HippocampusBackground
Hippocampus
Deep in the temporal lobe lies an ancient cortical structure called the hippocampus, which is Latin for "sea horse" due to its appearance in histological sections. The hippocampus plays a central role in memory formation and recall, and is implicated in a number of cortical pathologies including epilepsy and Alzheimer's disease. In this experiment, you will be recording electrical activity from the hippocampus of the mouse.
Oscillations
The brain runs on electricity.
If we record the electrical activity of a large group of cells by
sticking an electrode on (in which case we would be recording the EEG) or in
(as we will do in this lab) the brain, we can often record rhythmic electrical
signals that look like noisy sine waves.
These rhythmic signals are referred to as oscillations and represent the
activity of many cells doing the same thing at the same time, i.e. synchronous,
repetitive activity.
Depending on the
mechanism generating the oscillations, the frequency of the sine wave can be
fast or slow.
These oscillations have
been extensively studied over the years, and have been categorized based on
their frequency.
Two examples are
"theta" (5-10 Hz) and "gamma" (40 Hz) oscillations.
The reason brain rhythms
are interesting is that their occurrence and their properties change depending
on the behavioral state of the subject (e.g. attentive, bored, sleeping,
aroused), and depending on the region of the brain being studied.
Theta oscillations are especially prominent
in the hippocampus, and will be the focus of these two labs.
Although the function of brain oscillations
is not known, these rhythms are thought to act as timing signals in the brain,
sort of like a computer's clock cycle, organizing and coordinating cortical
activity amongst different regions of the brain.
How is synchronous, repetitive activity generated in the brain?
Consider the example of a sextet of musicians.
The tempo of the music can
either be imposed by the conductor, or can arise from musicians behaving as a
collective, listening and watching others in the group.
There are two analogous mechanisms for
generating synchrony in the brain: pacemaker cells (conductor) and network
monitoring (collective).
Often, both
mechanisms play a role: a network of cells may act as pacemakers to impose
their self-generated rhythm on other cells.
In the hippocampus and neocortex, there are two broad classes of cells: pyramidal cells (PCs) and inhibitory cells (GABAergic interneurons). Pyramidal cells receive excitatory input onto their dendrites from other pyramidal cells, and generate the output of the cortical structure. Interneurons regulate the activity of PCs and other interneurons via synapses onto the postsynaptic cells. Particularly relevant to this lab, networks of inhibitory cells in the hippocampus are thought to act as pacemakers, imposing their self-generated rhythms on pyramidal cells.
When
an interneuron fires an action potential, GABA is released at the synapse and
binds to GABAA receptors on the postsynaptic cell.
This causes a hyperpolarizing inhibitory
postsynaptic potential (IPSP) to occur in the pyramidal cell or interneuron
that is the target of this inhibition.
The duration and amplitude of the IPSP is determined to a large extent
by the properties of the receptor proteins.
Drugs that modulate these properties will change the duration and
amplitude of the IPSPs.
If the postsynaptic cell (PC or interneuron) is firing action
potentials at the time it gets inhibited, for example because of tonically
active excitatory inputs, the IPSP silences the postsynaptic cell. When the
postsynaptic cell gets hyperpolarized, its sodium channels get jazzed up and
when it recovers from the IPSP it's primed to start firing as soon as it's
able.
Since each interneuron is
connected to many PCs and other interneurons, all of these postsynaptic cells
will be inhibited simultaneously, and if the ongoing excitation in each cell is
similar, they all will tend to fire at the same time when they recover from the
inhibition.
(In the figure above, the
interneuron fires at the time marked by the black triangles, and the three
traces of action potentials are recorded from three cells that are inhibited
simultaneously.
If the interneuron is firing repetitively, for
example because it and all of its neighbors in the network are generating their
own theta rhythm, then the postsynaptic cells will be silenced repetitively,
i.e. the interneuron will impose on all of the cells it contacts a rhythmic inhibition,
sculpting the output of the postsynaptic cells. The duration and amplitude of the IPSP will determine the
frequency of the rhythm (i.e. the bigger and/or longer the IPSP, the longer the
postsynaptic cells will be silent and the slower the rhythm). Note that the interneurons rhythmically
inhibit each other, and in this way generate a rhythmicity within their
network. The interneuron network,
firing synchronously and repetitively, acts as a pacemaker by imposing its
rhythmicity on all of the pyramidal cells in the region.
Function of cortical oscillations
Oscillations serve to organize the firing activity
of cortical cells, restricting the occurrence of action potentials to certain
time periods. The interneurons generate a timing signal, and the pyramidal
cells generate their output at a fixed time relative to the ongoing
oscillation. What's the point of
organizing pyramidal cell activity in this way? One possible function is based on the idea that the exact timing
of the pyramidal cell action potentials will depend on how strong its
excitation is relative to the inhibition.
If a pyramidal cell is only weakly excited, then it will only be able to
fire when the inhibition has decayed back to zero. As the pyramidal cell gets more and more excited, it will tend to
fire earlier and earlier relative to the inhibition. Thus the phase of the pyramidal cell activity depends on the
strength of its excitatory inputs during that cycle of the rhythm. All the pyramidal cells that are equally
excited will tend to fire together, and cells that fire together are
interpreted by the brain as being related in some way, for example when forming
associative memories or when coding for different aspects of the same sensory
stimulus.
Behavioral effects on oscillations
One practical aspect of oscillations is that in a gross way, they can
tell us what is going on in the brain.
It turns out that the oscillation frequency and amplitude will change in
a predictable way depending on the behavioral state of the animal. For example, theta frequency is low when an
animal is at rest, and higher when an animal is exploring its environment. There are similar effects on other rhythms
such as gamma oscillations. One
clinical application of monitoring these rhythms that is being explored is
using oscillation frequency and amplitude to keep track of how deeply
anesthetized a patient is during surgery.
This is possible because oscillation frequency and amplitude is related
to awareness and consciousness. In the
first week of this lab you will explore how general anesthetics modulate the
properties of hippocampal theta oscillations.
In the second week of this lab, you will explore how different behaviors
correlate with the properties of theta oscillations.
Anesthetic effects on oscillations
If oscillations act as timing signals in the brain that organize conscious perception and cognition, anything that alters our level of consciousness should alter these timing signals. General anesthetics, i.e. drugs that cause you to lose consciousness, are a diverse class of drugs that are likely to have many overlapping mechanisms of action. (Incidentally, even though these drugs have been used for over 100 years and continue to be used routinely in every hospital in the world, their mechanism of action is still a mystery.) One effect that is common to many of these drugs is that they slow and ultimately eliminate cortical oscillations. Nearly all of these drugs also target GABAA receptors, and it is through their modulation of GABAA receptors that their effects on oscillations are likely to arise.