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Applications of Biology
Immunology
Immunity
ā€¢ This refers to the bodyā€™s ability to defend itself
against diseases.
ā€¢ Immunity is provided by the immune system.
ā€¢ The immune system recognizes foreign
material and produces chemicals to destroy it.
ā€¢ The defence provided by the immune system
can be physical, chemical and cellular.
Immunity conā€™t
ā€¢ Physical defence includes clotting
ā€¢ Cellular defence includes the barrier created
by epithelia and white blood cells.
ā€¢ Chemical defence include the secretion of
hydrochloric acid to destroy pathogens.
ā€¢ White blood cells play a very important role in
the immune system.
Immunity conā€™t
ā€¢ An antigen is a molecule which the body
recognizes as foreign.
ā€¢ Antigens have on their surfaces, large
molecules such as proteins, glycoproteins,
lipids and polysaccharides.
ā€¢ White blood cells are able to recognize
antigens.
White blood cells
ā€¢ White blood cells originate in the bone
marrow.
ā€¢ The two main groups involved in defence are
phagocytes and lymphocytes.
ā€¢ Phagocytes can be further classified into
neutrophils and macrophages.
Phagocytes
ā€¢ These are made throughout a personā€™s
lifetime in the bone marrow.
ā€¢ They are stored in the bone marrow before
they are distributed around the body.
ā€¢ Phagocytes act as scavengers by removing
dead cells as well as invasive microorganisms.
Neutrophils
ā€¢ Approximately 60% of white blood cells are
neutrophils.
ā€¢ They are transported by the blood throughout
the body.
ā€¢ They are often squeezed through the walls of
the capillaries (by a process known as
diapedesis) to ā€˜patrolā€™ the tissues.
Neutrophils conā€™t
ā€¢ They are short lived cells and are produced in
large amounts during an infection.
Macrophages
ā€¢ These are larger than neutrophils.
ā€¢ They are usually found in organs such as the
lungs, liver, spleen, kidney and in the lymph
nodes.
ā€¢ They are made in the bone marrow and travel
in the blood as monocytes.
ā€¢ Monocytes develop into macrophages once
they settle in the organs.
Macrophages conā€™t
ā€¢ Macrophages are long-lived.
ā€¢ They cut up pathogens displaying their
antigens so they can be easily recognized by
lymphocytes.
ā€¢ They therefore play a major role in initiating
immune response.
Phagocytosis
ā€¢ Cells that are being attacked by pathogens
produce histamine
ā€¢ Mast cells are body cells that produce
histamine and cause inflammation (see later)
ā€¢ The pathogens also release chemicals.
ā€¢ These chemicals from the pathogens along
with the histamine attract passing neutrophils
to the site of infection.
Phagocytosis conā€™t
ā€¢ Neutrophils have receptor proteins (opsonins)
on their surfaces which allow them to
recognise antibodies and chemicals produced
by the bacteria.
ā€¢ The pathogens may be clumped together and
covered in antibodies (secreted by
lymphocytes) which would also help to
stimulate action by the neutrophils.
Phagocytosis conā€™t
ā€¢ The neutrophils move towards the pathogens
and binds with the bacterium.
ā€¢ The binding stimulates the formation of a
pseudopodia and the formation of a vacuole
called a phagosome.
ā€¢ Lytic enzymes are released by lysozomes into
the phagosome which break down the
bacterium.
Phagocytosis conā€™t
ā€¢ Dead neutrophils collect as a site of infection
as pus. (See handout for illustration. Make
sure you can illustrate what is there)
ā€¢ The histamine released by mast cells cause
dilation of blood vessels making them leak.
ā€¢ Plasma and white blood cells flow out into the
infected area.
Phagocytosis conā€™t
ā€¢ Pus is formed from dead bacteria and white
blood cells (mainly phagocytes).
ā€¢ The inflamed area thus becomes red, hot and
swollen.
ā€¢ Sometimes a boil is formed which might
eventually burst because of the pressure of
the pus inside.
Phagocytosis conā€™t
ā€¢ Phagocytosis is enhanced by a group of blood
proteins called complement.
ā€¢ Complement proteins are made by
macrophages, monocytes and other cells in
the body especially those in the liver.
ā€¢ They are usually inactive.
ā€¢ When necessary they stick to invading micro-
organisms (mainly yeasts and bacteria)
Phagocytosis conā€™t
making them conspicuous to phagocytes as
foreign matter.
ā€¢ Some destroy the membranes of bacteria.
Lymphocytes
ā€¢ These are smaller than phagocytes and have a
large nucleus that fills most of the cell.
ā€¢ There are two types:
1. B lymphocytes
2. T lymphocytes
Origin and maturation of B
lymphocytes
ā€¢ As you already know, B cells are made in the
bone marrow.
