BB2 Revision5

Question 1

Which anti-epileptics should not be used in absence seizures, as they may exacerbate these types of seizures? [2]

Answer 1

Phenytoin
Carbamazepine

Question 2

Explain the DDI effect that phenytoin and carbamazepine have on other drugs [3]

Answer 2

Phenytoin and carbamazepine:
* both induce metabolizing liver enzymes.
* These liver enzymes are involved of transformation of many drugs / increased metabolism
* which may result in the loss of efficacy of other drugs (other drugs may need an increase in dose as a response)

Question 3

Explain what is meant by phenytoin’s dose dependent / zero order / saturation kinetics characteristics

Answer 3

Most drugs have first order elimination (rate of elimination is proportional to the plasma concentration).

However, with phenytoin, as the dose of drug is increased, because of saturated enzymes, the rate of elimination is no longer proportional to the concentration of drug in the plasma (i.e. there is saturation & so only a finite amount can be eliminated).

When this happens, small increases in drugs can cause large increases in plasma concentration

Question 4

Antiepileptic drugs:

Name two calcium channels that are used as anti-epileptic drugs [2]

Answer 4

Ethosuximide

Gabapentin / pregabalin (in the PBL)

Question 5

AEDs

What type of drug class does clonazepam belong to? [1]

State clonazepams MoA [1]

Answer 5

Benzodiazepines - GABA(A) receptor

positive allosteric modulators: enhance the frequency of GABA channel opening. (more GABA; causes more inhibition)

Question 6

AEDs

What type of drug class does phenobarbitone and stiripentol belong to? [1]

What is MoA? [1]

Answer 6

phenobarbitone and stiripentol:

• Drug class: Barbiturates: GABAA receptor positive allosteric modulators
• . Phenobarbitone (leads to microsomal enzyme induction)
  Enhances the duration of GABA channel opening. (more GABA; causes more inhibition

Question 7

AEDs

Which drug inhibits GABA metabolism? [1]

Answer 7

Vigabatrin

Question 8

Status elipeticus is a medical emergency. Name two drugs used to treat this conditon [2]

Answer 8

Lorezepam (IV)
Diazepam (IV)

Question 9

Alternatives to AEDs

Name 3 surgical procedures that could be used to treat epilepsy [3]

Answer 9

Lobe resection
Corpus callasotomy (reduces propogation of seizures from one cerebral hemisphere to the next)
Functional hemispherectomy

Question 10

Alternatives to AEDs

Name a type of diet that could help epilepsy [1]

Name a drug class for a potential new AED [1]

Answer 10

Keto diet

Cannabidiol

Question 11

Which of the following type of channel does pregabalin target?

Ca2+
GABA
Na+
Glutamate

Answer 11

Which of the following type of channel does pregabalin target?

Ca2+
GABA
Na+
Glutamate

Question 12

What is the MoA of Levetiracetam? [1]

Answer 12

Binds synaptic vesicle protein SV2A causing a reduction in conduction in neurones

SV2A protein is a part of secretory vesicle membranes that mediates calcium-dependent vesicular neurotransmitter release.

The binding of levetiracetam to SV2A appears to decrease the rate of vesicle release

Question 13

Name a drug that predominately blocks Na+ channels, but also acts on Ca2+ channels and causes the presynaptic inhibition of glutamate release.

Answer 13

Lamotrigine

(hint: tri gated?)

Question 14

AEDs

Focal Seizures Treatment:

First line: [] or []
Second line: [] or []

Answer 14

First line: carbamazepine or lamotrigine
Second line: sodium valproate or levetiracetam

Question 15

Management of tonic-clonic seizures is with:

First line: []
Second line: [] or []

Answer 15

Management of tonic-clonic seizures is with:

First line: sodium valproate
Second line: lamotrigine or carbamazepine

Question 16

Which drugs are used for absence seizures? [2]

Answer 16

ethosuximide, sodium valproate

Question 17

Myoclonic seizures:

First line: [1]
Other options: [3]

Answer 17

First line: sodium valproate
Other options: lamotrigine, levetiracetam or topiramate

Question 18

Describe the MoA of sodium channel active drugs like phenytoin and carbamazepine [1]

Answer 18

Stabilises Na+ channels inactivated state to decrease excitability

Question 19

Explain MoA of Sodium valproate [3]

