Dopaminergic pathways of the brain and drugs used to treat Parkinson’s Disease and Schizophrenia

Question 1

What are the three main dopaminergic pathways in the brain?

Answer 1

Nigrostriatal
Mesolimbic
Tuberoinfundibular system

Question 2

Where are each of these pathways found?

Answer 2

Nigrostriatal– projecting from the substantia nigra pars compacta to the striatum
Mesolimbic– projecting from the ventral tegmental area to the nucleus accumbens, frontal cortex, limbic cortex and olfactory tubercle
Tuburoinfundibular system– projecting from the arcuate nucleus in the hypothalamus to the median eminence and pituitary gland

Question 3

What are the roles of these pathways?

Answer 3

Nigrostriatal – control of movement
Mesolimbic – involved in emotion
Tuburoinfundibular system – regulate hormone secretion

Question 4

What are the two families of dopamine receptors and which receptors fall into each of these families?

Answer 4

D1 family – D1 + D5

D2 family – D2, D3 + D4

Question 5

Describe dopamine synthesis.

Answer 5

Tyrosine is converted by tyrosine hydroxylase to DOPA

DOPA is converted by DOPA decarboxylase to Dopamine

Question 6

Is Parkinson’s disease more common in males or females?

Answer 6

Males – 4:1

Question 7

What percentage of all cases of Parkinson’s disease is accounted for by familial Parkinson’s disease?

Answer 7

8%

The rest are idiopathic

Question 8

What are the possible causes of idiopathic Parkinson’s disease?

Answer 8

Possibly a combination of environmental, oxidative stress, altered protein metabolism and risk genes

Question 9

What are the cardinal signs of Parkinson’ disease?

Answer 9

Resting tremor (pill-rolling tremor)
Rigidity (stiffness – limbs feel weak and heavy)
Bradykinesia (slowness of movement)
Postural abnormality

Question 10

What are the presenting symptoms of Parkinson’s disease?

Answer 10

Pill-rolling resting tremor
Difficulty with fine movements (micrographia)
Poverty of blinking
Hypomimic face
Monotony of speech and loss of volume of voice
Disorders of posture – flexion of the neck and trunk
Lack of arm swing
Loss of balance – lack of righting reflex, retropulsion
Short steps, shuffling gait

Question 11

Describe the initial distribution of symptoms across the body.

Answer 11

Unilateral onset
Symptoms spread to both sides
Generally symptoms worsen with some patients becoming severely disabled

Question 12

What are some non-motor symptoms of Parkinson’s disease?

Answer 12

Depression  
Pain  
Taste/smell disturbances  
Cognitive decline/dementia  
Autonomic dysfunction (constipation, postural hypotension, urinary frequency/urgency, impotence, increased sweating)

Question 13

What is the main area of the brain that is affected by Parkinson’s disease?

Answer 13

Substantia nigra

Other brain areas affected: locus coeruleus, dorsal vagus nucleus, nucleus basalis of Mynert

Question 14

Describe the neuropathology of Parkinson’s disease.

Answer 14

Putamen-projecting pathways degenerate significantly  
Lewy bodies (large circular structure with bright core and white surrounding, packed with alpha-synuclein) also present – this is probably a defensive mechanism to protect against toxic altered proteins

Question 15

What are the stages of Parkinson’s disease?

Answer 15

1-2 = dorsal motor nucleus of vagus, raphe nucleus, locus coeruleus  
3 = substantia nigra pars compacta  
4 = amygdala, nucleus of Meynert, hippocampus  
5-6 = cingulate cortex, temporal cortex, frontal cortex, parietal cortex, occipital cortex

Question 16

What is the main biochemical change seen in Parkinson’s disease?

Answer 16

Marked reduction in the caudate nucleus/putamen dopamine content

Question 17

What proportion of dopaminergic neurones of the nigrostriatal dopaminergic pathway must be lost before symptoms occur?

Answer 17

80-85% of dopaminergic neurones and 70% of striatal dopamine must be depleted before symptoms appear

Question 18

What is the reason for this?

Answer 18

There are compensatory mechanisms e.g. neurone overactivity and increase in dopamine receptors

Question 19

What other type of drug has to be given with L-DOPA in dopamine replacement therapy and why?