ā€¢ Here the immature B cells divide by mitosis.
ā€¢ Each B cell is specific to an antigen.
ā€¢ It therefore means that many millions of B cell
types exist in our bodies.
ā€¢ During maturation, each B cell produces
antibodies.
Origin and maturation of B
lymphocytes conā€™t
ā€¢ The genes that code for antibodies change in a
variety of ways to code for different antibodies
during maturation.
ā€¢ Each B cell then divides to give a small number
of clones that are able to make the same
antibodies.
Origin and maturation of B
lymphocytes conā€™t
ā€¢ The antibodies formed during maturation of
the B cells do not leave the cell.
ā€¢ Rather, they form part of the plasma
membrane.
ā€¢ A part of each antibody forms a protein
receptor.
ā€¢ This receptor can combine with one type of
antigen.
Origin and maturation of B
lymphocytes conā€™t
ā€¢ If that antigen enters the body, there will be
some mature B cells with cell surface
receptors that recognise it. (See hand out for
diagram. Make sure you can illustrate what is
there)
Action of B lymphocytes
ā€¢ When pathogens enters the body for the first
time, some of them are take up by
macrophages (in lymph node etc).
ā€¢ The macrophages expose the antigens from
the pathogens on their surfaces.
ā€¢ Any B lymphocyte that has cell surface
receptors that are specific to the antigens
exposed divide repeatedly my mitosis.
Action of B lymphocytes conā€™t
ā€¢ Within a few weeks, a huge number of
identical B cells are produced.
ā€¢ Some pathogens have more than one antigen
on their surface.
ā€¢ This means that several B cells are activated
on entry of the pathogen.
ā€¢ As each type B cell divides, a polyclone is
formed (each type forms a clone)
Action of B lymphocytes conā€™t
ā€¢ Some of these B cells become plasma cells.
ā€¢ Others become memory cells.
ā€¢ Plasma cells are short lived.
ā€¢ They produce antibody molecules very quickly
(up to several thousand per second)
Action of B lymphocytes conā€™t
ā€¢ The antibody molecules are released into the
blood, lymph or onto the linings of the gut or
lungs.
ā€¢ The antibody molecules last longer than the
plasma cells. However, their concentrations
eventually decrease.
Action of B lymphocytes conā€™t
ā€¢ The memory cells remain in circulation within
the body for a very long time.
ā€¢ If the same pathogen enters the body again,
they divide rapidly forming more plasma cells
and memory cells.
ā€¢ This response occurs every subsequent time
the pathogen enters the body.
Action of B lymphocytes conā€™t
ā€¢ Thus the pathogen is prevented from causing
a disease. (See diagram on hand out ā€“ ensure
you are able to illustrate what is there)
ā€¢ The immunity offered by B lymphocytes is
called humoral immunity.
ā€¢ This is because antibodies are produced and
transported in body fluids (blood and lymph)
Primary and secondary responses
ā€¢ When the body encounters an antigen for the
first time, the response is slow because there
are a few B cells that are specific to the
particular antigen.
ā€¢ This first response is called a primary
response.
ā€¢ During this response, the body experiences
symptoms of the disease.
Primary and secondary responses
conā€™t
ā€¢ When the pathogen tries to enter the body
again, the response is much faster.
ā€¢ This is because there are many memory cells
which divide quickly to give plasma cells. Thus
more antibodies are produced.
Primary and secondary responses
conā€™t
ā€¢ This is called a secondary response. The body
does not experience symptoms of the disease.
ā€¢ Memory cells are the basis for immunological
memory. (See graph on handout ā€“ be able to
illustrate what is there)
Antibodies
ā€¢ So weā€™ve been talking about antibodies being
produced by B lymphocytes.
ā€¢ What really are antibodies?
ā€¢ They are globular glycoproteins and form the
group of plasma proteins called
immunoglobulins.
ā€¢ All antibodies has a basic strucure.
Structure of an antibody
http://tinyurl.com/77oeght
Antibodies conā€™t
ā€¢ All are made up of 4 polypeptide chains: two
long or heavy chains and two short or light
chains.
ā€¢ The chains are held together by disulphide
bridges.
ā€¢ Each antibody molecule has two identical
binding sites formed by both light and heavy
chains.
Antibodies conā€™t
ā€¢ The sequence of amino acids form a specific
three-dimensional shape which binds to only
one type of antigen.
ā€¢ This is called the variable region and varies for
different antibodies.
ā€¢ There is a hinge region formed between the
two heavy chains.
ā€¢ This provides flexibility.
Antibodies conā€™t
ā€¢ Antibodies work in different ways.
ā€¢ Their actions can be summarized into four
groups;
1. Agglutination ā€“ antibodies have two binding
sites. They can therefore bind to antigens on
two different pathogens. This can result in
pathogens being clumped together making
them more vulnerable to attack.
