Title: Trends in Biomedical Science
1Trends in Biomedical Science
2Some animations may have been used from
neurons.med.utoronto.ca/index.swf under the
conditions stated below
3- Nerve Conduction
- Nerve conduction is when nerve impulses are made
and move along our neurons. - None of our thoughts, or memories would be
possible without nerve conduction.
4- Nerve conduction is an electrochemical process.
- It uses electricity made with chemical molecules.
- The brains electricity is caused by the
movements of electrically charged molecules
through the neurons membranes.
5- The membrane of a neuron, like that of any other
cell, contains tiny holes known as channels. It
is through these channels that charged molecules
pass through the neural membrane.
6- The channels in neurons are so specialized that
they can coordinate the movements of these
charges across the membrane. - So they can conduct nerve impulses.
7- This sequence of events shows how a nerve impulse
is conducted. - (see figure one at this site)
8- In the resting state the channels in the neural
membrane create an unequal distribution of
charges.
9- The nerve impulses open and close ion channels.
Ions move across the membrane and change the
electrical potential across the membrane. For a
short time the inside becomes more positive than
the outside.
10- Other channels quickly re-establish the resting
potential, but next to this area the potential is
changed. http//thebrain.mcgill.ca/flash/d/d_01/d
_01_m/d_01_m_fon/d_01_m_fon.html
11- Ion Channels and Nerve Impulses
12- Ion transport proteins have a special role in the
nervous systems because voltage-gated ion
channels and ion pumps are needed to form a nerve
impulse.
13- Ion channels use energy to build and maintain a
concentration gradient of ions between the
extracellular fluid and the cells cytosol.
14- Channel proteins in the plasma membrane. Membrane
channel proteins (or channel proteins), allow the
movement of specific ions across the cell
membrane.
15- The concentration gradient results in electrical
potential energy building up across the membrane,
the basis for the conduction of a nerve impulse.
16- This concentration gradient results in a net
negative charge on the inside of the membrane and
a positive charge on the outside.
17- Ion channels and ion pumps are very specific
they allow only certain ions through the cell
membrane.
18- For example, potassium channels will allow only
potassium ions through, and the sodium-potassium
pump acts only on sodium and potassium ions.
19- All cells have an electrical charge which is due
to the concentration gradient of ions that exists
across the membrane.
20- All cells have an electrical charge which is due
to the concentration gradient of ions that exists
across the membrane.
20
21- The number of positively charged ions outside the
cell membrane is greater than the number of
positively charged ions in the cytosol. This
difference causes a voltage difference across the
membrane.
21
22- The number of positively charged ions outside the
cell membrane is greater than the number of
positively charged ions in the cytosol. This
difference causes a voltage difference across the
membrane.
23- The number of ions outside is greater than the
number of ions in the cytosol. This causes a
voltage difference across the membrane.
23
24- Voltage is electrical potential energy that is
caused by a separation of opposite charges, in
this case across the membrane. - The voltage across a membrane is called membrane
potential.
24
25- Voltage is electrical potential energy that is
caused by a separation of opposite charges, in
this case across the membrane. - The voltage across a membrane is called membrane
potential.
26- Membrane potential is the basis for the
conduction of nerve impulses along the cell
membrane of neurons. Ions that are important in
the formation of a nerve impulse include sodium
(Na) and potassium (K).
26
27- Membrane potential is the basis for the
conduction of nerve impulses along the cell
membrane of neurons. Ions that are important in
the formation of a nerve impulse include sodium
(Na) and potassium (K).
28- For revision if you need it
- How Diffusion Works
- and quiz
28
29- How Facilitated Diffusion Works
- And quiz
29
30- How the Sodium Potassium Pump Works
- And quiz
30
31- Receptors Linked to a Channel Protein
- And quiz
31
32- For review look at 3. Ions and Ion Transport
32
33 34- When a neuron is not conducting a nerve impulse,
it is said to be at rest. The resting potential
is the resting state of the neuron, during which
the neuron has an overall negative charge.
35- In neurons the resting potential is approximately
-70 milliVolts (mV). The negative sign indicates
the negative charge inside the cell relative to
the outside.
