Epilepsies in children, young people and adults

Ensure that people with Dravet syndrome have an adult or paediatric neurologist with expertise in epilepsy involved in their care.

Consider sodium valproate as first-line treatment for people with Dravet syndrome. Be aware that sodium valproate should be used with caution in women and girls, but it is recommended as first-line treatment for Dravet syndrome because of the severity of the syndrome and the lack of evidence for other effective first-line treatment options.

If sodium valproate first-line monotherapy is started or continued for Dravet syndrome in women and girls able to have children (including young girls who are likely to need treatment when they are old enough to have children):

• discuss the potential risks and benefits of treatment, including the risks to an unborn child

• take into account the likelihood of pregnancy and put in place a pregnancy prevention programme, if appropriate.
  
  Follow the MHRA safety advice on valproate use by women and girls.

If sodium valproate alone is unsuccessful as first-line monotherapy for Dravet syndrome, consider triple therapy with stiripentol and clobazam as first-line add-on therapy. Carefully titrate the additional drugs and review treatment frequently, including monitoring for adverse effects such as sedation.

In April 2022, these were off-label uses of clobazam as add-on therapy in children under 6 months, and stiripentol when it is started in adults over 18 years. See NICE's information on prescribing medicines.

If triple therapy is unsuccessful for Dravet syndrome and the child is over 2 years, consider cannabidiol in combination with clobazam as a second-line add-on treatment option in line with NICE's technology appraisal guidance on cannabidiol with clobazam for treating seizures associated with Dravet syndrome.

If triple therapy is unsuccessful for Dravet syndrome in a child aged under 2 years or second-line treatment is unsuccessful in a child aged over 2 years, consider 1 of the following add-on options under the supervision of a ketogenic diet team or a neurologist with expertise in epilepsy, as appropriate:

• ketogenic diet

• levetiracetam

• topiramate.
  
  If the first choice is unsuccessful, consider the other add-on options.
  
  In April 2022, these were off-label uses of levetiracetam and topiramate. See NICE's information on prescribing medicines.

If all other treatment options for Dravet syndrome are unsuccessful, consider potassium bromide under the guidance of a neurologist with expertise in epilepsy.

In April 2022, potassium bromide was not licensed for use in the UK. See NICE's information on prescribing medicines.

Be aware that the following medications may exacerbate seizures in people with Dravet syndrome:

• carbamazepine

• gabapentin

• lacosamide

• lamotrigine

• oxcarbazepine

• phenobarbital

• pregabalin

• tiagabine

• vigabatrin.
  
  NICE has produced technology appraisal guidance on fenfluramine for treating seizures associated with Dravet syndrome.

Ensure that people with Lennox–Gastaut syndrome have an adult or paediatric neurologist with expertise in epilepsy involved in their care.

Consider sodium valproate as first-line treatment for people with Lennox–Gastaut syndrome. Be aware that sodium valproate should be used with caution in women and girls, but it is recommended as first-line treatment for Lennox–Gastaut syndrome because of the severity of the syndrome and the lack of evidence for other effective first-line treatment options.

If sodium valproate treatment is started or continued for Lennox–Gastaut syndrome in women and girls able to have children (including young girls who are likely to need treatment when they are old enough to have children):

• discuss the risks and benefits of treatment, including the risks to an unborn child

• take into account the likelihood of pregnancy and put in place a pregnancy prevention programme, if appropriate.
  
  Follow the MHRA safety advice on valproate use by women and girls.

If first-line treatment is unsuccessful, consider lamotrigine as a second-line monotherapy or add-on treatment for people with Lennox–Gastaut syndrome.

In April 2022, this use of lamotrigine was off-label as monotherapy in children under 13 years and add-on therapy for children under 2 years. See NICE's information on prescribing medicines.

If second-line treatment is unsuccessful, consider the following as third-line add-on treatment options for people with Lennox–Gastaut syndrome:

• cannabidiol in combination with clobazam if the child is over 2 years, in line with NICE's technology appraisal guidance on cannabidiol with clobazam for treating seizures associated with Lennox–Gastaut syndrome

• clobazam

• rufinamide

• topiramate.
  
