100% tevredenheidsgarantie Direct beschikbaar na betaling Zowel online als in PDF Je zit nergens aan vast
logo-home
Eerder door jou gezocht
Eerder door jou gezocht
logo
Brain Tumours Exam/Essay Summary €6,77   In winkelwagen
Snel navigeren naar
Voorbeeld
  2.  
  3. University College London (UCL)
  4.  
  5. NEUR0010 Neurobiology of Brain Injury and Disease (NEUR0010)

Samenvatting

Brain Tumours Exam/Essay Summary

1 beoordeling
 16 keer bekeken  0 keer verkocht
  • Vak
  • NEUR0010 Neurobiology of Brain Injury and Disease (NEUR0010)
  • Instelling
  • University College London (UCL)

Summary of notes structured in exam and essay format complete with point, evidence, analysis, and critical thinking. Structured based on marking criteria.

Voorbeeld 2 van de 11  pagina's

Document informatie

  • 10 oktober 2022
  • 11
  • 2022/2023
  • Samenvatting

Onderwerpen

  • brain tumours

Geschreven voor

  • University College London (UCL)
  • Onbekend
  • NEUR0010 Neurobiology of Brain Injury and Disease (NEUR0010)
Alle documenten voor dit vak (17)

1  beoordeling

review-writer-avatar

Door: sobinya21 • 4 maanden geleden

Verkoper

avatar-seller
denh11323

Ontvangen beoordelingen

Voorbeeld van de inhoud

Part 1: Introduction
Seizures are defined as individual occurrences of abnormal electrical activity in the brain. Epilepsy is a
disease characterized by the propensity to have repeated spontaneous seizures. There are two main types
of seizures, focal and generalized.




Definition of Epilepsy
 Propensity to have spontaneous seizures
o Threshold for having seizures reduced because of
 Genetic predisposition – polygenic and mendelian
 Environmental factors – brain insult
 Combination of environment and genetic predisposition
 Prevalence: 0.5-1% (600,000 in UK)
 Lifetime chance of seizure: 5%
 Lifetime incidence of epilepsy: 3%
 Considered a spectrum from genetic to acquired
o Monogenic epilepsy – due to mutations that influence the thresholds of the brain
 Many of them but they are rare (McTague et al., 2016)
o Polygenic
o Brain insult
 Incidence with age: a curve – common in childhood, then increases again in adulthood
o Children: congenital, developmental, and genetic conditions
o 20-50: alcohol and head injury
o 40-60: stroke, dementia and tumour

Epileptogenesis: the development of the state of epilepsy  sequence of events that converts the normal
brain into one that supports recurrent spontaneous seizures

Types of Seizures
1. Focal seizures
a. Originating withing networks limited to one hemisphere

, b. May be discretely localised or more widely distributed
2. Generalised seizures
a. Originating at some point within, and rapidly engaging, bilaterally distributed networks
b. Can include cortical and subcortical structures – not necessarily include the entire cortex

Basis of argument  Epilepsy and seizures are not one and the same. While seizures are just
characterised by hyperexcitability of neurons, epilepsy is a chronic disorder characterised by recurring
spontaneous seizures. Therefore, an individual can experience a single seizure while not being diagnosed
with epilepsy. Due to this, there is particular interest in understanding what facilitates the transition from
seizures to epilepsy. In order to understand this, we first need to establish the neurobiological basis of
seizures, why they occur, and how they clinically manifest. From this, we can begin to expand on the effect
of chronic, recurring seizures on the brain and what facilitates the transition from normal brain functioning to
one that supports repeated seizures.

