L12 - correction of faulty neural circuits Flashcards

1
Q

what is channelrhodopsin

A

non-selective channel, stimulated with light, causing channel to open

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2
Q

what light is channel rhodopsin stimulated by

A

blue light 460nm

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3
Q

what happens if switch of the light

A

closes faster when stimulated with 360nm

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4
Q

what happens when switch on the light - channelrhodopsin

A

neuron is depolarised and sufficient to trigger a strike

the spike occurs everytime the neuron is stimulated

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5
Q

halorhodopsin

A

stimulated by yellow light 570nm. causes hyperpolarisation of the membrane

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6
Q

what is the problem with using rhodopsin channels in humans

A

don’t have the technologies to do so - express them in viruses which may not be safe

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7
Q

what can be used instead of channelrhodopsin

A

2 small molecules - optical isomers of each other

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8
Q

important parts of the small molecules

A

maleimide - binds to a specific channel
azobenzene - functions to change depending on stimulation of light
quaternary ammonium - serves as a block of the channel

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9
Q

at what light does the trans isomer turn into the cis isomer

A

380nm

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10
Q

at what light does the cis isomer turn back into the trans isomer

A

500nm

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11
Q

what does the trans isomer do?

A

block the channel - when turned into cis isomer, the block is removed

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12
Q

how does the small molecule work ?

A

enters the TRPV1 channel and acts on the channels from the inside of the cell

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13
Q

why is it important that it works inside the cell

A

stays inside the cell longer

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14
Q

what is the GABA receptor important for

A

regulating the overall excitability of the NS

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15
Q

what causes epileptic seizures

A

overexitability of neurons in the brain

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16
Q

what wavelength can activate the GABA receptors

A

380nm light

17
Q

what occurs when the GABA receptors are activated

A

hyper polarise the cells and remove hyperexcitabiltiy of the neurons

18
Q

what is retinitis pigmentosa

A

a disease in which the field of view becomes smaller and smaller until the patient becomes blind

19
Q

what causes retinitis pigmentosa

A

retinal degeneration which starts with the dying of the photoreceptors - rods and cones
as it progresses other cells in the retina become degernated (bipolar and ganglion cells)

20
Q

what is the treatment for retinitis pigmentosa

A

artificial retina or gene therapy

can use electrodes or tools to stimulate the visual system

21
Q

problems with using electrodes to stimulate neurons

A

chronic implantation of electrodes in the brain/retina will cause degeneration of the tissue around the electrodes as electrodes may hear up and kill surrounding neurons

22
Q

what are the 2 areas needed to stimulate to cure blindness

A

retina - for retinitis pigmentosa

visual cortex - when optic nerve didn’t develop/destroyed

23
Q

how are the retina and visual cortex stimulated

A

either by electric stimulation of channelrhodopsin and halorhodopsin

24
Q

problems with artificial stimulation of retina

A

stimulates ganglion cells but not photoreceptors or bipolar cells

25
Q

what are the 2 main classes of ganglion cells

A

parvocellular and magnocellualr

26
Q

size of parvocellular dendritic tree

A

small

27
Q

size of magnocellular dendritic tree

A

large

28
Q

what type of receptive fields to ganglion cells have

A

centre surround organisation

29
Q

what is a centre surround organisation

A

if stimulate ganglion cell in centre of the receptive field will have increase / decrease in spiking rate. if stimulate outside of receptive field will get opposite result in spiking rate

30
Q

what happens when switch of the light stimulating a ganglion cell

A

decrease in spiking rate

31
Q

what occurs when stimulate halorhodopsin in photoreceptors

A

get hyperpolarisation - leads to decrease in release of glutamate from the synapses

32
Q

what does intact centre surround organisation of RGCs in retinitis pigmentosa show

A

shows that can restore the basic properties of the cells

33
Q

what is intact during retinitis pigmentosa

A

diversity
center surround organisation
direction selectivity

34
Q

what are the 2 ways to control seizures

A
  • use halorhodopsin expressed in excitatory cells - hyperpolarise the excitatory cell

use channelrhodpsin - depolarise inhibitory cells - so when stimulate the cell with blue light they release more GABA

35
Q

what tools are used to inject a virus to treat seizures

A

ontogenetic tools

36
Q

questions needed to ask to treat

A

where to express optogenetic tools
where is the seizure of the origin
excitatory or inhibitory neurons