Lecture 29; Epilepsy

Question 1

What essentially is epilepsy?

Answer 1

An imbalance between excitation and inhibition

Very simplistic overview.

Question 2

What is the hallmark characteristic of epilepsy?

Answer 2

Abnormal, excessive electrical discharge from neurones (hypersynchronized discharge from the brain)

Often associated with Loss of Consciousness

But

Does not always produce Loss of Consciousness

Not all Loss of Consciousness due to epilepsy (people who faint can jerk a bit)

Question 3

What is epilepsy a symptom of?

Answer 3

Epilepsy is a symptom of brain dysfunction

Question 4

What are the possible causes of epilepsy?

Answer 4

Syndrome with many possible causes;
structural
genetic
metabolic / functional

Question 5

Define why epileptic seizures occur

Answer 5

Seizures occur as a result of abnormal synchronous activation of large numbers of hyperexcitableneurons which are connected in networks

Question 6

What pathways typically are seizure forming?

epiltogenesis

Answer 6

Seizures may be propagated via both normal and abnormal pathways

Seizures spread through synaptic and non synaptic pathways
- gap junctions (Bipasses synapses)

Everyone has neuronal circuitry that can generate seizures(ECT, Drugs)

Question 7

How many people have epilepsy and how does this differ from epilepsy?

Answer 7

0.5 –1 % of the population has epilepsy.

1 in 20 people will have a seizure at some time in their life.

Epilepsy is as a tendency to recurrent seizures.

Question 8

What are the two broad categories of electroclinical seizures?

Answer 8

Focal and Generalised

Question 9

Define focal seizures;

Answer 9

Focal

partial part of the brain

manifestations depend on which part of brain involved

Question 10

Describe generalised seizures;

Answer 10

generalised

Networks involving extensive regions of both hemispheres

Manifestations vary greatly

Question 11

What is the main functional test for seizures?

Answer 11

EEG

Question 12

What is EEG and what does it show?

Answer 12

An EEG is a 30 minute recording from 21 electrodes placed in standard positions on the scalp.

A single EEG will show epileptiform activity in 29-70% of patients with proven epilepsy.

Sensitivity improved by recordings during sleep.

Incidental epileptiform abnormalities are found in 0.5% of healthy young adults

Question 13

What does EEG identify?

Answer 13

EEG is important in identifying the seizure type and hence the correct seizure syndrome for an individual patient

Question 14

Describe what types of conscious focal seizures there are?

Answer 14

Consciousness may be preserved (Simple Partial)

Focal motor
Visual
Somatosensory
Auditory
Psychic

Question 15

What may lead to an impaired consciousness seizure?

Answer 15

Consciousness may be impaired

Complex partial - (aka) Dyscognitive

Patient is unresponsive with subsequent amnesia

Question 16

What sorts of brain lesions can be associated with focal seizures?

Answer 16

Cavernous Angionma

Focal Cortical Dysplasia

Hippocampal Sclerosis

Subependymall Hetrotopia

Question 17

What does GABA transmission do and what drugs allosterically bind to it / treat epilepsy?

Answer 17

x2 GABA bind - Cl in hyperpolarises

Allosteric binding sites for Benzodiazepines and Barbiturates (antiepileptic drugs)

Question 18

Are ion channels permanent?

Answer 18

No, they are all very plastic.

Ion channels demonstrate frequency dependent changes in synaptic efficiency

Excitatory synapses are potentiated when fire repetitively Inhibitory synapses decrease in efficacy when fire repetitively

NMDA LTP may be involved in long term chronic seizures.

Question 19

What does mutations in K channels lead to?

Answer 19

Mutations in voltage gated K channels

Benign familial neonatal epilepsy (children grow out of them)

2 different K channel mutations

Question 20

What can mutations in Na channels lead to?

Answer 20

Severe Myoclonic Epilepsy of Infancy (Dravet’sSyndrome) SCN1A

Benign familial Neonatal Epilepsy SCN2A

Generalised Epilepsy with Febrile Seizures plusSCN1A SCN1B SCN2A

Early onset absence seizures SCN1B

Genotype doesnt have consistent phenotype.

