Epileptic seizure

A seizure, formally known as an epileptic seizure, is a period of symptoms due to abnormally excessive or synchronous neuronal activity in the brain.[5] Outward effects vary from uncontrolled shaking movements involving much of the body with loss of consciousness (tonic-clonic seizure), to shaking movements involving only part of the body with variable levels of consciousness (focal seizure), to a subtle momentary loss of awareness (absence seizure).[3] Most of the time these episodes last less than 2 minutes and it takes some time to return to normal.[4][7] Loss of bladder control may occur.[3]

Epileptic seizure
Other namesEpileptic fit,[1] seizure, fit, convulsions[2]
Generalized 3 Hz spike and wave discharges in EEG
SpecialtyNeurology, emergency medicine
SymptomsVariable[3]
DurationTypically < 2 minutes[4]
TypesProvoked, unprovoked[5]
CausesProvoked: Low blood sugar, alcohol withdrawal, low blood sodium, fever, brain infection, concussion[3][5]
Unprovoked: Unknown, brain injury, brain tumor, previous stroke[4][3][5][6]
Diagnostic methodBased on symptoms, blood tests, medical imaging, electroencephalography[6]
Differential diagnosisSyncope, nonepileptic psychogenic event, tremor, migraine, transient ischemic attack[3][4]
TreatmentLess than 5 min: Place person on their side, remove nearby dangerous objects[7]
More than 5 min: Treat as per status epilepticus[7]
Frequency~10% of people (at one point in time)[4][8]

Seizures may be provoked and unprovoked.[5] Provoked seizures are due to a temporary event such as low blood sugar, alcohol withdrawal, low blood sodium, fever, brain infection, or concussion.[3][5] Unprovoked seizures occur without a known or fixable cause such that ongoing seizures are likely.[4][3][5][6] Unprovoked seizures may be triggered by stress or sleep deprivation.[3] Diseases of the brain, where there has been at least one seizure and a long term risk of further seizures, are collectively known as epilepsy.[5] Conditions that look like epileptic seizures but are not include fainting, nonepileptic psychogenic event, and tremor.[3]

A seizure that lasts for more than a brief period is a medical emergency.[9] Any seizure lasting longer than 5 minutes should be treated as status epilepticus.[7] A first seizure generally does not require long term treatment with anti-seizure medications unless a specific problem is found on electroencephalogram (EEG) or brain imaging.[6] Typically it is safe to complete the work-up following a single seizure as an outpatient.[3] In many, with what appears to be a first seizure, other minor seizures have previously occurred.[10]

Up to 10% of people have at least one epileptic seizure.[4][8] Provoked seizures occur in about 3.5 per 10,000 people a year while unprovoked seizures occur in about 4.2 per 10,000 people a year.[4] After one seizure, the chance of experiencing a second is about 50%.[11] Epilepsy affects about 1% of the population at any given time[8] with about 4% of the population affected at some point in time.[6] Nearly 80% of those with epilepsy live in developing countries.[8] Many places require people to stop driving until they have not had a seizure for a specific period.[4]

Signs and symptoms

The signs and symptoms of seizures vary depending on the type.[12] The most common type of seizure is convulsive (60%).[13] Two-thirds of these begin as focal seizures and become generalized while one third begin as generalized seizures.[13] The remaining 40% of seizures are non-convulsive, an example of which is absence seizure.[14]

Focal seizures

Focal seizures are often preceded by certain experiences, known as an aura.[12] These may include sensory, visual, psychic, autonomic, olfactory or motor phenomena.[15]

In a complex partial seizure a person may appear confused or dazed and can not respond to questions or direction. Focal seizure may become generalized.[15]

Jerking activity may start in a specific muscle group and spread to surrounding muscle groups—known as a Jacksonian march.[16] Unusual activities that are not consciously created may occur.[16] These are known as automatisms and include simple activities like smacking of the lips or more complex activities such as attempts to pick something up.[16]

Generalized seizures

There are six main types of generalized seizures: tonic-clonic, tonic, clonic, myoclonic, absence, and atonic seizures.[17] They all involve a loss of consciousness and typically happen without warning.[18]

  • Tonic-clonic seizures present with a contraction of the limbs followed by their extension, along with arching of the back for 10–30 seconds.[18] A cry may be heard due to contraction of the chest muscles.[18] The limbs then begin to shake in unison.[18] After the shaking has stopped it may take 10–30 minutes for the person to return to normal.[18]
  • Tonic seizures produce constant contractions of the muscles.[18] The person may turn blue if breathing is impaired.[18]
  • Clonic seizures involve shaking of the limbs in unison.[18]
  • Myoclonic seizures involve spasms of muscles in either a few areas or generalized through the body.[18]
  • Absence seizures can be subtle, with only a slight turn of the head or eye blinking.[15] The person often does not fall over and may return to normal right after the seizure ends, though there may also be a period of post-ictal disorientation.[15]
  • Atonic seizures involve the loss of muscle activity for greater than one second.[16] This typically occurs bilaterally (on both sides of the body).[16]

Duration

A seizure can last from a few seconds to more than five minutes, at which point it is known as status epilepticus.[19] Most tonic-clonic seizures last less than two or three minutes.[19] Absence seizures are usually around 10 seconds in duration.[14]

Postictal

After the active portion of a seizure, there is typically a period of confusion called the postictal period before a normal level of consciousness returns.[12] This usually lasts 3 to 15 minutes[20] but may last for hours.[21] Other common symptoms include: feeling tired, headache, difficulty speaking, and abnormal behavior.[21] Psychosis after a seizure is relatively common, occurring in between 6 and 10% of people.[22] Often people do not remember what occurred during this time.[21]

Causes

Seizures have a number of causes. Of those who have a seizure, about 25% have epilepsy.[23] A number of conditions are associated with seizures but are not epilepsy including: most febrile seizures and those that occur around an acute infection, stroke, or toxicity.[24] These seizures are known as "acute symptomatic" or "provoked" seizures and are part of the seizure-related disorders.[24] In many the cause is unknown.

