use oral solution if weight <20 kg
>16 years: Administer as in adults
ContraindicationsDocumented hypersensitivity
InteractionsNone reported
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsCaution in renal impairment (reduce dose); major adverse effects include somnolence, asthenia, incoordination, mild leukopenia (3%), and behavioral changes (eg, anxiety, hostility, emotional lability, depression and psychosis [1-2%], depersonalization); seizure frequency may increase following discontinuation (do so gradually); statistically significant decreases in RBCs and WBCs have been observed

Drug NamePregabalin (Lyrica)
DescriptionBinds to the alpha2-delta subunit site of voltage-gated calcium channels) in central nervous system tissues. Modulates calcium channel function and reduces release of multiple neurotransmitters.
Adult Dose50 mg PO tid initially; increase dose gradually, not to exceed 300 mg/d PO; adjust dose in reduced renal function
Pediatric DoseNot established
ContraindicationsDocumented hypersensitivity
InteractionsMay cause additive effects on cognitive and gross motor functioning when coadministered with drugs that cause dizziness or somnolence
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsDiscontinue gradually (over a minimum of 1 wk) to minimize increased seizure frequency in patients with seizure disorders; may cause insomnia, nausea, headache, or diarrhea with abrupt withdrawal; common adverse effects include dizziness, somnolence, blurred vision, weight gain, and peripheral edema; may elevate creatinine kinase level, decrease platelet count, and increase PR interval; doses >300 mg/d associated with higher rate of adverse effects and treatment discontinuation; decrease dose with renal impairment (ie, CrCl <60 mL/min)

Drug NameZonisamide (Zonegran)
DescriptionMay block sodium channels and reduce voltage-dependent, T-type Ca2+ currents and transient inward currents. Binds to the allosteric GABA/benzodiazepine receptor ionophore. Has weak carbonic anhydrase inhibiting activity.
Adult Dose100 mg/d PO for 2 wk, then increase by 100 mg/d PO q2wk, not to exceed 400 mg/d; may be given qd or bid
Pediatric DoseNot established
ContraindicationsDocumented hypersensitivity to sulfonamides or zonisamide
InteractionsMay increase serum carbamazepine levels; carbamazepine may increase concentrations; phenobarbital may decrease levels
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsMay cause drowsiness, weight loss, ataxia, nausea, and slowing of mental activity; pediatric patients have an increased risk for oligohidrosis and hyperthermia


FOLLOW-UP

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Patient Education

  • Patients with complex partial seizures is advised not to drive, operate potentially dangerous machinery, or perform any other activities that would put themselves or others at risk of injury from a seizure.
  • Every woman of childbearing potential should be given detailed information about the risks and benefits of anticonvulsant therapy, including the increased risk of congenital malformations and the need to take daily multivitamins and folate 1-5 mg/d.
  • For excellent patient education resources, visit eMedicine's Brain and Nervous System Center. Also, see eMedicine's patient education article Epilepsy.


MISCELLANEOUS

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Medical/Legal Pitfalls

  • Clinicians should document in writing that they have advised the patient not to operate a motor vehicle or dangerous machinery or to perform any other activities that would put the patient or others at risk of injury from a seizure. Clinicians should be familiar with regulations regarding driving in the states in which they practice.
  • Clinicians should document in writing that they have advised every woman of childbearing potential on the risks and benefits of anticonvulsant therapy, including the increased risk of congenital malformations and the need to take folate 1-5 mg/d.
  • Clinicians should document that they have advised women on the risk of oral contraceptive failure that may occur with hepatic enzyme inducing anticonvulsants.

Special Concerns

  • The benefits of controlled seizures outweigh the risks of drug therapy during pregnancy.
  • The risk of congenital malformations is increased 2-4 times with anticonvulsant therapy during pregnancy.
  • During pregnancy, a woman with epilepsy should receive the minimum dose and the minimum number of anticonvulsants that can control her seizures.
  • Supplementary folate 1-5 mg/d is recommended for all women of childbearing age who take anticonvulsants.
  • Phenytoin, phenobarbital, topiramate, and carbamazepine may cause oral contraceptives to fail.
  • The best anticonvulsant during pregnancy is the one that best controls the patients' seizures. Valproate has a higher risk of congenital malformations compared with that of other anticonvulsants. Lamotrigine does not appear to increase the risk of congenital malformations.
  • A common error during pregnancy is to switch the anticonvulsant to an apparently safer anticonvulsant though the patient's seizures are well controlled.
  • Use of enzyme-inducing anticonvulsants, particularly phenobarbital, may increase the risk of perinatal hemorrhagic complications. Supplementary vitamin K 10 mg/d is recommended during the last month of pregnancy.
  • The risk of congenital malformations increases during the switch-over period, when the mother is exposed to 2 anticonvulsants.
  • Changing the mother's current anticonvulsant to one that is less effective in controlling seizures may harm the mother and the baby.


MULTIMEDIA

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Media file 1:  MRI in a patient with temporal-lobe complex partial seizures due to a hippocampal tumor, which appears as an enlargement of the hippocampus (box).
Click to see larger pictureClick to see detailView Full Size Image
Media type:  MRI

Media file 2:  MRI in a patient with complex partial seizures due to biopsy-proven CNS vasculitis shows 2 high-signal-intensity lesions.
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Media type:  MRI

Media file 3:  Electroencephalographic recording of a temporal-lobe complex partial seizure shows the seizure pattern (boxes).
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Media type:  Rhythm Strip


REFERENCES

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Complex Partial Seizures excerpt

Article Last Updated: Oct 11, 2006