6-8

Question 1

What is an action potential?

Answer 1

A rapid, reversible change in membrane potential consisting of a depolarisation followed by a repolarisation

Question 2

Excitable cells

Answer 2

Muscle cells

neurones

Question 3

why use squid giant axons?

Answer 3

up to 1mm in diameter so hard to damage

Question 4

What is a nerve cells resting potential?

Answer 4

-70mV

Question 5

what are the phases of an action potential?

x 4

Answer 5

Rising phase
Repolarising phase
Hyper-polarisation
After hyper-polarisation

Question 6

What happens in the rising phase of an AP?

-the hodgekin cycle

Answer 6

Based on an increasing membrane permeability to Na+

• initial depolarisation above threshold causes some voltage gated Na+ channels to open
• then Na+ enters axon down electrochemical gradient
• further depolarisation towards E(Na)
• causing more VG channels to open and cycle keeps going
• Positive feedback

Question 7

What is an overshoot?

Answer 7

The membrane potential rises above 0mV and goes towards E(Na) and this shows that the axon doesn’t just become permeable to everything

Question 8

What happens in the repolarising phase?

Answer 8

• Na+ permeability falls as as the channels in-activate

- at a slight delay from the Na VG, the VG potassium channels open and so increase permeability to K+

Question 9

What causes hyper-polarisation?

Answer 9

• the Na+ and now closed but the K+ ones stay open for a few milliseconds later causing more K+ to move in causing more negative than resting potential

Question 10

After hyper-polarisation?

Answer 10

The VG K+ channels close and the permeabilities of Na+ and K+ return to normal and therefore so does membrane potential

Question 11

What do voltage-gated cation channels look like?

Answer 11

• 4 homologous polypeptide domains that form a pore between them
• Each domain made of 6 α-helices segments

DIAGRAM

Question 12

What are the three key characteristics of V-G cation channels?

Answer 12

1. Selectivity
2. Voltage sensitivity
3. Inactivation

Question 13

How are channels selective?

x 2 ways

Answer 13

• pore loops connecting segments 5 and 6 of each domain are the walls of the aqueous pore
• negatively charged amino acids found near both entrances repel anions
• now size, smaller channels for Na+ stop K+ which is too big
• K+ use selectivity filter of four carbonyl oxygen atoms to form bonds with K+ and replace water of hydration
• Na+ cannot form all 4 bonds and so still hydrated is too big to pass through
• snug-fit model

Question 14

How are channels voltage selective?

Answer 14

segment 4 of each domain has positively charged amino acids

- these move towards exterior and so outwards when membrane depolarises as ore negative on outside

Question 15

How do channels go through inactivation?

Answer 15

Most VG inactivate after being open for a period of time

• exact mechanisms differ
• Cue for inactivation is actually the original depolarisation but the process takes longer

Question 16

Na vs K channels?

2 differences apart from ion

Answer 16

1. Na+ channels open more quickly in response to depolarisation that K+
2. Na+ channels inactivate more rapidly too (1-2 msec)

Question 17

How is the behaviour of sodium channels stochastic?

Answer 17

Only a certain probability of a given channel being closed, open or inactive based on membrane potential and immediate history
- still random

Question 18

At what point is the activation threshold?

Answer 18

Where Na+ entry exceeds K+ loss

Question 19

What is the ARP? the absolute refractory period?

Answer 19

the time-period following the beginning of an AP when a second AP cannot be generated no matter how large the stimulus as there are too many inactive channels. (Na+)

Question 20

What is the RRP? The relative refractory period?

Answer 20

The time-period where a second AP can only be elicited with a stimulus of greater amplitude than normal.

Question 21

How does an action potential propagate?

Answer 21

• Na+ come into axon during AP and the positive charge (not the actual ions) will spread in both directions down potential gradient.
• in forwards direction then cause depolarisation as push ions away from outside of axon to make inside negative
• Cause a local circuit
• if backwards can’t cause depolarisation as in ARP

Question 22

What is Edgar Adrian’s All-or-Nothing idea?

