Behavioral Neuroscience Lecture 9 PDF

Summary

This document covers lecture notes on vision, part of a course called Introduction to Behavioral Neuroscience (PSYC 211). It discusses sensation, perception, sensory neurons, sensory transduction, photoreceptors, and the neural transduction of light.

Full Transcript

Introduction to Behavioral Neuroscience

PSYC 211
Lecture 9 of 24 – Vision (part 1 or 2)
Chapter 6-1, 6-2 (p173-188)

Professor Jonathan Britt
Questions? Concerns? Please write to [email protected]
 SENSATION VERSUS PERCEPTION

Sensation refers to how cells of the nervous system detect stimuli in the
environment (such as light, sound, heat, etc.), and how they
transduce (convert) these signals into a change in membrane
potential and neurotransmitter release.

Perception refers to the conscious experience and interpretation of sensory
information.
 SENSORY NEURONS

Sensory neurons are specialized cells that detect a specific category of
physical events, such as

– the presence of specific molecules
smell, taste, nausea, pain
– the presence (or absence) of physical pressure
touch, stretch, vibration, acceleration, gravity, balance, hearing, thirst, pain
– the temperature
heat, cold, pain
– the pH of a liquid (whether it is acidic or alkaline)
sour taste, suffocation, pain
– electromagnetic radiation (light)
vision

Some non-human animals have other senses, such as the ability to
detect electrical and magnetic fields, humidity, and water pressure.
 SENSORY TRANSDUCTION
Sensory neurons have specialized receptors that transduce sensory stimuli into
a change in membrane potential.

Sensory neurons come in all shapes and sizes.

Many sensory neurons do not have axons or action potentials,
but they all release neurotransmitter.

Sensory neurons that do not have action potentials release neurotransmitter
in a graded fashion, dependent on their membrane potential. The more
depolarized they are, the more neurotransmitter they release.
 PHOTORECEPTORS

Photoreceptor The sensory neurons responsible for vision.
cells These cells transduce the electromagnetic energy of visible light
into a change in membrane potential, which affects how much
neurotransmitter they release. These cells do not have action
potentials.

Opsins Light-sensitive proteins.
The opsins in photoreceptor cells are metabotropic receptors.
They are only sensitive to light because they bind a molecule of
retinal, which changes shape in response to light. The change in
the shape of retinal is what activates this metabotropic receptor.

Retinal Small molecule (synthesized from vitamin A) that attaches to the
opsin proteins in the photoreceptor cells in our eyes.
The retinal molecule is technically what absorbs the
electromagnetic energy of visible light that allows us to see.
 The two configurations of the retinal molecule

light

enzyme
+ ATP

retinal molecule

opsin protein
(embedded in the membrane
of photoreceptor cells)
When retinal absorbs a wavelength of visible light, it
activates the opsin protein (a metabotropic receptor).

This launches an intracellular g protein signaling
cascade that changes the membrane potential of the
photoreceptor cell, affecting how much
neurotransmitter it releases.
 NEURAL TRANSDUCTION OF LIGHT

4 types of photoreceptor cells contribute to our conscious perception of vision.

Each one expresses a different type of metabotropic opsin protein:

1) red cone cells express the red cone opsin
2) green cone cells express the green cone opsin
3) blue cone cells express the blue cone opsin
4) rod cells express the rhodopsin opsin

Each of these opsin proteins are sensitive to different wavelengths
of light according to how they hold the retinal molecule.

Rod cells (containing the rhodopsin protein) were the last to evolve;
they are 100 times more sensitive to light than the cone cells.

(Humans express a few other type of opsin proteins, but they are
not used for conscious vision perception.)
 WHAT THE EYES DETECT
Visible light refers to electromagnetic energy that has a wavelength between 380 and 760 nm.
We detect this light using four kinds of photoreceptor cells (1 rod cell & 3 cone cells).

blue green red
cone cone cone
 Cone Photoreceptors: Trichromatic Coding

Blue cone opsins are most sensitive
to short wavelengths of light

Green cone opsins are most sensitive
to medium wavelengths of light

Red cone opsins are most sensitive
to long wavelengths of light

The figure shows the absorption spectra of each of our cone opsins.
Notice that 610 nm wavelength light (orange) activates green cones 13%
of their maximum level and the red cones 75% of their maximum level.

Color perception is a function of the relative rates of activity across the three types of
cone cells (i.e. colors are discriminated by the ratio of activity across these cells).
 Cone Photoreceptors: Trichromatic Coding

The details get complicated because the three cone cells are not equally sensitivity to light.
For example, when people look at red, green, and blue lights of the same intensity, they often say that
the green light is brighter (because our green cone opsins are more sensitive to light in general).

But the key consideration for our brain for identifying color is how much each type of cone cell is
activated relative to its maximum level. Each color of the rainbow corresponds to a particular pattern
of activation across the three types of cones cells.
 Trichromatic Coding

When red and green light bulbs are so close
together that our eyes can’t differentiate
them, the color looks yellow to us.

There are 3 kinds of light bulbs here:
red, green and blue.

