willow

Question 1

what are the two mechanisms of cartilage production?

Answer 1

a) interstitial growth: from chondrocytes within the cartilage

b) appositional growth: undiff. cells at the surface of the cartilage (perichondrium)

Question 2

describe the intra and extracellular ion concentrations that sets up the cells resting membrane potential.

Answer 2

- Na+ greater outside cell

- K+ greater inside cell

- A- (proteins) greater inside cell

= creates a resting membreane potential: +ve outside, -ve inside

Question 3

how do cells get over asymmetrical ionic charge distribution caused by proteins not being permeable?

Answer 3

• *1. Active Na/K diffusion**
• 3Na+ from intracellular to extracellular
• 2K+ from extracellular to intracelluar

effects:
- high Na+ conc in extracellular space, low intracellular
- high K+ conc in intracellular space, low extracellular
32- results in +ve extraceullar space c.f. intracellluar space: sets up resting membrane potential

• *2. membrane permeability:**
• • K+ (50:1 difference): more +ve charged ions move out of the cell: sets up more -ve charge inside cell. neuron plasma membrane is 50-100 times more permeable to K+ than Na=
• resting membrane potential of cell: approx. -70mV

Question 4

how is resting membrane potential set up?

Answer 4

- passive ionic diffusion

- active ionic diffusion (e.g. Na / K pump)

- Gibbs-Donnan equilibrium (effect):

a) objective: obtain electroneutrality
b) impermeable protein ions: too big to diffuse through: causes asymmetrical distribution of charged ions (Na/K)

Question 5

which ion Na+ or K+ has more passive leaking out / in cell?

what is resting membrane potential of cell?

Answer 5

• K+ (50:1 difference): more +ve charged ions move out of the cell: sets up more -ve charge inside cell. neuron plasma membrane is 50-100 times more permeable to K+ than Na=
• resting membrane potential of cell: approx. -70mV

Question 6

* what is the resting membrane potential a consequence of? * [2]

Answer 6

concentration gradients of ions across the plasma membrane

AND
- relative ion impermeabilities of the membrane

Question 7

how does an AP work?

Answer 7

• resting potential starts at -70mV
• Na+ ions enter cell: depolarisation (more +ve mV). Na+ channels open
• leads to action potential
• 1ms after AP (3), inactivation gate of Na+ close, K+ channels open up: repolarisation (more -ve mV)
• K+ stay open longer than neccessary (4)
• K+ channels close

- Na/K ATPase pump, leak channels and proteins re-establish resting membrane potential

Question 8

explain whats going on at repolarisation of AP

explain whats going on at hyperpolarisation of AP

Answer 8

explain whats going on at repolarisation of AP

• after depol: fires AP
• *- Na channel ions close** (blockage of inactivation gate: ball on chain)
• K channel opens (repolarisation)

= restores intracellular -ve charge

explain whats going on at hyperpolarisation of AP

• **K+ channels stay open
• Na+ channels go back to resting state**

Question 9

explain what absolute v relative refractory periods are

Answer 9

refractory periods:

period time where cell membrane is resetting itself.

- absolute refractory period:

the period of time during which a second action potential absolutely cannot be initiated.

• occurs due to inactivation of Na channels

- relative refractory period:

• period after firing of nerve when partial repolirasation has occurred a greater than normal stimulis / depolarisation can stimulate a second response
• peak of AP will be lower (but still goes over threshold)
• recovering Na channels and open K channels

Question 10

how do local anaesthetics work?

Answer 10

- bind to open Na+ channel: become inactivated

• physically prevent Na+ reopening and generating AP: drugs stablises inactive state
• cant depolarise cell
• pain fibres cant send pain to brain

Question 11

how does resting state -> propogation of an action potention occur of an unmyelinated axon occur?

where is the trigger zone?

Answer 11

continous propogation:

trigger zone: axon hillock / aka axon initial segment

resting state: high conc of Na+ outside cell, extracellular env: +ve. -70mV inside cell

initiation: voltage gated Na+ channel opens: Na+ go to site A. creates a local zone in both extraceullar and intracellular fluid with a sudden change in charge.THEN go to Site B (which is an area of high conc negative charge) and sodium Na+ ions open here

propogation: Na+ at Site B attracted to -ve chrge –> go to site C. Also attracted to site A, but cant go back bc thats an absolute refractory period: only goes in one direction

propogation continues: Na+ go along site D etc. Site A is now region of repolarisation (new AP can occur)

Question 12

how does electrical synpase work?

Answer 12

• AP in presynaptic terminal goes through gap junction channel
• coupling potential

BOTH DIRECTIONS

Question 13

how do different excitatory or inhibitory NT work together / agaisnt each other on post-synaptic cleft.

what is the name for this?

Answer 13

• analogue (aka graded) potentials can arrive at trigger zone together and their sum create a suprathreshold signal to cause an AP

OR

• could get one inhibitory and two excitatory -> summed potentials are below threshold so no AP !

addition of excitatory and inhibtory signals = summation

Question 14

what is temporal summation?

what is spatial summation?

Answer 14

temporal summation

• post synaptic potentials at same syanpse (A&A) occur in rapid succession
• first potential doesnt have time to dissipate: next potentials add to previous once

spatial summation

• multiple postsynaptic potentials from different synapses (A+B) occur same time and add
• alone, EPSP not strong enough to cause AP. reinforce each other = AP.

Question 15

what is temporal summation?

what is spatial summation?

Answer 15

temporal summation

• post synaptic potentials at same syanpse (A&A) occur in rapid succession
• first potential doesnt have time to dissipate: next potentials add to previous once

spatial summation

• multiple postsynaptic potentials from different synapses (A+B) occur same time and add
• alone, EPSP not strong enough to cause AP. reinforce each other = AP.

Question 16

what are two methods that inhibitory post synpatic potentials can cause inhibition? [2]

Answer 16

• K+ permeability increased

OR
- increased Cl- perm.

Question 17

give an example of direct and indirect inhibitory post synaptic pontetial

Answer 17

indirect: Muscarinic ACh receptor:

• G-protein activated
• acts via 2nd messenger

- indirectly opens K+ channel

direct: GABA_A receptor:

• opens Cl- channel

BOTH: = hyperpolarisation

Question 18

what and describe are the two classes of cell surface receptor types for synapses?

Answer 18

ligand gate ion channels:

• opens pore for ions
• very fast
• aka ionotropic

G-protein coupled receptors (GPCR)

• activated receptor activates G proteins that affects enzymes
• metabotropic
• slow
• can have bigger effect

Question 19

describe basic overview of glutamate G-protein coupled receptor response?

Answer 19

G-protein coupled receptor –> G protein comple (intracellular) –> enzyme (+/-) –> 2nd messenger

its the second messenger which causes varied responses:

• e.g. cAMP released: inhibitory

- IP3 or DAG released: excitatory

Question 20

why do you need more ionotropic transport proteins cf. GPCRs?

Answer 20

GPRC: secondary messengers amplify signals to downstream target molecules - can need just one ligand binding to one GPCR

Question 21

how does receptor modulation by NTs occour?

Answer 21

receptor modulation by other NTs:

- NTs influence accumulation of opposite NTs on post-synaptic membrane

e.g. ionotropic glutamate receptor fires excitatory response BUT also feedback to GABA receptor and causes to disperse (and vice versa)

causes a balance of inhib and excitatory systems.

Question 22

what is tonic adaptation?
what is phasic adaptation?

Answer 22

Tonic receptors adapt slowly and inform about the presence and strength of a stimulus.

phasic receptors adapt rapidly