M&R Session 5

Question 0

What happens at the nerve terminal?

Answer 0

Depolarisation –> opens V-G calcium channels –> calcium influx –> release of neurotransmitter

Question 1

Which channels are found in the nerve terminal?

Answer 1

V-G sodium
V-G potassium
V-G calcium

Question 2

What is the difference between intracellular and extracellular calcium concentration?

Answer 2

10,000 fold

Question 3

Describe the structure of a V-G calcium channel.

Answer 3

Very similar to V-G sodium channels
Four repeats each consisting of 6 transmembrane domains
Porphyrin alpha subunit
Only one needed for channel formation

Question 4

What type of blockers act on L-type V-G calcium channels?

Answer 4

Dihydropyridines

Question 5

Describe the subunit composition of calcium channels.

Answer 5

Porphyrin alpha subunit associated w/other subunits which fine tune properties and allow correct regulation of activity

Question 6

How does calcium influx cause transmitter release?

Answer 6

Calcium influx –> binds to synaptotagmin –> brings vesicles close to plasma membrane –> snare complex makes fusion pore –> transmitter released through pore

Question 7

What is synaptotagmin?

Answer 7

A protein which brings vesicles close to plasma membrane

Question 8

How does increasing intracellular calcium affect transmitter release?

Answer 8

Increases

Question 9

What affect does an increase in the number of action potentials to the nerve terminal have?

Answer 9

Increases pulses of transmitter released

Question 10

How many subunits does a V-G calcium channel have?

Answer 10

5; incl. 2 alpha subunits

Question 11

Where are nicotinic AChR found?

Answer 11

NMJ

Fast synaptic receptors

Question 12

What feature of nAChR allows them to be used in fast synaptic receptors?

Answer 12

They allows fast depolarisation

Question 13

How is an nAChR activated?

Answer 13

2 ACh molecules bind causing a conformational change that opens channels

Question 14

What does the nACHR in an NMJ try to achieve with the membrane potential?

Answer 14

To reach -10 mV therefore causing depolarisation of the skeletal muscle fibre

Question 15

How selective is the sodium-potassium channel?

Answer 15

Not very - equally permeable to both so ion movement is determined by equilibrium potential

Question 16

What happens to the sodium-potassium channel at a membrane potential of -10 mV?

Answer 16

Reversal voltage is met
No net flow of charge
Current through channel reverses

Question 17

What causes the end-plate potential?

Answer 17

ACh action on nAChR

Question 18

How does decreasing extracellular calcium affect the end-plate potential?

Answer 18

Decreases amplitude

Question 19

What are the sequence of events during neuromuscular transmission?

Answer 19

AP in neurone –> ACh release –> activate nAChR –> brief depolarisation (end-plate potential) –> adjacent sodium channels activated by local spread of charge –> excitation-contraction coupling

Question 20

What are the two types of nAChR blockers?

Answer 20

Competitive

Depolarising

Question 21

What is the mechanism of activation of tubocurarine?

Answer 21

Competitive blocker
Binds to alpha subunit but does not cause a conformational change
Decreases depolarisation without changing ACh amount

Question 22

Can competitive nAChR blockers be overcome?

Answer 22

Yes - vastly increase ACh concentration

Question 23

Which enzyme breaks down succinylcholine?

Answer 23

Plasma cholinesterase

Question 24

Can depolarising nAChR blockers be overcome?

Answer 24

Nope

Question 25

Describe the action of depolarising nAChR blockers.

Answer 25

Binds to alpha subunit –> receptor opens –> no AChE caused degradation –> receptor remains open –> sustained depolarisation –> sodium channels inactivated and receptors desensitised

Question 26

What causes miniature end-plate potentials?

Answer 26

Spontaneous release of ACh vesicles w/out AP stimulus

Question 27

What is the rate of ACh release in a miniature end-plate potential?

Answer 27

~1 quanta per second

Question 28

What is the significance of the miniature end-plate potential?

Answer 28

It can be recorded (but does not reach anywhere near threshold potential)

Question 29

What is myasthenia gravis?

Answer 29

Autoimmune targeting of nAChR

Question 30

How are functional nAChR lost in myasthenia gravis?

Answer 30

Complement mediated lysis

Receptor degradation

Question 31

What measurement can be used to determine myasthenia gravis and what does it show?

