UMA’s summaries Flashcards
What is the retinal cellular pathways and the cells involved?
• VERTICAL PATHWAY (light to photoreceptor > bipolar cell > ganglion cell)
• HORIZONTAL (horizontal & amacrine cells)
• INTEGRATOR NEURONS: bipolar, horizontal, amacrine, ganglion
What are receptive fields and how do they present in the retina?
• Each neuron of retina covers an area in your field of vision.
• Receptive field = area in space where appropriate stimulus will modify activity of a neuron
• Towards the periphery - receptive fields larger & less specific
• Deeper layers of retina - more complex receptive field
How do photoreceptors activate and how do they converge?
• Photoreceptors are always hyperpolarised by light & depolarised by dark
• 130 million photoreceptors converge to RCG
• 1:1 at fovea, 500:1 periphery
What are rods? How do they work?
• Periphery
• Smaller than cones
• Scotopic conditions - no colour
• Hyperpolarise to DIM light - saturate quickly
• There are more rods than cones - more redundancy
• Spatial summation - photons don’t need to go to a specific rod to activate ganglion cell
Cone photoreceptors:
• Larger - 3 types: S, M L wavelength
• Fovea
• Hyperpolarise to brighter light (photopic)
• Less sensitive - saturate 2 log units slower
• Cones are only ‘on’ (hyperpolarising)
• Cones do not have centre surround organisation
What are the types of horizontal cells? What is their purpose ?
• Anatomical types: H1, H2, H3
• Receive input from R+C and make adjustments
• Provide surround information to bipolar cells
• Connect laterally
• INHIBITORY in nature, inhibit other cells selectively suppress signals (lateral inhibition)
• Purpose: only highest intensity output gets through which increases contrast and visual definition
• Communication in OPL, bodies in INL
What are Bipolar cells?
• Receive signals from photoreceptors
• Hyperpolarisation of photoreceptor = depolarisation of bipolar cell (inhibitory nature of synapse between them)
• Dendrites in OPL, axons IPL
• CONVERGENCE - signal neuron (bipolar or horizontal) collects info from more than one photoreceptor.
What are receptive fields?
• Circular
• Centre/surround, on/off
What are on centre cells?
• Light applied to centre = excitatory effect = depolarised (less negative)
• Light falls on surround = inhibitory effect = hyperpolarised (more negative)
• (cone in synapses with hyperpolarised, ON-centre bipolar cell depolarises)
What are off centre cells?
• Light applied to centre = inhibitory effect = hyperpolarisation
• Light falls on surround = excitatory effect = depolarisation
• Inhibited by light, excited by darkness
What are amacrine cells?
• Receive signals from bipolar cells & are involved in regulation/integration of bipolar and ganglion cells
• Functions of integrating ganglion cell output
• Excited by bipolar cells
What are ganglion cells?
• Do not absorb light - process neural information
• GC long axons = optic nerve
• End of intra-retinal processing, beginning of output to V1
• Small 1 million % contribute little/nothing to vision - neural information - circadian rhythms, pupils
ganglion receptive fields:
• Tightly fixed in space
• Mostly linear - wont response to light outside area of receptive field
• They do not have orientation selectivity
• Concentric
• ON/OFF centre - respond by increasing or decrease frequency of action potentials
(NOT by de/hyperpolarisation)
• DEPOLARISATION of bipolar cell = EXCITES ganglion cell = INCREASED firing rate of action potentials
• HYPERPOLARISATION of bipolar = INHIBITS ganglion cell = DECREASED firing rate
How are ganglion cells classified?
• Within the retina there are ganglion cells, which are classified based on their structural and anatomical physiological basis.
What are the two stream pathways?
• Y CELLS = Midget cells (P-CELLS) = > Parvocellular layer of LGN = > Ventral stream = Detail
• X-CELLS = Parasol (M-CELLS) = > Magnocellular layer of LGN = > Dorsal stream = Where
Y/P cells:
• Central retina - fovea
• Linear summation
• 80%
• Slow, sustained response (slow for detail)
• Small receptive fields (midget = small)
• Colour opponency, image detail
Best way to remember Parvocellular pathway
• Midget = small receptive fields for small detail
• P-cells = parvo = pardon = what stream, v in parvo = ventral
• Need more of these small cells so we can see lots of detail - detailed work in fovea
• Parvocellular pathway caries info from small RCGs > LGN (layers 3,4,5,6) > V1
What are X-cells/M-Cells?
• More peripheral retina
• Non-linear summation
• 10%
• Fast, transient response
• Parasol = large dendritic fields, complex
• Movement, achromatic
Tips to remember magnocellular pathway
• Parasol cells = large receptive field like a parasol
• M-cells = magna = motion = dorsal MD makes u move about so motion)
• Large receptive fields as motion over large area in periphery
• Magnocellular pathway carries info from large RCGs > LGN (layers 1&2) > V1
What are K cells/W cells?