36- The reasons for the overall negative charge of
the cell include
37- The sodium-potassium pump removes Na ions from
the cell by active transport. A net negative
charge inside the cell is due to the higher
concentration of Na ions outside the cell than
inside the cell.
38- The sodium-potasium pump is also called the
Na/K-ATPase (fully sodium-potassium adenosine
triphosphatase, also known as the Na/K pump, or
sodium pump, for short). - It is an enzyme (EC 3.6.3.9) located in the
plasma membrane in all animals. - As its name suggests, it uses ATP in its action.
38
3939
40- Animation of the sodium-potassium pump is at
- http//highered.mcgraw-hill.com/sites/0072495855/s
tudent_view0/chapter3/animation__sodium-potassium_
exchange_pump__quiz_1_.html
41- Na, K-ATPase and other ion pumps must work all
the time in our body. If they were to stop, our
cells would swell up, and might even burst, and
we would rapidly lose consciousness. A great deal
of energy is needed to drive ion pumps - in
humans, about 1/3 of the ATP that the body
produces.
42- Since neurons purposely allow Na to flood into
the cell and K to go out, we can assume that
neurons use much more energy for pumping
43- Ion pumps are affected by chemical substances.
- Digitalis plants contain a substance that
inhibits Na, K-ATPase which results in an
accumulation of sodium ions in cells. - Used as a pharmaceutical, it causes reinforced
heart muscle activity.
44- Most cells have potassium-selective ion channel
proteins that remain open all the time. The K
ions move down the concentration gradient
(passively) through these potassium channels and
out of the cell, which results in a build-up of
excess positive charge outside of the cell.
45- There are a number of large, negatively charged
molecules, such as proteins, inside the cell.
46- For review click on 4. Resting Membrane Potential
46
47- Potassium (K), which is positively charged,
passes most easily through a neural membrane in
its resting state. - Sodium (Na) and chloride (Cl-), which has a
negative charge, have more difficulty passing
through the membrane.
47
48- Large, negatively charged molecules inside the
neuron cannot get out but also influence the
membranes electrical potential. - The calcium ion (Ca) also plays an important
role, but in the process of synaptic
transmission.
48
49- Membrane ion-channel and ion-pumping proteins.
49
50 51- An action potential is an electrical charge that
travels along the membrane of a neuron. It is
made when a neurons membrane potential is
changed by chemical signals from a nearby cell.
52- In an action potential, the cell membrane
potential changes quickly from negative to
positive as sodium ions flow into and potassium
ions flow out of the cell through ion channels.
53- The movement of an action potential down an axon.
53
54- The movement of an action potential down an axon.
55- A chemical message from another nerve causes the
sodium ion channels at one point in the axon to
open. Sodium ions move quickly across the
membrane and cause the inside of the axon to
become positively charged (depolarized) because
the cell now contains more positive charges.
Potassium ion channels then open and potassium
ions flow out of the cell, which end the action
potential. The action potential then moves down
the axon membrane toward the synapse.
56- The cell becomes depolarized. An action potential
works on an all-or-nothing basis. This means, the
membrane potential has to reach a certain level
of depolarization, called the threshold,
otherwise an action potential will not start.
57- This threshold potential varies, but is generally
about 15 millivolts (mV) more positive than the
cell's resting membrane potential. If a membrane
depolarization does not reach the threshold
level, an action potential will not happen.
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60- The first channels to open are the sodium ion
channels, which allow sodium ions to enter the
cell. The resulting increase in positive charge
inside the cell (up to about 40 mV) starts the
action potential.
60
61- The first channels to open are the sodium ion
channels, which allow sodium ions to enter the
cell. The resulting increase in positive charge
inside the cell (up to about 40 mV) starts the
action potential.
62- Potassium ion-channels then open up, allowing
potassium ions out of the cell, which ends the
action potential.
62
63- Potassium ion-channels then open up, allowing
potassium ions out of the cell, which ends the
action potential.
64- Both of the ion channels then close, and the
sodium- potassium pump restores the resting
potential of -70 mV.
64
65- Both of the ion channels then close, and the
sodium- potassium pump restores the resting
potential of -70 mV.
66- The action potential will move down the axon
toward the synapse like a wave.
66
67- The action potential will move down the axon
toward the synapse like a wave.