Answer 31

End-plate potentials - each quanta released gives a decreased response in comparison to unaffected muscle

Question 32

S/S of myasthenia gravis?

Answer 32

Profound weakness
Muscle weakness increases w/exercise
Muscle fatigue

Question 33

Where are muscarinic AChR found?

Answer 33

NMJ of parasympathetic branch of the ANS

Question 34

Which give a faster response, nAChR or mAChR?

Answer 34

nAChR

Question 35

Summarise the activation of an mAChR in one sentence.

Answer 35

ACh binds to the receptor causing the associated G-protein to split, allowing the alpha G-protein subunit to modify the activity of the target effector

Question 36

Do both nAChR and mAChR use ligand binding?

Answer 36

Yes

Question 37

Why are mAChR slower to initiate a response than nAChR?

Answer 37

They are coupled to G-proteins which trigger a cascade of events in the cell to cause a response. They do not have an ion channel like nAChR

Question 38

What is calcium responsible for?

Answer 38

Bone and teeth integrity, fertilisation, proliferation, secretion, neurotransmission, metabolism, contraction, learning, memory, apoptosis, neurons etc.

Question 39

What is the advantage of having a large inward calcium gradient?

Answer 39

Changes in calcium are rapid w/small amounts of calcium ion movement

Question 40

What are the disadvantages of having a large inward calcium gradient?

Answer 40

Calcium overload is easy

Rapid loss of calcium regulation can lead to cell death

Question 41

How is the calcium gradient set-up and maintained?

Answer 41

Relative impermeability of the plasma membrane
Cell ability to expel calcium
Calcium buffers
Intracellular calcium buffers

Question 42

Which two transporter mechanisms are used to expel calcium across the CSM?

Answer 42

Calcium-ATPase

Sodium/calcium exchanger

Question 43

What is calmodulin?

Answer 43

A high affinity, low capacity trigger protein used for calcium expulsion

Question 44

Name three calcium binding proteins.

Answer 44

Synaptotagmin
Calmodulin
Troponin

Question 45

What factors of calcium binding molecules affect the diffusion of calcium?

Answer 45

Concentration

Saturation

Question 46

What two types of intracellular calcium stores are there?

Answer 46

Rapidly and non-rapidly releasable stores

Question 47

Where are rapidly releasable intracellular calcium stores found?

Answer 47

Sarcoplasmic reticulum

Endoplasmic reticulum

Question 48

What pump is used to release calcium from rapidly releasable stores?

Answer 48

SERCA

Question 49

What does SERCA require?

Answer 49

A low affinity, high capacity binding protein - e.g. Calsequestrin

Question 50

Where are non-rapidly releasing calcium stored found?

Answer 50

Mitachondria

Question 51

How does the calcium gradient across a mitochondria membrane compare to that across the cell membrane?

Answer 51

It is much greater

Question 52

When will mitochondria take up calcium?

Answer 52

When the intracellular concentration is high

Question 53

Why does mitochondrial uptake of calcium have to match energy demand and supply?

Answer 53

It requires ATPases

Question 54

Describe the mechanism of uptake of calcium by mitochondria.

Answer 54

Uniporter uses driving force from respiratory chain hydrogen ion production

Question 55

What are the properties of the uni porter used for calcium uptake in the mitochondria?

Answer 55

Low affinity

High capacity

Question 56

How is the internal calcium concentration elevated and returned to basal levels?

Answer 56

Calcium influx across the plasma membrane
Calcium release from rapidly releasable intracellular stores
Calcium release from non-rapidly releasable intracellular stores

Question 57

Which two channels are involved in influx of calcium across the plasma membrane?

Answer 57

V-G calcium channels

Receptor-operated calcium channels

Question 58

Give some examples of receptors used for receptor-operated calcium channels.

Answer 58

NMDA
AMPA
Glutamate receptors (especially in the brain)
Some nAChR

Question 59

What is the term given to describe receptor-operated calcium channels?

Answer 59

Inotropic channels

Question 60

How do V-G calcium channels operate?

Answer 60

Depolarisation –> conformational change

Question 61

How do receptor-operated calcium channels work?

Answer 61

Ligand/agonist binds –> opens aqueous pore –> calcium can move in

Question 62

Why will mitochondria take up calcium?

Answer 62

They need a high concentration to stimulate mitochondrial metabolism

Question 63

What is the role of mitochondria in calcium regulation?

