Topic 4: Neurotransmitters

Question 1

What are the 3 major classes of neurotransmitters? and what is the exception?

Answer 1

-amino acids
-amines (derived from amino acids)
-peptides (constructed from amino acids)
(ACh is exception, derived from actylel CoA and choline )

Question 2

What is the criteria of a molecule to be deemed a neurotransmitter?

Answer 2

1. The molecule must be synthesized and stored in the presynaptic neuron
2. the molecule must be released by the presynaptic axon terminal upon stimulation
3. the molecule, when experimentally applied, must produce a response in the postsynaptic cell that mimics the response produced by the release of neurotransmitter from the presynaptic neuron

Question 3

What is immunocytochemistry used for and what is it called when the same technique is applied to thin sections of tissue, including brain?

Answer 3

-used to anatomically localise particular molecules to particular cells –> used to localise any molecule for which a specific antibody can be generated, including synthesizing enzymes for transmitter candidates
-when used for thin sections of tissues including brain its referred to as immunohistochemistry.

Question 4

What is the method behind using immunohistochemistry in identifying a transmitter?

Answer 4

-once transmitter candidate has been chemically purified, it is injected under the skin or into the bloodstream of animal where it stimulates an immune response
-one feature of the immune response is the generation of large proteins called antibodies
-antibodies can bind tightly to specific site on foreign molecule aka the antigen, in this case the transmitter candidate
- these specific antibody molecules can be recovered from a blood sample of the immunized animal and chemically tagged with a colourful marker, so can be seen with microscope
-when these labelled antibodies are applied to a section of brain tissue, they will colour just those cells that contain transmitter candidate
-by using several different antibodies, each labelled with different marker colour, it is possible to distinguish several types of cells in the same region of the brain

Question 5

what is the use of immunocytochemistry being able to localise synthesising enzymes for transmitter candidates as well as any molecule for which antibody can be generated?

Answer 5

demonstrates that the transmitter candidate and its synthesizing enzyme are contained in the same neuron - or same axon terminal - which can help satisfy the criterion that the molecule is localised in and synthesised by a particular neuron

Question 6

What is the method in situ hybridization useful for?

Answer 6

-confirming that a cell synthesizes a particular protein or peptide
-method for localizing specific mRNA transcripts for proteins

Question 7

How does in situ hybridization work and the underlying mechanism behind it?

Answer 7

-There is unique mRNA molecule for every polypeptide synthesized by neuron –> mRNA transcript has 4 different nucleic acids linked together in various sequences to form a long strand
-Nucleic acid bind most tightly to complementary nucleic acid
-If sequence is nucleic acid in strand is known –> construct complementary strand (called a probe) that will stick like Velcro to mRNA molecule
-Process that probe bonds to mRNA called hybridization
- Chemically label the probe so it can stick to any complementary mRNA strands, then wash away all the extra probes that have not stuck, finally we search for neurons that contain the label.

Question 8

what are the ways the probes in in situ hybridization chemically tagged?

Answer 8

-make them radioactive, detected by laying brain tissue on sheet of special film sensitive to radioactive emissions, visible as white dots. Digital electronic imaging devices can be used to detect radioactivity –> called autoradiography
-another method, label with brightly coloured fluorescent molecules –> can be viewed directly with microscope –> fluorescent in situ hybridization is aka FISH

Question 9

Which approach helped Loewi and Dale identify ACh as transmitter at many peripheral synapses?

Answer 9

-In some cases, a specific set of cells or axons can be stimulated while taking samples of the fluids bathing their synaptic targets. The biological activity of the sample can then be tested to see if it mimics the effect of the intact synapses, and then the sample can be chemically analysed to reveal the structure of the active molecule.

Question 10

One way to collect the chemicals release by CNS is to use brain slices that are kept alive in vitro… explain this

Answer 10

To stimulate release, the slices are bathed in a solution containing a high K + concentration. This treatment causes a large membrane depolarization, thereby stimulating transmitter release from the axon terminals in the tissue. Because transmitter release requires entry of Ca 2+ into axon terminal, it must also be shown that the release of the neurotransmitter candidate from the tissue slice after depolarization occurs only when Ca 2+ ions are present in the bathing solution.

