Mer Scott
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PHCY320 (Neurology) Quiz on NE3 Epilepsy, created by Mer Scott on 09/10/2019.

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NE3 Epilepsy

Question 1 of 14

1

Epilepsy, the most common neurological disorder, is a brain disorder leading to recurring seizures.
A seizure is a sudden abnormal and excessive of neurons. It affects 1-2% of the population. 1/3 of epilepsy is . It can also be caused by: Brain injury, tumour, stroke, infections (), other brain disorders (Autism spectrum, dementia)
Challenges: Depression, disorders, ADHD, sleep, falls, issues, osteoporosis, risk of death.
Diagnosis involves .

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    4th
    firing
    genetic
    meningitis, encephalitis
    mood
    reproductive
    EEG and MRI

Explanation

Question 2 of 14

1

Types of epilepsy:
Note - Site of discharge and extent of spread affects symptoms.

(consciousness not affected) or (consciousness affected)
(begins and remains local) or (whole brain inc. reticular system)
Generalised can be classesd as: Absence, Myoclonic, Clonic, Tonic-clonic (very bad)

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    Simple
    Complex
    Focal
    Generalised

Explanation

Question 3 of 14

1

Neural mechanisms are poorly understood.
Epileptogenesis:
• Facilitation of neurotransmission
• Reduced transmission
• Abnormal of cells
Repeated epileptic causes cell death ()... this is brain damage.

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    excitatory
    inhibitory
    electrical properties
    excitotoxicity
    discharge

Explanation

Question 4 of 14

1

Which of these is NOT a drug that lowers seizure threshold?

Select one of the following:

  • Tramadol

  • Lithium

  • Antidepressants

  • Antipsychotics

  • Macrolides

Explanation

Question 5 of 14

1

Antiepileptic drug action is effective in 70-80% of patients.
Three main mechanisms:
• Inhibition of function
• Enhancement of action
• Inhibition of channel function (T type)

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    Na+ channel
    GABA
    Ca2+

Explanation

Question 6 of 14

1

Moa: Inhibition of sodium channels.
Affect membrane excitability. Inhibit high neuronal firing through their action on Na+ channels.

1. Phenytoin
seizures (not absence and myoclonic). kinetics – acute toxicity. > bound to plasma proteins. Hepatic metabolism CYP1A2 and 3A4. Toxicity signs: (uncontrolled eye movements), (double vision), slurred , ataxia, confusion, hyperglycaemia. Unwanted effects: GI, drowsiness, tremor, dizziness, headache,

2. Carbamazepine
Widely used: , only. Substrate and autoinducer of CYP3A4. half-life (3-5 wks, OK). Decreases , increases . Adverse effects are related and dose limiting: headache, N&V, ataxia, drowsiness, blurred vision,

3. Sodium Valproate
All forms of epilepsy. Chemically to other antiepileptics. Increases content, weak + block. Interactions: AEDs(), antidepressants, antimalarials, antipsychotics, carbapenems. Unwanted Effects: GI irritation, thrombocytopenia, transient , liver toxicity and pancreatitis.

4. Lamotrigine
Focal seizures, generalised tonic-clonic, . Valproate will its concentration. Carbamazepine and phenytoin will its concentration. SEs: Nausea, dizziness, ataxia, (serious) skin reactions

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    frequency
    Tonic-clonic and focal
    focal and generalised TC
    absence, Lennox-Gastaut syndrome
    Non-linear
    90%
    Nystagmus
    diplopia
    speech
    gingival hypertrophy, hirsuitism, acne.
    Variable
    warfarin
    erythromycin
    dose
    hyponatraemia.
    unrelated
    GABA
    Na
    hair loss
    increase
    decrease
    anti-epileptic drugs

Explanation

Question 7 of 14

1

Which two sodium channel inhibitors can never be used in pregnancy?

Select one of the following:

  • Carbamazepine, Valproate

  • Phenytoin, Lamotrigine

  • Carbamazepine, Lamotrigine

  • Phenytoin, Valproate

Explanation

Question 8 of 14

1

MoA: Enhancement of GABA.