Different causes of seizures are common in certain age groups.

  • Seizures in babies are most commonly caused by hypoxic ischemic encephalopathy, central nervous system (CNS) infections, trauma, congenital CNS abnormalities, and metabolic disorders.
  • The most frequent cause of seizures in children is febrile seizures, which happen in 2–5% of children between the ages of six months and five years.[25]
  • During childhood, well-defined epilepsy syndromes are generally seen.
  • In adolescence and young adulthood, non-compliance with the medication regimen and sleep deprivation are potential triggers.
  • Pregnancy and labor and childbirth, and the post-partum, or post-natal period (after birth) can be at-risk times, especially if there are certain complications like pre-eclampsia.
  • During adulthood, the likely causes are alcohol related, strokes, trauma, CNS infections, and brain tumors.[26]
  • In older adults, cerebrovascular disease is a very common cause. Other causes are CNS tumors, head trauma, and other degenerative diseases that are common in the older age group, such as dementia.[27]

Metabolic

Dehydration can trigger epileptic seizures if it is severe enough.[28] A number of disorders including: low blood sugar, low blood sodium, hyperosmolar nonketotic hyperglycemia, high blood sodium, low blood calcium and high blood urea levels may cause seizures.[18] As may hepatic encephalopathy and the genetic disorder porphyria.[18]

Structural

Medications

Both medication and drug overdoses can result in seizures,[18] as may certain medication and drug withdrawal.[18] Common drugs involved include: antidepressants, antipsychotics, cocaine, insulin, and the local anaesthetic lidocaine.[18] Difficulties with withdrawal seizures commonly occurs after prolonged alcohol or sedative use, a condition known as delirium tremens.[18]

Infections

Stress

Stress can induce seizures in people with epilepsy, and is a risk factor for developing epilepsy. Severity, duration, and time at which stress occurs during development all contribute to frequency and susceptibility to developing epilepsy. It is one of the most frequently self-reported triggers in patients with epilepsy.[33][34]

Stress exposure results in hormone release that mediates its effects in the brain. These hormones act on both excitatory and inhibitory neural synapses, resulting in hyper-excitability of neurons in the brain. The hippocampus is known to be a region that is highly sensitive to stress and prone to seizures. This is where mediators of stress interact with their target receptors to produce effects.[35]

Other

Seizures may occur as a result of high blood pressure, known as hypertensive encephalopathy, or in pregnancy as eclampsia when accompanied by either seizures or a decreased level of consciousness.[18] Very high body temperatures may also be a cause.[18] Typically this requires a temperature greater than 42 °C (107.6 °F).[18]

Electroconvulsive therapy (ECT) deliberately sets out to induce a seizure for the treatment of major depression.

Mechanism

Normally brain electrical activity is non synchronous.[15] In epileptic seizures, due to problems within the brain,[37] a group of neurons begin firing in an abnormal, excessive,[13] and synchronized manner.[15] This results in a wave of depolarization known as a paroxysmal depolarizing shift.[38]

Normally after an excitatory neuron fires it becomes more resistant to firing for a period of time.[15] This is due in part from the effect of inhibitory neurons, electrical changes within the excitatory neuron, and the negative effects of adenosine.[15] In epilepsy the resistance of excitatory neurons to fire during this period is decreased.[15] This may occur due to changes in ion channels or inhibitory neurons not functioning properly.[15] Forty-one ion-channel genes and over 1,600 ion-channel mutations have been implicated in the development of epileptic seizure.[39] These ion channel mutations tend to confer a depolarized resting state to neurons resulting in pathological hyper-excitability.[40] This long-lasting depolarization in individual neurons is due to an influx of Ca2+ from outside of the cell and leads to extended opening of Na+ channels and repetitive action potentials.[41] The following hyperpolarization is facilitated by γ-aminobutyric acid (GABA) receptors or potassium (K+) channels, depending on the type of cell.[41] Equally important in epileptic neuronal hyper-excitability, is the reduction in the activity of inhibitory GABAergic neurons, an effect known as disinhibition. Disinhibition may result from inhibitory neuron loss, dysregulation of axonal sprouting from the inhibitory neurons in regions of neuronal damage, or abnormal GABAergic signaling within the inhibitory neuron.[42] Neuronal hyper-excitability results in a specific area from which seizures may develop, known as a "seizure focus".[15] Following an injury to the brain, another mechanism of epilepsy may be the up regulation of excitatory circuits or down regulation of inhibitory circuits.[15][43] These secondary epilepsies occur through processes known as epileptogenesis.[15][43] Failure of the blood–brain barrier may also be a causal mechanism.[44] While blood-brain barrier disruption alone does appear to cause epileptogenesis, it has been correlated to increased seizure activity.[45] Furthermore, it has been implicated in chronic epileptic conditions through experiments inducing barrier permeability with chemical compounds.[45] Disruption may lead to fluid leaking out of the blood vessels into the area between cells and driving epileptic seizures.[46] Preliminary findings of blood proteins in the brain after a seizure support this theory.[45]

Focal seizures begin in one hemisphere of the brain while generalized seizures begin in both hemispheres.[17] Some types of seizures may change brain structure, while others appear to have little effect.[47] Gliosis, neuronal loss, and atrophy of specific areas of the brain are linked to epilepsy but it is unclear if epilepsy causes these changes or if these changes result in epilepsy.[47]

Seizure activity may be propagated through the brain's endogenous electrical fields.[48] Proposed mechanisms that may cause the spread and recruitment of neurons include an increase in K+ from outside the cell, and increase of Ca2+ in the presynaptic terminals.[41] These mechanisms blunt hyperpolarization and depolarizes nearby neurons, as well as increasing neurotransmitter release.[41]

