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Neuropharmacology > GABA neurotransmission > Flashcards

GABA neurotransmission Flashcards

1
Q

Name 2 fast inhibitory neurotransmitters in the brain and list their receptors

A 
•	GABA
GABAA, GABAB
•	Glycine
GlyR
o	No metabotropic Gly receptor known
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2
Q

GABA(A)R pharmacology - agonists:

A
  • GABA
  • Muscimol from Amanita muscaria
  • Gabadoxadol
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3
Q

GABA(A)R pharmacology - antagonists:

A

• Bicuculline (competitive)
• GABAzine (competitive)
• Picrotoxin (non-competitive; combination of picrotoxinin and picrotin)
U93631

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4
Q

GABA(A)R pharmacology - modulators:

A
  • Benzodiazepines (BZDs)
  • Barbiturates
  • Neurosteroids
  • Anaesthetics
  • Alcohol
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5
Q

Where are GABA(A)Rs found?

A

Not on dendritic spines - usually found in the membrane of the postsynaptic neuron. They signal in the normal mechanism for an ionotropic receptor

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6
Q

Explain feed-forward inhibition, using a diagram

A

• Excitatory neuron stimulates GABAergic and Glutamatergic neurons –> EPSP, then IPSP (caused by GABA release)

diagram: https://neurology.mhmedical.com/data/books/1049/kan_ch2_f008.png

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7
Q

Using a diagram, explain feedback (recurrent) inhibition

A

• 2nd excitatory cells feeds back onto itself
• Is ‘doubly inhibited’
• There are 3 synapses; 2 of them inhibitory
Diagram: https://neurology.mhmedical.com/data/books/1049/kan_ch2_f008.png

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8
Q

Using a diagram, explain inhibition of inhibition and what it leads to

A

–> excitation (overall)
GABA neuron inhibits GABA neuron – cancels out release of GABA from 2nd neuron; prevents inhibition ∴ allows excitation

Diagram: https://neurology.mhmedical.com/data/books/1049/kan_ch2_f008.png

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9
Q

Explain why inhibitions are needed

A 
GABA antagonists induce seizures
	Epilepsy in rats
	Give PTZ --> seizures
	∴ GABA agonists can be used as anticonvulsants 
	Zebrafish assay
•	Tetanus toxin --> lockjaw/tetanus
o	Without inactivation with formaldehyde --> muscle spasm
o	Stops inhibitory synapses from working
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10
Q

Explain how strychnine achieves its inhibitory effects and their consequences:

A 
Antagonises GlyRs
	Alkaloid
	Comes from Quaker’s buttons
	Inhibits synapses of spinal inhibition of motor neurons --> spasms
	Renshaw cell:
	Glycinergic 
	 Sits in spinal cord
	α muscle neurons excite these; Renshaw cells feed back and inhibit motor neurons (FF inhibition via Gly)
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11
Q

With the aid of a diagram, explain Glycine receptor structure and subunit composition

A 
‘Cys-loop’ family members
	4 TMDs
	long intracellular loop connects TM3 and 4
	either:
	5 α subunits
	Or 2α + 3β

diagram: https://www.researchgate.net/figure/Structure-of-the-glycine-receptor-A-Membrane-topology-of-the-a-subunit-with-the-four_fig1_11904296

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12
Q

List the features of a glycine receptor

A 
Ligand-gated ion channel
	5 subunit genes:
	α1-4
	No α4 in humans
	β1
	Large single channel conductance – 50-110pS
	Anion pore; selects for Cl- ions
	Activated by Glycine (β-alanine + taurine)
	Potently inhibited by:
	Strychnine
	RU5135
	Pore can be blocked by picrotoxinin, as with GABAAR
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13
Q

Explain GABA structure (chirality), synthesis, transport, and receptors

A

• GABA has no chiral centre – no L/D form
• Not usually on dendritic spines
• Synthesized by GAD67 (in cell) and GAD65 (nerve terminal)
o GAD = Glu decarboxylase
• GAT1 and 3 transport GABA into cells
• VGAT gets GABA (and Gly) into vesicles
• GABAA,B,C receptors bind GABA
• GABA function terminated by diffusion and uptake by GATs