68- Video
- http//highered.mcgraw-hill.com/sites/0072495855/s
tudent_view0/chapter14/animation__the_nerve_impuls
e.html
69 70- In myelinated neurons, ion flows occur only at
the nodes of Ranvier. As a result, the action
potential signal is quickly pushed along the axon
membrane, from node to node, rather than
spreading smoothly along the membrane, as they do
in axons that do not have a myelin sheath.
71- The quick pushing of the action potential signal
along the axon membrane, from node to node, is
called saltatory conduction.
71
72- Comparison
- http//faculty.stcc.edu/AandP/AP/AP1pages/nervssys
/unit11/saltator.htm
72
73- Saltatory conduction
- Saltatory conduction is faster than smooth
conduction. Some typical action potential
velocities
Fiber Diameter AP Velocity
Unmyelinated 0.2-1.0 micron 0.2-2 m/sec
Myelinated 2-20 microns 12-120 m/sec
73
74- The action potential is increased at the Nodes of
Ranvier. This is due to clustering of Na and K
ion channels at the Nodes of Ranvier.
74
75- Unmyelinated axons do not have Nodes of Ranvier
and ion channels in these axons are spread over
the entire membrane surface.
76- Video-
- The Schwann Cell and Action Potential
- http//www.knowmia.com/watch/lesson/433
77- For review go to this page and click on 5. Action
Potential
77
78- Communication Between Neurons
79- Neurons communicate with each other at
specialized junctions called synapses. Synapses
are also found at junctions between neurons and
other cells, such as muscle cells.
80- Neuromuscular junction
- Axon
- Synaptical junction
- Muscle fiber
- Myofibrils
81- There are two types of synapses
- - chemical synapses use chemical signaling
molecules as messengers - - electrical synapses use ions as messengers
- We will look at chemical synapses.
82- The axon terminal of one neuron usually does not
touch the other cell at a chemical synapse.
Between the axon terminal and the receiving cell
is a gap called a synaptic cleft.
83- The transmitting cell is called the presynaptic
neuron, and the receiving cell is called the
postsynaptic cell or if it is another neuron, a
postsynaptic neuron.
84- The brain has a huge number of synapses. Each of
the 1012 (one trillion) neurons, including glial
cells, has on average 7,000 synaptic connections
to other neurons.
85- It has been estimated that the brain of a three
year-old child has about 1016 synapses (10
quadrillion). This number declines with age, and
levels off by adulthood.
86- An adult has between 1015 and 5 x 1015 synapses
(1 to 5 quadrillion).
87 88- A neurotransmitter is a chemical message that is
used to relay electrical signals between a neuron
and another cell.
89- Neurotransmitter molecules are made inside the
presynaptic neuron and stored in vesicles at the
axon terminal.
90- Some neurons make only one type of
neurotransmitter, but most neurons make two or
more types of neurotransmitters.
91- When an action potential reaches the axon
terminal, it causes the neurotransmitter vesicles
to fuse with the terminal membrane, and the
neurotransmitter is released into the synaptic
cleft.
92- The neurotransmitters then diffuse across the
synaptic cleft and bind to receptor proteins on
the membrane of the postsynaptic cell.
93- The synaptic cleft. Neurotransmitter that is
released into the synaptic cleft diffuses across
the synaptic membrane and binds to its receptor
protein on the post synaptic cell.
94- Neuromuscular junction
- presynaptic terminal
- sarcolemma
- synaptic vesicles
- Acetylcholine receptors
- mitchondrion
95- At a synapse, neurotransmitters are released by
the axon terminal. They bind with receptors on
the other cell.
95
96- The location of synapses. Synapses are found at
the end of the axons (called axon terminals) and
help connect a single neuron to thousands of
other neurons. Chemical messages called
neurotransmitters are released at the synapse and
pass the message onto the next neuron or other
type of cell.
96
97 98- Many types of neurotransmitters exist.
- Neurotransmitters can have an excitatory or
inhibitory effect on the postsynaptic cell.
