Synaptic Plasticity

Question 1

What is M=NPQ?

Answer 1

Formula for synaptic strength

P= Probability of release of a synaptic vesicle after an action potential (ranges from 0 to 1)
Q= Amplitude of the post-synaptic potential (PSP) resulting from the release of one vesicle.
N= number of vesicle release spots.
M is term for size of synaptic strength

Question 2

What 3 factors can influence the probability of vesicle release?

Answer 2

Amount of Calcium entering with an action potential: More calcium, more release

Number of primed vesicles

Coupling of Calcium entry to fusion of the vesicle; More coupling, more release

Question 3

What can be inferred from a readily releasable pool procedure (RRP)?

Answer 3

The RRP can be measured using an independent way of releasing vesicles, such as hypertonic shock that disrupts the membrane.
This releases all vesicles that are primed

PROVIDES A MEASURE OF P

Question 4

How can P be modulated?

Answer 4

PPF, PPD, PTP, modulatory neurotransmission (e.g. STF in aplysia)

Question 5

What determines whether paired pulse facilitation or depression occurs?

Answer 5

PPF occurs if initial probability of release is low
PPD occurs if initial probability of release is high

Question 6

How can PPF be used to probe whether a change in synaptic strength results from a change in P or Q?

Answer 6

If there is increased synaptic strength but no change in PPF, it means that the underpinning change comes from Q, not P

Question 7

If there is an increase in PPF, this means p _____
If there is a decrease in PPF, this means p _____
If there is no change in PPF, one can argue that p is _____.

Answer 7

If there is an increase in PPF, this means p decreased
If there is a decrease in PPF, this means p went up
If there is no change in PPF, one can argue that p is unchanged.

Question 8

What is PPF due to?

Answer 8

residual calcium from previous firing

Question 9

What sensor is mediating PPF? Why?

Answer 9

Syt 3 and 7 bc. sensitive to small amounts of calcium.

Question 10

True or false: In PPF, calcium binding to just the Syt 7/Syt 3 releases VS.

Answer 10

False: Calcium binding to just the Syt 7/Syt 3 complexin site makes the vesicle more primed, but is not sufficient for fusion (need calcium binding to Syt 1,2,9 site as well)

Question 11

What variable mainly influences PPD?

Answer 11

Time

Question 12

True or false: The higher the probability of release, the more pronounced depression will be.

Answer 12

True, as more of the RRP will be secreted.

Question 13

Is post-tetanic potentiation also relying on residual calcium?

Answer 13

Yes, indirectly

Question 14

What are three calcium sensors involved in mediating PTP?

Answer 14

Munc13
PKC
Synaptotagmin 3

BUT THESE ARE CELL SPECIFIC

Question 15

What does Syt3/7 increase during stimulus?

Answer 15

RRP

Question 16

What is EGTA?

Answer 16

high affinity calcium sensory competing with Syt3 for clacium -> high affinity like Syt 7!!!

Question 17

How can Munc13 increase RRP in PTP?

Answer 17

Munc13 binds calmodulin = calcium sensitivity -> calcium binding would accelerate Munc13’s ability to remove the inhibitory effect of Munc18 on syntaxin = increase in RRP

Question 18

How can unc-13 be regulated to increase priming? Is it important for PTP?

Answer 18

DAG can bind to C1 domain of unc-13 and increase priming

PKC also phosphorylates both munc13 and munc18, promoting priming

YES

Question 19

What is the time course of involvement of Munc13 and Syt3 during PTP?

Answer 19

During stimulus train Syt is important
Munc13 important afterward bc. binds calcium for longer

Question 20

In terms of homeostasis, why are PPF and PTP important?

Answer 20

increasing probability of release when the neuron is firing is an attempt to keep p constant during a long train of action potentials

Question 21

Short-term facilitation in aplysia is related to cellular habituation or sensitization?

Answer 21

Sensitization

Question 22

Short-term facilitation is caused by an increase in P or Q?