Diagnosis

The 2017 ILAE classification of seizure types and the epilepsies (click to read full text)

Seizures may be divided into provoked and unprovoked.[5] Provoked seizures may also be known as "acute symptomatic seizures" or "reactive seizures".[5] Unprovoked seizures may also be known as "reflex seizures".[5] Depending on the presumed cause blood tests and lumbar puncture may be useful.[6] Hypoglycemia may cause seizures and should be ruled out. An electroencephalogram and brain imaging with CT scan or MRI scan is recommended in the work-up of seizures not associated with a fever.[6][49]

Classification

Seizure types are organized by whether the source of the seizure is localized (focal seizures) or distributed (generalized seizures) within the brain.[17] Generalized seizures are divided according to the effect on the body and include tonic-clonic (grand mal), absence (petit mal), myoclonic, clonic, tonic, and atonic seizures.[17][50] Some seizures such as epileptic spasms are of an unknown type.[17]

Focal seizures (previously called partial seizures[13]) are divided into simple partial or complex partial seizure.[17] Current practice no longer recommends this, and instead prefers to describe what occurs during a seizure.[17]

Physical examination

An individual who has bitten the tip of their tongue while having a seizure

Most people are in a postictal state (drowsy or confused) following a seizure. They may show signs of other injuries. A bite mark on the side of the tongue helps confirm a seizure when present, but only a third of people who have had a seizure have such a bite.[51] When present in people thought to have had a seizure, this physical sign tentatively increases the likelihood that a seizure was the cause.[52]

Tests

An EEG can aid in locating the focus of the epileptic seizure.

An electroencephalography is only recommended in those who likely had an epileptic seizure and may help determine the type of seizure or syndrome present. In children it is typically only needed after a second seizure. It cannot be used to rule out the diagnosis and may be falsely positive in those without the disease. In certain situations it may be useful to prefer the EEG while sleeping or sleep deprived.[53]

Diagnostic imaging by CT scan and MRI is recommended after a first non-febrile seizure to detect structural problems inside the brain.[53] MRI is generally a better imaging test except when intracranial bleeding is suspected.[6] Imaging may be done at a later point in time in those who return to their normal selves while in the emergency room.[6] If a person has a previous diagnosis of epilepsy with previous imaging repeat imaging is not usually needed with subsequent seizures.[53]

In adults, testing electrolytes, blood glucose and calcium levels is important to rule these out as causes, as is an electrocardiogram.[53] A lumbar puncture may be useful to diagnose a central nervous system infection but is not routinely needed.[6] Routine antiseizure medical levels in the blood are not required in adults or children.[53] In children additional tests may be required.[53]

A high blood prolactin level within the first 20 minutes following a seizure may be useful to confirm an epileptic seizure as opposed to psychogenic non-epileptic seizure.[54][55] Serum prolactin level is less useful for detecting partial seizures.[56] If it is normal an epileptic seizure is still possible[55] and a serum prolactin does not separate epileptic seizures from syncope.[57] It is not recommended as a routine part of diagnosis epilepsy.[53]

Differential diagnosis

Differentiating an epileptic seizure from other conditions such as syncope can be difficult.[12] Other possible conditions that can mimic a seizure include: decerebrate posturing, psychogenic seizures, tetanus, dystonia, migraine headaches, and strychnine poisoning.[12] In addition, 5% of people with a positive tilt table test may have seizure-like activity that seems due to cerebral hypoxia.[58] Convulsions may occur due to psychological reasons and this is known as a psychogenic non-epileptic seizure. Non-epileptic seizures may also occur due to a number of other reasons.

Prevention

A number of measures have been attempted to prevent seizures in those at risk. Following traumatic brain injury anticonvulsants decrease the risk of early seizures but not late seizures.[59]

In those with a history of febrile seizures, medications (both antipyretics and anticonvulsants) have not been found effective for prevention. Some, in fact, may cause harm.[60]

There is no clear evidence that antiepileptic drugs are effective or not effective at preventing seizures following a craniotomy,[61] following subdural hematoma,[62] after a stroke,[63][64] or after subarachnoid haemorrhage,[65] for both people who have had a previous seizure, and those who have not.

Management

Potentially sharp or dangerous objects should be moved from the area around a person experiencing a seizure, so that the individual is not hurt. After the seizure if the person is not fully conscious and alert, they should be placed in the recovery position. A seizure longer than five minutes, or two or more seizures occurring within the time of five minutes is a medical emergency known as status epilepticus.[19][66] Contrary to a common misconception, bystanders should not attempt to force objects into the mouth of the person suffering a seizure, as doing so may cause injury to the teeth and gums.[67]

Treatments of a person that is actively seizing follows a progression from initial response, through first line, second line, and third line treatments.[68] The initial response involves ensuring the person is protected from potential harms (such as nearby objects) and managing their airway, breathing, and circulation.[68] Airway management should include placing the person on their side, known as the recovery position, to prevent them from choking.[68] If they are unable to breathe because something is blocking their airway, they may require treatments to open their airway.[68]

Medication

The first line medication for an actively seizing person is a benzodiazepine, with most guidelines recommending lorazepam.[49][69] Diazepam and midazolam are alternatives. This may be repeated if there is no effect after 10 minutes.[49] If there is no effect after two doses, barbiturates or propofol may be used.[49] Benzodiazepines given by a non-intravenous route appear better than those given by intravenous, as the intravenous takes longer to have an effect.[70]

Second-line therapy for adults is phenytoin or fosphenytoin and phenobarbital for children.[71] Third-line medications include phenytoin for children and phenobarbital for adults.[71]

