AEDs Flashcards

1
Q

Know the general classification of epilepsy based on partial and generalised seizures

A

Partial/Focal –> simple (conscious)/complex (unconscious)

Generalised –> aclonic/myoclonic/tonic-clonic/absence

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2
Q

Understand the difference between primary and secondary causes of epilepsy

A

Primary - idiopathic

Secondary - vascular disease, tumours etc.

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3
Q

Describe some of the major recognised precipitants of epilepsy

A
Sensory
Brain disease/trauma
Metabolic disturbances
Infections
Therapeutics
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4
Q

Understand the broad models of how epilepsy is generated within the brain

A

Increased excitatory or decreased inhibitory –> loss of homeostatic control –> spread of neuronal hyperactivity

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5
Q

Appreciate that untreated epilepsy can be a life threatening condition

A
Physical injury
Hypoxia
SUDEP
Brain dysfunction/damage
Cognitive impairment
Psychiatric disease
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6
Q

Describe the method of action, ADRs and DDIs of carbamazepine

A

MOA - prolongs VGSC inactivation, affects own phase 1 metabolism
ADRs - dizziness, drowsy, ataxia, motor disturbances, numbness, neutropenia
DDIs - phenytoin, warfarin, COCP, antidepressants

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7
Q

Describe the method of action, ADRs and DDIs of phenytoin

A

Blocks voltage gated sodium channels
Non linear kinetics, CYP450 inducer
ADRs - CNS, gingival hyperplasia, rash, Stevens Johnsons syndrome
DDIs - valproate, NSAIDs, COCP

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8
Q

Describe the method of action, ADRs and DDIs of lamotrigine

A
Blocks voltage gated sodium channel, calcium channel blocker? Lowers glutamate? 
Linear kinetics, no CYP450 induction 
ADRs - CNS, nausea, rash
DDIs - valproate, COCP 
*safe in pregnancy
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9
Q

Describe the method of action, ADRs and DDIs of sodium valproate

A

Inhibits GABA inactivation enzymes, stimulates GABA synthesis enzymes, linear kinetics
ADRs - CNS, weight gain, liver damage
DDIs - antidepressants, antipsychotics, aspirin
*not safe in pregnancy –> causes neural tube defects, congenital malformations (therefore take folate, vitamin K)

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10
Q

Describe the method of action, ADRs and DDIs of benzodiazepine

A

Positive allosteric modulator, increases total conduction of chloride ions
ADRs - dizziness, drowsiness, withdrawal, tolerance, seizure trigger, respiratory and CNS depression
DDIs - COCP, antidepressants, antifungals carbamazepine, phenytoin

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11
Q

Describe the safety concerns of anticonvulsant therapy in pregnancy

A

Ensure anti-epileptic is not a teratogen (NOT valproate, only lamotrigine is safe)
Monitor for pre-eclampsia/eclampsia

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12
Q

Appreciate the value of therapeutic drug monitoring in phenytoin therapy

A

Phenytoin has non-linear kinetics so monitoring is very important to prevent toxicity

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13
Q

Differentiate between the terms ‘seizures’, ‘epilepsy’ and ‘status epilepticus’

A

Seizures - episodic discharge of abnormal high frequency electrical activity in the brain, clinical manifestation of abnormal and excessive excitation and synchronisation of population of cortical neurons
Epilepsy - >2 unprovoked episodes
Status Epilepticus - seizure >5 minutes or fits following one another without recovery of consciousness between them

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14
Q

Describe the dietary supplements needed during pregnancy

A
Folate - reduce risk of neural tube defects
Vitamin K (10mg/day in last trimester) - prevent coagulopathy and cerebral haemorrhage in new born
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15
Q

Describe the treatment of status epilepticus

A

Benzodiazepine (IV/PR lorazepam)
IV phenytoin
Midazolam/Pentobarbital/Propofol
–> ITU for paralysis/ventilation if failing

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