Answer 22

P

Question 23

Explain the cascade resulting in STF (from shock to release of transmitter)

Answer 23

Shock -> release of 5-HT -> G-prot -> cAMP -> PKA -> closing of K+ via phosphorylation -> slow repolarization after AP -> broader AP -> increase calcium influx -> more transmitter release

Question 24

True or false: Amplitude of miniature EPSPS (minis) are most often probes for postsynaptic changes

Answer 24

Yes, but sometimes vesicle content can change (e.g., changing uptake rate)

Question 25

RRP is increased after STF, what does that indicate?

Answer 25

In addition to be caused by a larger calcium influx, STF is also caused by increase in priming

Question 26

Is short term depression acting directly on RRP? How can it be reversed?

Answer 26

No, RRP is intact in depression -> therefore caused by a loss in calcium secretion coupling, which might be due to an untethering of the calcium channel and SV

PKC can restore calcium depression coupling at depressed synapses

Question 27

What properties are required of a physiological basis for memory

Answer 27

Persistence
Input Specificity
Associativity

Question 28

What kind of stimulation does it take to induce LTP?

Answer 28

Tetanic stimulation (100Hz) or Theta-Burst stimulation

Question 29

What molecular structure mediates the associativity of LTP?

Answer 29

NMDA receptors (coincidence detection)

Question 30

Why does LTP require calcium? And what allows the influx of calcium?

Answer 30

NMDA receptors allow Ca influx ->activation of CamKII

Question 31

How does LTP decrease failure rate?

Answer 31

By upregulating AMPA receptors in the postsynaptic neuron

Question 32

What is the evidence that LTP is not caused by increase in P?

Answer 32

Only increase in AMPA response (more vesicles released would not discriminate which receptor gets activated)

Question 33

How can LTP “unsilence” AMPA postsynaptic responses?

Answer 33

In synapses that express no AMPA receptors, expression of AMPA via NMDA increases the responsitivity of the postsynaptic neuron by 100% from 0%.

Question 34

What channel property of AMPA and NMDA allows to record NMDA currents almost entirely independently from AMPA currents?

Answer 34

AMAP currents shut off rapidly, while NMDA currents last longer -> simply wait for the AMPA currents to be off to record NMDA currents WITH magnesium block and CHANGING input voltage to separate NMDA (+40) and AMPA (-60) currents

Question 35

What is the pathway by which LTP leads to the insertion of more AMPA receptors

Answer 35

NMDA -> CamKII -> PKC -> substrate phosphorylation -> AMPA insertion

Question 36

How can you measure AMPA-R insertion during learning?

Answer 36

Use AUDITORY FEAR CONDITIONING = one-trial learning that takes place in the lateral amygdala where auditory inputs from the thalamus project

Need a way to distinguish newly inserted AMPA-Rs from previously present AMPA-Rs ->
ELECTROPHYSIOLOGICAL TAGGING – viral overexpression of GluA1 results in the formation of GluA1 homotetrameric AMPA- Rs that exhibit inward rectification. Normally AMPA-Rs are heterotetramers and non-rectifying.

Question 37

True or false: Preventing new GluA1 insertion was sufficient to prevent learning during fear conditioning.

Answer 37

True.

Question 38

How is L-LTP induced?

Answer 38

Multiple spaced trains of high-frequency stimulation

Question 39

What intracellular process does L-LTP require?

Answer 39

CREB activation and dendritic protein synthesis

Question 40

By which protein kinase is CREB phosphorylated by?

Answer 40

PKA

Question 41

L-LTP shows synapse specificity, how possible since in involves protein synthesis?

Answer 41

synaptic tagging:

L-LPT induces expression of “goodies” (plasticity related proteins)
+
Synapse would be tagged by initial AMPA trafficking event
= L-LTP

Question 42

What characterizes a successful synaptic capture in the case of L-LTP?

