Fixing faulty neural circuits

Question 1

What is channelrhodopsin selective for?

Answer 1

Cations (Na+, Ca2+, H+, K+)

Question 2

What happens when channelrhodopsin opens?

Answer 2

The cell depolarises

Question 3

How is channelrhodopsin activated?

What wavelength?

Answer 3

By blue light

460nm

Question 4

How can expressing ChR in different brain areas do?

Answer 4

• Modify behaviour

- Help to recover the function of a specific brain area

Question 5

What travels through halorhodopsin?

Answer 5

Chloride ions (Cl)

Question 6

What is HR activated by?

What wavelength?

Answer 6

Yellow light

570nm

Question 7

What happens when HR is activated?

Answer 7

Hyperpolarisation of the cell

Question 8

What can HR be used in?

Answer 8

Correction in the circuitry when the brain is OVER EXCITABLE (eg. treatment for epilepsy)

Question 9

What can be used to fix faulty neural circuits instead of ChR?

What is the structure of these compounds?

Answer 9

Small organic compounds

Structure - double bond and a part that binds to an ion channel

Question 10

What happens when shine light onto the small organic compounds?

How?

Answer 10

Change the configuration of the compound from trans- to cis- configuration

By rotation around the double bond

Question 11

How are small organic compounds administered when correcting faulty neural circuits?

Answer 11

They are injected into the eye or brain

Question 12

What do the small organic molecules do in trans- configuration?

Cis-configuration?

Answer 12

Block the channel in trans- configuration

Don’t block the channel in cis- configuration

Question 13

How do small organic molecules act on the target channels?

Which is more prolonged?

Answer 13

1) From the OUTSIDE of the membrane

2) From the INSIDE of the membrane - more prolonged as they don’t diffuse away

Question 14

How do the small organic molecules act from the inside of the membrane?

Answer 14

They go through channels (TRPV1 or P2XR)

Question 15

Are the methods of correcting neural circuits with ChR specfic?

HR?

Small organic molecules?

Answer 15

Non of them are very specific

Question 16

Describe the photocontrol of GABA receptors

Answer 16

• Substitution of the part of a compound that binds to the ion channel with a LIGAND for the receptor
• The configuration of the compound can be changed using a specific wavelength of light
• In ONE configuration: ligand will bing and activate the channel
• In the OTHER configuration: ligand doesn’t activate the channel (ligand is AWAY from the binding site of the GABA receptor)

Question 17

What happens when GABA receptors are activated?

What is this used for?

Answer 17

Hyperpolarisation of the membrane

Used to calm down the brain

Question 18

How can photocontrol be used on other receptors?

What does the outcome depend upon?

Answer 18

Outcome depends on the channel and expression of the channel:

• AchR = hyperpolarisation
• Na channels = hyperpolarise
• Glutamate R = hyperpolarise or depolarise depending upon the glutamate channel and the cell

Question 19

What can optical stimulation be used for?

Answer 19

To cure blindness

Question 20

What is retinitis pigmentosa?

Answer 20

Where the visual field becomes smaller and smaller until the patient cannot see anything

Question 21

What is the main cause of RP?

Answer 21

Photoreceptors dying - therefore no transduction

Question 22

What drug can be used to stop photoreceptors from dying?

Answer 22

No drugs can be used to stop them dying

Question 23

What can be used to reverse the effects of RP?

Answer 23

Artificial retina, containing:

• Light activated electrodes
• ChR
• HR

Question 24

With an artificial retina, when is it best to stimulate the retina itself?

Answer 24

Mostly for retinitis pigmentosa

Question 25

With an artificial retina, when is it best to stimulate the visual cortex?

Answer 25

When the optic nerve is damaged or not formed

Question 26

Why is it important to activate as early as anatomically possible in the visual pathway?

Examples?

Answer 26

The further downstream in the pathway, the more difficult it becomes:

• Even at the level of the retina - large diversity of neurons that perform complex computations
• Different ganglion cells have different functions and project to different brain areas

Question 27

When are motion sensitive retinal ganglion cells active?

Answer 27

Only when there is motion

Question 28

What are the disadvantages of activating the artificial retina with electrodes?

How can this be overcome?

Answer 28

Disadvantages:
- Electrodes don’t survive for very long (tissue around the electrodes die with time)

• Have to stimulate ganglion cells or cortical cells with electrodes (other cells are more difficult) and these cells are very complex

Overcome by:
- Activating the artificial retina/visual cortex with ChR or HR

Question 29

Why is it easier to activate ganglion cells than bipolar cells/photoreceptors using electrodes?

Answer 29

Ganglion cells face the inner eye

Bipolar cells and retinal cells are the other side of the tissue and are harder to get to

Question 30

Why is it useless to stimulate retinal ganglion cells using electrodes?

Answer 30

Very complicated:
- Different types of ganglion cells (P-type, M-type) that respond to different stimuli

• Each ganglion cell also have centre-surround organisation of their receptive fields
• Also presence of direction selective cells
• Also have different responses to light in different colours

Question 31

How do they cells in the cortex become even more complicated to stimulate using electrodes?

Answer 31

Hypercomplex cells

Question 32

What is the optimal way to stimulate the retina to reconstruct the activity (before suffering with RP)?

Answer 32

Using light to stimulate the DEEPER layers of the retina:

• Bipolar cells
• Remaining photoreceptors

Question 33

How can HR be used to reverse the effects of reinitis pigmentosa?

Answer 33

• Express halorhodopsin in the remains of the photoreceptors
• Illuminate with YELLOW light
• ON cells spike
• OFF cells stop spiking

Question 34

Why is HR expressed in the remaining photoreceptors and not ChR?

Answer 34

Photoreceptors must HYPERPOLARISE in response to light

Question 35

What is seen when the size of the yellow spot on the receptive field is increased? (When there is HR expressed)

Answer 35

• Increase in spike rate
• Until the yellow spot covers the whole of the receptive field, where the response of the ganglion cells gets smaller and smaller, until no activation

Question 36

When HR is artificially expressed, what does moving yellow spots cause?

Answer 36

Activation of halorhodopsin:

- However, some cells respond to movement in one direction (preferred) more and the the other direction (null) less

Question 37

What experiments show that everything past the photoreceptors is still intact?

What does this mean?

Answer 37

The same results are seen as would be in a normal retina when:

• Increase the spot of yellow light
• Use a moving spot of yellow light

Means if stimulate the remains of the photoreceptors - can restore vision to a very large extent

Question 38

Why is stimulating the remains of the photoreceptors a disadvantage?

How can this be overcome?

Answer 38

The remains of the photoreceptors are also likely to degenerate

This can be overcome by:
- Expressing 2 different ion channels very close to the photoreceptors (in the dendrites of bipolar cells?)

OR

• Injecting small organic molecules into the eye

Question 39

What ion channel is expressed next to ON cells?

Answer 39

ChR

Question 40

What ion channel is expressed next to OFF cells?

Answer 40

HR

Question 41

How are ChR/HR expressed in the dendrite of different bipolar cells?

Answer 41

Using specific promoters:

- Different for ON/OFF cells

Question 42

What are the disadvantages of using small organic molecules?

Answer 42

Less specificity

Question 43

What cells is it better the stimulate when trying to recover the function of the retina?

Why?

Answer 43

Bipolar cells

• Less complicated than ganglion cells
• Remaining photoreceptors are likely to continue to degenerate