Antibodies conā€™t
2. Precipitation ā€“ some antigens are soluble.
Some antibodies bind them together into
large units which are then precipitated out of
solution. This way they are more easily
digested by phagocytes.
3. Neutralization ā€“ some antibodies bind to
toxins released by pathogens preventing
harm.
Antibodies conā€™t
4. Lysis ā€“ when some antibodies attach to a
pathogen, they act as a binding site for a
number of blood proteins (complement
system). Some of these proteins are
enzymes and cause breakdown of the
pathogen.
ā€¢ Immunoglobulin E (IgE) binds to the
receptors of mast cells activating them to
release histamine.
Origin and maturation of T
lymphocytes
ā€¢ As you already know, T lymphocytes are made
in the bone marrow.
ā€¢ Here the immature T cells dived by mitosis.
ā€¢ They then travel to the thymus gland where
they mature.
ā€¢ They develop specific receptors which are
displayed in the plasma membrane.
Origin and maturation of T
lymphocytes conā€™t
ā€¢ The mature T cells circulate in the body. (see
hand out ā€“ be able to illustrate)
ā€¢ Some form T helper cells, some form T
cytotoxic cells, some form T suppressor cells
and some form memory T cells.
Action of T lymphocytes
ā€¢ T cells are activated when they recognize an
antigen in contact with a host cell. Eg. A
macrophage which has cut up a pathogen
displaying its antigen (a help signal).
ā€¢ The T cell with matching receptors divide by
mitosis to form a clone.
ā€¢ The cells differentiate to form several types of
cells, the two main types being T helper cells
and killer T cells.
Action of T lymphocytes conā€™t
ā€¢ Cytokines are secreted by T helper cells when
they are activated.
ā€¢ Cytokines stimulate appropriate B cells to
divide and develop plasma cells which secrete
antibodies.
ā€¢ Some secrete cytokines that stimulate
macrophages to carry out phagocytosis more
vigilantly.
Action of T lymphocytes conā€™t
ā€¢ The cytokines these T cells secrete belong to a
group of proteins called lymphokines.
ā€¢ Another lymphokine is called interferons.
These inactivate the protein making
machinery of the infected cell. This therefore
inhibits the replication of viruses.
Action of T lymphocytes conā€™t
ā€¢ T cytotoxic cells search for body cells that are
invaded with pathogens and are displaying the
antigens.
ā€¢ The killer T cells attach themselves to the
infected cells and secrete toxic substances
such as hydrogen peroxide killing these
infected cells and the pathogens. (see
handout ā€“ be able to illustrate)
Action of T lymphocytes conā€™t
ā€¢ T suppressor cells ā€“ these control the immune
system. Once an infection has been
eliminated, these cells suppress the activities
of the lymphocytes.
ā€¢ T memory cells ā€“ these remain in the body
and become very active during a secondary
response to antigens.
Active and passive immunity
ā€¢ Active immunity refers to resistance to disease
derived by the body producing antibodies on
exposure to antigens.
ā€¢ Active immunity is long term and can be
either natural or artificial.
ā€¢ When pathogens enter the body by natural
means (air borne, food borne etc.), B
lymphocytes make antibodies to destroy
them.
Active and passive immunity conā€™t
ā€¢ As you would remember, memory cells are
formed which make the body immune the
next time the pathogen invades the body.
ā€¢ This is natural active immunity.
ā€¢ In some cases antigens are injected or taken
orally into the body.
ā€¢ The body then makes antibodies which
protect the body from those antigens.
Active and passive immunity conā€™t
ā€¢ Passive immunity refers to resistance to
disease that is short lived and is not derived
by any action of the body.
ā€¢ Passive immunity can also be natural or
artificial.
ā€¢ Natural passive immunity is obtained when
antibodies pass by natural means into the
body.
Active and passive immunity conā€™t
ā€¢ Babies have natural passive immunity.
ā€¢ This is a result of antibodies passing across the
placenta from the mother to the foetus.
ā€¢ After birth, the colostrum which the baby
receives is rich in IgA which prevents the
growth of bacteria.
ā€¢ Because immunity is passive it is short lived.
Active and passive immunity conā€™t
ā€¢ Depending on the nature of a disease or
infection, antibodies may need to be injected
into the body.
ā€¢ If the body were allowed to make its own
antibodies, the person would die. Eg. Tetanus.
ā€¢ This is artificial passive immunity.
Vaccinations
ā€¢ A vaccine is a preparation of antigenic
material designed to stimulate the production
of antibodies and develop immunity within
the body.
ā€¢ Immunity derived from exposure to live
pathogens is the best but not always realistic.
ā€¢ Some vaccines are very effective and one
injection is sufficient. Some need
vaccinations.