Question 11

What method enables activation of just one specific types of synapse at a time? and how is it done?

Answer 11

optogenetics, genetic methods are used to induce one particular population of neurons to express light-sensitive proteins, and then those neurons can be stimulated with brief flashes of light that have no effect on the surrounding cells. Any transmitters released are likely to have come from the optogenetically selected type of synapse.

Question 12

Even when it has been shown that a transmitter candidate is released upon depolarization in a calcium-dependent manner, can we be sure that the molecules collected in the fluids was released from the axons terminals, why/why not?

Answer 12

No, because they may have been released as a secondary consequence of synaptic activation. These technical difficulties make the second criterion— that a transmitter candidate must be released by the presynaptic axon terminal upon stimulation— the most difficult to satisfy unequivocally in the CNS.

Question 13

What is the microiontophoresis method used for?

Answer 13

To assess the postsynaptic actions of a transmitter candidate

Question 14

Describe the microiontophoresis method

Answer 14

-Neurotransmitter candidate –>dissolved in solutions –>acquire a net electrical charge.
-A glass pipette with a very fine tip (few micrometres), filled with ionized solution. The tip of the pipette positioned next to postsynaptic membrane of neuron; transmitter candidate ejected in very small amounts by passing electrical current through the pipette.
-Neurotransmitter candidates can also be ejected from fine pipettes with pulses of high pressure. A microelectrode in the postsynaptic neuron can be used to measure the effects of the transmitter candidate on the membrane potential.

Question 15

What happens if iontophoretic or pressure application from microiontophoresis causes electrophysiological changes that mimic effects of transmitter and the other criteria of localisation, synthesis and release are met?

Answer 15

Then the molecule and the transmitter are usually considered to be the same chemical

Question 16

as a rule, no 2 neurotransmitters bind to the same…

Answer 16

receptor, however one neurotransmitter can bind to many different receptors

Question 17

What are the 3 methods that are particularly useful in studying different receptor subtypes?

Answer 17

-neuropharmacological analysis of synaptic transmission
-ligand-binding methods
-molecular analysis of receptor proteins

Question 18

What is an example of neuropharmacological analysis discovering receptor subtypes?

Answer 18

ACh receptors –nicotine receptor agonist in skeletal muscle no responses in heart, muscarine agonist in heart, no response in skeletal muscle.
–>curare antagonist to ACh nicotinic receptors, atropine antagonist to muscarine receptor

Question 19

how many subtypes for glutamate receptors and describe them

Answer 19

AMPA, NMDA and kainate receptors

-glutamate activates all three
-AMPA only acts on AMPA receptors
-NMDA only acts on NMDA receptor
-Kainate only acts on Kainate receptor

Question 20

What is Noradrenaline and GABA subtypes?

Answer 20

noradrenaline - alpha and beta receptor
GABA - GABAa and GABAb

Question 21

What is the ligand binding method?

Answer 21

The technique of studying receptors using radioactively or nonradioactively labelled ligands is called the ligand binding method. Notice that a ligand for a receptor can be an agonist, an antagonist, or the chemical neurotransmitter itself. Specific ligands were invaluable for isolating neurotransmitter receptors and determining their chemical structure. Ligand-binding methods have been enormously important for mapping the anatomical distribution of different neurotransmitter receptors in the brain.

Question 22

What is a ligand?

Answer 22

Any chemical compound that binds to a specific site on a receptor is called a ligand for that receptor

Question 23

what are the 2 groups of receptors proteins?

Answer 23

-transmitter-gated ion channels
-G-protein-coupled (metabotropic) receptors

Question 24

What is Dale’s principle?

Answer 24

that a neuron has only one neurotransmitter –> many peptide-containing neurons violate Dale’s principle

Question 25

What are co-transmitters?

Answer 25

When 2 or more transmitters are releases from one nerve terminal these are co-transmitters – e.g., glycine and GABA

Question 26

What specific enzyme does ACh require for making it? and where is it manufactured?