Answer 22

As long as the stimulus (original) goes over threshold then AP occurs, if it doesn’t then no AP. So different magnitude stimuli cause same AP provided over threshold

Question 23

What is a myelin sheath

Answer 23

layer of specialised cell membranes wrapped several hundred times around nerve axon

• high resistance and low capacitance

Question 24

Where does myelin come from

Answer 24

In peripheral nervous system it is Schwann Cells but CNA it is oligodendrocytes

Question 25

What are the sections of myelin called?

Answer 25

The myelinated regions are internodes and the breaks are the Nodes of Ranvier (this is where all the sodium channels are)

Question 26

Why does myelin work?

Answer 26

Causes saltatory conduction which is where the local currents are elongated. Makes transmission quicker
- increases length constant λ

Question 27

How do the two adaptations for increased speed of AP work?

Answer 27

picture

Question 28

How does temperature affect transmission?

Answer 28

Higher temperatures cause faster transmission—>kinetics

Question 29

How does making axons wider work?

Answer 29

Reduce resistance and so AP increase speed

Question 30

Resistances present in nerves

Answer 30

• Re = external resistance of extracellular fluid
• Ra = axonal resistance = inversely proportional to axon’s cross sectional are
• Rm = membrane resistance for unit length of axon ( inverse proportion to membrane area and density of background ion channels)

Question 31

What is the length constant?

Answer 31

The distance over which the voltage change caused by the sustained injection of current at position x=0 decays to 1/e (37%) of original value.

Question 32

Why does the voltage change decrease?

Answer 32

leakage of current due to resistance and capacitance.

- so make less leaky or axon wider.

Question 33

What is the decay of the voltage change?

Answer 33

Vx = V0 * (e*(-x/λ))

Question 34

What is the length constant equal to?

Answer 34

λ = sqrt (Rm/Ra)

Question 35

What is τ (time constant)

Answer 35

The time it takes for the membrane potential to rise from baseline to 63% (1-1/e) of its final (when x=λ)

Question 36

What is τ equal to

Answer 36

Vt = Vinfinity (1-(e*(-t/τ)))

where τ = RmCm

Question 37

How do we increase transmission in terms of λ and τ

Answer 37

increase λ and decrease τ

Question 38

What is a synapse?

Answer 38

A specialised region of communication between two cells-> one needs to be an excitable cell

Question 39

What is a gap junction?

Answer 39

An electrical synapse where ionic current can pass directly between two cells. Cells shared cytoplasm.
- like between muscle cells

Question 40

Which is faster? Chemical or electrical synapses?

Answer 40

Electrical. Chemical have a synaptic delay of 0.5 to 2 ms

Question 41

What is the neuromuscular junction?

Answer 41

The point where and α motor neurone with it’s bod in the ventral horn of the spinal cord
- innervates skeletal muscle

Question 42

What is a muscle fibre?

Answer 42

A single muscle cell

Question 43

What is a motor unit?

Answer 43

Where a group of fibres is innervated by same axon and will act together

Question 44

What is another name for a NMJ (neuromuscular junction)?

Answer 44

Moto end-plates

Question 45

What is the neurotransmitter in NMJs

Answer 45

acetylcholine (ACh)

Question 46

Diagram of NMJ

Answer 46

Picture

Question 47

How wide is the synaptic cleft?

Answer 47

50nm

Question 48

What are junctional folds?

Answer 48

Folds in the post-synaptic membrane of muscle cell—>increase surface area

Question 49

How is the ACh released into synaptic cleft?

Answer 49

1. AP reaches terminal bouton
2. Depolarisation causes opening of VG calcium channels on pre-synaptic membrane
3. These close to active zones fo calcium into cell and then interacts with synaptotagmin (calcium sensor)
4. Synaptotagmin promotes interaction between t-SNARE and v-SNARE to cause exocytosis of ACh (roughly 100-300 vesicles)

Question 50

How does ACh cause AP in muscle cell?

Answer 50

1. post-synaptic membrane has high density of NAChR (nicotinic acetylcholine receptors)
2. One ACh molecule binds to each α-subunit to open channel
3. both Na+ K+ can pass (but Na+ higher rate as greater gradient)
4. cause depolarisation of muscle cell membrane

Question 51

Structure of NAChR

Answer 51

ligand-gated ion channel

• in adult mammals it is a pentameric α2βδε structure (subscript 2)
• opened when ACh molecule bind to each of α subunits

Question 52

2 Examples of toxins can affect the NMJ and how they work

Answer 52

1. α-latrotoxin-from black widow spider
   - makes membrane unusually permeable to Ca2+ and so over stimulates
2. Tubocurarine
   - block NAChR

Question 53

What are end-plate potentials?

