Epileptic seizure

Epileptic seizure
Epileptic seizure
Classification and external resources
ICD-10 G40, P90, R56
ICD-9 345.9, 780.3
DiseasesDB 19011
eMedicine neuro/694 neuro/415
MeSH D012640

An epileptic seizure, occasionally referred to as a fit, is defined as a transient symptom of "abnormal excessive or synchronous neuronal activity in the brain".[1] The outward effect can be as dramatic as a wild thrashing movement (tonic-clonic seizure) or as mild as a brief loss of awareness. It can manifest as an alteration in mental state, tonic or clonic movements, convulsions, and various other psychic symptoms (such as déjà vu or jamais vu). Sometimes it is not accompanied by convulsions but a full body "slump", where the person simply will lose control of their body and slump to the ground. The medical syndrome of recurrent, unprovoked seizures is termed epilepsy, but seizures can occur in people who do not have epilepsy.

About 4% of people will have an unprovoked seizure by the age of 80 and the chance of experiencing a second seizure is between 30% and 50%.[2][3] Treatment may reduce the chance of a second one by as much as half.[3] Most single episode seizures are managed by primary care physicians (emergency or general practitioners), whereas investigation and management of ongoing epilepsy is usually by neurologists. Difficult-to-manage epilepsy may require consultation with an epileptologist, a neurologist with an interest in epilepsy.

Contents

Classification

Clinicians organize different types of seizure according to whether the source of the seizure within the brain is localized (partial- or focal-onset seizures) or distributed (generalized seizures). Partial seizures are further divided on the extent to which consciousness is affected (simple partial seizures and complex partial seizures). If consciousness is unaffected, then it is a simple partial seizure; otherwise it is a complex partial seizure. A partial seizure may spread within the brain—a process known as secondary generalization. Generalized seizures are divided according to the effect on the body, but all involve loss of consciousness. These include absence, myoclonic, clonic, tonic, tonic–clonic, and atonic seizures. A mixed seizure is defined as the existence of both generalized and partial seizures in the same patient.[4]

Following standardization proposals published[by whom?] in 1970, outdated terms such as "petit mal", "grand mal", "Jacksonian", "psychomotor", and "temporal-lobe seizure" have fallen into disuse.

Signs and symptoms

The signs and symptoms of seizures vary depending on the type.[5] Seizures may cause involuntary changes in body movement or function, sensation, awareness, or behavior. Seizures are often associated with a sudden and involuntary contraction of a group of muscles and loss of consciousness. However, a seizure can also be as subtle as a fleeting numbness of a part of the body, a brief or long term loss of memory, visual changes, sensing/discharging of an unpleasant odor, a strange epigastric sensation, or a sensation of fear and total state of confusion. A seizure can last from a few seconds to status epilepticus, a continuous group of seizures that is often life-threatening without immediate intervention. Therefore seizures are typically classified as motor, sensory, autonomic, emotional or cognitive. After the active portion of a seizure, there is typically a period referred to as postictal before a normal level of consciousness returns.[5]

In some cases, the full onset of a seizure event is preceded by some of the sensations described above, called vertiginous epilepsy. These sensations can serve as a warning to that a generalized tonic–clonic seizure is about to occur. These warning sensations are cumulatively called an aura and are due to a focal seizure.[5]

Some patients are able to tell when a seizure is about to happen. Some symptoms experienced by the person before a seizure may include dizziness, lightheadedness, tightening of the chest, and some experience things in slow-motion just prior to the seizure. Symptoms experienced by a person during a seizure depend on where in the brain the disturbance in electrical activity occurs. Partial and frontal seizures and focal epileptic discharges tend to happen more during sleep than during wakefulness. In contrast, psychogenic nonepileptic seizures are rare between midnight and 6 a m. and never occur during sleep.[6] Generalized epilepsy but not focal epilepsy is higher in the morning probably reflecting a diurnal variation in cortical excitability.[7] A person having a tonic–clonic seizure may cry out, lose consciousness and fall to the ground, and convulse, often violently. A person having a complex partial seizure may appear confused or dazed and will not be able to respond to questions or direction. Some people have seizures that are not noticeable to others. Sometimes, the only clue that a person is having an absence seizure is rapid blinking, extreme confusion for a few seconds or sometimes into hours.[citation needed]

Causes

Unprovoked seizures are often associated with epilepsy and related seizure disorders.

Causes of provoked seizures include:

Some medications produce an increased risk of seizures and electroconvulsive therapy (ECT) deliberately sets out to induce a seizure for the treatment of major depression. Many seizures have unknown causes.

Seizures which are provoked are not associated with epilepsy, and people who experience such seizures are normally not diagnosed with epilepsy. However, the seizures described above resemble those of epilepsy both outwardly, and on EEG testing.