Answer 26

choline acetyltransferase (ChAT), manufactured in soma and transported to axon terminal –> only cholinergic neurons contain ChAT –> transfers an acetyl group from acetyl CoA to choline (from extracellular fluid)

Question 27

what is the role of the ACh transporter?

Answer 27

Neurotransmitter is concentrated in synaptic vesicles by the actions of a vesicular ACh transporter

Question 28

What is the rate-limiting step in ACh synthesis?

Answer 28

the transport of choline into the neuron

Question 29

What is AChE?

Answer 29

acetylcholinesterase, degradative enzyme, secreted in cleft, degrades ACh into choline and acetic acid

Question 30

What is the amino acid tyrosine a precursor to?

Answer 30

structures called catecholamines
-dopamine
-noradrenaline
-adrenaline

Question 31

What is tyrosine hydroxylase (TH)

Answer 31

contained in all catecholaminergic neurons –> first step in catecholamine synthesis, the synthesis of tyrosine to dopa
-TH is rate limiting for catecholamine synthesis

Question 32

What is the precursor to dopamine and what does it use to convert into DA?

Answer 32

Dopa, uses enzyme dopa decarboxylase to convert dopa into DA

Question 33

What is the precursor to noradrenaline and what does it use to convert into noradrenaline?

Answer 33

Dopamine, uses enzyme called dopamine beta-hydroxylase (DBH)
- created in synaptic vesicles

Question 34

What is the precursor to adrenaline and what does it use to covert it into adrenaline?

Answer 34

noradrenaline, uses enzyme phentolamine N-methyltransferase (PNMT)
- synthesised in cytosol, NA made in vesicles and released in cytosol to convert into adrenaline

Question 35

How are catecholamines removed from cleft?

Answer 35

selective reuptake back into axon terminal via Na+ dependent transporters

Question 36

What happens after uptake of catecholamines?

Answer 36

Can be reused or broken down by action of monoamine oxidase (MAO) –> found on outer membrane of mitochondria

Question 37

Describe serotonin (5-HT)

Answer 37

-amine
-derived from amino acid tryptophan
-relatively few serotoninergic neurons
-important for regulation of mood, emotional behaviour and sleep

Question 38

describe the synthesis of serotonin.

Answer 38

-first step, tryptophan converted into 5-hydroxytryptophan (5-HTP) by enzyme tryptophan hydroxylase
-second step, 5-HTP converted to 5-HT by enzyme 5-HTP decarboxylase
-limited by availability of tryptophan

Question 39

how is 5-HT remove from cleft? and then what?

Answer 39

by reuptake by transporter –> can be reused or broken down by MAO

Question 40

What are the main amino acids that serves as neurotransmitters?

Answer 40

-glutamate (Glu)
-glycine (Gly)
-gamma-aminobutyric acid (GABA)

Question 41

What are glutamate and glycine synthesised from?

Answer 41

glucose and other precursors by actions of enzymes that exist in cells

Question 42

What is GABA derived from?

Answer 42

glutamate, key synthesizing enzyme is glutamic acid decarboxylase (GAD)

Question 43

how are the amino acid transmitters removed from cleft? and then what?

Answer 43

selective reuptake into presynaptic terminals and glia, by Na+ dependent transporters, then GABA is metabolized by enzyme GABA transaminase

Question 44

What is adenosine triphosphate (ATP)?

Answer 44

-key molecule in cellular metabolism – also transmitter
- directly excites neurons by gating cation channels
-binds to purinergic receptors
-following release from synapses, ATP degraded by extracellular enzyme yielding adenosine

Question 45

What are endocannabinoids (endogenous cannabinoids)?

Answer 45

-small lipid molecules
-released from postsynaptic and act on presynaptic terminals
-this communication called retrograde signalling thus they are retrograde messengers
-serve as feedback system to regulate conventional forms of transmission

Question 46

describe the structure of nicotinic ACh channel at neuromuscular junction

Answer 46

-pentamer, amalgam of five protein subunits arranged like staves of barrel to form a single pore through membrane
-4 different types of polypeptides are used as subunits for the nicotinic receptor, α, β, γ, and δ
-mature channel is made form α2βγδ (2 alpha one of each of others)
-one binding site to each alpha subunit –> simultaneous binding of ACh to both sides are required for channel to open

Question 47

describe the structure of nicotinic ACh receptor on neuron

Answer 47

-pentamer, made up of α3β2

Question 48

What does the nicotinic ACh, GABAa and glycine receptor have in common?