Ongoing anti-epileptic medications are not typically recommended after a first seizure except in those with structural lesions in the brain.[49] They are generally recommended after a second one has occurred.[49] Approximately 70% of people can obtain full control with continuous use of medication.[37] Typically one type of anticonvulsant is preferred. Following a first seizure, while immediate treatment with an anti-seizure drug lowers the probability of seizure recurrence up to five years it does not change the risk of death and there are potential side effects.[72]

In seizures related to toxins, up to two doses of benzodiazepines should be used.[73] If this is not effective pyridoxine is recommended.[73] Phenytoin should generally not be used.[73]

There is a lack of evidence for preventative anti-epileptic medications in the management of seizures related to intracranial venous thrombosis.[64]

Other

Helmets may be used to provide protection to the head during a seizure. Some claim that seizure response dogs, a form of service dog, can predict seizures.[74] Evidence for this, however, is poor.[74] At present there is not enough evidence to support the use of cannabis for the management of seizures, although this is an ongoing area of research.[75][76] There is tentative evidence that a ketogenic diet may help in those who have epilepsy and is reasonable in those who do not improve following typical treatments.[77]

Prognosis

Following a first seizure, the risk of more seizures in the next two years is 40%–50%.[6] The greatest predictors of more seizures are problems either on the electroencephalogram or on imaging of the brain.[6] In adults, after 6 months of being seizure-free after a first seizure, the risk of a subsequent seizure in the next year is less than 20% regardless of treatment.[78] Up to 7% of seizures that present to the emergency department (ER) are in status epilepticus.[49] In those with a status epilepticus, mortality is between 10% and 40%.[12] Those who have a seizure that is provoked (occurring close in time to an acute brain event or toxic exposure) have a low risk of re-occurrence, but have a higher risk of death compared to those with epilepsy.[79]

Epidemiology

Approximately 8-10% of people will experience an epileptic seizure during their lifetime.[80] In adults, the risk of seizure recurrence within the five years following a new-onset seizure is 35%; the risk rises to 75% in persons who have had a second seizure.[80] In children, the risk of seizure recurrence within the five years following a single unprovoked seizure is about 50%; the risk rises to about 80% after two unprovoked seizures.[81] In the United States in 2011, seizures resulted in an estimated 1.6 million emergency department visits; approximately 400,000 of these visits were for new-onset seizures.[80] The exact incidence of epileptic seizures in low-income and middle-income countries is unknown, however it probably exceeds that in high-income countries.[82] This may be due to increased risks of traffic accidents, birth injuries, and malaria and other parasitic infections.[82]

History

Epileptic seizures were first described in an Akkadian text from 2000 B.C.[83] Early reports of epilepsy often saw seizures and convulsions as the work of “evil spirits”.[84] The perception of epilepsy, however, began to change in the time of Ancient Greek medicine. The term “epilepsy” itself is a Greek word, which is derived from the verb “epilambanein”, meaning “to seize, possess, or afflict”.[83] Although the Ancient Greeks referred to epilepsy as the “sacred disease”, this perception of epilepsy as a “spiritual” disease was challenged by Hippocrates in his work “On The Sacred Disease”, who proposed that the source of epilepsy was from natural causes rather than supernatural ones.[84]

Early surgical treatment of epilepsy was primitive in Ancient Greek, Roman and Egyptian medicine.[85] The 19th century saw the rise of targeted surgery for the treatment of epileptic seizures, beginning in 1886 with localized resections performed by Sir Victor Horsley, a neurosurgeon in London.[84]  Another advancement was that of the development by the Montreal procedure by Canadian neurosurgeon Wilder Penfield, which involved use of electrical stimulation among conscious patients to more accurately identify and resect the epileptic areas in the brain.[84]

Society and culture

Economics

Seizures result in direct economic costs of about one billion dollars in the United States.[6] Epilepsy results in economic costs in Europe of around 15.5 billion Euros in 2004.[13] In India, epilepsy is estimated to result in costs of US$1.7 billion or 0.5% of the GDP.[37] They make up about 1% of emergency department visits (2% for emergency departments for children) in the United States.[26]

Driving

Many areas of the world require a minimum of six months from the last seizure before people can drive a vehicle.[6]

Research

Scientific work into the prediction of epileptic seizures began in the 1970s. Several techniques and methods have been proposed, but evidence regarding their usefulness is still lacking.[86]

Two promising areas include gene therapy,[87] and seizure detection and seizure prediction.[88]

Gene therapy for epilepsy consists of employing vectors to deliver pieces of genetic material to areas of the brain involved in seizure onset.[87]

Seizure prediction is a special case of seizure detection in which the developed systems is able to issue a warning before the clinical onset of the epileptic seizure.[86][88]

