W9 -Neurotransmitters Systems III: Monoamines

Question 1

Why is it important?

Answer 1

It is involved in behavioural effects, eg. motivation, rewards, pleasure, movement, learning and cognition, arousal and moods.
They are identified to lead to mental health issues - like depression, schizophrenia, psychosis, Parkingson’s disease, drugs abuse, dementia, Alzheimer’s.
Important to know to develop drugs.

Question 2

What do Venalfaxine, Citalopram and Prozac, Olanzapine, Levodopa and Aricept do?

Answer 2

Drugs:
Venlafaxine = Antidepressants - increases serotonin and noradrenaline.
Citalopram and Prozac = antidepressants that target the serotonin transporter. Increases serotonin.
Olanzapine = Antipsychotic by blocking dopamine D2 receptor.
Levodopa = Precursor of dopamine - manage symptoms of Parkingsonism like rigidity.
Aricept = Management of dementia and alzheimers - inhibits anti cholinesterase.

Recreational drugs also affects the monoamine system.

Question 3

What are CNS systems that control behaviour?

Answer 3

• Autonomic nervous system
• Hypothalamic-pituitary neurohormones
• Diffuse monoamine system

Question 4

What is the sympathetic nervous system?

Answer 4

Increases, fear, fights, flight, sexual stimulation.
Autonomic nervous system.

Question 5

What is the parasympathetic nervous system?

Answer 5

Relaxation, recovery, growth, digestion takes place.

Question 6

What is The Diffuse Modulatory Systems of
the Brain (monoamines)?

Answer 6

The modulatory system is the system that releases monoamines.

• Four systems with common principles:
  – Small set of neurons at core
  – Arise from brain stem
  – One neuron influences many others
  – Synapses release transmitter molecules into extracellular fluid
• Four main systems:
  – Noradrenergic Locus Coeruleus - Noradrenaline
  – Serotonergic Raphe Nuclei - Serotonin
  – Dopaminergic Substantia Nigra and Ventral tegmental Area - Dopamine
  – Cholinergic Basal Forebrain and Brain Stem Complexes - Acetylcholine

Question 7

What are the behavioural effect: The Diffuse Modulatory Systems of the Brain

Answer 7

A: Point to point communication
-Fast, restricted
B: Diffuse modulatory systems
-slower, widespread
Behavioural effects: Mood, memory, reward, movement, motivation

These don’t inhibit or excite, they modulate the excitation. This is why they are attractive pharmacologically. They don’t completely change, they modulate.

Question 8

What are some examples of metabotropic receptors?

Answer 8

5-HT1
Inhibits AC
5-HT2
Stimulates PLC
Dopamine D1
Stimulates AC
Dopamine D2
Inhibits AC
Noradrenaline
Stimulates AC
Noradrenaline
1 Stimulates PLC
Noradrenaline
2 Inhibits AC

Question 9

What is the monoamine: Noradrenaline (NA)?

Answer 9

Noradrenergic Locus Coeruleus (LC)- Noradrenaline
 Arousal
 Wakefullness
 Exploration and mood (low NA in depressed)
 Blood pressure
 Addiction/gambling
These neurones project in certain areas such as the cortical region, amygdala (involved in emotions), hypothalamus (thermogenesis, appetite regulation, endocrine centre etc), cerebellum (motor coordination) and down to the spinal cord.

Question 10

What is the synthesis of catecholamines?

Answer 10

The precursor of Dopamine is the amino acid Tyrosine.
Tyrosine + Tyrosine hydrolase = DOPA
DOPA + DOPA decarboxylase = Dopamine
Dopamine + Dopamine B-hydroxylase = Noradrenaline
Noradrenaline + Phenylethanolamine N-methyltransferase = adrenaline

Question 11

How is NA regulated?

Answer 11

• Post-synaptic
  – Carry on the message
• Pre-synaptic (autoreceptors)
  – Usually inhibitory
  – Negative feedback mechanism
• Reserpine-depletes NA stores by inhibiting vesicular uptake - basically, blocks NA getting inside vesicles. This means NA gets depleted in the synaptic cleft. This drug is associated with negative moods. Also used as an antihypertensive.
• Amphetamine (indirect sympathomimetic)-enters
  vesicles displacing NA. Into cytoplasm, increase NA leakage out of neuron. This is a psychostimulant. The NA leaks out and accumulates in the synaptic cleft. Results in a big surge of NA. This is the excitement people feel.

In a neurone, the NA gets inside a NA vesicle. Once they are inside, they release the content in the synaptic vesicle. It activated NA receptors.