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14
Q

With the aid of a diagram, explain GABA(A)R structure and potential subunit composition, as well as the 3 most common conformations

A 
Ligand-gated ion channel assembly
	Channel is inherent to receptor
	Ligand-binding enables channel opening
	Pentameric - α,β,γ
	19 subunits:
	α1-6
	β1-3
	γ1-3
	δ
	ϵ
	π
	θ
	ρ1-3
	Most receptors have 2α, 2β, 1γ/δ subunit
	Other conformations include:
α1β2γ2, α1βγ2
	different subunits = different localisations – α6 is only in the cerebellum

• In the transmembrane domain the terms “plus side”, which is formed by parts of TM2 and TM3 of the principal subunit; and “minus side”, formed by parts of TM2 and TM1 of the complementary subunit, are also commonly used

Diagram: https://upload.wikimedia.org/wikipedia/commons/3/3a/GABAa_receptor.gif

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15
Q

Use a diagram to show where on the GABA(A)R benzodiazepines bind, and explain their potential effects

A

Bind α-γ subunit interface

Don’t work on α4,6-containing receptors

Classically, are PAMs of GABA-mediate channel activation:
They increase frequency of bursts of channel opening
Are anticonvulsants; promote sleep; reduce anxiety
Can be very addictive
Temazepam sleeping pills
Drug users tend to prefer short-acting and intermediate-acting barbiturates. The most commonly used are amobarbital (Amytal), pentobarbital (Nembutal), and secobarbital (Seconal). A combination of amobarbital and secobarbital (called Tuinal) is also highly used. Short-acting and intermediate-acting barbiturates are usually prescribed as sedatives and sleeping pills. These pills begin acting fifteen to forty minutes after they are swallowed, and their effects last from five to six hours.

Are also BDZ-site inverse agonists
Anxiogenic
Seizure-promoting
E.g. DCM

And competitive antagonists:
Flumazenil
Treats overdose

Some BDZ-site ligands have subtype selectivity:
Can lead to more focused therapeutic use with fewer side-effects
α1,5 –> sedation (ataxia, amnesia)
α2,3 –> anxiolytic (stop anxiety)
Barbiturates and (neuro)steroids
Different binding site to BDZs:
PAMs at [low]
Activate receptors directly at [higher]
Tend to increase duration of bursts of channel opening
Sodium thiopental/pentobarbital – used in lethal injections (as with midazolam)

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16
Q

Briefly summarise the structure and pharmacology of GABA(B) and GABA(C) receptors

A

GABAB:
GPCR
Signal via intracellular G-proteins to 2nd messenger cascades
Obligate dimer

GABAC:
AKA GABAA-ρ
Insensitive to bicuculline and GABAzine (unlike GABAA)
Structurally similar to GABAA – Cys-loop pentameric Cl- channel

17
Q

How many types of GABAergic cells are there?

A

• There are many kinds of GABAergic cell types
o 3 types of pyramidal cell are accompanied by at least 21 classes of interneuron in hippocampal CA1 area
• Basket cells mediate FF and FB inhibition
o Depends on which branch of the basket cell is being activated

18
Q

Explain the immediate potentiating effect of GABA(A)R-mediated synaptic transmission, how this can be blocked and enhanced, and why this has no effect on the long, slow portion.

A

GABAAR-mediated synaptic transmission is the most common form of GABAergic synaptic signalling
–>IPSP; short-lived. Completely blocked by bicuculline, GABAzine, picrotoxin. Enhanced by BDZs, barbiturates, neurosteroids

Some GABAergic IPSPs are longer, and biphasic
Blocking GABAARs does not block the long, slow portion of the IPSP
GABABRs mediate this long slow IPSP via G-protein linked Inwardly Rectifying K+ (GIRK) channels
Initially identified by pharmacology – a receptor which was activated by GABA, not blocked by GABAAR antagonists and activated by a selective antagonist:
Baclofen:
Hyperpolarises postsynaptic cells via increased K+ conductance (∴ causes IPSP)
Reduces NT release from presynaptic terminals (via inhibition of VDCCs)
Reduces production of cAMP by adenylyl cyclase
∴ coactivation of GABAARs and GABABRs causes long-lasting, biphasic IPSPs