Seizures can occur after a subject witnesses a traumatic event. This type of seizure is known as a psychogenic non-epileptic seizure and is related to posttraumatic stress disorder.

Diagnosis

Only about 25 percent of people who have a seizure or develop status epilepticus have epilepsy.[8] It is important to distinguish primary epileptic seizures from secondary causes. Blood tests, lumbar puncture or toxicology screening can be helpful in specific circumstances suggestive of an underlying cause like alcohol or benzodiazepine withdrawal, meningitis or drug overdose, but there is insufficient evidence to support their routine use in the work-up of an adult with an apparently unprovoked first seizure.[9] A 2007 review recommends an electroencephalogram and brain imaging with CT scan or MRI scan in the work-up.[10] MRI is more sensitive in a first apparently unprovoked seizure.

Physical examination

Most patients are in a postictal state following a seizure. In this state they are drowsy and often confused. There may be signs of other injuries. A small study found that finding a bite to the side of the tongue was very helpful when present: while only a quarter of those with seizures had such a bite (sensitivity of 24%), the finding was very specific for seizures, with only 1% due to other causes (specificity of 99%).[11]

Serum prolactin level

Two meta-analyses have quantified the role of an elevated serum prolactin. The first meta-analysis found that[12]: "If a serum prolactin concentration is greater than three times the baseline when taken within one hour of syncope, then in the absence of test "modifiers":

  1. the patient is nine times more likely to have suffered a GTCS as compared with a pseudoseizure positive LR = 8.92 (95% CI (1.31 to 60.91)), SN = 0.62 (95% CI (0.40 to 0.83)), SP = 0.89 (95% CI (0.60 to 0.98))
  2. five times more likely to have suffered a GTCS as compared with non-convulsive syncope positive LR 4.60 (95% CI (1.25 to 16.90)), SN = 0.71 (95% CI (0.49 to 0.87)), SP = 0.85 (95% CI (0.55 to 0.98)). "

The second meta-analysis found:[13]

  1. "Elevated serum prolactin assay, when measured in the appropriate clinical setting at 10 to 20 minutes after a suspected event, is a useful adjunct for the differentiation of generalized tonic-clonic or complex partial seizure from psychogenic nonepileptic seizure among adults and older children (Level B)."
  2. "Serum prolactin assay does not distinguish epileptic seizures from syncope (Level B).
  3. "The use of serum PRL assay has not been established in the evaluation of status" epilepticus, repetitive seizures, and neonatal seizures (Level U)."

The serum prolactin level is less sensitive for detecting partial seizures.[14]

EEG

An isolated abnormal electrical activity recorded by an electroencephalography examination without a clinical presentation is called subclinical seizure. They can identify background epileptogenic activity, as well as help identify causes of seizures.

Determining the underlying cause

Additional diagnostic methods include CT Scanning and MRI imaging or angiography. These may show structural lesions within the brain and heart, but the majority of those with epilepsy show nothing unusual.

As seizures have a broad differential diagnosis, it is common for patients to be simultaneously investigated for cardiac and endocrine causes. Checking glucose levels, for example, is a mandatory action in the management of seizures as hypoglycemia may cause seizures, and failure to administer glucose would be harmful to the patient. Other causes typically considered are syncope and cardiac arrhythmias, and occasionally panic attacks and cataplexy. In addition, 5% of patients with a positive tilt table test may have seizure-like activity that seems to be due to cerebral hypoxia.[15] For more information, see non-epileptic seizures.

Differential

Differentiating an epileptic seizure from other conditions such as syncope can be difficult.[5] Other possible conditions that can mimic a seizure include: decerebrate posturing, psychogenic seizures, dystonia, migraine headaches, and strychnine poisoning.[5]

Management

Potentially sharp or dangerous objects should also be moved from the vicinity, 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 is a medical emergency. Caregivers may carry medicine.

Medication

The treatment of choice for someone who is actively seizing is lorazepam.[10] This may be repeated if there is no effect after 10 minutes.[10] If there is no effect after two doses, barbiturates or propofol may be used.[10] Ongoing medication is not typically needed after a first seizure and is generally only recommended after a second has occurred or those with structural lesions in the brain.[10]

Other

A seizure response dog can be trained to summon help or ensure personal safety when a seizure occurs. These are not suitable for everybody. Rarely, a dog may develop the ability to sense a seizure before it occurs.[16] Helmets may be used to provide protection of the head during a seizure.