References

  1. Shorvon, Simon (2009). Epilepsy. OUP Oxford. p. 1. ISBN 9780199560042.
  2. "Seizures - National Library of Medicine". PubMed Health. Retrieved 16 October 2018.
  3. Misulis, Karl E.; Murray, E. Lee (2017). Essentials of Hospital Neurology. Oxford University Press. p. Chapter 19. ISBN 9780190259433.
  4. Ferri, Fred F. (2018). Ferri's Clinical Advisor 2019 E-Book: 5 Books in 1. Elsevier Health Sciences. p. 959. ISBN 9780323550765.
  5. Fisher, RS; Acevedo, C; Arzimanoglou, A; Bogacz, A; Cross, JH; Elger, CE; Engel J, Jr; Forsgren, L; French, JA; Glynn, M; Hesdorffer, DC; Lee, BI; Mathern, GW; Moshé, SL; Perucca, E; Scheffer, IE; Tomson, T; Watanabe, M; Wiebe, S (April 2014). "ILAE official report: a practical clinical definition of epilepsy". Epilepsia. 55 (4): 475–82. doi:10.1111/epi.12550. PMID 24730690.
  6. Wilden, JA; Cohen-Gadol, AA (15 August 2012). "Evaluation of first nonfebrile seizures". American Family Physician. 86 (4): 334–40. PMID 22963022.
  7. "The Epilepsies and Seizures: Hope Through Research". National Institute of Neurological Disorders and Stroke. Retrieved 16 October 2018.
  8. "Epilepsy". World Health Organization. 8 February 2018. Retrieved 16 October 2018.
  9. "What Is A Seizure Emergency". epilepsy.com. Retrieved 8 May 2018.
  10. Angus-Leppan H (2014). "First seizures in adults". BMJ. 348: g2470. doi:10.1136/bmj.g2470. PMID 24736280.
  11. Berg, AT (2008). "Risk of recurrence after a first unprovoked seizure". Epilepsia. 49 Suppl 1: 13–8. doi:10.1111/j.1528-1167.2008.01444.x. PMID 18184149.
  12. Shearer, Peter. "Seizures and Status Epilepticus: Diagnosis and Management in the Emergency Department". Emergency Medicine Practice. Archived from the original on 30 December 2010.
  13. National Institute for Health and Clinical Excellence (January 2012). "Chapter 1: Introduction" (PDF). The Epilepsies: The diagnosis and management of the epilepsies in adults and children in primary and secondary care. National Clinical Guideline Centre. pp. 21–28. Archived (PDF) from the original on 16 December 2013.
  14. Hughes, JR (August 2009). "Absence seizures: a review of recent reports with new concepts". Epilepsy & Behavior. 15 (4): 404–12. doi:10.1016/j.yebeh.2009.06.007. PMID 19632158.
  15. Hammer, edited by Stephen J. McPhee, Gary D. (2010). "7". Pathophysiology of disease : an introduction to clinical medicine (6th ed.). New York: McGraw-Hill Medical. ISBN 978-0-07-162167-0.CS1 maint: extra text: authors list (link)
  16. Bradley, Walter G. (2012). "67". Bradley's neurology in clinical practice (6th ed.). Philadelphia, PA: Elsevier/Saunders. ISBN 978-1-4377-0434-1.
  17. National Institute for Health and Clinical Excellence (January 2012). "Chapter 9: Classification of seizures and epilepsy syndromes" (PDF). The Epilepsies: The diagnosis and management of the epilepsies in adults and children in primary and secondary care. National Clinical Guideline Centre. pp. 119–129. Archived (PDF) from the original on 16 December 2013.
  18. Simon, David A. Greenberg, Michael J. Aminoff, Roger P. (2012). "12". Clinical neurology (8th ed.). New York: McGraw-Hill Medical. ISBN 978-0-07-175905-2.
  19. Trinka, E; Höfler, J; Zerbs, A (September 2012). "Causes of status epilepticus". Epilepsia. 53 Suppl 4: 127–38. doi:10.1111/j.1528-1167.2012.03622.x. PMID 22946730.
  20. Holmes, Thomas R. (2008). Handbook of epilepsy (4th ed.). Philadelphia: Lippincott Williams & Wilkins. p. 34. ISBN 978-0-7817-7397-3. Archived from the original on 7 May 2016.
  21. Panayiotopoulos, CP (2010). A clinical guide to epileptic syndromes and their treatment based on the ILAE classifications and practice parameter guidelines (Rev. 2nd ed.). [London]: Springer. p. 445. ISBN 978-1-84628-644-5. Archived from the original on 28 April 2016.
  22. James W. Wheless, ed. (2009). Advanced therapy in epilepsy. Shelton, Conn.: People's Medical Pub. House. p. 443. ISBN 978-1-60795-004-2. Archived from the original on 6 May 2016.
  23. Stasiukyniene, V.; Pilvinis, V.; Reingardiene, D.; Janauskaite, L. (2009). "[Epileptic seizures in critically ill patients]". Medicina. 45 (6): 501–7. doi:10.3390/medicina45060066. PMID 19605972.
  24. Thurman DJ, Beghi E, Begley CE, Berg AT, Buchhalter JR, Ding D, Hesdorffer DC, Hauser WA, Kazis L, Kobau R, Kroner B, Labiner D, Liow K, Logroscino G, Medina MT, Newton CR, Parko K, Paschal A, Preux PM, Sander JW, Selassie A, Theodore W, Tomson T, Wiebe S (September 2011). "Standards for epidemiologic studies and surveillance of epilepsy". Epilepsia. 52 Suppl 7: 2–26. doi:10.1111/j.1528-1167.2011.03121.x. PMID 21899536.
  25. Graves, RC; Oehler, K; Tingle, LE (15 January 2012). "Febrile seizures: risks, evaluation, and prognosis". American Family Physician. 85 (2): 149–53. PMID 22335215.