Vaccinations conā€™t
ā€¢ The materials used in vaccinations can be
grouped:
1. Living attenuated organisms ā€“ these are
pathogens that are treated (for example,
using heat) so that they can multiply but are
unable to cause the symptoms of the
disease. Even though they are harmless,
they stimulate the production of antibodies.
Eg. Measles, tuberculosis, poliomyelitis
Vaccinations conā€™t
2. Toxoids ā€“ the toxins which result from certain
diseases can stimulate the body to produce
antibodies. These toxins are modified to
prevent them causing symptoms of the
disease (eg. Treating it with formaldehyde)
and then administered by injection. Eg.
Diphtheria, tetanus
Vaccinations conā€™t
3. Dead microorganisms ā€“ the pathogens are
killed and then injected. Even though they are
dead, they are able to stimulate the
production of antibodies in the same way they
would if they were living. Eg. Typhoid,
cholera, whooping cough.
Vaccinations conā€™t
4. Extracted antigens ā€“ chemicals with antigenic
properties are extracted from the pathogens
and injected. Eg. Influenza vaccine
5. Artificial antigens ā€“ Genetic engineering is
used to transfer genes for the production of
antigens from the pathogen to a harmless
organism. These are grown in a laboratory
for the production of antigens which are later
used. Eg. Hepatitis B
Problems with vaccines
ā€¢ Despite the benefits derived from vaccines,
there are several problems associated with
them.
1. Poor response ā€“ due to weakened immune
systems or malnourishment some persons do
not develop the necessary B and T cell clones.
Persons that are vaccinated with live viruses
can pass it to others in faeces. Herd immunity
is therefore ideal.
Problems with vaccines conā€™t
ā€¢ Antigenic variation ā€“ when pathogens mutate
causing minor changes in the antigens they
produce, this is called antigenic drift.
Sometimes the memory cells will still
recognise them and cause a secondary
response. Sometimes there is an antigenic
shift where the mutation is so great that there
is a drastic change in antigen structure (eg.
Influenza). This results in the vaccine being
Problems with vaccines conā€™t
changed every year. Also, some pathogens are
eukaryotes eg. Plasmodium which causes
malaria and Trypanosoma which causes
sleeping sickness. Being eukaryotes, they
have many more genes than viruses and
bacteria and can have many hundreds or
thousands of antigens (each stage in the life
cycle has different antigens). There are
therefore no effective vaccines against these
diseases.
Problems with vaccines conā€™t
ā€¢ Large invaders like nematodes and
platyhelminthes of the body are too large to
be dealt with by the phagocytes.
Eosinophils produce materials including
enzymes that breakdown the body walls of
these parasites and protect the body.
Basophils and mast cells produce chemicals like
histamine that stimulate action of the immune
system.
Problems with vaccines conā€™t
ā€¢ Antigenic concealment ā€“ some pathogens are
able to hide inside body cells before an
immune response can be waged. They are
ā€˜protectedā€™ by being in the body cell eg.
Plasmodium in red blood cells. Some remain
in the intestines eg. Vibrio cholerae where
they cannot be reached by antibodies. To
combat this oral vaccines have been
developed against cholera
Problems with vaccines conā€™t
Some pathogens parasitize macrophages eg.
Myobacterium tuberculosis. Others parasitize
T helper cells eg. HIV. These suppress the
immune system.
ā€¢ Recently, there have been concerns about
vaccines influencing the development of
autism. There have also been concerns about
chemicals used to treat pathogens. Eg.
Mercury and chloroform
Monoclonal antibodies
ā€¢ Since B lymphocytes produce specific
antibodies, it would be ideal to be able to
produce antibodies outside the body.
ā€¢ Until recently it was difficult to produce pure
cultures.
ā€¢ In 1975 two persons (Cesar Milsten and
Georges Kohler) succeeded in producing pure
cultures.
Monoclonal antibodies conā€™t
ā€¢ They did this by fusing antibody secreting cells
with tumour cells.
ā€¢ The resulting cells are called HYBRIDOMAS.
ā€¢ These hybridomas secrete antibodies and are
considered ā€˜immortalā€™.
ā€¢ These hybridoma cells can be cultured as pure
clones and each type of antibody collected.
Monoclonal antibodies conā€™t
ā€¢ The antibodies collected this way are called
monoclonal antibodies.
Using monoclonal antibodies
1. They can be used to treat a range of
infections.
2. They can be used to separate a particular
antigen from a complex mixture ā€“ to do this
the monoclonal antibodies for the required
antigen are immobilized on resin beads
which are then packed in a column. When
the mixture is passed over the beads, only
the required antigen is removed.
Using monoclonal antibodies conā€™t
ā€¢ The antigen can then be washed from the
beads using a chemical which causes the
antibodies to release it.