Part 2: Neurobiology of Seizures
Scharfman, 2007
While seizures can be caused by a variety of factors and mechanisms (environmental or genetic), they all
arise via a disruption of mechanisms that maintain a balance of excitation and inhibition of neurons.
 Neurons have mechanisms by which they control or facilitate their action potential discharge – an
imbalance of this, whether it be facilitatory or inhibitory, will lead to excess excitation that leads to
seizures
 As such, disruption of mechanisms that bring neurons close to firing thresholds or inhibition of
neurons is thought to prevent seizure activity

Electrical basis of nerve cell function
https://www.ncbi.nlm.nih.gov/books/NBK2510/#!po=18.8889
 Basic mechanism of neuronal excitability is the action potential caused by membrane depolarization
through shifts in membrane potential
 This hyperexcitable state can result from increased neurotransmission, changes in voltage-gated
channels, inhibitory transmission, or a change in the intracellular and extracellular concentrations
 Resting membrane potential  ensures neurons are not constantly firing but close to threshold so
that they can discharge
o High conc of intracellular K+ and extracellular NA+  -60mV resting potential
 When this balance of ions is disrupted, it can lead to depolarization leading to aberrant excitation
and activation of neurons
o Terminals depolarize  transmitter release  neurons depolarize  AP discharge
 Seizures can lead to changes in transmembrane gradients  elevation in extracellular K+ that will
further depolarize neurons

Argument: Seizures are caused by a synchronization of neurons
 Excessive discharge alone does not directly cause a seizure. A seizure is caused by
synchronization of a network of neurons
 There are many ways that neurons can synchronize
 Circuitry Associated with Spike-Wave Discharge
o EEG manifestations of epilepsy due to highly synchronised firing between cortical and
thalamic neurons  rhythmic periods of rapid increased activity and quiescence on EEG
o Connectivity of thalamocortical networks explains alternating activity
o Thalamic neurons normally act as a conduit for information propagation into the cortex
 Excitatory projections relay sensory and other subcortical signals through the
thalamus to pyramidal neurons in multiple cortical layers for processing
 These projections are also sent to thalamic reticular nucleus (layer of GABAergic
cells in lateral thalamus)
 The thalamic reticular nucleus projects to all thalamic nuclei  also receives cortical
input
 Participates in thalamo-thalamic and cortico-thalamic negative feedback
o This negative feedback circuitry of the thalamic reticular nucleus produces the rhythmic
spike-wave discharge
 Increased firing in cortex causes increased activity via afferents into the nRT
 Results in inhibitory GABAergic firing onto other thalamic nuclei

Voordelen van het kopen van samenvattingen bij Stuvia op een rij:

√ Verzekerd van kwaliteit door reviews

√ Verzekerd van kwaliteit door reviews

Stuvia-klanten hebben meer dan 700.000 samenvattingen beoordeeld. Zo weet je zeker dat je de beste documenten koopt!

Snel en makkelijk kopen

Snel en makkelijk kopen

Je betaalt supersnel en eenmalig met iDeal, Bancontact of creditcard voor de samenvatting. Zonder lidmaatschap.

Focus op de essentie

Focus op de essentie

Samenvattingen worden geschreven voor en door anderen. Daarom zijn de samenvattingen altijd betrouwbaar en actueel. Zo kom je snel tot de kern!

Veelgestelde vragen

Wat krijg ik als ik dit document koop?

Je krijgt een PDF, die direct beschikbaar is na je aankoop. Het gekochte document is altijd, overal en oneindig toegankelijk via je profiel.

Tevredenheidsgarantie: hoe werkt dat?

Onze tevredenheidsgarantie zorgt ervoor dat je altijd een studiedocument vindt dat goed bij je past. Je vult een formulier in en onze klantenservice regelt de rest.

Van wie koop ik deze samenvatting?

Stuvia is een marktplaats, je koop dit document dus niet van ons, maar van verkoper denh11323. Stuvia faciliteert de betaling aan de verkoper.

Zit ik meteen vast aan een abonnement?

Nee, je koopt alleen deze samenvatting voor €6,77. Je zit daarna nergens aan vast.

Is Stuvia te vertrouwen?

4,6 sterren op Google & Trustpilot (+1000 reviews)

Afgelopen 30 dagen zijn er 77254 samenvattingen verkocht

Opgericht in 2010, al 14 jaar dé plek om samenvattingen te kopen

Start met verkopen
€6,77
  • (1)
  Kopen