Question 21

What causes absence epilepsy?

Answer 21

Absence seizures and Ca++ channelsAbsence seizures due to abnormal activation of T-type calcium channels in the thalamus

Hyperpolarisation of thalamic relay neurones produces synchronous depolarisation of the cortex via excitatory neurones

GAERS rats –mutations of T-type calcium channel

Question 22

What are the possible mutations in ligand gated ion channels?

Answer 22

AutosomalDominant Nocturnal Frontal Lobe Epilepsy Mutation of Nicotinic AChreceptor

Generalised Epilepsy with Febrile Seizures plus Mutation of GABAa receptor

Angelman’s syndrome
- Deletion of part of Chr15 -contains genes for several GABAareceptor subunits

Question 23

What does surgery on epileptics show?

Answer 23

Surgically resected temporal lobe specimens show changes in the ratio and function of Na channels

Question 24

What do epileptic animal models show in terms of changes in brain structure?

Answer 24

Overexpression of low threshold Ca currents in thalamic neurones in rats produces model of human absence epilepsydensity, distribution, molecular structure and function of ion channels is altered after seizures

Question 25

What can induce seizures?

Answer 25

Blocking Gaba a receptors
Activating glutamate receptors
Blocking some K channels

Question 26

What drugs block GABAa receptors?

Answer 26

Blockade of GABAa receptors

bicuculline(competitive antagonist)

picrotoxin(non-competitive antagonist),

penicillin –enters open GABA channels and occludes them

Question 27

What activates glutmate receptors? causing siezures

Answer 27

kainate, domoicacid unblocking of NMDA receptors by low Mg2+

Question 28

What antiepileptic drugs target Na channels?

Answer 28

Na+ channel blockers –presynaptic

Prevent sustained repetitive firing from extended depolarisation

i.e
carbamazepin
ephenytoin
lamotrigin
esodium valproate

Question 29

What drugs enhance GABA transmission?

Answer 29

vigabatrin
tiagabine
sodium valproat
ebenzodiazepines  (diazepam, lorazepam)
barbiturates  (phenobarbitone)
topirimate

Question 30

What drugs act on Ca channels?

Answer 30

Ethosuxamide

Sodium valproate

Question 31

What drugs block glutamate?

Answer 31

Topirimate
Lamotrigine
Felbamate
Perampanel (AMPA receptors)

Question 32

What are some autoantibody induced epileptic syndromes

?

Answer 32

Anti-voltage gated potassium channels (LGI1):

Anti-NMDA receptor

Question 33

What results from Anti-voltage gated potassium channels (LGI1):?

Answer 33

Limbic encephalitis, (prominent amnesia)Focal (dyscognitive) seizures –complex partial seizuresFacio-brachial dystonicseizuresHyponatraemi

Question 34

What results from anti-NMDA receptor antibodies?

Answer 34

Psychiatric features

DyskinesiasFocal (dyscognitive) seizures –complex partial seizures

Question 35

What are the effects of seizures?

Answer 35

Kindling (theory)

Repetitive exposure to (initially) subthreshold electrical stimulation eventually produces spontaneous seizures

Theory that seizures may beget seizures

Question 36

How do seizures affect the neuronal circuits?

Answer 36

Anatomic rearrangements of local circuits

Excitatory axons have collateral branches feedback inhibition and / or excitationusually inhibition more powerful

With neuronal death, there is sprouting of unlesioned axons occurs to fill in dendritic regions

Question 37

How do seizures affect the dengate gyrus?

Answer 37

Mossy fibres of granule cells in dentate gyrusinnervate pyramidal cells of CA3 region (inappropriate)

When granule cells die, surviving neurons develop collaterals that form new connections

Form recurrent excitatory connections - alter normal balance between feedback inhibition and excitation

Question 38

What did they find in sprouting in epilepsy associated with?

Answer 38

Degree of sprouting correlates with number of evoked seizures

Sprouting may occur even in the absence of overt cell death