Parkinson's

Question 1

Projection pathway of corticobulbar tract

Answer 1

Motor neurons project to the brainstem nuclei via internal capsule

Question 2

What does the corticobulbar tract control?

Answer 2

movement of the face, tongue, and pharyngeal muscles

Question 3

Projection pathway of the corticospinal tract

Answer 3

Motor neurons project via the posterior internal capsule to the cerebral peduncle. From here it divides into three distinct tracts.
1. Lateral corticospinal tract (80%): decussate at the medulla
2. Ventral/anterior corticospinal tract (10%): decussate at terminal spinal cord
3. Corticospinal tract (10%): remain ipsilateral

Question 4

What does the corticospinal tract control?

Answer 4

skilled voluntary movement involving the neck and limbs

Question 5

What is the role/participants of the extrapyramidal pathway

Answer 5

The Extra-pyramidal pathways provide additional information and modulation to optimise the motor programme.
- Premotor cortex: early motor programme development
- Cerebellum: controls the timing of muscle contractions within the motor programme
- Basal Ganglia: selection of appropriate motor programme
- (motor) Thalamus: integrates information from BG and cerebellum

Question 6

Describe the circuitry of the basal ganglia

Answer 6

The VTA/SNpc send dopaminergic projections to the striatum, where dopamine acts on two distinct groups of spiny projection neurons/MSNs. The direct group contains Substance P, and expresses the D1 type dopamine receptor. The indirect group contains enkephalin, and expresses the D2 type receptor. The direct pathway sends GABAergic projections to the GPi/SNpr, which are the major output nuclei of the basal ganglia. The indirect pathway sends inhibitory projections to the GPe, which has inhibitory projections to STN. The STN projects excitatory glutamate onto the output nuclei. The output nuclei SNpr/GPi send GABAergic projections to the thalamus.

Question 7

What occurs in the BG when there is a phasic spike of DA?

Answer 7

In the direct pathway, DA binds to D1 receptors, causing an increase in cAMP and increased cellular activation, therefore release of GABA and inhibition of GPi/SNpr.

In the indirect pathway DA binding to D2 receptors leads to a decreased firing rate. Thus there is less GABA released onto the GPe. This causes an inhibition of the STN, and thus less excitation of the output nuclei.

Less GABA released from GPi/SNpr onto thalamus = disinhibition of the thalamus

Question 8

List the symptoms of PD

Answer 8

Motor: Bradykinesia (Slow Movement), Dyskinesia, Rigidity, Postural instability, Resting tremor, akinesia (inability to initiate movement)

Non motor: Cognitive impairments, sleep disorders, depression, memory deficits

Question 9

What is the hallmark pathology of PD?

Answer 9

Death of dopaminergic cells in the substantia nigra pars compacta and VTA. Formation of Lewy bodies in dopaminergic cells, which occur due to accumulation of the alpha-synuclein protein in the cytoplasm.

Question 10

At what stage in the parkinson’s pathology do symptoms appear?

Answer 10

After death of ≥65% of the dopaminergic cells in the SNpc/VTA.

Question 11

What are the available treatments for parkinsons?

Answer 11

1. Physical therapy/exercise
2. environmental adjustments
3. L-DOPA
4. Surgery for deep brain stimulation

Question 12

What is the net affect to the basal ganglia in parkinsons?

Answer 12

Decreased dopamine release leads to an increased inhibition of the thalamus AND abnormal, prolonged synchronous firing

Question 13

What should a good animal model of PD possess?

Answer 13

progressive death of dopaminergic cells in the SNpc/VTA, and formation of lewy bodies. Should show motor deficits including akinesia, bradykinesia, rigidity, postural instability, and resting tremor. Should respond to treatment with levodopa/DBS.

Question 14

What does the 6OHDA animal model involve?

Answer 14

Injection of 6-OH DA into the SNpc/medial forebrain bundle (SNpc/VTA projection fibres)/striatum into a single hemisphere.

6OHDA taken up by dopaminergic and noradrenergic cells (if you want dopaminergic specificity, also inject a noradrenaline uptake blocker). Within the cells, the 6OHDA interferes with mitochondrial metabolism causing production of radical oxygen species which promote cell death.

Data compared to un-lesioned hemisphere, or a sham lesion.