Answer 48

all pentameric complexes of subunits

Question 49

describe the glutamate channel

Answer 49

-tetramer (4)
-M2 region does not span the membrane, instead hairpin that both enters and exits from inside membrane

Question 50

describe amino-acid gated channels

Answer 50

-mediate most fast synaptic transmission in CNS

-several properties distinguish them from one another and define their functions within brain
–The pharmacology of their binding sites describes which transmitters affect them and how drugs interact with them.
–The kinetics of the transmitter binding process and channel gating determine the duration of their effect.
–The selectivity of the ion channels determines whether they produce excitation or inhibition and whether Ca 2+ enters the cell in significant amounts.
–The conductance of open channels helps determine the magnitude of their effects

all of these properties are direct result of molecular structure of channels

Question 51

which glutamate subtypes mediates bulk of brains fast excitatory transmission?

Answer 51

AMPA- and NMDA-gated channels –> kainate receptors not fully understood

Question 52

What are AMPA-gated channels permeable to?

Answer 52

Na+ and K+, most not permeable to Ca2+

Question 53

how do NMDA-gated channels differ from AMPA?

Answer 53

(1) NMDA-gated channels are permeable to Ca 2+
(2) inward ionic current through NMDA-gated channels is voltage dependent

Question 54

What happens when NMDA-gated channels open?

Answer 54

-Ca 2+ and Na + enter the cell (and K + leaves)
-at normal negative resting membrane potentials, the channel becomes clogged by Mg 2+ ions, and this “magnesium block” prevents other ions from passing freely through the NMDA channel. –Mg 2+ pops out when the membrane is depolarized, which usually follows the activation of AMPA channels at the same and neighbouring synapses.
-Both glutamate and depolarization must coincide before the channel will pass current. This property has a significant impact on synaptic integration at many locations in the CNS.

Question 55

What mediates most inhibition in CNS?

Answer 55

GABA mediates most, glycine mediates most of the rest

Question 56

What do GABAa and glycine receptor gate?

Answer 56

a chloride channel

Question 57

What do benzodiazepines and barbiturates do?

Answer 57

when GABA is present benzodiazepines increase frequency of channel opening and barbiturates increase duration of channel opening

Question 58

What are the steps of G-protein couple receptors action?

Answer 58

(1) binding of the neurotransmitter to the receptor protein,
(2) activation of G-proteins
(3) activation of effector systems

Question 59

what is the structure of G-protein couple receptors?

Answer 59

-consist of a single polypeptide containing seven membrane-spanning alpha helices.
-Two of the extracellular loops of the polypeptide form the transmitter binding sites. Structural variations in this region determine which neurotransmitters, agonists, and antagonists bind to the receptor.
-Two of the intracellular loops can bind to and activate G-proteins. Structural variations here determine which G-proteins and, consequently, which effector systems are activated in response to transmitter binding.

Question 60

Describe the G-protein mode of operation

Answer 60

1. Each G-protein has three subunits, termed α, β, and γ. In the resting state, a guanosine diphosphate (GDP) molecule is bound to the Gα subunit, and the whole complex floats around on the inner surface of the membrane.
2. If this GDP-bound G-protein bumps into the proper type of receptor and if that receptor has a transmitter molecule bound to it, then the G-protein releases its GDP and exchanges it for a GTP that it picks up from the cytosol.
3. The activated GTP-bound G-protein splits into two parts: the Gα subunit plus GTP and the Gβγ complex. Both can then move on to influence various effector proteins.
4. The Gα subunit is itself an enzyme that eventually breaks down GTP into GDP. Therefore, Gα eventually terminates its own activity by converting the bound GTP to GDP
5. The Gα and Gβγ subunits come back together, allowing the cycle to begin again

Question 61

What is the subdivisions of G-proteins?