  In April 2022, these were off-label uses of clobazam as add-on therapy in children under 6 months, rufinamide in children under 1 year, and topiramate in children under 2 years. See NICE's information on prescribing medicines.

When starting an add-on treatment in people with Lennox–Gastaut syndrome, carefully titrate the additional medicine and review treatment frequently, including monitoring for adverse effects such as sedation.

If seizures continue with third-line treatments for Lennox–Gastaut syndrome, consider a ketogenic diet as an add-on treatment under the supervision of a ketogenic diet team.

If all other treatment options for Lennox–Gastaut syndrome are unsuccessful, consider felbamate as add-on treatment under the supervision of a neurologist with expertise in epilepsy.

In April 2022, felbamate was not licensed for use in the UK. See NICE's information on prescribing medicines.

Be aware that the following medications may exacerbate seizures in people with Lennox–Gastaut syndrome:

• carbamazepine

• gabapentin

• lacosamide

• lamotrigine

• oxcarbazepine

• phenobarbital

• pregabalin

• tiagabine

• vigabatrin.

If a child under 2 years has suspected or confirmed infantile spasms, within 24 hours seek guidance from, and refer the child urgently to, a tertiary paediatric neurologist to ensure rapid assessment, including a sleep electroencephalogram (EEG), and rapid treatment to stop spasms.

Review children under 2 years with infantile spasms at least weekly during treatment and repeat sleep EEG at 2 weeks after starting treatment.

When infantile spasms have stopped, review children monthly and repeat sleep EEG if spasms recur or there are clinical concerns.

Offer combination therapy with high-dose oral prednisolone and vigabatrin as first-line treatment for infantile spasms that are not due to tuberous sclerosis, unless the child is at high risk of steroid-related side effects.

In April 2022, this was an off-label use of vigabatrin in combination with prednisolone. See NICE's information on prescribing medicines.

Consider vigabatrin alone as first-line treatment for infantile spasms in children at high risk of steroid-related side effects.

Offer vigabatrin alone as first-line treatment for infantile spasms due to tuberous sclerosis. If vigabatrin is ineffective after 1 week, add high-dose oral prednisolone.

In April 2022, this was an off-label use of vigabatrin in combination with prednisolone. See NICE's information on prescribing medicines.

Before starting oral prednisolone for infantile spasms:

• discuss the possible side effects of steroid treatment with parents and carers

• test whether the child has antibodies to the varicella zoster virus

• give the parents and carers a steroid card and information about when to seek medical help for side effects.

When using oral prednisolone to treat infantile spasms, follow the advice in the BNF for children on prednisolone dosages. Monitor blood pressure and urinary glucose weekly during treatment.

See recommendations on managing glucocorticoid withdrawal in NICE's guideline on adrenal insufficiency.

When using vigabatrin to treat infantile spasms, increase the dose as outlined in the BNF for children on vigabatrin. Discuss further dose increases with a tertiary paediatric neurologist if the spasms do not stop (clinically and on EEG).

If first-line treatment for infantile spasms is unsuccessful, discuss further treatment with a tertiary paediatric epilepsy specialist.

Consider the following as a second-line monotherapy or add-on treatment options for infantile spasms, guided by a ketogenic diet team or tertiary paediatric epilepsy specialist, as appropriate:

• ketogenic diet

• levetiracetam

• nitrazepam

• sodium valproate

• topiramate.
  
  If the first choice is unsuccessful, consider the other second-line options.
  
  In April 2022, these were off-label uses of levetiracetam, nitrazepam and topiramate. See NICE's information on prescribing medicines.

Discuss with children and young people with self-limited epilepsy with centrotemporal spikes, and their families or carers as appropriate, whether they wish to start treatment. In particular, discuss:

• frequency and severity of seizures

• possible hazards of ongoing seizures (including the small risk of death)

• possible side effects of treatment.

