Monoamines: Catecholamines Flashcards
What are monoamines?
Monoamines (biogenic amines) are a group of neurotransmitters / hormones that share a common single amine functional group.
- Includes epinephrine, norepinephrine, dopamine and serotonin
What are catecholamines?
Catecholamine neurotransmitters have common structure (with individual variations)
- includes epinephrine, norepinephrine and dopamine
what is VMAT?
VMAT is the transporter that loads
dopamine into synaptic vesicles
What is reserpine?
Reserpine inhibits VMAT and depletes DA and NE as cytosolic catecholamines are rapidly degraded
Reserpine treatment causes sedation in animals and induces depression in humans
How does
cocaine and amphetamine affect DAT function?
Cocaine and amphetamine affect DAT function
Cocaine & amphetamines inhibits
DAT preventing dopamine reuptake
- Increases dopamine in the synapse
- Prolongs dopamine signalling
- Hyperactivity of dopaminergic circuits
Describe dopaminergic synapse
Presynaptic cell rich in anabolic enzymes (TH, DOPA decarboxylase)
VMAT expressed on vesicles for loading dopamine
Dopamine receptors in postsynaptic membrane
Autoreceptors in presynaptic membrane for feedback inhibition
Dopamine transporter (DAT)
responsible for reuptake
What is the difference between D1 and D2 receptors?
D1 family [D1, D5] – G-protein coupled receptors signalling through Gsα to ↑cAMP (Excitatory)
D2 family [D2, D3, D4] – G-protein coupled receptors signalling through Giα to ↓ cAMP (Inhibitory)
Describe dopaminergic terminals
Unlike classical synapses, dopamine can often synapse onto the neck of dendritic spines
This allows dopamine to modulate the activity of the synapse
Dopamine can gate the signals at dendritic spines – increasing or decreasing signal transmission
Describe dopaminergic pathways
Dopamine accounts for 90% of catecholamine neurotransmission in the CNS
- Nigrostriatal system
- projects from substantia nigra and ventral tegmental area to striatum (caudate and putamen)
- Tuberoinfundibular system
- projects from the hypothalamus to the medial eminence to stimulate the pituitary
- prolactin secretion
- Mesolimbic/mesocortical system
- Projects from the ventral tegmental area to the limbic system, nucleus accumbens, mesial frontal, anterior cingulate, and entorhinal cortex
Describe dopaminergic lesions
6-hydroxydopamine (6-OHDA) is a selective neurotoxin.
BBB impermeable, taken up by catecholaminergic neurons (after injection using a stereotactic apparatus).
Bilateral nigrostriatal lesion – sensory neglect, motivational deficits, motor impairment.
Unilateral lesion of nigrostriatal pathway results in postural asymmetry and turning.
Describe the nigrostriatal system
- Projects to the striatum
- Involved in motor control
- D1 and D2 family receptors
- Degradation in Parkinson’s leads to motor symptoms
- Treatment includes L-DOPA, precursor to dopamine
- MPTP (1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine) is a neurotoxin that degrades dopaminergic neurons in the substantia nigra and produces
Parkinson’s symptoms - Resistant to L-DOPA treatment
Describe nigrostriatal dopaminergic pathways
- Degeneration of dopaminergic neurons in the nigrostriatal system central to the pathophysiology of Parkinson’s disease
- tremors,rigidity,forward-flexed posture and shuffling steps, bradykinesia (slowed movement)
- Targets enriched with D1 and D2 receptors in the basal ganglia
- Degradation of neurons in the substantia nigra in Parkinson’s disease
Describe NIGROSTRIATAL DOPAMINE
- Genetic modification of dopamine function induces locomotor effects
- DAT knockout causes hyperactivity
- Decreased re-uptake prolongs DA signalling at the synapse
What leads to cocaine’s hyper locomotion
- Cocaine (inhibiting DAT activity) has comparable effects on locomotion to DAT knockout.
- D1 receptor knockout ablates cocaine’s hyperlocomotion.
Describe mesolimbic pathways
- Targets enriched in D1,D2 family receptors
- Limbic connections are proposed to mediate memory, learning, and affect
- The nucleus accumbens is proposed to act to modify salience of information flow, implicated in motivation & addictions (motivational salience), and psychosis (sensory salience)