Answer 19

Peripheral DOPA decarboxylase inhibitor

This prevents the conversion of L-DOPA to dopamine by peripheral DOPA decarboxylase (this can cause nausea and vomiting)

Question 20

State two different preparation of dopamine replacement therapy.

Answer 20

Sinamet = Carbodopa + L-DOPA 
Madopar = Benserazide + L-DOPA

Question 21

What does L-DOPA treat?

Answer 21

Hypokinesia
Tremor
Rigidity

Question 22

Describe how the dosage of L-DOPA is changed with continued treatment.

Answer 22

It is started low and increased until maximum benefit of drug is achieved without side effects
Effectiveness of L-DOPA declines with time

Question 23

What are the acute side effects of L-DOPA?

Answer 23

Nausea (prevented by domperidone)  
Hypotension 
Psychological effects (schizophrenia like syndrome with dellusions, hallucinations, confusion, disorientation and nightmares)

Question 24

What are the chronic side effects of L-DOPA?

Answer 24

Dyskinesias (abnormal movement of limbs and face – can occur within 2 years of treatment – disappear with reduced dose)
Rapid fluctuations in clinical state (off periods may last for minutes to hours

Question 25

Name three dopamine agonists.

Answer 25

Bromocriptine Ropinerol Pergolide

Question 26

Which receptors do they act on?

Answer 26

D2 receptor

Question 27

What are the benefits of dopamine agonists over L-DOPA?