NA is regulated by the reuptake via NA transporter. Its function is to take up excess NA in the synaptic cleft and break it down and metabolised by the enzynme Monoamine (MAO), which destroys NA.

Question 12

Where do the various pathways of adrenaline/noradrenaline do?

Answer 12

There are a and B adrenaline/noradrenaline receptors.
a subdivides to a1 and a2.

a1 = Phosphlipase C = PIP, IP3 DAG
IP3 = Ca2+ = smooth muscle contraction glycogenolysis.

a2= inhibits adenyl cyclase. This decreases cAMP = smooth muscle contraction.
a2 = Also inhibits release of noradrenaline due to Ca+ decrease

B = stimulation of Adenyl cyclase = cAMP = Contraction of cardiac muscle, smooth muscle relaxation glycogenolysis.

Question 13

What is noradrenaline?

Answer 13

• Reserpine-depletes NA stores by inhibiting
  vesicular uptake
• Amphetamine (indirect sympathomimetic)-enters
  vesicles displacing NA into cytoplasm, increase NA leakage out of neuron
• Cocaine-blocks NA re-uptake
• Noradrenaline (NA)
  – Main action inhibitory (β)
• Also excitatory (⍺ / β)
  – Termination: neuronal uptake and MAO
  – Main cell body in locus coeruleus
• NAergic neurons active when ‘awake’
• Amphetamine -  alertness and exploratory behaviour
  – High density in brainstem, hypothalamus & medial temporal lobe
  – Functions:
• Arousal, wakefullness, exploration and mood (low NA in depressed patients)
• Blood pressure regulation, (antihypertensive e.g. clonidine 2)
• (Addiction/gambling)

Question 14

What is the monoamine: Dopamine (DA)?

Answer 14

Dopaminergic Substantia Nigra (SN) and Ventral tegmental Area (VTA) - Dopamine is released in the striatum.
Involved in: Movement, Reward, Inhibition of prolactin release, Memory consolidation

Parkinson’s Disease - result of Nigrostriatal neurone degradation- characterised by difficulty in movement.
Schizophrenia - overstimulation of the mesolimbic dopaminergic areas lead to positive reactions such as hallucinations.
Addiction, Emesis, ADHD

The mesolimbic pathway consisting of Dopaminergic neurones with cell bodies located in that area of the brain (VTA). These project to various ridges of brain including the nucleus accumbens (Ac) - rewards and pleasure. Also extends to Am - emotions and also the hyppocampus- memory and learning.

Mesocortical pathway leads from directly the SN to the frontal cortex. The Tubero-hypophyseal pathways stem from the hyppocampus releasing dopamine.This is closely related to portal system, where it is transferred via circulation to pituitary. Here it will act on the D2 receptor to inhibit release of prolactin.
Dopamine is also present in the chemoreceptor trigger zone (CTZ) - induce vomiting.

Question 15

How is dopamine regulated?

Answer 15

L-dopa get metabolised by Dopa decarbohydroxylase to Dopamine.
Dopa gets inside synaptic vesicles, the content gets released and they activate D1 and D2 receptors.
D2 are found pre and post synaptically.

Too high = psychosis, addiction etc
Too low = impairment in movement etc

Excess dopamine in the synaptic cleft = Dopamine transporters collect it and pushes it back to the presynaptic neurone. Once inside, it would get metabolised and broken down by an isoenzyme of monoamine oxydase B (MAOB) - completely destroying Dopamine.

One way to increase dopamine is to administer L-dopa. Can also block dopamine transporters. Inhibiting MAOB.

Question 16

What are the pathways and functions of dopamine receptors?

Answer 16

• Dopamine (DA)
  – Inhibits central neurons (K+ channels)
  – D1 (D1 & D5) and D2 (D2, D3, D4) receptors
• D1 and D2 receptors in striatum, limbic system, thalamus & hypothalamus
• D3 receptors in limbic system NOT striatum
• D4 receptors in cortex & limbic system
  – Termination: MAO, neuronal uptake
  – Main pathways
• Substantia nigra to basal ganglia (Parkinson’s disease)
• Midbrain to limbic cortex (schizophrenia)
  – Functions / disorders
• Movement, addiction, stereotypy, hormone release, vomiting

Question 17

What is the monoamine: Serotonin (5-HT)?

Answer 17

Serotonergic Raphe Nuclei - Serotonin/5-HT is release.
The neurones project to different regions including the cortex, the striatum, the thalamus (relaying of all info), projects to hypothalamus, hyppocampus, amygdala, cerebellum and spinal cord.

Consequences of release of serotonin: Heightened perceptions, stimulations, elevated mood, reduced appetite.
Eg. Ecstasy works mainly by increasing serotonin.