  26. Martindale JL, Goldstein JN, Pallin DJ (2011). "Emergency department seizure epidemiology". Emerg. Med. Clin. North Am. 29 (1): 15–27. doi:10.1016/j.emc.2010.08.002. PMID 21109099.
  27. Harrison's Principles of Medicine. 15th edition
  28. "diet and nutrition". 8 May 2013. Archived from the original on 29 June 2015.
  29. Hildebrand, J (July 2004). "Management of epileptic seizures". Curr Opin Oncol. 16 (4): 314–7. doi:10.1097/01.cco.0000127720.17558.38. PMID 15187884.
  30. Bhalla, D.; Godet, B.; Druet-Cabanac, M.; Preux, PM. (June 2011). "Etiologies of epilepsy: a comprehensive review". Expert Rev Neurother. 11 (6): 861–76. doi:10.1586/ern.11.51. PMID 21651333.
  31. "Management of Convulsion in Children, a Health concern in Nigeria". Public Health Nigeria. October 2018. Archived from the original on 18 October 2018. Retrieved 18 October 2018.
  32. Carlson, Neil (22 January 2012). Physiology of Behavior. Neurological Disorders. 11th edition. Pearson. p. 550. ISBN 978-0-205-23939-9.
  33. Nakken, Karl O.; Solaas, Marit H.; Kjeldsen, Marianne J.; Friis, Mogens L.; Pellock, John M.; Corey, Linda A. (2005). "Which seizure-precipitating factors do patients with epilepsy most frequently report?". Epilepsy & Behavior. 6 (1): 85–89. doi:10.1016/j.yebeh.2004.11.003. PMID 15652738.
  34. Haut, Sheryl R.; Hall, Charles B.; Masur, Jonathan; Lipton, Richard B. (13 November 2007). "Seizure occurrence: precipitants and prediction". Neurology. 69 (20): 1905–1910. doi:10.1212/01.wnl.0000278112.48285.84. ISSN 1526-632X. PMID 17998482.
  35. Gunn, B.G.; Baram, T.Z. (2017). "Stress and Seizures: Space, Time and Hippocampal Circuits". Trends in Neurosciences. 40 (11): 667–679. doi:10.1016/j.tins.2017.08.004. PMC 5660662. PMID 28916130.
  36. Bushara, KO (April 2005). "Neurologic presentation of celiac disease". Gastroenterology. 128 (4 Suppl 1): S92–7. doi:10.1053/j.gastro.2005.02.018. PMID 15825133.
  37. "Epilepsy". Fact Sheets. World Health Organization. October 2012. Archived from the original on 11 March 2016. Retrieved 24 January 2013.
  38. Somjen, George G. (2004). Ions in the Brain Normal Function, Seizures, and Stroke. New York: Oxford University Press. p. 167. ISBN 978-0-19-803459-9. Archived from the original on 6 May 2016.
  39. Wei, Feng; Yan, Li-Min; Su, Tao; He, Na; Lin, Zhi-Jian; Wang, Jie; Shi, Yi-Wu; Yi, Yong-Hong; Liao, Wei-Ping (August 2017). "Ion Channel Genes and Epilepsy: Functional Alteration, Pathogenic Potential, and Mechanism of Epilepsy". Neuroscience Bulletin. 33 (4): 455–477. doi:10.1007/s12264-017-0134-1. ISSN 1995-8218. PMC 5567559. PMID 28488083.
  40. Ropper, A (2014). Adams and Victor's Principles of Neurology (10th ed., p. Chapter 16. Epilepsy and Other Seizure Disorders). New York: McGraw-Hill.
  41. Lowenstein DH. Seizures and Epilepsy. In: Jameson J, Fauci AS, Kasper DL, Hauser SL, Longo DL, Loscalzo J. eds. (2018) Harrison's Principles of Internal Medicine, 20e New York, NY: McGraw-Hill.
  42. Liu, Yu-Qiang; Yu, Fang; Liu, Wan-Hong; He, Xiao-Hua; Peng, Bi-Wen (December 2014). "Dysfunction of hippocampal interneurons in epilepsy". Neuroscience Bulletin. 30 (6): 985–998. doi:10.1007/s12264-014-1478-4. ISSN 1995-8218. PMC 5562563. PMID 25370443.
  43. Goldberg, EM; Coulter, DA (May 2013). "Mechanisms of epileptogenesis: a convergence on neural circuit dysfunction". Nature Reviews. Neuroscience. 14 (5): 337–49. doi:10.1038/nrn3482. PMC 3982383. PMID 23595016.
  44. Oby, E; Janigro, D (November 2006). "The blood-brain barrier and epilepsy". Epilepsia. 47 (11): 1761–74. doi:10.1111/j.1528-1167.2006.00817.x. PMID 17116015.
  45. van Vliet, E.A.; Aronica, E.; Gorter, J.A. (2015). "Blood–brain barrier dysfunction, seizures and epilepsy". Seminars in Cell & Developmental Biology. 38: 26–34. doi:10.1016/j.semcdb.2014.10.003. ISSN 1084-9521. PMID 25444846.
  46. Marchi, Nicola; Banjara, Manoj; Janigro, Damir (2016). "Blood–brain barrier, bulk flow, and interstitial clearance in epilepsy". Journal of Neuroscience Methods. 260: 118–124. doi:10.1016/j.jneumeth.2015.06.011. ISSN 0165-0270. PMC 4835226. PMID 26093166.
  47. Jerome Engel, Jr.; Timothy A. Pedley, eds. (2008). Epilepsy : a comprehensive textbook (2nd ed.). Philadelphia: Wolters Kluwer Health/Lippincott Williams & Wilkins. p. 483. ISBN 978-0-7817-5777-5.
  48. Qiu, Chen; Shivacharan, Rajat S; Zhang, Mingming; Durand, Dominique M (2015). "Can Neural Activity Propagate by Endogenous Electrical Field?". The Journal of Neuroscience. 35 (48): 15800–11. doi:10.1523/JNEUROSCI.1045-15.2015. PMC 4666910. PMID 26631463. electric fields can be solely responsible for spike propagation at ... This phenomenon could be important to explain the slow propagation of epileptic activity and other normal propagations at similar speeds.
  49. "Current Guidelines For Management Of Seizures In The Emergency Department" (PDF). Archived from the original on 30 December 2010.