3. They can be used in immunoassays ā€“ this is
the use of monoclonal antibodies to
determine the amount of a particular antigen
in a mixture. The antibodies are labelled eg.
With radioactive or fluorescent material for
easy detection.
Using monoclonal antibodies conā€™t
ā€¢ If they are added to a test sample they will
attach to their specific antigen. If the sample
is washed in a special solution, the unattached
antibodies are removed. The amount of
antigens in the sample is revealed by the
degree of radioactivity or fluorescence.
4. ELISA (Enzyme Linked Immunosorbant Assay)
ā€“ this is used in athletes drugs tests,
pregnancy test kits and HIV tests.
Using monoclonal antibodies conā€™t
ā€¢ The antibodies are immobilized and the test
solution passed over them. If the antibody is
specific for antigen X and X is present in the
test solution, it will bind to the antibody. A
second set of antibodies with an enzyme
attached is added to the solution. It combines
with antibody/antigen X complex. If a
substrate is added whose colour the enzyme
will change , the amount of chemical X can be
Using monoclonal antibodies conā€™t
determined.
5. Anticancer drugs are linked to monoclonal
antibodies which are attracted to the cancer
cells.
6. ADEPT (Antibody Direct Enzyme Prodrug
Therapy) ā€“ Monoclonal antibodies are tagged
with an enzyme which converts an inactive
form of the cytotoxic drug (prodrug) into an
active form.
Using monoclonal antibodies conā€™t
ā€¢ Once injected these antibodies link with the
cancer cells. The inactive form of the drug is
administered in large doses. It is only effective
on the cancer cells.
ā€¢ Monoclonal antibodies are used in the cancer
treatment Mabthera. The active ingredient is
rituximab and is used to treat non-Hodgkins
lymphoma which is a cancer affecting B cells.
Using monoclonal antibodies conā€™t
ā€¢ Rituximab binds to a specific protein on the
surface of the affected B lymphocytes
stimulating the immune system to get rid of
the cancer cells.

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Immunity

  • 2. Immunity ā€¢ This refers to the bodyā€™s ability to defend itself against diseases. ā€¢ Immunity is provided by the immune system. ā€¢ The immune system recognizes foreign material and produces chemicals to destroy it. ā€¢ The defence provided by the immune system can be physical, chemical and cellular.
  • 3. Immunity conā€™t ā€¢ Physical defence includes clotting ā€¢ Cellular defence includes the barrier created by epithelia and white blood cells. ā€¢ Chemical defence include the secretion of hydrochloric acid to destroy pathogens. ā€¢ White blood cells play a very important role in the immune system.
  • 4. Immunity conā€™t ā€¢ An antigen is a molecule which the body recognizes as foreign. ā€¢ Antigens have on their surfaces, large molecules such as proteins, glycoproteins, lipids and polysaccharides. ā€¢ White blood cells are able to recognize antigens.
  • 5. White blood cells ā€¢ White blood cells originate in the bone marrow. ā€¢ The two main groups involved in defence are phagocytes and lymphocytes. ā€¢ Phagocytes can be further classified into neutrophils and macrophages.
  • 6. Phagocytes ā€¢ These are made throughout a personā€™s lifetime in the bone marrow. ā€¢ They are stored in the bone marrow before they are distributed around the body. ā€¢ Phagocytes act as scavengers by removing dead cells as well as invasive microorganisms.
  • 7. Neutrophils ā€¢ Approximately 60% of white blood cells are neutrophils. ā€¢ They are transported by the blood throughout the body. ā€¢ They are often squeezed through the walls of the capillaries (by a process known as diapedesis) to ā€˜patrolā€™ the tissues.
  • 8. Neutrophils conā€™t ā€¢ They are short lived cells and are produced in large amounts during an infection.
  • 9. Macrophages ā€¢ These are larger than neutrophils. ā€¢ They are usually found in organs such as the lungs, liver, spleen, kidney and in the lymph nodes. ā€¢ They are made in the bone marrow and travel in the blood as monocytes. ā€¢ Monocytes develop into macrophages once they settle in the organs.
  • 10. Macrophages conā€™t ā€¢ Macrophages are long-lived. ā€¢ They cut up pathogens displaying their antigens so they can be easily recognized by lymphocytes. ā€¢ They therefore play a major role in initiating immune response.
  • 11. Phagocytosis ā€¢ Cells that are being attacked by pathogens produce histamine ā€¢ Mast cells are body cells that produce histamine and cause inflammation (see later) ā€¢ The pathogens also release chemicals. ā€¢ These chemicals from the pathogens along with the histamine attract passing neutrophils to the site of infection.
