Neurotransmitters & synapses Flashcards

1
Q

How are neurotransmitters packaged into vesicles?

A
  • enzymes that are needed to make small molecule transmitters are synthesized in the cell body and move to presynaptic terminal
  • substrates transported to pre synaptic terminal
  • transported into vesicles
  • large neuropeptide precursors are synthesised in the cell body packaged into vesicles & transported along microtubule
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2
Q

How are neurotransmitters released?

A
  • small vesicles docked near ca2+ channels
  • AP invades terminal
  • Ca2+ channels open & Ca2+ enters
  • vesicles fuse with presynaptic membrane and release contents
  • vesicle membrane recycled
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3
Q

Describe neurotransmission

A
  • AP arrives at nerve terminal which opens Ca2+ channels
  • Ca2+ entry causes vesicle fusion and transmitter release
  • receptor channels open, transmitter binds to receptor and causes Na2+ ion channel to open
  • Na2+ enters the postsynaptic cell and vesicles recycle
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4
Q

what is an axosomatic synapse?

A

synapse between the axon of one neuron and the body of another

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5
Q

what is a axodendritic synapse?

A
  • synapse between dendrite of one cell and a dendrite of another
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6
Q

what is a axo-axonic synapse?

A
  • type of synapse, formed by one neuron projecting its axon terminals onto another neuron’s axon
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7
Q

What is a mixed cation ion channel?

A
  • channel that for example lets Na+ enter and K+ leave
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8
Q

what is an excitatory postsynaptic potential? EPSP

A
  • Postsynaptic potential that makes the postsynaptic neuron more likely to fire an action potential
  • temporary depolarization of the postsynaptic membrane
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9
Q

Compare EPSP vs IPSP

A
  • excitatory (EPSP) = depolarization of postsynaptic cell - sufficient depolarisation could produce AP, eg glutamate in CNS binding to AMPA receptors
  • Inhibitory (IPSP) = hyperpolarisation or repolarisation of postsynaptic cell , prevents action potential, eg GABA binding to receptors
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10
Q

whats the difference between GABA a and GABA b?

A
  • IPSP, due to Cl- entering the cell (GABA a type) or K+ ions leaving the cell (GABA b type)
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11
Q

what happens if EPSP’s summate (adding up together) ?

A
  • EPSP’s can summate to cause the cell to depolarise sufficiently to allow the cell to fire an action potential
  • causes the cell to communicate with the next nueron
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12
Q

compare and contrast spatial summation vs temporal summation

A
  • Spatial - input to different dendrites
  • Temporal - repetitive input onto the same terminal in a dendrite
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13
Q

what are the important steps for transmission at a chemical synapse?

A
  1. neurotransmitter synthesis either in presynaptic terminal or in the neuronal cell body
  2. concentration and packaging of neurotransmitter molecules in preparation for release
  3. release of neurotransmitter into synaptic cleft
  4. Binding of neurotransmitter by post synaptic receptor molecules
  5. termination of neurotransmitter action preparing the synapse for subsequent (coming after something in time , following ) release of neurotransmitter
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14
Q

what is the priming stage of neurotransmitter recycling?

A
  • vesicles in the reserve pool undergo priming to enter readily reversible pool
  • involves assembly of SNARE complexes
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15
Q

What are snare proteins and what is their function?

A
  • large protein family
  • they mediate vesicle fusion - the fusion of vesicles with target membrane or membrane bound compartments
  • examples : synaptotagmin & synaptobrevin
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16
Q

what is the function of synaptotagmin?

A
  • functions as a calcium sensor
  • entering Ca2+ binds to synaptotagmin and Ca2+ bound synaptotagmin catalyses membrane fusion
17
Q

what are the two types of postsynaptic receptors?

A
  1. Ionotropic
  2. Metabotropic -
18
Q

What is the difference between ionotropic and metabotropic receptors?

A
  • they are both ligand gated transmembrane proteins
  • ionotropic receptors change shape when they are bound to a ligand - channels open and ions flow in eg nAchR
  • metabotropic receptors do not have a channel that opens or closes, instead they are linked to a ‘ G protein’, ligand binds to receptor which activates G protein which activates a secondary messenger
19
Q

what is a secondary messenger?

A
  • A secondary messenger is a chemical whose function is to go and activate other particles
20
Q

How is a neurotransmitter removed after release?

A
  • uptake by glial cells
  • enzymatic degradation eg acetylcholinesterase
  • internalization by postsynaptic process
21
Q

explain the pathway steps of neurotransmitters

A
22
Q

what is an example of a fast ionotropic receptor?

A
  • Nicotinic Ach receptors
  • pentameric receptor - 5 subunits
  • Ach binds to the 2 alpha subunits which causes conformational change which ooens ion channel
23
Q

what are the 2 ionotropic glutamate receptors?

A
  • AMPA
  • NMDA
  • excitatory throughout CNS
24
Q

what is LTP induction?

A
  • long term potentiation
  • induction of the NMDA receptor is a chemical synapse in the brain - substantial rise in calcium ion conc in postsynaptic cell
25
Q

what are the main inhibitory neurotransmitters?

A
  • Glycine - mainly spinal chord ( activates Cl- channels)
  • GABA released by many inhibitory CNS inter neurons
  • GABA a - receptor activation opens Cl- channels ( Cl- enters and causes hyperpolarisation)
  • GABA b -metabotropic receptor opens K+ channels - K+ exits cell and causes hyperpolarisation
26
Q

what are neuropeptides?

A
  • chemical messengers made up of small chains of amino acids that are synthesized and released by neurons