Neurochemistry

Question 1

What are ependymal cells?

Answer 1

Cells that line the ventricles

They produce, monitor, and circulate CSF

Question 2

What type of cell is an olfactory or retinal cell?

Answer 2

Bipolar neuron

Question 3

What are basket cells?

Answer 3

Inhibitory interneurons that form dense plexus of terminals around the soma of target cells

Found in the cerebellum and cortex

Question 4

What are betz cells?

Answer 4

Large motor neurons

Question 5

What type of cell forms most of the corpus striatum?

Answer 5

Medium spiny neurons

Question 6

What are Purkinje cells?

Answer 6

Huge neurons in the cerebellum

Question 7

What are Renshaw cells?

Answer 7

Neurons with both ends linked to alpha motor neurons

Question 8

What are granule cells?

Answer 8

The smallest type of neurons, found in the cerebellum

Question 9

What are anterior horn cells?

Answer 9

Motor neurons located in the spinal cord

Question 10

What are spindle cells?

Answer 10

Interneurons that connect widely separated areas of brain

Question 11

What are the main types of circuits neurons can form?

Answer 11

▪️Divergence (same or multiple pathways)
▪️Convergence (single or multiple sources)
▪️Reverberating circuit
▪️Parallel after-discharge circuit

Question 12

How are neurotransmitters transported down an axon?

Answer 12

I’m vesicles

Question 13

What evokes the release of neurotransmitters from vesicles?

Answer 13

Influx of calcium caused by action potential

Question 14

Where do vesicles go after releasing neurotransmitters?

Answer 14

Back up the axon to the soma

Question 15

What are the two types of axonal transport?

Answer 15

▪️Slow (1-5mm/day)
▪️Fast (200-400mm/day)

Question 16

What is transported via fast axonal transport?

Answer 16

▪️Neurotransmitters
▪️Growth factors
▪️Toxins/pathogens (e.g. HSV, tetanus)

Question 17

What is slow axonal transport important for?

Answer 17

▪️Transporting complex products (e.g. axoplasm to terminals)
▪️Neuronal growth
▪️Part of mature neuron function

Question 18

What are the 3 main types of synapses?

Answer 18

▪️Axodendritic
▪️Axosomatic
▪️Axoaxonic

Question 19

What targets are relevant for neurotransmitters?

Answer 19

▪️Receptors (ionotropic, metabotropic)
▪️Enzymes
▪️Transporters
▪️Nuclear/mitochondrial receptors

Question 20

What are ionotropic receptors?

Answer 20

Receptors with a channel that opens up when a ligand (NT) binds to it, changing its shape, and allowing ions to flow across the membrane.

(Aka neurotransmitter-gated or ligan-gated channels)

Question 21

What are cations?

Answer 21

Ions with a positive charge (e.g., Na+, K+, Ca+)

Question 22

How does the opening of an ionotropic receptor effect the membrane?

Answer 22

Has direct and fast effects of neural membrane excitability.

Question 23

How does synaptic transmission with metabotropic receptors compare to ionotropic receptors?

Answer 23

Much slower

Question 24

What happens when a neurotransmitter binds to a metabotropic receptor?

Answer 24

▪️ G-protein coupled with the receptor is activated and produces effector
▪️ Effector stimulates secondary messenger synthesis
▪️ Secondary messenger activates intercellular process, which opens the channel

Question 25

What pathways can be activated by G-proteins (GPCR/7TM)?

Answer 25

▪️ Canonical pathway (which activates cyclic AMP or phosphatidylinositol pathway)
▪️ Alternative pathways (via beta-arrestins, GRKs and SrcKs)

Question 26

Why might different molecules activating the same metabotropic receptor lead to different effects?

Answer 26

Depends on which pathway is activated (show bias for different ones)

Question 27

What can control metabotropic receptor activity?

Answer 27

G-protein coupling

Question 28

G-protein coupling has a _________________________

Answer 28

Dynamic equilibrium (at any one time some will be coupled and some wont, changes very quickly)

Question 29

Which metabotropic receptors do agonists show higher affinity for?