  • 12. Phagocytosis conā€™t ā€¢ Neutrophils have receptor proteins (opsonins) on their surfaces which allow them to recognise antibodies and chemicals produced by the bacteria. ā€¢ The pathogens may be clumped together and covered in antibodies (secreted by lymphocytes) which would also help to stimulate action by the neutrophils.
  • 13. Phagocytosis conā€™t ā€¢ The neutrophils move towards the pathogens and binds with the bacterium. ā€¢ The binding stimulates the formation of a pseudopodia and the formation of a vacuole called a phagosome. ā€¢ Lytic enzymes are released by lysozomes into the phagosome which break down the bacterium.
  • 14. Phagocytosis conā€™t ā€¢ Dead neutrophils collect as a site of infection as pus. (See handout for illustration. Make sure you can illustrate what is there) ā€¢ The histamine released by mast cells cause dilation of blood vessels making them leak. ā€¢ Plasma and white blood cells flow out into the infected area.
  • 15. Phagocytosis conā€™t ā€¢ Pus is formed from dead bacteria and white blood cells (mainly phagocytes). ā€¢ The inflamed area thus becomes red, hot and swollen. ā€¢ Sometimes a boil is formed which might eventually burst because of the pressure of the pus inside.
  • 16. Phagocytosis conā€™t ā€¢ Phagocytosis is enhanced by a group of blood proteins called complement. ā€¢ Complement proteins are made by macrophages, monocytes and other cells in the body especially those in the liver. ā€¢ They are usually inactive. ā€¢ When necessary they stick to invading micro- organisms (mainly yeasts and bacteria)
  • 17. Phagocytosis conā€™t making them conspicuous to phagocytes as foreign matter. ā€¢ Some destroy the membranes of bacteria.
  • 18. Lymphocytes ā€¢ These are smaller than phagocytes and have a large nucleus that fills most of the cell. ā€¢ There are two types: 1. B lymphocytes 2. T lymphocytes
  • 19. Origin and maturation of B lymphocytes ā€¢ As you already know, B cells are made in the bone marrow. ā€¢ Here the immature B cells divide by mitosis. ā€¢ Each B cell is specific to an antigen. ā€¢ It therefore means that many millions of B cell types exist in our bodies. ā€¢ During maturation, each B cell produces antibodies.
  • 20. Origin and maturation of B lymphocytes conā€™t ā€¢ The genes that code for antibodies change in a variety of ways to code for different antibodies during maturation. ā€¢ Each B cell then divides to give a small number of clones that are able to make the same antibodies.
  • 21. Origin and maturation of B lymphocytes conā€™t ā€¢ The antibodies formed during maturation of the B cells do not leave the cell. ā€¢ Rather, they form part of the plasma membrane. ā€¢ A part of each antibody forms a protein receptor. ā€¢ This receptor can combine with one type of antigen.
  • 22. Origin and maturation of B lymphocytes conā€™t ā€¢ If that antigen enters the body, there will be some mature B cells with cell surface receptors that recognise it. (See hand out for diagram. Make sure you can illustrate what is there)
  • 23. Action of B lymphocytes ā€¢ When pathogens enters the body for the first time, some of them are take up by macrophages (in lymph node etc). ā€¢ The macrophages expose the antigens from the pathogens on their surfaces. ā€¢ Any B lymphocyte that has cell surface receptors that are specific to the antigens exposed divide repeatedly my mitosis.
  • 24. Action of B lymphocytes conā€™t ā€¢ Within a few weeks, a huge number of identical B cells are produced. ā€¢ Some pathogens have more than one antigen on their surface. ā€¢ This means that several B cells are activated on entry of the pathogen. ā€¢ As each type B cell divides, a polyclone is formed (each type forms a clone)
  • 25. Action of B lymphocytes conā€™t ā€¢ Some of these B cells become plasma cells. ā€¢ Others become memory cells. ā€¢ Plasma cells are short lived. ā€¢ They produce antibody molecules very quickly (up to several thousand per second)
  • 26. Action of B lymphocytes conā€™t ā€¢ The antibody molecules are released into the blood, lymph or onto the linings of the gut or lungs. ā€¢ The antibody molecules last longer than the plasma cells. However, their concentrations eventually decrease.
  • 27. Action of B lymphocytes conā€™t ā€¢ The memory cells remain in circulation within the body for a very long time. ā€¢ If the same pathogen enters the body again, they divide rapidly forming more plasma cells and memory cells. ā€¢ This response occurs every subsequent time the pathogen enters the body.
  • 28. Action of B lymphocytes conā€™t ā€¢ Thus the pathogen is prevented from causing a disease. (See diagram on hand out ā€“ ensure you are able to illustrate what is there) ā€¢ The immunity offered by B lymphocytes is called humoral immunity. ā€¢ This is because antibodies are produced and transported in body fluids (blood and lymph)
  • 29. Primary and secondary responses ā€¢ When the body encounters an antigen for the first time, the response is slow because there are a few B cells that are specific to the particular antigen. ā€¢ This first response is called a primary response. ā€¢ During this response, the body experiences symptoms of the disease.
