Differences

This shows you the differences between two versions of the page.

--- content:neonatal_seizures [2020/02/23 12:52] – [Prognosis] icna
+++ content:neonatal_seizures [2020/02/23 15:39] – [Neonatal seizures] icna
@@ Line 3: / Line 3: @@
   * Neonatal epileptic seizures occur from birth to the end of the neonatal period.
   * The neonatal period is defined as the first 28 days of life of a full-term infant.
-  * Most neonatal seizures are acute (pro-voked, occasional, reactive) symptomatic seizures caused by an acute illness such as hypoxic–ischaemic encephalopathy, stroke or infection.
+  * Most neonatal seizures are acute symptomatic seizures caused by an acute illness such as hypoxic–ischaemic encephalopathy, stroke or infection.
   * seizures are the most common and important sign of acute neonatal encephalopathy
   * neonatal seizures are a major risk for death or subsequent neurological disability and, by themselves, may contribute to an adverse neuro-developmental outcome.
@@ Line 55: / Line 55: @@
-==== Duration ====
+The duration of neonatal seizures is usually brief (10 s to 1–2 min) and repetitive with a median of 8 min in between each seizure. Longer seizures and status epilepticus develop more readily at this age, but convulsive neonatal status epilepticus is not as severe as that of older infants and children.
-  * The duration of neonatal seizures is usually brief (10 s to 1–2 min) and repetitive with a median of 8 min in between each seizure
-  * Longer seizures and status epilepticus develop more readily at this age, but convulsive neonatal status epilepticus is not as severe as that of older infants and children.
 ==== Non-epileptic neonatal seizures ====
@@ Line 138: / Line 135: @@
   * ‘decoupling response’ - commonly seen after starting AEDs where AEDs may suppress the clinical manifestations of seizures but not the EEG ictal discharge
   * may arise from foci not consistently echoed by surface electrodes[(:cite:1764139>{{pubmed>1764139}})]
+==== Differential diagnosis ====
+  * [[hyperekplexia]]
+  * [[benign neonatal sleep myoclonus]]
+  * [[Benign Non-Epileptic Myoclonus of Early Infancy]] ([[benign non-epileptic infantile spasms]])
+    * paroxysmal, non-epileptic movement disorder of otherwise healthy infants who have normal EEG and development[(:cite:889296>{{pubmed>889296}})][(:cite:889296>{{pubmed>889296}})][(:cite:10937134>{{pubmed>10937134}})][(:cite:11292215>{{pubmed>11292215}})]
+    * ‘benign non-epileptic infantile spasms’ is descriptively more accurate than myoclonus[(:cite:3960282>{{pubmed>3960282}})]
+    * thought to be the same condition as ‘shuddering attacks’[(:cite:11118798>{{pubmed>11118798}})].
 ==== Prognosis ====
   * depends on the underlying cause[(:cite:panayitopoulos2005>Panayiotopoulos CP. (2005). **The Epilepsies: Seizures, Syndromes and Management**. Oxfordshire (UK): Bladon Medical Publishing)]
@@ Line 158: / Line 161: @@
     * EEG persistence of immature patterns
     * Frequent or prolonged clonic seizures and clonic status epilepticus
+==== Management ====
+=== Investigations ===
+  * Neuroimaging
+    * CT, MRI, Cranial USS
+  * EEG
+  * Blood tests
+  * CSF studies
+=== Treatment ===
+{{page>template:sectionupdate}}
+There is limited evidence regarding the best pharmacologic treatment for neonatal seizures. World Health Organisation recommends electrographic seizures should be treated in the same way as clinical seizures[(:cite:who2011>World Health Organisation . Guidelines on neonatal seizures. Geneva: World Health Organisation; 2011)].