Answer 53

caused by opening of NAChR leads to depolarisation of post-synaptic membrane at about 20-40mV in amplitude and only local

• it stimulates VG sodium channels so only AP if this over threshold
• looks like small hump before depolarisation near NMJ

Question 54

What feature of normal AP do skeletal muscle APs not have?

Answer 54

no hyperpolarisation

Question 55

what are miniature end-plate potentials

Answer 55

around 0.4mV when one vesicle released

• small depolarisation
• in discrete intervals

Question 56

How to stop response at NMJ

Answer 56

Acetylcholinesterase

• breaks ACh into acetate and choline
• acetate diffuse into cells
• choline cannot be synthesised by motor nerve terminal so actively transported back across pre-synaptic membrane
• made back into ACh using acetate from acetyl coenzyme A
• new vesicles from endocytosis
• Ca2+ actively pumped out of cell

Question 57

What is an Excitatory post-synaptic potential?

Answer 57

Small depolarisations of the dendrites that increase the probability that the cell will come to threshold and fire and AP

• often glutamate as transmitter
• increase Na+ entry

Question 58

What is an inhibitory post-synaptic potentials

Answer 58

decrease the probability that the cell experiencing them comes to threshold

• Ofter GABA (brain) or glycine (spinal cord) as transmitter
• usually increase Cl- permeability
• Dont know how decreases chance of getting to threshold

Question 59

Roughly how many synapses can a brain cell have

Answer 59

100,000

Question 60

Where is the AP initiated?

Answer 60

axon initial segment which has a high density of VG sodium channels
- located just after axon hillock

Question 61

How to increase depolarisation

Answer 61

Temporal or spacial summation

Question 62

What does myogenic mean

Answer 62

The type of action potential generated by myocytes (muscle cells)

Question 63

What is the pacemaker of the heart

Answer 63

SAN- Sino-atrial node

Question 64

What is the funny current in myocytes?

Answer 64

The point when Na+ enters—> which is after repolarisation

Question 65

How are AP made in myocytes

Answer 65

funny current causes Ca2+ entry through channels

• causes pacemaker potential and then causes AP when threshold
• AP in SAN cells based on Ca2+ entering through L-type VG channels
• spike is slower and much longer than neuronal AP
• repolarises when calcium channels inactivate and K+ leaves cell through VG delayed rectifier

Question 66

Autonomic nervous system controls slope of pacemaker potential and so controls rater—> what does it not control

Answer 66

The initiation

Question 67

What fibres in the spinal cord make up the peripheral nervous system?

—questionable

Answer 67

The spinal nerves and cranial nerve

Question 68

What is the structure of spinal nerves?

Answer 68

all have a dorsal root, through which sensory axons enter the cord
- and a ventral root through which the motor axons leave

Question 69

What are cranial and spinal nerves split into?

Answer 69

Efferent fibres (leave CNS)
Afferent fibres (sensory)

Question 70

What two roles do efferent fibres have?

Answer 70

1. somatic motor system-> to skeletal muscle

2. Autonomic nervous system (to smooth muscle, cardiac muscle and glands)

Question 71

Where do sensory nerve fibres have their cell bodies?

Answer 71

the dorsal root ganglia

- the axons go on to synapse with grey matter of spinal cord

Question 72

what types of motor neurones supply skeletal muscle?

Answer 72

α motor neurones

Question 73

What happens in a monosynaptic reflex arc?

Answer 73

1. sensory and somatic motor fibres are directly coupled within the spinal cord

Question 74

Where are the cell bodies of α motor neurones located? And where do their axons leave?

Answer 74

the ventral horn of the spinal cord

- axons leave via the ventral root and go directly to skeletal muscle

Question 75

few skeletal muscles are involved in homeostasis. Give two examples

Answer 75

1. Ventilation - involved in control of blood gas concentrations and pH
   - use diaphragm and chest-wall muscles
2. Shivering - body temp control
   - mediated by most skeletal muscles

Question 76

How is smooth muscle innervated?