Answer 63

Buffering
Signalling
Match energy demand and supply
Apoptosis
Altered redox potential

Question 64

By which two methods is the release of calcium from rapidly releasable intracellular stores mediated?

Answer 64

G-protein coupled receptors

Calcium-induced calcium release

Question 65

Describe the mechanism of GPCRs in calcium release from non-rapid stores.

Answer 65

Ligand/agonist binds to GPCR –> turns receptor on –> effector molecules activated –> cellular response

Question 66

Which two effector molecules are stimulated by activation of GPCRs?

Answer 66

Plasma channels

Muscarinic receptors

Question 67

How can the activation of GPCRs lead to different cellular responses in different cells?

Answer 67

Different muscarinic receptors are present in different cells - M1 to M5

Question 68

What is the function of alpha-q once it has split from the 7-transmembrane domain of the GPCR?

Answer 68

It activates phospholipase C which activates IP3 and diacylglycerol

Question 69

What is the action of IP3?

Answer 69

Ligand-gated ion channels found in the sarcoplasmic/endoplasmic reticulum which have a pore permeable to calcium, allowing its efflux from the S/ER to increase cellular calcium levels

Question 70

What is the action of diacylglycerol?

Answer 70

Protein kinase C regulation

Question 71

What molecule do alpha-s and alpha-I have opposite actions on?

Answer 71

Adenyl cyclase

Question 72

What is the mechanism of adenylyl cyclase action?

Answer 72

Produces cAMP –> phosphorylates protein kinase A

Question 73

Where are M3 receptors found?

Answer 73

Walls of the airways

Question 74

What does activation of the M3 receptors cause?

Answer 74

Contraction of smooth muscle in the airways

Question 75

Where is ryanodine derived from?

Answer 75

Plants

Question 76

Where are ryanodine receptors found?

Answer 76

In the sarcoplasmic/endoplasmic reticulum

Question 77

How are ryanodine receptors activated?

Answer 77

Conformational coupling with voltage operated calcium channels
Depolarisation

Question 78

How does calcium exit through ryanodine receptors?

Answer 78

Acts as an agonist –> conformational change –> released

Question 79

How does depolarisation of the T-tubule cause calcium release?

Answer 79

V-G sodium channels open

VOCC open

Question 80

Why are the ryanodine receptors so important for calcium release?

Answer 80

Give explosive release of 85% of calcium

Located directly adjacent to contractile proteins

Question 81

What happens in the cardiac myocyte when calcium levels decrease?

Answer 81

Ryanodine receptor stops
SERCA pumps calcium into stores
NCX reverses –> calcium into T-tubule for minor store

Question 82

What restores normal function of the NCX following decreased calcium levels?

Answer 82

Sodium removal

Question 83

What causes the plateau in the cardiac action potential before repolarisation occurs?

Answer 83

Calcium influx via VOCC

Question 84

What is the role of calcium in muscle contraction?

Answer 84

Bind with tropomyosin and roll it out of the way

Exposes binding sites for cross-bridge recycling

Question 85

How are microdomains formed?

Answer 85

Strategically placed calcium channels allow local variations in calcium levels

Question 86

Why does repetitive signalling need restoration of basal calcium levels?

Answer 86

Too much calcium for too long is toxic

Question 87

How do cells return intracellular calcium concentrations to basal levels?

Answer 87

Use of transient signals

Question 88

What does return of calcium to basal levels require?

Answer 88

Termination of signal
Calcium ion removal
Calcium ion store refilling

Question 89

How are calcium stores refilled?

Answer 89

Recycling of released cytosolic calcium
VOCC
Capacitative/store operated calcium channel

Question 90

Describe the mechanism of recycling released calcium.

Answer 90

In cardiac myocytes effectively release and grab back cytosolic calcium

Question 91

Describe the mechanism of channel led calcium store refilling.

Answer 91

Deleted signal to membrane allows more calcium in

Specific proteins interact to activate the channel

Question 92

What is STIM-ER?

Answer 92

ER membrane located calcium sensor w/motif that binds to calcium which causes a conformational change

Question 93

What is ORAI?

Answer 93

A plasma membrane channel which allows entry of calcium

Question 94

Can channel led calcium store refilling regulate physiological processes?

Answer 94

Yes

Question 95

Is the mechanism of calcium regulation always the same?

Answer 95

No, it may be dependent on cell type and circumstance