Question 15

What does the MPTP model involve

Answer 15

Injection of MPTP (i.v ,.i.m.) into the bloodstream, from which it will travel to the brain. The injection can be given to any mammal expressing the MAO B enzyme (not rats), but is mainly given to primates. Injection must occur repetitively over days/weeks to ensure no behavioural recovery.

MPTP is metabolised by MAO B into MPP+, which is selectively taken up by dopamine cells resulting in mitochondrial dysfunction and production of free radicals.

Data is collected from a control animal, or with primates, prior to injection for comparison as primates are a limited (and thus expensive) resource.

Question 16

How is dopamine antagonism used to model PD?

Answer 16

An acute model of PD that can be used in all models, but does not model the pathology. Antagonist can be D1/D2 selective or generalised, and acts to temporarily block the effects of dopamine.

A caveat is that this treatment affects all dopamine cells (not just SNpc/VTA), and does not reflect clinical features such as response to treatment.

Data is compared to the same animal with saline injection.

Question 17

How is animal model pathology assessed?

Answer 17

Pathology can be assessed qualitatively using the step test, apomorphine test, cylinder test, open field test or rotarod or quantitatively through immunohistochemistry or high performance liquid chromotography

Question 18

Step Test

Answer 18

animals (must be trained) are dragged 1m across surface at a specific angle, direction, and speed. Number of ‘steps’ in measured. Less steps = less DA.

Question 19

Apomorphine test

Answer 19

apomorphine is a dopamine agonist, and is injected systemically into animals that are parkinsonian in one hemisphere. Because the Parkinsonian side adapts to low dopaminergic input, there is a significantly greater number of DA receptors in the striatum. When agonist is added this stimulation far outweighs the normal side, causing the rat to spin around

Question 20

cylinder test

Answer 20

the rat is placed in a tube, and assessed on number of paw touches to the wall of cylinder. Relatively low placements on side contralateral to lesion indicates DA loss.

Question 21

rotarod

Answer 21

a general motor behaviour test, where rats ability to learn to stay on a rotating rod is assessed. PD animals tend to lack learning ability, thus will continue to fall off across multiple trials.

Question 22

immunohistochemistry markers

Answer 22

Tyrosine hydroxylase or the dopamine transport (DAT)

TH is less specific as also stains noradrenaline, DAT is more complex (expensive, time consuming) but more selective

Question 23

How is PD pathology assessed in humans?

Answer 23

1. Simple reaction and movement time studies,
2. the Hoehn & Yahr scale (which rates the motor symptoms of PD)
3. The UPDRS, which accounts for all factors that are affect in PD (cognitive level, daily living, motor level, drug complications)

Question 24

Pros/Cons of in vitro

Answer 24

Pros: Controlled, Sensitive to small changes, Can guide more complex experiments
Cons: No behavioural data, lacks biological complexity (neurons do not exist in isolation but in a complex 3D matrix of connections)

Question 25

Pros/Cons of ex vivo

Answer 25

Pros: More physiologically relevant, can test substances not possible in live animals, can examine the function of small scale circuits = preservation of circuits
Cons: Lacks true biological complexity, no behavioural data

Question 26

Pros/Cons of in vivo

Answer 26

Pros: Behavioural data, physiological conditions
Cons: Hard to control, more variance, highly susceptible to other influences, therefore should be repeated multiple times to obtain significant results

Question 27

Pros/Cons of drug stimulation

Answer 27

+ : receptor specific
- : poor time resolution
Injection can be systemic (easy, but off-target effects, must account for metabolism) or into the neural structure (difficult, requires small volume of drug)

Question 28

Pros/Cons of electrical stimulation

Answer 28

+ great time resolution
- : poor neuronal specificity
Stimulation often affects surrounding soma/axons/dendrites. To minimise this, you should use the lowest current possible

Question 29

Pros/Cons of optogenetic stimulation

Answer 29

+ : functional causality, good time resolution, good neuronal specificity
- : tight regulatory control, requires more money, staff, and time. More points where the experiment can fail.

Question 30

What are the main features of a virus?

Answer 30

• Genetic code
• Capsid
• Envelope
• Glycoproteins (neuronal specificity)

Question 31

What changes are made to the genetic code of a virus for optogenetics?