• Don’t fit into X/Y categories
• Non-concentric receptive fields
• More common in lower animals
What experiment was done to map out ON-OFF regions of RF ganglion cells?
• Anaesthetised animal set up with viewing screen, where small lights can he flashed
• Extracellular single unit electrode inserted into animals optic nerve, which records action potentials
• Electrode connected to amplifier, which feeds amplified signals an oscilloscope, for viewing the signal, an audio amplifier for listening and recording action potentials
• Small spots of light were flashed at various locations and their direct effect on cells spontaneous firing rate was assessed
• If firing rate increased when light is flashed, that location is considered ON part of receptive field
• It firing rate decreased, considered OFF part of receptive field
From recording these locations, one can construct a receptive field
Why is retinal processing needed?
RETINAL PROCESSING is needed to adjust the gain of the retina (make pupil bigger), and code information for efficient transmission to the brain.
What are the 6 steps in post retinal processing?
- GANGLION CELLS leave retina at OD
- ON crosses at chiasm (nasal cross to opposite sides, temporal remain uncrossed)
- Axons are now part of the OPTIC TRACT
- Most axons from optic tract terminate in LGN (visual part of thalamus)
- Axons can also project to SUPERIOR COLLICULUS in midbrain (rapid eye movement), SUPERCHIASMATIC NUCLEUS of the hypothalamus for circadian rhythms. - Most axons from LGN > OPTIC RADIATIONS
- OPTIC RADIATIONS > PRIMARY VISUAL CORTEX (cerebral cortex)
a. Axons with info about superior VF = occipital lobe via Meyers loop
b. Axons with info about inferior VF = parietal cortex
Describe the LGN
LGN (LATERAL GENICULATE NUCLEUS)
• Located in the posterior end of the thalamus
• Gets info from optic tract
• Sends input to V1
• LGN is a relay station for all sensory signals on their way to the cerebral cortex
• Introduces coding efficiencies by cancelling out redundant info from the retina
• Helps visual system focus on most important info & can direct us to points in space
What are the layers of the LGN and the differentiations?
• 6 layers (laminae) - each layer contains a retinotopic map of half the VF
- Layers 1,4,6 = contralateral eye (opposite eye - nasal input)
- Layers 2,3,5 = ipsilateral eye (same eye - temporal input)
• M CELL bodies in layer 1+2 = large (magnocellular bodies, parasol) bottom = where
• P CELL bodies layers 3,4,5,6 = small (parvocellular bodies, midget) top = detail
• More dorsal (top) LGN = controls how much of the signal gets to V1 - has inhibitory circuits
Tips for remembering which layers of LGN are magno and same eye input:
• Magno = first 2 layers which are at the bottom
• Input from same side (uncrossed) = 2+3 = 5 which is right so its not crossed (ipsilateral)
What is the receptive field of the LGN??
• Large, concentric ON/OFF
• Stronger surround inhibition = cells amplify differences in luminance
midbrain’s structures important for visual processing:
• SUPERIOR COLLICULUS = orientation movements of eye towards objects, inter/motor sensory eye movements of head/eyes - no pattern analysis. Contains the retinotopic map.
- Receptive field= simple, ill-defined, centre surround, surround is strictly inhibitory
• Red nucleus, basal ganglia, cerebellum = coordinate movement
What, and where is the striate cortex?
• Striate cortex = part of the cerebral cortex which is responsible for processing visual information
• Location = calcarine fissure in occipital lobe
• The whole visual cortex takes up all of occipital lobe, inferior temporal lobe, parts of the parietal and frontal lobes (divided into ~ 30 interconnected regions after V1)
Where does the striate cortex receive inputs, and what does it analyse?
• Input to V1 - receives input directly from LGN
• Analyses = lines, spatial frequencies, direction, orientation (yet we perceive complex 3D images)
How is the retinotopic map represented in v1?
• V1 contains a retinotopic map
• Retinotopic organisation fovea represented at back of brain - overrepresented
• peripheral VF = more anterior location
• upper VF = more ventral
Columnar architecture in V1
• Orientation, directional selectively etc - eventually all this information goes to the extra striate cortex where images are formed from information which is integrated in the primary visual cortex.
• Electrode moves vertically, more neurons have same selectivity
Ocular dominance columns
• Cells from LGN layer will project to target cells in layer 4 (monocular) of V1
• Groups of cells form alternating stripes in layer 4
• Above & below layer 4 = most cells are driven binocularly
• Move electrode across the cortex, cells respond to left eye inputs, then binocular, then right eye, then binocular, then left eye etc