Answer 27

``` Longer duration of action Smoother and more sustained response Actions independent of dopaminergic neurones Incidence of dyskinesias is less NOTE: L-DOPA is still the gold standard ```

Question 28

What are the adverse effects of dopamine agonists?

Answer 28

Common – confusion, dizziness, nausea/vomiting, hallucinations Rare – constipation, headache, dyskinesia

Question 29

What structure used to be present in older dopamine agonists that caused quite serious clinical problems?

Answer 29

Ergot ring | This caused problems with heart valves

Question 30

What has been the consequence of the removal of this structure within dopamine agonists?

Answer 30

Development of addictive behaviour e.g. gambling

Question 31

Name two MAO inhibitors.

Answer 31

Deprenyl (selegiline) | Rasagiline

Question 32

What are the effects of Deprenyl?

Answer 32

Selective for MAO-B (this predominates in dopaminergic areas of CNS) Does NOT have the peripheral side effects of non-selective MAO inhibitors Can be given in combination with L-DOPA (reduce dose of L-DOPA by 30-50%)

Question 33

What are the side effects of Deprenyl?

Answer 33

RARE Hypotension Nausea/vomiting Confusion and agitation

Question 34

What are the effects of Rasagiline?

Answer 34

It has neuroprotective properties by inhibiting apoptosis (promotes anti-apoptosis genes) NOTE: early clinical trials show this drug might slow down the progression of disease but subsequent studies haven’t been so promising

Question 35

Name two COMT inhibitors.

Answer 35

Tolocapone (CNS + PNS) | Entacapone (PNS)

Question 36

What are the effects of COMT inhibition in the CNS?

Answer 36

Prevents breakdown of dopamine in the brain

Question 37

What are the effects of COMT inhibition in the peripheral nervous system?

Answer 37

Peripheral COMT converts L-DOPA to 3-O-methyl DOPA (3-OMD) 3-OMD competes with L-DOPA for the transport system that transports it across the BBB COMT inhibitors stop 3-OMD production and hence there is less competition for L-DOPA Result: REDUCE L-DOPA DOSAGE

Question 38

What are the side effects of COMT inhibitors?

Answer 38

Cardiovascular complications

Question 39

What percentage of the general population is affected by schizophrenia?

Answer 39

1%

Question 40

What are the symptoms of schizophrenia?

Answer 40

Positive Symptoms (overt symptoms that should NOT be present)  Hallucinations  Delusions  Disorganised thoughts Negative Symptoms (lack of characteristics that SHOULD be present)  Reduced speech  Lack of emotional and facial expression  Diminished ability to begin and sustain activity  Decreased ability to find pleasure in everyday life  Social withdrawal Cognitive deficits  Memory  Attention  Planning  Decision making

Question 41

What appears to have quite a strong contribution to the development of schizophrenia?

Answer 41

Genetics

Question 42

Once schizophrenia has been diagnosed, what are the four main outcomes for patients?

Answer 42

1 – illness resolves completely, with or without treatment and never returns (10-20%) 2 – illness recurs repeatedly with full recovery between episodes (30-35%) 3 – illness recurs repeatedly with incomplete recovery and a persistent defective state develops, becoming more profound with each successive relapse (30-35%) 4 – illness pursues down a downhill course from the beginning (10-20%) NOTE: most cases are relapsing and remitting

Question 43

Describe the involvement of dopamine in schizophrenia.

Answer 43

Positive symptoms – results from excessive dopamine transmission in the mesolimbic and striatal region (D2-mediated) Negative symptoms – results from dopamine deficit in the pre-frontal region (D1-mediated)

Question 44

What evidence has arisen that supports this hypothesis?

Answer 44

Dopamine agonists can induce various psychotic reactions | Typical antipsychotics are dopamine receptor antagonists (blocking D2 receptors)

Question 45

Describe the involvement of glutamate in schizophrenia.

Answer 45

NMDA is a glutamate receptor Glutamate exerts an excitatory influence over the GABA-ergic striatal neurones and dopamine exerts an inhibitory influence These GABA-ergic striatal neurones project to the thalamus and constitute a sensory ‘gate’ Too little glutamate or too much dopamine disables this gate, allowing uninhibited sensory input to reach the cortex NOTE: you find reduced glutamate concentration and reduced glutamate receptors in post-mortem schizophrenic brains. Also NMDA receptor antagonists can produce psychotic symptoms

Question 46

What is the most robust gene associated with schizophrenia?

Answer 46

Neuregulin-1

Question 47

What are all the susceptibility genes for schizophrenia associatedwith?

Answer 47

Dopamine and glutamate neurotransmission

Question 48

What type of drug are all neuroleptics?

Answer 48

Dopamine receptor antagonists (D2 receptors) | NOTE: most neuroleptics block other receptors

Question 49

Which symptoms do neuroleptic drugs treat?

Answer 49

Positive symptoms ONLY

Question 50

What are the initial effects of neuroleptic drugs?

Answer 50

Initial increase in dopamine synthesis and neuronal activity – this declines with time

Question 51

What is meant by an atypical antipsychotic?

Answer 51

Newer antipsychotics are given this term – they have fewer extrapyramidal side effects

Question 52

Name an atypical antipsychotic.

Answer 52

Clozapine

Question 53

Name a typical antipsychotic.

Answer 53

Haloperidol

Question 54

What is an important other action of neuroleptics?

Answer 54

Anti-emetic Because they block dopamine receptors in the chemotactic trigger zone Phenothiazine is a neuroleptic that is really good at preventingnausea/vomiting caused by drugs NOTE: many neuroleptics also block histamine receptors – this is effective at controlling motion sickness

Question 55

What are the extrapyramidal side effects of antipsychotics caused by?

Answer 55

Blockade of dopamine receptors in the nigrostriatal system can induce Parkinson-like side effects

Question 56

What are the two main extra-pyramidal side effects? Acute Dystonia

Answer 56

 Involuntary movements  Muscle spasm, protruding tongue, fixed upward gaze, neck spasm etc.  Often accompanied by Parkinson’s like features  Occur in the FIRST FEW WEEKS and often decline with ongoing therapy  Reversible with withdrawal of the drug or anti-cholinergics Tardive Dyskinesias  Involuntary movements  Involving the face and tongue, but also trunk and limbs  Occur in 20% of patients after SEVERAL MONTHS/YEARS of therapy  Made WORSE by drug withdrawal or anti-cholinergics

Question 57

What are the unwanted effects of antipsychotics?

Answer 57

Endocrine effects – loss of inhibition of prolactin secretion leads to hyperprolactinaemia (can lead to breast swelling and sometimes lactation) Blocking alpha-adrenoceptors – postural hypotension Blocking 5-HT receptors – weight gain Blockade of muscarinic receptors – typical anti-muscarinic effects e.g. blurring of vision, increased intra-ocular pressure, dry mouth, constipation, urinary retention