Answer 42

Strong L-LTP induction at synapse A = prod. of goodies + tag
Weak E-LTP induction at synapse B = no prod. of goodies + tag
Goodies expressed from strong L-LTP induction at synapse A will be capture BOTH by the tags of synapses A AND B

Question 43

What kind of stimulation provokes LTD?

Answer 43

Low freq. stimulation

Question 44

Is the downstream pathway of LTD similar to LTP?

Answer 44

Calcium is also needed in LTD, but afterward phosphatases and not kinases are the effectors

Question 45

How is LTD ultimately implemented?

Answer 45

Endocytosis of AMPA receptors

Question 46

What determines whether LTP or LTD occurs?

Answer 46

Intracellular concentration of calcium (det. by freq. of stimulation)
Kinases haev low. calcium affinity = requires a lot of calcium = intense stimulation = LTP
Phosphatases have high calcium affinity = requires a little bit a calcium = weak stimulation = LTD

Question 47

Which phosphatase is known to play a role in LTD?

Answer 47

Calcineurin

Question 48

Under which more realistic conditions than trains of stimulus are LTP and LTD happening? What is the name of the process?

Answer 48

Spike timing-dependent plasticity coordinates pre-synaptic activity with post-synaptic firing

Question 49

Pre- before post- results in ____
Post- before pre- results in ____

Answer 49

Pre- before post- results in LTP
Post- before pre- results in LTD

Question 50

What property of action potential is particularly important for spike timing-dependent plasticity?

Answer 50

Back propagation to the dendrites (synapse location)

Question 51

If 100% is the theoretical sum of calcium entry from EPSP and AP when measured independently, how much calcium do you get when:

AP comes before EPSP
EPSP comes before AP

Answer 51

AP (post) comes before EPSP (pre) = 50% = LTD
EPSP (pre) comes before AP (post) = 150% = LTP

Question 52

Are LTD postsyn or presyn at mossy fiber synapses? Provide respective pathway.

Answer 52

Presyn.
LTP = presyn. influx of Ca = activation of AC1 -> cAMP -> PKA = increase release prob.
LTD = glu retroactivating presyn. mGluR2 -> inhibition of AC1 -> cAMP -> PKA = decrease release prob.

Question 53

Is LTD at the cerebellar synapse (PC-PF) postsyn. or presyn.? Provide pathway. What is counter-intuitive about this mechanism?

Answer 53

Postsyn.
mGluR activation postsyn. -> PLC -> PKC -> phosphorylation (COUNTER-INTUITIVE) of AMPA receptors C-tails -> internalization of AMPAr

Question 54

Endocannabinoids usually increase or decrease transmitter release? Are they acting pre- or post-synaptically?

Answer 54

Endogenous cannabinoids are released presynaptically and act retrogradely on CB1 receptors to generate different forms of synaptic depression:

depolarization-dependent suppression of inhibition (DSI)
depolarization-dependent suppression of excitation (DSE)
LTD

Question 55

How is CB1 activation preventing presyn. transmitter release?

Answer 55

CB1 G prot. blocks calcium entry pre syn.

Question 56

Name one blocker of CB1r.

Answer 56

Rimonabant.

Question 57

What is the goal of homeostasis of neural activity?

Answer 57

Reach a target firing rate that lays between seizure and cell death

Question 58

With neuronal cultures, how can you demonstrate activity homeostasis?

Answer 58

Adding TTX, washing off = increase in spike activity
Adding bicuculline (GABA antagonist silencing inhibition, so increasing excitability), washing off = decrease in spike activity

Question 59

Is non-Hebbian plasticity (homeostasis) driven by change at specific synapses? On what molecular mechanism does it rely on? How does synaptic scaling relate to that?

Answer 59

No, whole circuit modification

Large scale trafficking of AMPA receptors

Synaptic scaling = all synapses of a regulated network conserve their relative synaptic strengths and are all regulated in the same manner (increase, decrease)

Question 60

Are NMDA receptors necessary for homeostatic plasticity?

Answer 60

No

Question 61

In inhibitory synapses, what receptors get regulated?