1. Clobazam, clonazepam - Enhances , facilitates Cl- channel ( threshold for AP)

2. Tiagabin - .
• Confusion, difficulty , mild , paraesthesia
Overdose: lethargy,

3. Vigabatrin - . (GABA transaminase inhibitor.)
• 1/3 experience field disturbances
adverse effects

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    activation of GABA(A) R
    opening
    inhibits GABA uptake
    prevents GABA breakdown
    speaking
    sedation
    respiratory depression, tachycardia
    visual
    behavioural
    raise

Explanation

Question 9 of 14

1

MoA: Inhibition of calcium channels.

1. Ethosuximide
• Specific block of T type Calcium channels (thalamic relay)
seizures
• Side Effects: dizziness, hypersensitivity (rarely)

2. Gabapentin (Pregabalin)
• T type calcium channels ( voltage activated)

Relatively SE free: . Abuse/addiction/safety risks.

3. Levetiracetam
w/wo generalisation; prophylaxis post
• Binds to a , SV2A
• Inhibits calcium channels ( type)
• No CYP450 interactions
• 100% oral bioavailability
Side Effects: ataxia, dizziness, headache, tremor, behavioural disturbances, GI,

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    Absence
    Nausea, anorexia, lethargy,
    Low
    Adjunct
    sedation, ataxia
    Focal
    neurosurgery
    synaptic vesicle glycoprotein
    presynaptic
    N
    suicidal ideation

Explanation

Question 10 of 14

1

Drag the drug to match the interactions and unwanted side effects. (Assessable Task...)

1.
UE: GI, drowsiness, tremor, dizziness, headache, gingival hypertrophy, hirsuitism, acne
Interactions: MANY including amiodarone, trimethoprim, SSRIs, TCAs, MAOIs, warfarin

2.
UE: • headache, N&V, ataxia, drowsiness, blurred vision, hyponatraemia. blood, hepatic and skin disorders.
Interactions: warfarin, clopidogrel, simvastatin, oestrogens/progesterone, erythromycin

3.
UE: GI irritation, thrombocytopenia, transient hair loss, liver toxicity and pancreatitis
Interactions: /AEDs, antidepressants, antimalarials, antipsychotics, carbapenems

4.
UE: Nausea, dizziness, ataxia, (serious) skin reactions (SJS and TEN). hypersensitivity syndrome)
Interactions: valproate, carbamazepine, phenytoin

5.
UE: Confusion, difficulty speaking, mild sedation, paraesthesia

6.
UE: Nausea, anorexia, lethargy, dizziness, hypersensitivity (rarely)

7.
UE: Sedation, ataxia

8.
UE: ataxia, dizziness, headache, tremor, behavioural disturbances, GI, suicidal ideation

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    Phenytoin
    Levetiracetam
    Gabapentin (Pregabalin)
    Ethosuximide
    Tiagabine
    Lamotrigine
    Sodium Valproate
    Carbamazepine
    Anti-epileptics

Explanation

Question 11 of 14

1

Antiepileptic hypersensitivity syndrome: , potentially fatal. Between wks exposure. lymphadenopathy. Danger of multi-organ failure.
Risk meds: Carbamazepine, lacosamide, lamotrigine, oxcarbazepine, phenobarbital, phenytoin, primidone

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    1-8
    Rare
    Fever, rash,

Explanation

Question 12 of 14

1

Treatment is initiated after the first seizure to decrease risk and time to second seizure.

Select one of the following:

  • True
  • False

Explanation

Question 13 of 14

1

Common comorbidities:
disorders (depression, anxiety)
• Cognitive disorders
• Migraine
disorders
More common in people with epilepsy:
• Cardiovascular
• Respiratory
• Inflammatory disorders
Other:
- SUDEP (Sudden unexpected death in epilepsy)
- 2-6 times greater risk of , 35% attributed to seizures

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    Sleep
    Psychiatric
    fractures

Explanation

Question 14 of 14

1

Pregnancy:
Dose adjustment needed because of clearance
Increased risk of teratogenicity - esp. trimester, > drugs. Valproate = defects, cognitive outcomes.
Breastfeeding:
Encouraged with monotherapy
Infant = sedation, feeding , weight , developmental milestones

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    increased
    first
    2
    neural tube
    monitoring
    difficulties
    gain

Explanation