99- Common Neurotransmitters and Their Receptors
Name Receptor Name and Type Ions Involved
Glutamate (glutamic acid) Glutamate receptors (ligand-gated ion channels and G protein-coupled receptors) Ca2, K, Na
Acetylcholine Acetylcholine receptors (ligand-gated ion channel) Na
Norepinephrine (noradrenaline) Adrenoceptors (G protein-coupled receptors) Ca2
Epinephrine (adrenaline) Adrenoceptors (G protein-coupled receptors) Ca2
Serotonin (5-hydroxytryptamine) 5-HT receptors 5-HT3 is a ligand-gated ion channel 5-HT1, 5-HT2, 5-HT4, 5-HT5A, 5-HT7 are G protein-coupled receptors K, Na
Gamma-aminobutyric acid (GABA) GABAA and GABAC (ligand-gated ion channels) GABAB (G protein-coupled receptors) Cl- K
Histamine Histamine receptors (H1, H2, H3, H4) (G protein-coupled receptors)
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101- An excitatory neurotransmitter initiates an
action potential and an inhibitory
neurotransmitter prevents one from starting.
102- Glutamate is the most common excitatory
transmitter in the body while GABA and glycine
are inhibitory neurotransmitters.
103 104- The release of acetylcholine, an excitatory
neurotransmitter causes an inflow of positively
charged sodium ions (Na) into the postsynaptic
neuron.
105- This inflow of positive charge causes a
depolarization of the membrane at that point. The
depolarization then spreads to the rest of the
postsynaptic neuron.
106- The effect of a neurotransmitter also can depend
on the receptor it binds to. So, a single
neurotransmitter may be excitatory to the
receiving neuron, or it may inhibit such an
impulse by causing a change in the membrane
potential of the cell.
107- Synapses too can be excitatory or inhibitory and
will either increase or decrease activity in the
target neuron, based on the opening or closing of
ion channels.
108- Neurotransmitter receptors can be gated ion
channels that open or close through
neurotransmitter binding or they can be
protein-linked receptors.
109- Protein-linked receptors are not ion channels
instead they cause a signal transduction that
involves enzymes and other molecules (called
second messengers) in the postsynaptic cell.
110- Video-
- http//highered.mcgraw-hill.com/sites/0072495855/s
tudent_view0/chapter14/animation__transmission_acr
oss_a_synapse.html
111 112- Side journey. How we can see how cells are
connected with many synapses. - Beautiful 3-D brain
113- Removal of Neurotransmitter
114- Many neurotransmitters are removed from the
synaptic cleft by neurotransmitter transporters
in a process called reuptake. Reuptake is the
removal of a neurotransmitter from the synapse by
the pre-synaptic neuron.
115- Reuptake happens after the neurotransmitter has
transmitted a nerve impulse. - Without reuptake, the neurotransmitter molecules
might continue to stimulate or inhibit an action
potential in the post-synaptic neuron.
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117- A synapse before and during reuptake.
118- Re-uptake is carried out by transporter proteins
which bind to the released transmitter and
actively transport it across the plasma membrane
into the pre-synaptic neuron.
119- Removal of neurotransmitters
- Section 8
120- Reuptake of neurotransmitter as a medical target.
121- The reuptake of neurotransmitter is the target of
some types of medicine. - For example, serotonin is a neurotransmitter that
is produced by neurons in the brain.
122- Serotonin is believed to play an important role
in the regulation of mood, emotions, and
appetite. -
123- After release into the synaptic cleft, serotonin
molecules either attach to the serotonin
receptors (5-HT receptors) of the post-synaptic
neuron, or they attach to receptors on the
surface of the presynaptic neuron that produced
the serotonin molecules, for reuptake.
124- Reuptake is a form of recycling because the
neuron takes back the released neurotransmitter
for later use.
125- Medicines called selective serotonin reuptake
inhibitors (SSRIs) block the reuptake of the
neurotransmitter serotonin. - This blocking action increases the amount of
serotonin in the synaptic cleft, which prolongs
the effect of the serotonin on the postsynaptic
neuron.
126- Some scientists hypothesize that decreased levels
of serotonin in the brain are linked to clinical
depression and other mental illnesses. - So SSRI medications such as sertraline and
fluoxetine are often prescribed for depression
and anxiety disorders.
127- Another way that a neurotransmitter is removed
from a synapse is digestion by an enzyme.
128- L-Monoamine oxidases (MAO) (EC 1.4.3.4) are a
family of enzymes that catalyze the oxidation of
monoamines - They are found bound to the outer membrane of
mitochondria in most cell types in the body. - They belong to the protein family of
flavin-containing amine oxidoreductases.