Question 18

How is serotonin/5HT regulated?

Answer 18

Tryptophan is the precursor.

Tryptophan + Tryptophan hydrolase = 5-Hydroxyltryptophan

5-Hydroxyltryptophan + L-Aromatic acid decarvoxylase (=dopa decarboxylase) = 5-Hydroxyltryptamine (serotonin)

5-Hydroxyltryptamine + Monoamine oxidase = 5-hydroxylincoleacetylaldehyde.

5-hydroxylincoleacetylaldehyde + aldehyde dehydrogenase = Hydroxyindoleacetic acid (5-HIAA)

Serotonin can get inside serotonergic vesicles. This means the content of the serotonergic vesicles are released once the neurone is activated, which inturn activates serotonin receptors. 5-HT3 is the only ion gated channel receptor.

Serotonin receptors are mostly found post-synaptically. 5HT1D Autoreceptors on presynaptic neurones release 5HT.

High serotonin = serotonin syndrome, seizures, cardiac collapse
Low = depression,

5-HT is a serotonin transporter on the presynaptic vesicle that absorbs the serotonin. Once serotonin enters, it gets metabolised by MAO, terminating serotonin.

Treat depression:
Block 5-HT transporter and MAO.

Question 19

What are the specifics of serotonin?

Answer 19

• Serotonin (5-HT)
  – 5-HT receptors (14 subtypes)all G-protein coupled except 5-HT3
• 5-HT1 inhibitory, limbic system – mood, migraine
• 5-HT2 (5-HT2A), excitatory, hallucinogenic, limbic system & cortex
• 5-HT3 excitatory, medulla – vomiting
• 5-HT4 presynaptic facilitation (ACh) – cognitive enhancement
• 5-HT6 and 5-HT7 – novel targets, cognition, sleep
  – Termination – MAO, neuronal uptake
  – Function / disorders
• Mood (anxiety/depression)
• Psychosis (5HT antagonism antipsychotic)
• Sleep / wake (5-HT linked to sleep, 5-HT2 antagonists inhibit REM sleep)
• Feeding behaviour (5HT2A antagonist increase apetite, weight gain; antidepressants decrease apetite
• Pain, migraine (5-HT inhibits pain pathway, synergistic with opioids)
• Vomiting,

Question 20

What are autoreceptors?

Answer 20

Inhibit cell firing and transmitter release at the terminal regions found presynaptically.
These receptors can also be found post-synaptically.
The role is to control the release of neurotransmitters.
They are found on cell bodies too.
5-HT1D
D2 or D3
a2

Question 21

What are monoamine transporters?

Answer 21

• 12TMDs
  -Both ends intracellular
• Pump monoamines in neuron
  -DA, NA, 5HTtransporters

Question 22

How do Transporters work?

Answer 22

Transporters usually take the neurotransmitter
back up into the pre-synaptic terminal

Question 23

How does the monoamine: Acetylcholine (ACh) work?

Answer 23

Involved in:Memory, learning, Motor control (striatum), Reward, Arousal

This means the degeneration causes:

Alzheimer’s
Pain
Addiction
Epilepsy (nAChR genes)
Schizophrenia
ADHD
Depression
Anxiety,

Cholinergic Basal Forebrain and Brain Stem Complexes - Acetylcholine. These stem from the nucleus basalis to different regions including the cortex where acetylcholine gets released. Also gets released from the septum to the hyppocumpus. Also goes from SN to the thalamus.

Question 24

What is acetylcholine?

Answer 24

• Acetylcholine (ACh)
  – Abundant in basal forebrain, hippocampus
  and striatum
  – Termination – acetylcholinesterase (AChE)
  – ACh excitatory neurotransmitter
• Nicotinic (ionotropic / fast)
• Muscarinic (G-protein coupled / slow)
  – M1 excitatory ( M1 receptors in dementia)
  – M2 presynaptic inhibition (inhibit Ach release)
  – M3 excitatory glandular/smooth muscle effects (side effects)
  – M4 and M5 function not well known

– Functions:
* Arousal
* Epilepsy (mutations of nAChR genes)
* Learning and memory (KO mice)
* Motor control (M receptors inhibit DA), pain, addiction
* Involved in schizophrenia, ADHD, depression, anxiety, Alzheimers

Question 25

How does the uptake of acetylecholine work?

Answer 25

AcCoA + Choline = Acetylcholine
These get into cholinergic vesicles via a specific carrier. Once the neurone is activated, acetylcholine is released into the synaptic cleft. These activate either nicotinic or muscurinic receptors. Some of these are found presynaptically. The effects of acetylecholine is terminated by the breakdown into Choline and Acetate with acetylcholinesterase. This means the choline gets back inside the neurone via the choline carrier.