Prognosis

In adults, after 6 months seizure free, after a first seizure the risk of a subsequent seizure in the next year is less than 20% regardless of treatment.[17] Up to 7% of seizure that present to the emergency are in status epilepticus.[10] In those with a status epilepticus mortality is between 10 and 40%.[5]

Epidemiology

About 7 per 1000 people in the United States have a seizure in a given year.[5] Rates are highest in those less than 1 year of age and greater than 55.[5]

History

Seizures were long viewed as an otherworldly condition being referred to by Hippocrates in 400B.C. as "the sacred disease".[5]

References

  1. ^ Fisher R, van Emde Boas W, Blume W, Elger C, Genton P, Lee P, Engel J (2005). "Epileptic seizures and epilepsy: definitions proposed by the International League Against Epilepsy (ILAE) and the International Bureau for Epilepsy (IBE)". Epilepsia 46 (4): 470–2. doi:10.1111/j.0013-9580.2005.66104.x. PMID 15816939. http://www.blackwell-synergy.com/doi/full/10.1111/j.0013-9580.2005.66104.x. 
  2. ^ Herman, ST. (2004). "Single Unprovoked Seizures". Curr Treat Options Neurol 6 (3): 243–255. doi:10.1007/s11940-004-0016-5. PMID 15043807. 
  3. ^ a b Hosey, MM; Tao, M (1977). "Protein kinases of rabbit and human erythrocyte membranes. Solubilization and characterization.". Biochimica et biophysica acta 482 (2): 348–57. PMID 18184. 
  4. ^ Chen LS, Mitchell WG, Horton EJ, Snead OC (April 1995). "Clinical utility of video-EEG monitoring". Pediatr. Neurol. 12 (3): 220–4. doi:10.1016/0887-8994(95)00021-7. PMID 7619188. 
  5. ^ a b c d e f g h i Shearer, Peter. "Seizures and Status Epilepticus: Diagnosis and Management in the Emergency Department". Emergency Medicine Practice. http://www.ebmedicine.net/topics.php?paction=showTopic&topic_id=77. Retrieved 2 March 2011. 
  6. ^ Bazil, CW; Walczak, TS. (1997). "Effects of sleep and sleep stage on epileptic and nonepileptic seizures". Epilepsia 38 (1): 56–62. doi:10.1111/j.1528-1157.1997.tb01077.x. PMID 9024184. 
  7. ^ Badawy, RA; MacDonell, RA; Jackson, GD; Berkovic, SF (2009). "Why do seizures in generalized epilepsy often occur in the morning?". Neurology 73 (3): 218–22. doi:10.1212/WNL.0b013e3181ae7ca6. PMID 19620610. 
  8. ^ Stasiukyniene, V.; Pilvinis, V.; Reingardiene, D.; Janauskaite, L. (2009). "[Epileptic seizures in critically ill patients]". Medicina (Kaunas) 45 (6): 501–7. PMID 19605972. 
  9. ^ Krumholz, A; Wiebe, S; Gronseth, G; Shinnar, S; Levisohn, P; Ting, T; Hopp, J; Shafer, P et al. (2007). "Practice Parameter: evaluating an apparent unprovoked first seizure in adults (an evidence-based review): report of the Quality Standards Subcommittee of the American Academy of Neurology and the American Epilepsy Society.". Neurology 69 (21): 1996–2007. doi:10.1212/01.wnl.0000285084.93652.43. PMID 18025394. 
  10. ^ a b c d e f "Current Guidelines For Management Of Seizures In The Emergency Department" (PDF). http://www.ebmedicine.net/topics.php?paction=showTopic&topic_id=212. 
  11. ^ Benbadis SR, Wolgamuth BR, Goren H, Brener S, Fouad-Tarazi F (1995). "Value of tongue biting in the diagnosis of seizures". Arch. Intern. Med. 155 (21): 2346–9. doi:10.1001/archinte.155.21.2346. PMID 7487261. 
  12. ^ Ahmad S, Beckett MW (2004). "Value of serum prolactin in the management of syncope". Emergency medicine journal : EMJ 21 (2): e3. doi:10.1136/emj.2003.008870. PMC 1726305. PMID 14988379. http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pmcentrez&artid=1726305. 
  13. ^ 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. 
  14. ^ Shukla G, Bhatia M, Vivekanandhan S, et al. (2004). "Serum prolactin levels for differentiation of nonepileptic versus true seizures: limited utility". Epilepsy & behavior : E&B 5 (4): 517–21. doi:10.1016/j.yebeh.2004.03.004. PMID 15256189. 
  15. ^ Passman R, Horvath G, Thomas J, et al. (2003). "Clinical spectrum and prevalence of neurologic events provoked by tilt table testing". Arch. Intern. Med. 163 (16): 1945–8. doi:10.1001/archinte.163.16.1945. PMID 12963568. 
  16. ^ Dalziel D, Uthman B, Mcgorray S, Reep R (2003). "Seizure-alert dogs: a review and preliminary study". Seizure 12 (2): 115–20. doi:10.1016/S105913110200225X. PMID 12566236. 
  17. ^ Bonnett, LJ; Tudur-Smith, C, Williamson, PR, Marson, AG (2010-12-07). "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. PMID 21147743. 

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