Answer 76

The autonomic nervous system

Question 77

What three divisions make up the autonomic nervous system?

Answer 77

1. sympathetic
2. parasympathetic
3. enteric

• both 1 and 2 are completely efferent fibres

Question 78

What is the structure of the neurones in the parasympathetic and sympathetic pathways

Answer 78

same

• 1. pre-ganglionic is usually myelinated and has cell body in CNA
     
     2. axon out of CNS to autonomic ganglion
     3. there is has cholinergic synapse with a number of post-ganglionic neurones
     4. cell bodies of these post are in ganglion and axons, usually unmyelinated go to innervate organ in question

Question 79

What is the intermediolateral column?

Answer 79

where sympathetic nerve fibres have their cell bodies and then axon to sympathetic chain ganglia
- pre nerves are short and post are long-go to organs

Question 80

What is the neurotransmitter of the SNS?

Answer 80

ACh which works of NAChR which is different from the NAChR in the NMJ in pre to post neurone

• at organ it releases noradrenaline
  (often co-transmitted with neuropeptide Y or ATP)

Question 81

What are chromaffin cells

Answer 81

cells in the adrenal medulla that release adrenaline

- when ach from preganglionic nerve of SNS

Question 82

What are adrenergic receptors?

Answer 82

the g-coupled receptors that adrenaline and noradrenaline work on
- 2 classes
α and β
both activate both but noradrenaline stimulates α1 and β1 more than adrenaline
- same with 2 for adrenaline

Question 83

What are β-receptors of adrenoceptors coupled with?

Answer 83

Excitory g-proteins which release cAMP as secondary messenger in cell as activate adenylyl cyclase

Question 84

What are the α-receptors?

Answer 84

α2) coupled with inhibitory g-proteins to stop cAMP

α1) works to activate inositol phospholipid pathway via another g-protein

Question 85

Are the PNS and SNS always opposite?

Answer 85

NO
- salivary glands work together

SNS=enzyme secretion
PNS=Liquid secretion

Question 86

PNS nerves

Answer 86

pre = emerge from brain and carried within cranial nerves to target organs
- like vagus nerve (which is a mixed nerve)
-

Question 87

Autonomic control of the heart

Answer 87

Increased - adrenaline and noradrenaline- SNS

decreased by ACh form PNS

• at rest subject to tonic parasympathetic stimulation (PNS)
• from vagus

Question 88

How is heart rate increased?

Answer 88

β1 receptors on SAN cells respond to catecholamines-activate GCPR so increased cAMP

• opening of Na+ and Ca2+
• speed up depolarisation rate
• shorten pacemaker potential

Question 89

What is the pacemaker potential?

Answer 89

slow, positive increase in voltage across the cell’s membrane (the membrane potential) that occurs between the end of one action potential and the beginning of the next action potential.

Question 90

How slow heart down

Answer 90

Vagal ACh works of muscarinic receptors-GCPRs in SAN

• α-subunit inhibits adenylyl cyclase so reduce cAMP (so longer pacemaker potential)
• also βγ subunit opens K+ channels directly and hyperpolarises cell to -70mV rather than -60mV so longer to get to threshold

Question 91

SNS on blood vessels

Answer 91

• noradrenergic fibres activate α subunits and maintain basal level of vasoconstriction=sympathetic tone
• changing tone can constrict or dilate vessel
• in skeletal muscle via β2 causes vasodilation (adrenaline at normal levels)

Question 92

How can PNS affect blood flow?

Answer 92

Only in some areas like salivary glands

- very little influence of total peripheral resistance, unlike SNS

Question 93

Fight or flight response

x 7

Answer 93

1. heart rate increases
2. exercising muscle arterioles dilate and others constrict
3. Bronchioles dilate
4. Glucose mobilised
5. Gastrointestinal activity put on hold
6. Pupils dilate
7. Hair stands on end

Question 94

How to end autonomic effects

Answer 94

1. most noradrenaline from SNS is taken back via presynaptic membrane transporter (uptake 1 mechanism)
2. Circulating adrenaline taken up into many different tissues (by uptake 2 transporters) enzymatically degraded in the cells
   - end products secreted in urine (1-3 min half life)
3. ACh rapidly broken down by acetylcholinesterase in synaptic cleft