Answer 29

G-coupled receptors (compared to uncoupled)

Question 30

How does the affinity of antagonists at metabotropic receptors differ when it is G-coupled compared to when it is uncoupled?

Answer 30

No difference

Question 31

What happens with chronic agonist stimulation of a metabotropic receptor?

Answer 31

Desensitisation - internalisation of receptors, some get destroyed, some get recycled but regeneration of new ones cannot keep up with the number destroyed so total amount reduces

Question 32

What happens with chronic antagonist stimulation of a metabotropic receptor?

Answer 32

Hypersensitisation - prevents internalisation and destruction of receptors, leading to increased number of receptors on the surface

(Reaction to less stimulation to try and increase stimulation!)

Question 33

What controls second messenger cellular concentrations?

Answer 33

Specific enzyme pathways (e.g., cyclic nucleotides)

Question 34

What happens if there is too much secondary messenger?

Answer 34

Increase affinity of the breakdown enzyme for its substrate to increase the breakdown of the messenger

Question 35

How might one metabotropic receptor interact with another?

Answer 35

Secondary messengers provide a path between them so activity of one can modulate activity of another

Question 36

What is an excitatory neurotransmitter?

Answer 36

One that enhances the probability of an action potential

Depolarises or increased probability of depolarisation

Question 37

What is an inhibitory neurotransmitter

Answer 37

Hyperpolarises the membrane and reduces probability of action potential

Question 38

Can the same neurotransmitter have both excitatory and inhibitory effecrs?

Answer 38

Yes! - depending on the circuit and the receptor it binds to

Question 39

What controls neurotransmitter release?

Answer 39

▪️ Activity (e.g., change in neuronal firing rate modulated by somatodendritic auto-receptors)
▪️ Synaptic neurotransmitter concentration
▪️ Other neurotransmitters released from other terminals that activate pre-synaptic hetero-receptors

Question 40

What modulates synaptic membrane excitability and local neurotransmitter release?

Answer 40

Pre-synaptic auto-receptors

Question 41

What terminates neurotransmitter activity?

Answer 41

▪️ Dissociation of NT from receptor
▪️ Receptor internalisation (typically in response to agonist binding for metabotropic receptors)
▪️ Synaptic “free” NT concentration drops

Question 42

What causes synaptic “free” NT concentration to drop?

Answer 42

▪️ NT diffuses away
▪️ Re-uptake into pre-synaptic terminal or glia via re-uptake transporters
▪️ Catabolism by extracellular (e.g., acetylcholinesterase, COMT) or intracellular enzymes (e.g., MAO)

Question 43

What are the main modulatory monoamines?

Answer 43

▪️ Dopamine
▪️ Noradrenaline
▪️ Histamine
▪️ Serotonin (5-HT)

Question 44

What type of molecule is glutamate, GABA, and glycine?

Answer 44

Amino acids

Question 45

What constitutes the majority of neurotransmitters in the brain?

Answer 45

Glutamate and GABA

Question 46

What is GABA?

Answer 46

▪️ Principle inhibitory NT
▪️ Typically acts on ionotropic receptors attached to chloride channels
▪️ Increase of chloride ions = increasingly negative potential (hyperpolarisation)

Question 47

What is glutamate?

Answer 47

▪️ Principle excitatory NT
▪️ Typically acts on receptors coupled with cation channels - depolarisation!

Question 48

What is glutamate involved in?

Answer 48

Cognition, memory, and learning

Question 49

What are the main glutamatergic ionotropic receptors?

Answer 49

NMDA, AMPA, and kainate

Question 50

What role does glutamate play in neurodegenerative disease?

Answer 50

Insult to brain = increased glutamate release = excitotoxicity = cells self-destruct

Question 51

What are the most prominent glutamate pathways?

Answer 51

▪️ Cortico-cortical
▪️ Thalamo-cortical
▪️ Cortico-striatal

(also pathways been cortex, substantia nigra, subthalamic nucleus, and pallidum)

Question 52

What does GABA regulate?