+  * **phenobarbital**
+    * often recommended as first-line treatment[(:cite:16777818>{{pubmed>16777818}})]
+    * recommended as first line treatment in the UK[(:cite:25824891>{{pubmed>25824891}})]
+    * included in RCTs of first-line treatment of neonatal seizure
+    * most studied anti-epileptic medication in animals
+    * historical precedence as the first-line antiepileptic drug for neonates
+    * extremely limited evidence on the effect of phenobarbital on long-term neonatal neurodevelopment
+    * U.S. Food and Drug Administration (FDA) has never approved phenobarbital for use in any patient population[(:cite:17342837>{{pubmed>17342837}})]
+    * animal studies have raised concerns that neonatal phenobarbital exposure induces neuronal apoptosis, disruption of synaptic development in the striatum, and other behavioral deficits[(:cite:29315524>{{pubmed>29315524}})]
+  * **Levetiracetam**
+    * effective as second-line treatments for neonatal seizures that are unresponsive to phenobarbital
+    * FDA-approved for children as young as one-month of age[(:cite:fda>U.S. Dept. of Health and Human Services. [cited 2012 Oct 5];Food and Drug Administration Center for Drug Evaluation and Research. Application Number NDA 21505/S-026 [Internet] Available from: http://www.accessdata.fda.gov)]
+    *  efficacy and safety profile has not been adequately studied in term or preterm neonates within the first month of life
+    * current literature suggests loading doses of 10 to 20 mg/kg are appropriate and effective in neonates, with a maintenance dose range of 10 to 80 mg/kg/day divided twice daily[(:cite:25964725>{{pubmed>25964725}})]
+    * dosing of 40–50mg/kg bolus has also been suggested [(:cite:21397167>{{pubmed>21397167}})]
+    * a recent open labelled RCT (Level III neonatal unit; 100 neonates) used Levetiracetam (20 mg/kg) or Phenobarbitone (20 mg/kg) intravenously and concluded that Levetiracetam achieves better control than Phenobarbitone for neonatal clinical seizures when used as first-line antiepileptic drug, and is not associated with adverse drug reactions[(:cite:31477643>{{pubmed>31477643}})]
+  * phenytoin/fosphenytoin
+    * effective as second-line treatments for neonatal seizures that are unresponsive to phenobarbital
+    * requires frequent blood-level monitoring
+    * erratic oral absorption & needs 6-8hrly oral dosing
+  * **lidocaine**
+    * effective as second-line treatments for neonatal seizures that are unresponsive to phenobarbital.
+    * narrow therapeutic window and the potential to cause cardiac arrhythmias or hypotension
+    * can induce seizures at high doses
+    * may be considered in status epilepticus if phenytoin was no previously given
+  * Benzodiazepines (midazolam)
+    * sedation is a serious side effect
+    * may be considered as a second- or third-line therapy choice, especially in already intubated neonates
+Other considerations
+  * consider pyridoxine challenge when other antiepileptics provide no response
+  * minimal data for many antiepileptics including topiramate, which is being increasingly used in neonates
+  * steroids and / or [[vigabatrin]] are considered in epileptic spasms
+  * Low-dose carbamazepine (CBZ) should be considered as first-line treatment for benign familial neonatal epilepsy (BNFE), even in cases of status epilepticus[(:cite:27888506>{{pubmed>27888506}})]
+  * there is equipoise on levetiracetam vs phenobarbitone as first line treatment[(:cite:31992265>{{pubmed>31992265}})]
+  * The 2011 World Health Organization (WHO) guidelines for neonatal seizures[(:cite:who2011)] and the 2010 Queensland Maternity and Neonatal Clinical Guidelines for neonatal seizures[(:cite:queensland2013>Queensland Department of Health. Queensland Clinical guidelines. Translating evidence into best clinical practice: maternity clinical guidelines. http://www.health.qld.gov.au/qcg/html/publications.asp#Neonatal. Accessed March 10, 2013)] recommend phenobarbital as the first-line agent for treatment of neonatal seizures, followed by phenytoin, and then benzodiazepines
 ===== References =====
 ~~REFNOTES cite~~