Consider lamotrigine or levetiracetam as first-line treatment for self-limited epilepsy with centrotemporal spikes. If either lamotrigine or levetiracetam is unsuccessful, try the other of these options.

In April 2022, these were off-label uses of lamotrigine in children under 13 years, and levetiracetam in children under 16 years. See NICE's information on prescribing medicines.

If first-line treatments for self-limited epilepsy with centrotemporal spikes are unsuccessful, consider the following as second-line monotherapy treatment options:

• carbamazepine

• oxcarbazepine

• zonisamide.
  
  If the first choice is unsuccessful, consider the other second-line monotherapy options.
  
  In April 2022, these were off-label uses for oxcarbazepine in children under 6 years, and zonisamide in adults and children. See NICE's information on prescribing medicines.

If second-line treatments tried are unsuccessful for self-limited epilepsy with centrotemporal spikes, consider sulthiame as monotherapy or add-on treatment, but only after discussion with a tertiary paediatric neurologist.

In April 2022, sulthiame was not licensed for use in the UK. See NICE's information on prescribing medicines.

Be aware that carbamazepine, oxcarbazepine and lamotrigine may rarely exacerbate seizures or the development of another epilepsy syndrome, or affect cognitive performance, in a small number of children and young people with self-limited epilepsy with centrotemporal spikes.

If there is concern about the school performance of a child or young person having antiseizure medication, seek guidance from an epilepsy specialist and consider:

• sleep electroencephalogram (EEG) to exclude exacerbation of epileptic activity (electrical status epilepticus during sleep) and

• neuropsychology assessment to review academic performance.

If a child or young person having antiseizure medication treatment develops other seizure types, consider a sleep EEG to exclude exacerbation of epileptic activity (developmental epileptic encephalopathy with spike-wave activation in sleep).

Offer follow up at a frequency and with a healthcare professional appropriate to the child or young person's individual needs. Discuss discontinuing treatment if a child or young person with self-limited epilepsy with centrotemporal spikes is seizure-free for at least 2 years or at age 14 years.

Discuss the treatment and management of epilepsy with myoclonic-atonic seizures in children with a tertiary paediatric neurologist.

Consider levetiracetam or sodium valproate as first-line treatments for epilepsy with myoclonic-atonic seizures. If either levetiracetam or sodium valproate is unsuccessful, try the other of these options.

In April 2022, this was an off-label use of levetiracetam. See NICE's information on prescribing medicines.

If sodium valproate is started or continued for epilepsy with myoclonic-atonic seizures in girls or women able to have children (including young girls who are likely to need treatment when they are old enough to have children):

• discuss the risks and benefits of treatment, including the risks to an unborn child

• take into account the likelihood of pregnancy and put in place a pregnancy prevention programme, if appropriate.
  
  Follow the MHRA safety advice on valproate use by women and girls.

If first-line treatments for epilepsy with myoclonic-atonic seizures are unsuccessful, consider a ketogenic diet as a second-line monotherapy or add-on treatment, under the supervision of a ketogenic diet team.

If second-line treatment for epilepsy with myoclonic-atonic seizures is unsuccessful, consider the following as third-line monotherapy or add-on treatment options:

• clobazam

• ethosuximide

• topiramate

• zonisamide.
  
  If the first choice is unsuccessful, consider the other third-line options.
  
  In April 2022, these were off-label uses of clobazam as monotherapy in adults and children, and add-on therapy in children under 6 months, and topiramate and zonisamide in adults and children. See NICE's information on prescribing medicines.

Do not use any of the following medications because they may exacerbate seizures in people with epilepsy with myoclonic-atonic seizures:

• carbamazepine

• gabapentin

• oxcarbazepine

• phenytoin

• pregabalin

• vigabatrin.

Consider discontinuing antiseizure medication treatment in children with epilepsy with myoclonic-atonic seizures who are seizure-free for 2 years.