Alzheimer’s treatment = block acetylcholinesterase.

Question 26

What are some other transmitter/modulator substanes?

Answer 26

• Histamine
  – H1 (arousal) and H3 (presynaptic / constitutively active)
  – Functions: sleep / wake, vomiting
• Purines
  – Adenosine (A1, A2A/2B) and ATP (P2X)
  – Functions: sleep, pain, neuroprotection, addiction, seizures, ischaemia, anticonvulsant
• Neuropeptides
  – Opioid peptides
• u, delta, K
  – Tachykinins (Substance P, neurokinin A & neurokinin B)
• NK1 (Substance P), NK2 (neurokinin A), NK3 (neurokinin B)
  – Functions: pain

Question 27

What are opioid peptides and opioid receptors?

Answer 27

Opioid peptide families:

Proopioimelanocortin (B-endorphin)
Proenkephalin (Enkephalins)
Prodynorphin (Dynorphins)
Pronociceptin (Nociceptin/OFQ)

Question 28

What are some Other Transmitter / Modulator Substances

Answer 28

• Lipid mediators
  -Products of conversion of eicosanoids to
  endocanabinoids
  -act on CB1 (inhibit GABA, glutamate release)
  
  • involved in vomiting (CB1 agonist block it, MS, pain,
    anxiety, weight loss/rimonabant CB1 antogonist)
• Melatonin
  -MT1, MT2 receptors
  
  • involved in sleep regulation, circadian rhythmicity,
    agonists for jet lag and insomnia

Question 29

What are some Drugs interacting with the diffuse system Psychostimulants: Amphetamine

Answer 29

• Amphetamine-like drugs (Amphetamine-like drugs (methylphenidate & MDMAmethylphenidate & MDMA))
• Release cytosolic monoamines (DA)Release cytosolic monoamines (DA)
• Prolonged use neurotoxic
  Prolonged use neurotoxic
  ** Degeneration of amine-containing nerve terminals, cell deathDegeneration of amine-containing nerve terminals, cell death
• Pharmacological effects:Pharmacological effects:
  -alertness and alertness and locomotor stimulation (locomotor stimulation ( aggression) aggression)
  -Euphoria / excitement Euphoria / excitement
• Stereotyped behaviourStereotyped behaviour
• AnorexiaAnorexia
• decrease physical and mental fatigue (improves monotonous tasks) physical and mental fatigue (improves monotonous tasks)
• Peripheral sympathomimetic actions (Peripheral sympathomimetic actions (increase blood pressure & blood pressure & decrease gastric motility) gastric motility) - appetite repressor.
• Confidence improves/lack of tirednessConfidence improves/lack of tiredness
• Therapeutic uses
  Therapeutic uses
• ADHD (ADHD (methylphenidatemethylphenidate), appetite suppressants, narcolepsy

Question 30

What do the central stimulants: Cocaine do?

Answer 30

• Blocks catecholamine reuptake Blocks catecholamine reuptake
  ((increase DA, stimulant effect)DA, stimulant effect)
• Pharmacological effects:Pharmacological effects:
• EuphoriaEuphoria
• Locomotor stimulationLocomotor stimulation
  ** Fewer stereotyped behaviours than amphetamineFewer stereotyped behaviours than amphetamine
• Heightened pleasureHeightened pleasure
  ** Lower tendency for delusions, hallucinations and paranoiaLower tendency for delusions, hallucinations and paranoia
• Pharmacokinetics:Pharmacokinetics:
• HCl salt, inhaled and i.v. administrationHCl salt, inhaled and i.v. administration
  ** Nasal inhalation less intense, leads to necrosis of nasal mucosaNasal inhalation less intense, leads to necrosis of nasal mucosa
• Freebase form (‘crack’), smoked, as intense as i.v route

Question 31

What are the effects of drugs of abuse on other diffuse
modulatory systems

Answer 31

• MDMA (ecstasy)MDMA (ecstasy) Inhibits monoamine transporters (mainly Inhibits monoamine transporters (mainly
  5-HT)5-HT)
  ** Large Large increase 5-HT (followed by depletion) 5-HT (followed by depletion)
  ** increase 5-HT linked to psychotomimetic 5-HT linked to psychotomimetic
  effectseffects
  ** increase DA linked to euphoria (followed by DA linked to euphoria (followed by rebound dysphoria)rebound dysphoria)

LSD, Psylocybin (magic mushrooms)
* Hallucinogenic effect by
acting on 5HT2 receptors

Psychostimulants
* Also increase 5HT and NA
* Cocaine block DAT, NET, SERT