Green light (530nm) activates the green cone opsin more than the red cone opsin.
Red light (680nm) activates the red cone opsin more than the green cone opsin.
The combination of red and green light causes the red and green cone opsins to
be activated at similar amounts, which is what happens with yellow light (580nm).
 Additive versus Subtractive Color
The primary colors of light The primary colors of paint

Sunlight is white light,
since it contains an
equal mixture of all
the colors.

Paint doesn’t produce light; it absorbs some wavelengths of light and reflects others.
Yellow, magenta, and cyan are the three primary colors of office printers because each of these dyes only
absorbs (subtracts) one color from white light (from sunlight), while reflecting the other colors.

For example, yellow is a primary paint color because it only absorbs one color (blue) from white light.
Yellow paint reflects green and red light, which in combination we perceive as yellow.

Red is not a primary paint color because red paint simultaneously absorbs both blue and green light.
Printers create red by mixing yellow and magenta paint, which absorb blue and green light, respectively.
Note that it is advantageous to paint with chemicals that only absorb one color, because otherwise you
quickly end with black when mixing different paints together (when all light is absorbed, none is reflected).
You do not need to know about paint or the concept of subtractive color for this class.
 PERCEPTUAL DIMENSIONS OF COLOR & LIGHT
Our perception of light and color has three dimensions to it:

1) Brightness – intensity (luminance, amount)
2) Saturation – purity (in terms of wavelength mixture)
3) Hue – dominant wavelength (color) 0 to 360
100% 0%
degrees
If brightness is zero, the image is
completely black. Hue and saturation
have no impact without brightness.

If there is (bright) light, the next question
is whether the light is saturated with a
particular wavelength (color). If
saturation is 0%, then you are in the http://jamiewayne.com/wp-content/uploads/2011/05/hsb.jpg

middle of the color cone where there is
an equal contribution from all visible
wavelengths. An image with 0%
saturation is grayscale (black and
white), because all wavelengths are
present in equal amounts.

If saturation is >0%, the hue indicates
the color that the light is saturated with. 0
 COLOR VISION DEFICIENCY
Protanopia Absence of the red cone opsin (1% of males). People with this condition
have trouble distinguishing colors in the green-yellow-red spectrum.
Visual acuity is normal because red cone cells switch to using the green
cone opsin.
Simple mutations in of the red cone opsin (1% of males) produce less
pronounced deficits in color vision.

Deuteranopia Absence of the green cone opsin (1% of males). Visual acuity is normal
because green cone cells switch to using the red cone opsin.
People with this inherited condition have trouble distinguishing colors in the
Mutations in the red cone opsin
green-yellow-red section of the spectrum.
hinder color vision if they make
Simple mutations in of the green cone opsinit(6% of males)
act more produce
like the less
green opsin
pronounced deficits in color vision. (in terms of what light it can
detect).

Tritanopia Absence of the blue cone opsin (1% of the population).
Blue cone cells do not compensate for this in any way, but since the blue
cone opsin is not that sensitive to light anyway, visual acuity is not
noticeably affected.
 COLOR VISION DEFICIENCY
Protanopia Absence of the red cone opsin (1% of males). People with this condition
have trouble distinguishing colors in the green-yellow-red spectrum.
Visual acuity is normal because red cone cells switch to using the green
cone opsin.
Simple mutations in of the red cone opsin (1% of males) produce less
pronounced deficits in color vision.

Deuteranopia Absence of the green cone opsin (1% of males). People with this condition
have trouble distinguishing colors in the green-yellow-red spectrum.
Visual acuity is normal because green cone cells switch to using the red
cone opsin.
Simple mutations in of the green cone opsin (6% of males) produce less
pronounced deficits in color vision.

Tritanopia Absence of the blue cone opsin (1% of the population).
Blue cone cells do not compensate for this in any way, but since the blue
cone opsin is not that sensitive to light anyway, visual acuity is not
noticeably affected.
 COLOR VISION DEFICIENCY
Normal Vision Deuteranopia
(no green
cone)

Protanopia Tritanopia
(no red (no blue
cone) cone)

True color blindness is called achromatopsia. It is typically caused by mutations
in the g protein signaling cascade that is used by all the cone opsins.
 WHAT THE EYES DETECT
Visible light refers to electromagnetic energy that has a wavelength between 380 and 760 nm.
We detect this light using four kinds of photoreceptor cells (1 rod cell & 3 cone cells).

rhodopsin

blue green red
cone cone cone

Rod cells are 100x more sensitive
to light than any of the cone cells.
They are in a different category.

Cone cells are useful because
there are three of them, and they
are sensitive to different
wavelengths, which is necessary
for color vision.
 ANATOMY OF THE EYE
The conjunctiva is a mucous
membranes that line the eyelid

The cornea is the
outer, front layer of
the eye. It focuses
incoming light a
fixed amount.

The sclera is opaque and
does not permit entry of light
 ANATOMY OF THE EYE

The iris is a ring of muscle.
The contraction and
relaxation of this muscle
determines the size of the
pupil, which determines how
much light enters the eye.

The lens consists of several transparent layers.
We change the shape of this lens to focus near versus far,
a process known as accommodation.
 ANATOMY OF THE EYE

The interior lining (furthest back part) of the eye is the retina. Photoreceptor cells are
located in the furthest back layer of the retina.