Answer 61

Gs stimulatory and Gi inhibitory

Question 62

What are the 2 types of ways G-proteins exert their effect?

Answer 62

-binding to G-protein-gated ion channels and to G-protein-activated enzymes (second messenger cascades)
-G-protein-gated ion channel binding aka shortcut pathway because doesn’t involved other chemical intermediaries (or membrane-delimited pathway)

Question 63

Describe the G-protein-gated ion channels (aka the shortcut pathway)

Answer 63

-βγ subunits migrate laterally along the membrane until they bind to the right type of potassium channel and induce it to open.
-30-100 msec for responses
-localised, cannot move very far, thereby only close channels can affect it
-referred to as membrane-delimited pathway because all action occurs within membrane
-(e.g., muscarinic receptors in heart take shortcut pathway)

Question 64

Describe the second messenger cascades

Answer 64

-trigger elaborate series of biochemical reactions, often ends in activation of other “downstream” enzyme that alter neural function
-between first enzyme and last there are several second messengers –> this process called second messenger cascades`

Question 65

describe the noradrenaline β receptor and cAMP

Answer 65

-cAMP second messenger cascade initiated by activation of noradrenaline β receptors
- begins with β receptor activating the stimulatory G-protein, Gs, which proceeds to stimulate the membrane bound enzyme adenylyl cyclase.
-Adenylyl cyclase converts ATP to cAMP. The subsequent rise of cAMP in the cytosol activates a specific downstream enzyme called protein kinase A (PKA).

Question 66

what is the push-pull method and how is it used in cAMP inhibition?

Answer 66

-means one to stimulate and one to inhibit
-activation of the second type of noradrenaline receptor called alpha-2 receptor, leads to activation of Gi (inhibitory G-protein). Gi suppresses the activity of adenylyl cyclase (converts ATP to cAMP), and this effect can take precedence over the stimulatory system

Question 67

describe how activation of various G-proteins can cascades branches

Answer 67

-Activation of various G-proteins can stimulate phospholipase C (PLC), an enzyme that floats in the membrane-like adenylyl cyclase.
-PLC acts on a membrane phospholipid, splitting it to form two molecules that serve as second messengers: diacylglycerol (DAG) and inositol-1,4,5triphosphate (IP3).
-DAG, a lipid-soluble, stays within the plane of the membrane where it activates a downstream enzyme, protein kinase C (PKC).
-At the same time, the water-soluble IP3 diffuses away in the cytosol and binds to specific receptors on the smooth ER and other membrane-enclosed organelles in the cell.
-These receptors are IP-3 -gated calcium channels, so IP-3 causes the organelles to discharge their stores of Ca 2+.

Question 68

What can elevations in cytosolic Ca2+ trigger?

Answer 68

widespread and long-lasting effects. one effect is the activation of the enzyme calcium-calmodulin-dependent protein kinase (CaMK)

Question 69

What is phosphorylation?

Answer 69

The process of protein kinases transferring phosphate from ATP floating in cytosol to proteins

Question 70

Consider example of Beta type of noradrenaline receptors on cardiac muscle in terms of subsequent rise in cAMP, describe it

Answer 70

rise in cAMP activates PKA, which phosphorylates the cell’s voltage-gated calcium channels, this enhances activity, more Ca2+ flows and heart beats stronger

Question 71

What do protein phosphatases do?

Answer 71

act rapidly to remove phosphate groups. The degree of channel phosphorylation at any moment therefore depends on the dynamic balance of phosphorylation by kinases and dephosphorylation by phosphatases.

Question 72

what are the advantages of G-protein-coupled receptors?

Answer 72

-signal amplification, activation of one can lead to activation of many ion channels
-signal over distance
-sites for further regulation
-generate long-lasting chemical changes in cells

Question 73

what is divergence?

Answer 73

ability for one transmitter to activate more than one subtype of receptor and cause more than one type of postsynaptic response

Question 74

What is convergence?

Answer 74

multiple transmitters each activating their own receptor type, can converge to influence the same effector system