Answer 19

Potentiates GABA receptor;
Stops breakdown of GABA
Blocks voltage gated sodium channels and T-type calcium channels

Question 20

State the veins from blue & red arrow [2]

Answer 20

Red arrow = vein of Trolard (superior anastomotic vein)
Blue arrow = vein of Labbe (inferior anastomotic vein)

Question 21

What are the two types of strokes [2] & their causes [2]

Answer 21

Ischaemic (thrombotic; embolic): 80%
Haemorrhagic stroke (trauma; spontaneous): 20%

Question 22

Name the leading causes of hemorrhagic stroke [5]

Answer 22

Major causes of hemorrhagic stroke
* Hypertension
* Aneurysm
* Elderly
* Head injury (trauma)
* Alcoholics
* Arteriovenous malformation

Question 23

What are the two leading causes of non-traumatic hemorrhagic stroke? [2]

Answer 23

HTN
Aneursym

Question 24

Describe MCA stroke if occurs on the:

• Left
• Right

Answer 24

MCA Left stroke
* Global aphasia
* Sensorimotor loss on contralateral face, upper limb and trunk

Right MCA Stroke:
* Neglect syndrome

Question 25

Which artery is effected here? [1]

Answer 25

Lenticulostriate

Question 26

Split brain syndrome

Describe how a patient with split brain syndrome would percieve & verbalise an object in their right visual field & their right hand

Describe how a patient with split brain syndrome would percieve & verbalise an object in their left visual field & their left hand

Answer 26

Human anatomy; the right hemisphere receives visual input from the left visual field and controls the left hand

Transfer of visual learning between the hemispheres is abolished

right visual field the patient responds correctly verbally and with his/her right hand.

Left visual field the patient verbally states that he/she saw nothing, and identifies the object accurately with the left hand only

Question 27

Describe the effects of PCA stroke [3]

Answer 27

• Contralateral homonymous hemianopsia (a field loss deficit in the same halves of the visual field of each eye,)
• Reading and writing deficits
• Impaired memory

Question 28

Why do TIAs commonly present with temporary blindness? [1]

Answer 28

Opthalmic artery

Question 29

Which type of intra-axial bleed causes the most mortality? [1]

Which type of veins are commonly ruptered to cause this? [1]

Answer 29

Subdural hematoma - due to bridging veins rupturing

Question 30

Which arteries are commonly affected during extradural (epidural) hematoma? [2]

Answer 30

Middle meningeal Artery(temperoparital area, pterion)

Ant. Ethmoidal A. (frontal)

Question 31

Which cranial nerve is commonly effected by extradural (epidural) hematoma [1]

What happens to visual field? [1]

What happens to feelings of extremities? [1]

Answer 31

CN III damaged

Loss of visual field opposite to lesion (compress of PCA)

Weakness of extremities on opposite side of lesion (crossed pyramid pathways)

Question 32

Describe the onset of SAH [1]

Describe pain experienced in SAH [1]

Answer 32

Rapid onset: thunderclap headache

Question 33

What are the two types of cerebral aneurysm? [2]

Answer 33

Saccular (berry is a sub-type)
Fusiform

Question 34

Which artery supplies the midbrain & thalamus? [1]

Answer 34

PCA

Question 35

What is Xanthochromia?

Which type of hematoma does it occur in? [1]

Answer 35

Xanthochromia is the presence of bilirubin in the cerebrospinal fluid and is sometimes the only sign of an acute subarachnoid hemorrhage.

Question 36

Which type of hematoma can present with blood in lumbar puncture? [1]

Answer 36

Subarachnoid hematoma
Lumbar puncture - Evidence of blood in 3% of people with normal CT

Question 37

Label A-C

Answer 37

A: ICH
B: SDH
C: SAH

Question 38

Which the following is SAH and which is ICH?

Answer 38

L: SAH
R: ICH

Question 39

Define primary and secondary headaches [2]

Answer 39

Primary headaches
Diagnosis is made on the history in the absence of physical signs

Secondary headaches
Diagnosis is made on the history in the presence of physical signs

Question 40

State the characteristics of cluster headaches:

• How long do they last? [1]
• When do they occur? [1]
• Name an immediate trigger of cluster headaches [1]

Answer 40

• Typically last 15-180 mins
• Seasonal: often last 6-8 weeks
• Alcohol is an immediate trigger

Question 41

Define cluster headaches

Answer 41

a neurological disorder characterized by recurrent severe headaches on one side of the head, typically around the eye(s).