  • 30. Primary and secondary responses conā€™t ā€¢ When the pathogen tries to enter the body again, the response is much faster. ā€¢ This is because there are many memory cells which divide quickly to give plasma cells. Thus more antibodies are produced.
  • 31. Primary and secondary responses conā€™t ā€¢ This is called a secondary response. The body does not experience symptoms of the disease. ā€¢ Memory cells are the basis for immunological memory. (See graph on handout ā€“ be able to illustrate what is there)
  • 32. Antibodies ā€¢ So weā€™ve been talking about antibodies being produced by B lymphocytes. ā€¢ What really are antibodies? ā€¢ They are globular glycoproteins and form the group of plasma proteins called immunoglobulins. ā€¢ All antibodies has a basic strucure.
  • 33. Structure of an antibody http://tinyurl.com/77oeght
  • 34. Antibodies conā€™t ā€¢ All are made up of 4 polypeptide chains: two long or heavy chains and two short or light chains. ā€¢ The chains are held together by disulphide bridges. ā€¢ Each antibody molecule has two identical binding sites formed by both light and heavy chains.
  • 35. Antibodies conā€™t ā€¢ The sequence of amino acids form a specific three-dimensional shape which binds to only one type of antigen. ā€¢ This is called the variable region and varies for different antibodies. ā€¢ There is a hinge region formed between the two heavy chains. ā€¢ This provides flexibility.
  • 36. Antibodies conā€™t ā€¢ Antibodies work in different ways. ā€¢ Their actions can be summarized into four groups; 1. Agglutination ā€“ antibodies have two binding sites. They can therefore bind to antigens on two different pathogens. This can result in pathogens being clumped together making them more vulnerable to attack.
  • 37. Antibodies conā€™t 2. Precipitation ā€“ some antigens are soluble. Some antibodies bind them together into large units which are then precipitated out of solution. This way they are more easily digested by phagocytes. 3. Neutralization ā€“ some antibodies bind to toxins released by pathogens preventing harm.
  • 38. Antibodies conā€™t 4. Lysis ā€“ when some antibodies attach to a pathogen, they act as a binding site for a number of blood proteins (complement system). Some of these proteins are enzymes and cause breakdown of the pathogen. ā€¢ Immunoglobulin E (IgE) binds to the receptors of mast cells activating them to release histamine.
  • 39. Origin and maturation of T lymphocytes ā€¢ As you already know, T lymphocytes are made in the bone marrow. ā€¢ Here the immature T cells dived by mitosis. ā€¢ They then travel to the thymus gland where they mature. ā€¢ They develop specific receptors which are displayed in the plasma membrane.
  • 40. Origin and maturation of T lymphocytes conā€™t ā€¢ The mature T cells circulate in the body. (see hand out ā€“ be able to illustrate) ā€¢ Some form T helper cells, some form T cytotoxic cells, some form T suppressor cells and some form memory T cells.
  • 41. Action of T lymphocytes ā€¢ T cells are activated when they recognize an antigen in contact with a host cell. Eg. A macrophage which has cut up a pathogen displaying its antigen (a help signal). ā€¢ The T cell with matching receptors divide by mitosis to form a clone. ā€¢ The cells differentiate to form several types of cells, the two main types being T helper cells and killer T cells.
  • 42. Action of T lymphocytes conā€™t ā€¢ Cytokines are secreted by T helper cells when they are activated. ā€¢ Cytokines stimulate appropriate B cells to divide and develop plasma cells which secrete antibodies. ā€¢ Some secrete cytokines that stimulate macrophages to carry out phagocytosis more vigilantly.
  • 43. Action of T lymphocytes conā€™t ā€¢ The cytokines these T cells secrete belong to a group of proteins called lymphokines. ā€¢ Another lymphokine is called interferons. These inactivate the protein making machinery of the infected cell. This therefore inhibits the replication of viruses.
  • 44. Action of T lymphocytes conā€™t ā€¢ T cytotoxic cells search for body cells that are invaded with pathogens and are displaying the antigens. ā€¢ The killer T cells attach themselves to the infected cells and secrete toxic substances such as hydrogen peroxide killing these infected cells and the pathogens. (see handout ā€“ be able to illustrate)
  • 45. Action of T lymphocytes conā€™t ā€¢ T suppressor cells ā€“ these control the immune system. Once an infection has been eliminated, these cells suppress the activities of the lymphocytes. ā€¢ T memory cells ā€“ these remain in the body and become very active during a secondary response to antigens.