Light passed through the lens and crosses
the vitreous humor, a clear, gelatinous fluid.

The central region of the retina
is called the fovea. It primarily
contains cone cells.

The periphery of the retina only
contains rod cells.

The optic disk is where blood
vessels enter and leave the eye.
It is also where the optic nerve
exits the eye, carrying visual
information to the brain. There
are no photoreceptors in this
spot, so it is a blind spot.
THE BLIND SPOT
 MOVEMENTS OF THE EYE

Eyes are suspended in bony sockets
in the front of the skull called orbits.

Our eyes never sit still for very long.

Our eyes scan a scene by making
saccadic eye movements – rapid,
jerky shifts in gaze from one point to
another.

However, when we maintain focus
on an object that is moving (relative
to us) our eyes exhibit pursuit
movements. This is the only time
are eyes appear to calm down and
move smoothly, slowly.

Six extraocular muscles are attached to the sclera: the tough, outer white of the eye.
These muscles rotate the eye and hold it in place.
 ORGANIZATION OF THE RETINA
Visual information propagates from photoreceptor cells → bipolar cells → retinal ganglion cells → brain.
So, when light enters our eyes, it must pass through each of the cell layers in the retina before it can reach the
opsin proteins in photoreceptor cells. There does not seem to be a good reason for this awkward arrangement.

Opsin proteins
Light
are here, in the
furthest back of
the retina.

neural activity

to the
brain
 RETINA FOVEA VERSUS PERIPHERY
In the fovea, there is an equal number of photoreceptor cells, bipolar cells, and retinal ganglion cells.
This means there is no compression of information. The fovea is the only part of our retina where our
visual acuity is good enough to read text (20/20 vision). And the photoreceptor cells in our fovea are
mostly cone cells, which support color vision, so the fovea supports high resolution, color vision.

Outside the fovea (in the periphery of our retina), there is a massive compression (averaging) of
information, since there are 100x more photoreceptor cells than retinal ganglion cells. Our visual acuity
in peripheral vision is about 20/200, which is quite blurry. It is also gray scale. We can make out
general shapes but not any details. Yet, the periphery of our retina contains a high density of rod cells,
which are very sensitive to light, allowing us to easily detect dim light and movements of light.

❖ Our fovea supports high resolution color
vision, but only when there is a sufficient
amount of light. At night, the moon must be at
least half full for us to see in color (if there are
no other sources of light.)

Light

❖ Our peripheral vision is very sensitive to dim
light, but it only provides low resolution
grayscale images. What we see in peripheral
vision 20 feet away is as detailed as what we
see in our fovea 200 feet away.
PERIPHERAL VISION

People have poor visual acuity and
are not great at identifying colors in
their peripheral vision.

We can still make out general
shapes, but images look blurry,
unfocused.

The high visual acuity needed for
reading is only possible in the
fovea, where we also see in color.
ROD AND CONE PHOTORECEPTORS
 NEURONS IN THE RETINA

Back of Light
eye

Photoreceptor cells are located in the furthest back part of the retina. They express
the opsin proteins that transduce light. Photoreceptor cells synapse on bipolar cells.
Bipolar cells relay information from photoreceptor cells to retinal ganglion cells.
Retinal ganglion cells are the only cells that send information out of the eye.
Their axons form the optic nerve, which exits the retina through the optic disc
(the blind spot of the retina).

Horizontal cells and amacrine cells interconnect cells within each layer, which gives
rise to complex interactions between neighboring cells (within a layer).
VISUAL INFORMATION PATHWAYS
Retinal ganglion cells have action potentials, unlike most
other cells in the retina. Their axons go to 3 places:

Thalamus (specifically the lateral geniculate nucleus),
which in turn projects to primary visual cortex (area
V1) in the occipital lobe where visual information
enters consciousness. This retina→thalamus→V1
pathway creates an internal (mental) representation of
your entire visual space: the objects in it, their position,
and their attentional value.

Midbrain (specifically the superior colliculi): Visual
information is used here to control fast visually-guided
reflexive movements. The midbrain doesn’t know what
you are looking at, but it can draw attention to
unexpected visual events.

Hypothalamus: Visual information is used here to
control circadian rhythms such as sleep-wake cycles.
The hypothalamus doesn’t know what you are looking
at, but it knows how much light is present in your
environment.
VISUAL CORTEX WIRING DIAGRAM

The wiring diagram of visual information
processing as it was understood in the 1970s.

This diagram is an oversimplification because
there are actually tons more pathways and most of
them are bidirectional (bottom-up and top-down).

One interesting theory of sensory processing is
the predictive coding theory. The idea is that each
node in the network tries to predict what its
ascending inputs will look like in the next moment,
based on previous experience.

The idea is that top-down (descending) activity
represents sensory predictions that neutralize
(cancel out) any correctly predicted bottom-up
ascending signals. Thus, what propagates up
through the network may only be prediction error
signals, which inform the brain of how the current
moment differs from what was expected.

The prediction error signals that ascend through
the network would cause learning to improve
future predictions.