Question 42

Name acute [2] and prophylactic [1] treatment for cluster headaches

Answer 42

Acute:
* oxygen (15L/min 100% through non-rebreather mask – acts as vasoconstrictor);
* -triptans

Prophylactic
* : has to be quick. High dose of verapamil

Question 43

Primary headaches:

Name the 3 questions need to ask for diagnosis of a migraine [need score of 2/3]

Answer 43

Light bothers you (a lot more than when you don’t have headache)

Your headaches limit your ability to work, study or do what you need to do?

You feel nauseated or sick

Question 44

Primary headaches:

What is the difference of length of migraines between episodic and chronic migraines? [2]

Answer 44

Episodic
* <15 days/month

Chronic
* Headache occurring on ≥15 or more days/month for more than three months. At least 8 days/month have the features of migraine headache

Question 45

Migraine pathophysiology

Name 4 examples that can cross migraine threshold (& cause migraine)

Answer 45

• Lack of sleep
• Lack of food
• Dehydration
• Hormonal trigger

Question 46

Describe the NT that influences migraines [1]

What urinary metabolite would be high in migraine attacks? [1]

Answer 46

Seratonin released (90% from gut, 10% platelets, 1-2% brain)

Increase urinary metabolites 5HIAA in attacks

Question 47

Describe 5 symptoms of premonitory phase of migraine

Answer 47

Food craving
Yawning
Neck pain
Heightened perception
Fluid retention

Question 48

What are the 5 stages of migraine? [5]

Answer 48

Premonitory
Aura
Heachache
Resolution
Recovery

Question 49

Describe the pathophysiology of aura of migraine

Answer 49

A transient and local suppression (depression)
…of spontaneous electrical activity in the visual cortex (cortical)
…which moves slowly across the brain (spreading)

(Note: occurs rom visual cortex not the eyes)

Question 50

Describe the trigeminovascular pathways that causes migraine

Answer 50

Increase in serotonin causes BV on the dura to vasodilate

This causes a release of neuropeptides

This begins a cascade reaction causing further inflammation: particularly release of CGRP: potent vasodilator

CGRP activate the nerve pathways & the nerves send pain signals to the trigeminal ganglion

The trigeminal ganglion, once activated by CGRP, is what causes peripheral sensitisation which is responsible for the throbbing pain in a migraine

Trigeminal ganglion transmits pain impulses to SpV (spinal trigeminal nucleus caudalis)

SpV then relays to the thalamus and from the thalamus to the cerebral cortex where pain is decoded

Question 51

Where do acute [1] and chronic [1] treatments for migraines target?

Answer 51

Acute:
Acute medication given for migraine primarily acts peripherally, at the trigeminal ganglion

Preventive medication for migraine acts more centrally (i.e. the trigeminal nucleus caudalis)

Question 52

What drug classes are used to acutely treat migraine? [3]

Answer 52

Triptans: (5HT1D/B agonists)
* Vasoconstrictive Agents

Ditans (5HT1F agonists)
* Neurally Active Anti-Migraine Agent

Gepants: small molecule CGRP receptor antagonists

Question 53

Describe the difference between peripheral and central sensitisation that occurs during migraine pathophysiology [2]

come back x

Answer 53

Peripheral sensitisation:
* Sensitization of peripheral trigeminovascular neurons in the trigeminal ganglion mediates the throbbing pain

Question 54

Name first line treatment for migraine? [1]

Answer 54

Sumatriptan

Question 55

Describe action of CGRP monoclonal antibodies (mAbs)

Answer 55

Prevent vasodilation

Question 56

Describe MoA of triptans [1]
Where are 3 possible sites of action? [3]

Answer 56

Triptans:
* 5-HT1D/B agonists.
* 3 possible sites of action: 1. cranial vasoconstriction, 2. peripheral neuronal inhibition and 3. inhibition of transmission through second order neurones of the trigeminal ganglion.

Question 57

What is the role of CGRP and when is it released? [1]

Answer 57

CGRP is a potent vasodilator released from the meninges in response to increased serotonin-induced vasodilation in the premonition phase of a headache.