Answer 31

• The DNA code that allows the virus to spread, and the pathological DNA is removed, and is replaced with the genetic code for a light-activation ion channel/to reduce target protein expression via RNA interference.
• The viruses surface proteins can be specialised via promoter region to recognise neurons expressing certain proteins- for instance the dopamine transporter DAT.
• Viruses also transfected with a fluorophore, such as mCHERRY or GFP, to allow confirmation post mortem.

Question 32

What differs the use of AAVs/lentiviruses for optogenetics?

Answer 32

Lentiviruses have better neuronal specificity, but a lower transduction rate than AAVs.

Question 33

How does VSVg transfect neurons?

Answer 33

The vesicular stomatitis virus enters neurons at the soma

Question 34

How does RVg transfect neurons?

Answer 34

The rabies virus enters neurons at the axon terminals and undergoes retrograde transport to the soma.

Question 35

What is the most important thing to consider when using optogenetics?

Answer 35

The stimulation pattern. Actual firing ≠ average firing.

Question 36

MCx Layer 1

Answer 36

Primarily dendrites of MSNs, with a small number of soma.
- Receives input from thalamus and other cortical areas.

Question 37

MCx Layer 2

Answer 37

Contains cell bodies of medium spiny neurons of the extrapyramidal tract, ACh interneurons, and GABAergic interneurons.
- Projects to, and receives from other cortical areas.

Question 38

MCx Layer 3

Answer 38

Contains cell bodies of medium spiny neurons of the extrapyramidal tract, ACh interneurons, and GABAergic interneurons.
- Projects to, and receives from other cortical areas.

Question 39

MCx Layer 4

Answer 39

404: DOES NOT EXIST

Question 40

MCx Layer 5

Answer 40

contains the cell bodies of large spiny neurons/projection neurons/pyramidal neurons/Betz cells which form the corticospinal tract

Question 41

MCx Layer 6

Answer 41

contain MSNs that project to thalamus in the extrapyramidal tract

Question 42

motor neuron disease

Answer 42

caused by the degeneration of betz cells (layer V pyramidal cells)

Question 43

What is the normal functioning pattern of motor cortex neurons?

Answer 43

The pyramidal cells of the motor cortex generally have a low rate of firing (≤10 spikes/s), and exhibit transient burst patterns during movement.
- 60% of neurons respond to movement with excitation
- 30% with inhibition
- 10% with mixed

Question 44

What questions need to be answered to understand neural generation of movement?

Answer 44

• How do we activate agonist & antagonist movement in correct sequence?
• How do we move in three dimensions when muscle only move in 2?

Question 45

What is the cortical cell assembly model?

Answer 45

The cortical cell model states that movement-related cells code for a movement vector (strength and direction). The sum of these vectors from a cluster of neurons determines the executed movement. The order of activation aligns to cell’s muscle role – agonist/antagonist. Neurons that fire together wire together- clusters become linked through LTP.

Question 46

What are the recorded neuronal changes during bradykinesia?

Answer 46

In Bradykinesia, there is a decrease in strength of resting and movement related firing. This results in increased movement time.
- Impaired firing rate of some pyramidal neurons -> reduction in temporal summation, and reduced recruitment of a-motor neurons

Less bursty patterns, when they did occur they were reduced

Less transient synchronous activity within cell clusters -> Reduced spatial summation & insufficient engagement of cortical cell assembly

Question 47

MPTP & Ethics
How was the MPTP primate model “discovered”?

Answer 47

Four individuals who injected a ‘synthetic heroin’ containing MPPP and MPTP experienced an acute onset of Parkinson’s disease.

Question 48

What are the “3 R” guiding principles of humane use of animals in research?

Answer 48

Replacement (of animals with other techniques), Reduction (of animal number used), Refinement (to minimise pain & stress).

Question 49

The medial forebrain bundle

Answer 49

Contains all the axons from the SNpc and VTA. Cutting it prevent all dopamine from reaching the striatum.

Question 50

What other drug is usually administered with L-dopa to prevent degradation in the periphery?

Answer 50

Carbidopa

Question 51

What are the motor-related thalamic nuclei?

Answer 51

The ventromedial/anterior and ventrolateral

Question 52

The ventromedial thalamic nuclei receives input from…

Answer 52

the basal ganglia output nuclei (SNpr/GPi)

Question 53

The ventrolateral thalamic nuclei receives input from….

Answer 53

the cerebellum