  50. Simon D. Shorvon (2004). The treatment of epilepsy (2nd ed.). Malden, Mass.: Blackwell Pub. ISBN 978-0-632-06046-7. Archived from the original on 6 May 2016.
  51. Peeters, SY; Hoek, AE; Mollink, SM; Huff, JS (April 2014). "Syncope: risk stratification and clinical decision making". Emergency Medicine Practice. 16 (4): 1–22, quiz 22–3. PMID 25105200.
  52. Brigo, Francesco; Nardone, Raffaele; Bongiovanni, Luigi Giuseppe (1 October 2012). "Value of tongue biting in the differential diagnosis between epileptic seizures and syncope". Seizure. 21 (8): 568–572. doi:10.1016/j.seizure.2012.06.005. ISSN 1059-1311. PMID 22770819.
  53. National Institute for Health and Clinical Excellence (January 2012). "4" (PDF). The Epilepsies: The diagnosis and management of the epilepsies in adults and children in primary and secondary care. National Clinical Guideline Centre. pp. 57–83.
  54. Luef, G (October 2010). "Hormonal alterations following seizures". Epilepsy & Behavior. 19 (2): 131–3. doi:10.1016/j.yebeh.2010.06.026. PMID 20696621.
  55. Ahmad S, Beckett MW (2004). "Value of serum prolactin in the management of syncope". Emergency Medicine Journal. 21 (2): 3e–3. doi:10.1136/emj.2003.008870. PMC 1726305. PMID 14988379.
  56. Shukla G, Bhatia M, Vivekanandhan S, et al. (2004). "Serum prolactin levels for differentiation of nonepileptic versus true seizures: limited utility". Epilepsy & Behavior. 5 (4): 517–21. doi:10.1016/j.yebeh.2004.03.004. PMID 15256189.
  57. Chen DK, So YT, Fisher RS (2005). "Use of serum prolactin in diagnosing epileptic seizures: report of the Therapeutics and Technology Assessment Subcommittee of the American Academy of Neurology". Neurology. 65 (5): 668–75. doi:10.1212/01.wnl.0000178391.96957.d0. PMID 16157897.
  58. Passman R, Horvath G, Thomas J, et al. (2003). "Clinical spectrum and prevalence of neurologic events provoked by tilt table testing" (PDF). Arch. Intern. Med. 163 (16): 1945–8. doi:10.1001/archinte.163.16.1945. PMID 12963568.
  59. Weston, J; Greenhalgh, J; Marson, AG (4 March 2015). "Antiepileptic drugs as prophylaxis for post-craniotomy seizures". The Cochrane Database of Systematic Reviews (3): CD007286. doi:10.1002/14651858.CD007286.pub3. PMID 25738821.
  60. Offringa, Martin; Newton, Richard; Cozijnsen, Martinus A.; Nevitt, Sarah J. (2017). "Prophylactic drug management for febrile seizures in children". The Cochrane Database of Systematic Reviews. 2: CD003031. doi:10.1002/14651858.CD003031.pub3. ISSN 1469-493X. PMC 6464693. PMID 28225210.
  61. Weston, Jennifer; Greenhalgh, Janette; Marson, Anthony G. (4 March 2015). "Antiepileptic drugs as prophylaxis for post-craniotomy seizures". The Cochrane Database of Systematic Reviews (3): CD007286. doi:10.1002/14651858.CD007286.pub3. ISSN 1469-493X. PMID 25738821.
  62. Ratilal, BO; Pappamikail, L; Costa, J; Sampaio, C (6 June 2013). "Anticonvulsants for preventing seizures in patients with chronic subdural haematoma". The Cochrane Database of Systematic Reviews. 6 (6): CD004893. doi:10.1002/14651858.CD004893.pub3. PMID 23744552.
  63. Sykes, L; Wood, E; Kwan, J (24 January 2014). "Antiepileptic drugs for the primary and secondary prevention of seizures after stroke". The Cochrane Database of Systematic Reviews (1): CD005398. doi:10.1002/14651858.CD005398.pub3. hdl:10722/194712. PMID 24464793.
  64. Price, Michelle; Günther, Albrecht; Kwan, Joseph S. K. (21 April 2016). "Antiepileptic drugs for the primary and secondary prevention of seizures after intracranial venous thrombosis". The Cochrane Database of Systematic Reviews. 4: CD005501. doi:10.1002/14651858.CD005501.pub4. hdl:10722/226344. ISSN 1469-493X. PMID 27098266.
  65. Marigold, R; Günther, A; Tiwari, D; Kwan, J (5 June 2013). "Antiepileptic drugs for the primary and secondary prevention of seizures after subarachnoid haemorrhage". The Cochrane Database of Systematic Reviews. 6 (6): CD008710. doi:10.1002/14651858.CD008710.pub2. hdl:10722/194540. PMID 23740537.
  66. Al-Mufti, F; Claassen, J (October 2014). "Neurocritical care: status epilepticus review". Critical Care Clinics. 30 (4): 751–64. doi:10.1016/j.ccc.2014.06.006. PMID 25257739.
  67. O’connor, Anahad (22 April 2008). "The Claim: During a Seizure, You Can Swallow Your Tongue". The New York Times. Archived from the original on 6 March 2017.
  68. Betjemann, John (23 November 2015). "Current Trends in Treatment of Status Epilepticus and Refractory Status Epilepticus". Seminars in Neurology. 35 (6): 621–628. doi:10.1055/s-0035-1564304. ISSN 0271-8235. PMID 26595862.
  69. De Waele, Liesbeth; Boon, Paul; Ceulemans, Berten; Dan, Bernard; Jansen, Anna; Legros, Benjamin; Leroy, Patricia; Delmelle, Francoise; Ossemann, Michel (10 September 2013). "First line management of prolonged convulsive seizures in children and adults: good practice points". Acta Neurologica Belgica. 113 (4): 375–380. doi:10.1007/s13760-013-0247-x. hdl:1854/LU-4182539. ISSN 0300-9009. PMID 24019121.