Answer 52

▪️ Neuronal excitability
▪️ Muscle tone
▪️ Levels of alertness

Question 53

What are the two main types of GABA receptors?

Answer 53

▪️ GABA a = ionotropic (opens Cl- and K+ channels)
▪️ GABA b = metabotropic (works via GPCRs)

Question 54

Where is GABA taken into and what is it converted to?

Answer 54

▪️ Astrocytes
▪️ Converted into glutamate and glutamine

Question 55

What happens to glutamine when it is released by astrocytes?

Answer 55

▪️ Taken up by neurons
▪️ Converted into glutamate and then GABA

Question 56

What are the two acetylcholine receptors?

Answer 56

▪️ Nicotinic (typically excitatory)
▪️ Muscarinic (either excitatory or inhibitory)

Question 57

What is the main role of acetylcholine?

Answer 57

Cognitive function - possible role in AD/AD treatment

Question 58

What is the monoamine synthetic pathway?

Answer 58

1. L-tyrosine
2. L-DOPA
3. Dopamine
4. Noradrenaline
5. Adrenaline

Question 59

Where are the cell bodies for dopamine synthesis?

Answer 59

Midbrain nuclei - substantia nigra, ventral tegmental area

Question 60

What are the main functions of D1 and D5 receptors?

Answer 60

▪️ Excitatory
▪️ Increase cAMP which enhances cation channel opening

Question 61

What are the main functions of D2, D3, and D4?

Answer 61

▪️ Inhibitory
▪️ Decrease cAMP

Question 62

How many dopamine receptors are there and what kind of receptor are they all?

Answer 62

▪️ 5
▪️ All GPCRs (metabotropic)

Question 63

How is dopamine taken back into presynaptic terminals and what can inhibit this?

Answer 63

▪️ Via dopamine transporters (DAT)
▪️ Inhibited by amphetamine, cocaine, and methylphenidate - increase reward!

Question 64

How are dopamine and noradrenaline catabolised?

Answer 64

▪️ By MAO-A in the neurons
▪️ By MAO-B in glial
▪️ By COMT extracellularly

Question 65

What conditions are associated with abnormal dopamine?

Answer 65

▪️ Schizophrenia (increased in PFC)
▪️ ADHD (decreased)
▪️ Parkinson’s (severe deficiency due to cell death in substantia nigra)

Question 66

Why is Parkinson’s treated with L-DOPA instead of dopamine?

Answer 66

Dopamine cannot cross the BBB and has severe adverse cardiac effects

Question 67

Where is noradrenaline synthesised?

Answer 67

Noradrenergic neurons in locus coeruleus

Question 68

Where does noradrenaline take effect?

Answer 68

▪️ Brain stem
▪️ Spinal cord
▪️ Cerebellum
▪️ Hypothalamus
▪️ Amygdala
▪️ Neocortex

Question 69

What are the two types of CNS noradrenaline receptors?

Answer 69

▪️ Alpha-2 = inhibitory
▪️ Beta-2 = excitatory

Question 70

Where else are noradrenaline receptors typically found?

Answer 70

On vasculature

Question 71

How are dopamine, noradrenaline, and serotonin transported?

Answer 71

In synaptic vesicles by vesicular monoamine transporter (VMAT)

Question 72

What is the main role of adrenaline?

Answer 72

Attention and focus

Question 73

What conditions have been associated with abnormal noradrenaline in the brain?

Answer 73

▪️ ADHD
▪️ Depression
▪️ Schizophrenia

Question 74

What is serotonin derived from?

Answer 74

Tryptophan

Question 75

What neurons are modulated by serotonin?

Answer 75

Glutamatergic and GABAnergic

Question 76

Where are serotonergic cell bodies found?

Answer 76

Raphe nuceli

Question 77

How many receptors are associated with serotonin?

Answer 77

17

Question 78

What type of receptor are serotonin receptors?

Answer 78

All metabotropic (GPCRs) except for 5-HT3 which is a ligand-gated ion channel

Question 79

How is serotonin taken back into pre-synaptic terminals?