19
Q

With the aid of a diagram, describe GABA(B)R structure and the effect of knocking out the subtypes

A

• Formed from 2 interacting proteins
o Both proteins have ‘classic’ GPCR structure
 7TMDs
o GABA binds GABABR1; G-proteins interact with GABABR2
o 2 N-terminal splice variants of GABABR1
o KO of either Receptor subtype blocks all GABAB-type responses

diagram: https://www.google.com/url?sa=i&url=https%3A%2F%2Fwww.semanticscholar.org%2Fpaper%2FTargeting-GABAB-receptors-for-anti-abuse-drug-Phillips-Reed%2Fa049643bb25c8631e0267a40182e6d310d1f31fb%2Ffigure%2F0&psig=AOvVaw3ajPOqHuT8aaF5_1c8tkgU&ust=1577221072651000&source=images&cd=vfe&ved=0CAIQjRxqFwoTCIDWj8DUzOYCFQAAAAAdAAAAABAO

20
Q

List 2 GABA(B)R agonists

A

• Agonists:
o GABA
o Baclofen
o SKF-97541

21
Q

List 2 GABA(B)R antagonists

A

• Antagonists:
o Saclofen
o CGP-55845
o SCH-50911

22
Q

List 2 GABA(B)R positive allosteric modulators

A

o Rac BHFF

o GS-39783

23
Q

Name a GABA(B)R negative allosteric modulator

A

o CLH304a

24
Q

Which signalling pathway are GABA(B)Rs linked to? What downstream effects does this have?

A

Are Gi/o linked, ∴ GABABRs:
Inhibit cAMP production
Activate GIRK K+ channels –> long-lasting IPSP
Inhibit VDCCs

25
Q

Where are GABA(B)Rs found on a synapse? What are the subsequent effects?

A

• Are found pre- and post-synaptically
o Presynaptic GABABRs can inhibit VDCCs on the presynaptic neuron (autoreceptor), inhibiting further GABA release from the presynaptic neuron
o Presynaptic GABABRs can depress Glu release

26
Q

What effect can GABA(B)Rs have on CA1 pyramidal cells?

A

GABABRs can mediate short-term plasticity in CA1 pyramidal cells:
If 2 identical stimuli are given in rapid succession (30-1000ms of each other), the 2nd IPSP is smaller
This is because the first GABA ‘wave’ inhibits the cell’s VDCCs ∴ i[Ca2+] is decreased
∴ Ca2+ less available; so can’t cause cytoskeletal rearrangement and vesicle release
∴ less GABA is able to be released, so the second IPSP is smaller
GABABR antagonists can block this!

27
Q

What do neurogliaform cells produce?

A

• Neurogliaform cells (NGFs) produce GABAB-mediated IPSPs
o GABAB-mediated synaptic responses normally come from these
• Applying a GABAAR antagonist blocks the short, fast portion of the biphasic response
o Leaves the long, slow portion – GIRK-mediated
o Shown with paired cell recordings (recording pre- and post-synaptic cells at the same time)
• NGFs can affect other NGFs in this manner too! (inhibition of inhibition)
• NGFs utilise GABAergic volume transmission (sprinkler, not hosepipe-like wired transmission)
o This can activate astroglia

28
Q

Explain GABA(B)R-mediated heterosynaptic short-term plasticity

A

• Glu synapse with GABAB
• You can get released GABA to bind to and activate presynaptic GABABRs on Glutamatergic nerve terminals
• Activity at 1 synapse can transiently affect activity at another synapse
o Due to GABA ‘spill-over’ during conditioning (short-term plasticity)
o GABA diffuses between synapses; accesses GABABR on presynaptic neuron of glutamatergic nerve terminal  heterosynaptic short-term plasticity
• GABABR antagonist removes this depression – Glu release remains the same when GABABR antagonist is applied

Neuropharmacology (16 decks)

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