129- In humans there are two types of MAO MAO-A and
MAO-B. - Both are found in neurons and astroglia.
- Outside the central nervous system
- MAO-A is also found in the liver,
gastrointestinal tract, and placenta. - MAO-B is mostly found in blood platelets.
129
130- They are well known enzymes in pharmacology,
since they are the substrate for the action of a
number of monoamine oxidase inhibitor drugs. - Both MAOs are inactivate monoaminergic
neurotransmitters, for which they display
different specificities.
130
131- Serotonin, melatonin, norepinephrine, and
epinephrine are mainly broken down by MAO-A. - Phenethylamine and benzylamine are mainly broken
down by MAO-B. - Both forms break down dopamine, tyramine, and
tryptamine equally
131
132- MAO dysfunction (too much or too little MAO
activity) is thought to be responsible for a
number of psychiatric and neurological disorders.
132
133- For example, unusually high or low levels of MAOs
in the body have been associated with depression,
schizophrenia, substance abuse, attention deficit
disorder, migraines, and irregular sexual
maturation.
133
134- Monoamine oxidase inhibitors are one of the major
classes of drug prescribed for the treatment of
depression. - MAO-A inhibitors act as antidepressant and
antianxiety agents, whereas MAO-B inhibitors are
used alone or in combination to treat Alzheimers
and Parkinsons diseases.
134
135- MAO is also heavily depleted by use of tobacco
cigarettes.
135
136- 7. Post-synaptic mechanisms
136
137- Neurotransmitters and Disease
137
138- Before we begin
- We often think of disease (or the cause of
disease) as a bad functioning of the cells or
systems. - But the proper functioning may be the underlying
cause of disease.
139- Before we begin
- We often think of disease (or the cause of
disease) as a bad functioning of the cells or
systems. - But the proper functioning may be the underlying
cause of disease. - When we look at diseases which are caused by
compulsive or addiction related behaviors,
remember that they may be based on the proper
functioning of neurotransmitters or their
receptors.
140- Diseases that affect nerve communication can have
serious consequences.
140
141- A person with Parkinson's disease has a
deficiency of the neurotransmitter dopamine. - Progressive death of brain cells that produce
dopamine increases this deficit, which causes
tremors, and a stiff, unstable posture.
141
142- L-dopa is a chemical related to dopamine that is
given as a medicine to ease some of the symptoms
of Parkinsons disease. - The L-dopa acts as a substitute neurotransmitter,
but it cannot reverse the disease.
142
143- The soil bacterium Clostridium tetani produces a
neurotoxin that causes the disease tetanus. - The bacteria usually get into the body through an
injury caused by an object that is contaminated
with C. tetani spores.
143
144- The C. tetani neurotoxin blocks the release of
the neurotransmitter GABA, which causes skeletal
muscles to relax after contraction. - When the release of GABA is blocked, the muscle
tissue does not relax and remains contracted.
144
145- Tetanus can be fatal when it affects the muscles
used in breathing. - Tetanus is treatable and can be prevented by
vaccination.
145
146146
147- An electrical synapse is a link between two
neighboring neurons that is formed at a narrow
gap between the pre- and postsynaptic cells
called a gap junction.
147
148- At gap junctions, cells are about 3.5 nm from
each other, a much shorter distance than the 20
to 40 nm distance that separates cells at
chemical synapses.
148
149- Electrical synapses. The image at the bottom
right shows the location of gap junctions between
cells.
149
150- Each gap junction has many channels which cross
the plasma membranes of both cells. Gap junction
channels are wide enough to allow ions and even
medium sized molecules like signaling molecules
to flow from one cell to the next.
150
151- For example, when positive ions move through the
channel into the next cell, the extra positive
charges depolarize the postsynaptic cell.
151
152- Signaling at electrical synapses is faster than
the chemical signaling that occurs across
chemical synapses.
152
153- Ions directly depolarize the cell without the
need for receptors to recognize chemical
messengers, which occurs at chemical synapses.
153
154- Such fast communication between neurons may
indicate that in some parts of the brain large
groups of neurons can work as a single unit to
process information.
154
155- There are many electrical synapses in the retina
and cerebral cortex.
155
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