Answer 79

Via serotonin transporters (SERT)

Question 80

What inhibits serotonin reuptake?

Answer 80

▪️ MDMA
▪️ Amphetamine
▪️ Cocaine
▪️ Tricyclic antidepressants
▪️ SSRIs

Question 81

How is serotonin catabolised?

Answer 81

By MAO-A

Question 82

What role does serotonin play physiologically?

Answer 82

▪️ Well-being
▪️ Happiness
▪️ Mood
▪️ Appetite
▪️ Sleep

Question 83

What conditions have been associated with abnormal levels of serotonin?

Answer 83

▪️ Depression
▪️ Anxiety
▪️ Eating disorder
▪️ Parkinson’s disease?

Question 84

What are the main histamine receptors in the CNS?

Answer 84

H1 and H3 (all metabotropic)

Question 85

How is histamine formed and where?

Answer 85

▪️ By decarboxylation of L-histidine
▪️ In the tuberomammillary nuclei in posterior hypothalamus

Question 86

What is physiological role of histamine?

Answer 86

Regulation of sleep, appetite, and body temperature

Question 87

What conditions have been associated with abnormal histamine levels?

Answer 87

Schizophrenia

Question 88

What are the main purines in the brain?

Answer 88

Adenosine and ATP

Question 89

What is the main role of adenosine receptors?

Answer 89

Co-localise with other receptors, such as D2, affecting their function

Question 90

What can block adenosine 2A receptors and what is the effect of this?

Answer 90

Caffeine - decreases function of D2 thus increases the effect of dopamine

Question 91

What do endorphins do?

Answer 91

▪️ Generally inhibitory
▪️ Act via opioid receptors
▪️ General pain control and feelings of happiness

Question 92

How are endocannabinoids transported through the cytoplasm?

Answer 92

Via endocannabinoid transporter proteins (eCBTs) because they are very hydrophobic

E.g., heat shock proteins, fatty acid binding proteins

Question 93

What are the two main endocannabinoids?

Answer 93

▪️ Anandamide
▪️ 2-Arachidonoylglycerol

Question 94

What are the two main cannabinoid receptors?

Answer 94

▪️ CB1 - one of the most abundant of all CNS receptors
▪️ CB2 - mainly on activated glia, role in immune activation?

Question 95

How are cannabinoids broken down?

Answer 95

▪️ Fatty acid amide hydrolase (FAAH)
▪️ Monoacyl glycerol lipase (MAGL)

Question 96

What are the main physiological roles of cannabinoids?

Answer 96

▪️ Feeding behaviour
▪️ Motivation
▪️ Pleasure

Question 97

What is the Hebbian theory of neuronal plasticity?

Answer 97

Circuits that get used often will be reinforced, making it easier for those cells to communicate

Conversely, connections used less often will die off

Question 98

What is long-term potentiation?

Answer 98

Persistent strengthening of synapses:

▪️ Strong depolarisation leads to removal of NMDAR Mg2+ block
▪️ Rapid flow of Ca2+ into the cell
▪️ Activation of protein kinases
▪️ Trigger insertion into postsynaptic membrane

Question 99

What is the cellular basis of synaptic plasticity?

Answer 99

▪️ At resting potential, ion flow through NMDAR is blocked by extracellular Mg2+
▪️ Mg2+ is displaced by depolarisation of post-synaptic membrane
▪️ Pattern of this and presynaptic glutamate release determines extent of NMDAR activation and Ca2+ influx
▪️ Ca2+ activates second messenger pathways
▪️ Pathways enable easier activation of pathway with lower amounts of glutamate

Question 100

What is long-term depression?

Answer 100

Synapses become less efficient

▪️ Weka depolarisation leads to lesser degree of removal of NMDAR Mg2+ block
▪️ Modest increase in Ca2+
▪️ Activation of protein phosphatases
▪️ Trigger removal from postsynaptic membrane

Question 101

How is the best way to measure in vivo neurochemistry?

Answer 101

▪️ PET
▪️ SPECT

Question 102

What is SV2A used for?

Answer 102

A marker of synapses, giving a measure of synaptic density