  70. Alshehri, A; Abulaban, A; Bokhari, R; Kojan, S; Alsalamah, M; Ferwana, M; Murad, MH (25 March 2017). "Intravenous versus Non-Intravenous Benzodiazepines for the Abortion of Seizures: A Systematic Review and Meta-analysis of Randomized Controlled Trials". Academic Emergency Medicine. 24 (7): 875–883. doi:10.1111/acem.13190. PMID 28342192.
  71. Marx, J. A., Hockberger, R. S., Walls, R. M., Adams, J., & Rosen, P. (Eds.). (2013). Rosen's emergency medicine: concepts and clinical practice (8th ed). Philadelphia: Mosby/Elsevier.
  72. Leone, MA; Giussani, G; Nolan, SJ; Marson, AG; Beghi, E (6 May 2016). "Immediate antiepileptic drug treatment, versus placebo, deferred, or no treatment for first unprovoked seizure". The Cochrane Database of Systematic Reviews. 5 (5): CD007144. doi:10.1002/14651858.CD007144.pub2. PMC 6478062. PMID 27150433.
  73. Sharma, AN; Hoffman, RJ (February 2011). "Toxin-related seizures". Emergency Medicine Clinics of North America. 29 (1): 125–39. doi:10.1016/j.emc.2010.08.011. PMID 21109109.
  74. Doherty, MJ; Haltiner, AM (23 January 2007). "Wag the dog: skepticism on seizure alert canines". Neurology. 68 (4): 309. CiteSeerX 10.1.1.1003.1543. doi:10.1212/01.wnl.0000252369.82956.a3. PMID 17242343.
  75. Gloss, D; Vickrey, B (5 March 2014). "Cannabinoids for epilepsy". The Cochrane Database of Systematic Reviews. 3 (3): CD009270. doi:10.1002/14651858.CD009270.pub3. PMID 24595491.
  76. Belendiuk, KA; Baldini, LL; Bonn-Miller, MO (21 April 2015). "Narrative review of the safety and efficacy of marijuana for the treatment of commonly state-approved medical and psychiatric disorders". Addiction Science & Clinical Practice. 10 (1): 10. doi:10.1186/s13722-015-0032-7. PMC 4636852. PMID 25896576.
  77. Martin, K; Jackson, CF; Levy, RG; Cooper, PN (9 February 2016). "Ketogenic diet and other dietary treatments for epilepsy". The Cochrane Database of Systematic Reviews. 2: CD001903. doi:10.1002/14651858.CD001903.pub3. PMID 26859528.
  78. Bonnett, LJ; Tudur-Smith, C; Williamson, PR; Marson, AG (7 December 2010). "Risk of recurrence after a first seizure and implications for driving: further analysis of the Multicentre study of early Epilepsy and Single Seizures". BMJ (Clinical Research Ed.). 341: c6477. doi:10.1136/bmj.c6477. PMC 2998675. PMID 21147743.
  79. Neligan, A; Hauser, WA; Sander, JW (2012). The epidemiology of the epilepsies. Handbook of Clinical Neurology. 107. pp. 113–33. doi:10.1016/B978-0-444-52898-8.00006-9. ISBN 9780444528988. PMID 22938966.; Sander JW, Shorvon SD (1996). "Epidemiology of the epilepsies". J Neurol Neurosurg Psychiatry. 61 (5): 433–43. doi:10.1136/jnnp.61.5.433. PMC 1074036. PMID 8965090.
  80. Gavvala, JR; Schuele, SU (27 December 2016). "New-Onset Seizure in Adults and Adolescents: A Review". JAMA. 316 (24): 2657–2668. doi:10.1001/jama.2016.18625. PMID 28027373.
  81. Camfield, P; Camfield, C (June 2015). "Incidence, prevalence and aetiology of seizures and epilepsy in children". Epileptic Disorders. 17 (2): 117–23. doi:10.1684/epd.2015.0736. PMID 25895502.
  82. Ba-Diop, A; Marin, B; Druet-Cabanac, M; Ngoungou, EB; Newton, CR; Preux, PM (October 2014). "Epidemiology, causes, and treatment of epilepsy in sub-Saharan Africa". The Lancet. Neurology. 13 (10): 1029–44. doi:10.1016/S1474-4422(14)70114-0. PMC 5497080. PMID 25231525.
  83. Magiorkinis, Emmanouil; Sidiropoulou, Kalliopi; Diamantis, Aristidis (January 2010). "Hallmarks in the history of epilepsy: Epilepsy in antiquity". Epilepsy & Behavior. 17 (1): 103–108. doi:10.1016/j.yebeh.2009.10.023. ISSN 1525-5050. PMID 19963440.
  84. Ali, Rohaid; Connolly, Ian D.; Feroze, Abdullah H.; Awad, Ahmed J.; Choudhri, Omar A.; Grant, Gerald A. (June 2016). "Epilepsy: A Disruptive Force in History". World Neurosurgery. 90: 685–690. doi:10.1016/j.wneu.2015.11.060. ISSN 1878-8750. PMID 26709155.
  85. Meador, Kimford J.; Loring, David W.; Flanigin, Herman F. (January 1989). "History of epilepsy surgery". Journal of Epilepsy. 2 (1): 21–25. doi:10.1016/0896-6974(89)90054-6. ISSN 0896-6974.
  86. Litt B, Echauz J (May 2002). "Prediction of epileptic seizures". Lancet Neurol. 1 (1): 22–30. doi:10.1016/S1474-4422(02)00003-0. PMID 12849542.
  87. Walker, Matthew C.; Schorge, Stephanie; Kullmann, Dimitri M.; Wykes, Robert C.; Heeroma, Joost H.; Mantoan, Laura (2013). "Gene therapy in status epilepticus". Epilepsia. 54: 43–45. doi:10.1111/epi.12275. ISSN 0013-9580. PMID 24001071.
  88. Mormann, F.; Andrzejak, R. G.; Elger, C. E.; Lehnertz, K. (1 February 2007). "Seizure prediction: the long and winding road". Brain. 130 (2): 314–333. doi:10.1093/brain/awl241. ISSN 0006-8950. PMID 17008335.
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