  • 46. Active and passive immunity ā€¢ Active immunity refers to resistance to disease derived by the body producing antibodies on exposure to antigens. ā€¢ Active immunity is long term and can be either natural or artificial. ā€¢ When pathogens enter the body by natural means (air borne, food borne etc.), B lymphocytes make antibodies to destroy them.
  • 47. Active and passive immunity conā€™t ā€¢ As you would remember, memory cells are formed which make the body immune the next time the pathogen invades the body. ā€¢ This is natural active immunity. ā€¢ In some cases antigens are injected or taken orally into the body. ā€¢ The body then makes antibodies which protect the body from those antigens.
  • 48. Active and passive immunity conā€™t ā€¢ Passive immunity refers to resistance to disease that is short lived and is not derived by any action of the body. ā€¢ Passive immunity can also be natural or artificial. ā€¢ Natural passive immunity is obtained when antibodies pass by natural means into the body.
  • 49. Active and passive immunity conā€™t ā€¢ Babies have natural passive immunity. ā€¢ This is a result of antibodies passing across the placenta from the mother to the foetus. ā€¢ After birth, the colostrum which the baby receives is rich in IgA which prevents the growth of bacteria. ā€¢ Because immunity is passive it is short lived.
  • 50. Active and passive immunity conā€™t ā€¢ Depending on the nature of a disease or infection, antibodies may need to be injected into the body. ā€¢ If the body were allowed to make its own antibodies, the person would die. Eg. Tetanus. ā€¢ This is artificial passive immunity.
  • 51. Vaccinations ā€¢ A vaccine is a preparation of antigenic material designed to stimulate the production of antibodies and develop immunity within the body. ā€¢ Immunity derived from exposure to live pathogens is the best but not always realistic. ā€¢ Some vaccines are very effective and one injection is sufficient. Some need vaccinations.
  • 52. Vaccinations conā€™t ā€¢ The materials used in vaccinations can be grouped: 1. Living attenuated organisms ā€“ these are pathogens that are treated (for example, using heat) so that they can multiply but are unable to cause the symptoms of the disease. Even though they are harmless, they stimulate the production of antibodies. Eg. Measles, tuberculosis, poliomyelitis
  • 53. Vaccinations conā€™t 2. Toxoids ā€“ the toxins which result from certain diseases can stimulate the body to produce antibodies. These toxins are modified to prevent them causing symptoms of the disease (eg. Treating it with formaldehyde) and then administered by injection. Eg. Diphtheria, tetanus
  • 54. Vaccinations conā€™t 3. Dead microorganisms ā€“ the pathogens are killed and then injected. Even though they are dead, they are able to stimulate the production of antibodies in the same way they would if they were living. Eg. Typhoid, cholera, whooping cough.
  • 55. Vaccinations conā€™t 4. Extracted antigens ā€“ chemicals with antigenic properties are extracted from the pathogens and injected. Eg. Influenza vaccine 5. Artificial antigens ā€“ Genetic engineering is used to transfer genes for the production of antigens from the pathogen to a harmless organism. These are grown in a laboratory for the production of antigens which are later used. Eg. Hepatitis B
  • 56. Problems with vaccines ā€¢ Despite the benefits derived from vaccines, there are several problems associated with them. 1. Poor response ā€“ due to weakened immune systems or malnourishment some persons do not develop the necessary B and T cell clones. Persons that are vaccinated with live viruses can pass it to others in faeces. Herd immunity is therefore ideal.
  • 57. Problems with vaccines conā€™t ā€¢ Antigenic variation ā€“ when pathogens mutate causing minor changes in the antigens they produce, this is called antigenic drift. Sometimes the memory cells will still recognise them and cause a secondary response. Sometimes there is an antigenic shift where the mutation is so great that there is a drastic change in antigen structure (eg. Influenza). This results in the vaccine being
  • 58. Problems with vaccines conā€™t changed every year. Also, some pathogens are eukaryotes eg. Plasmodium which causes malaria and Trypanosoma which causes sleeping sickness. Being eukaryotes, they have many more genes than viruses and bacteria and can have many hundreds or thousands of antigens (each stage in the life cycle has different antigens). There are therefore no effective vaccines against these diseases.
  • 59. Problems with vaccines conā€™t ā€¢ Large invaders like nematodes and platyhelminthes of the body are too large to be dealt with by the phagocytes. Eosinophils produce materials including enzymes that breakdown the body walls of these parasites and protect the body. Basophils and mast cells produce chemicals like histamine that stimulate action of the immune system.
  • 60. Problems with vaccines conā€™t ā€¢ Antigenic concealment ā€“ some pathogens are able to hide inside body cells before an immune response can be waged. They are ā€˜protectedā€™ by being in the body cell eg. Plasmodium in red blood cells. Some remain in the intestines eg. Vibrio cholerae where they cannot be reached by antibodies. To combat this oral vaccines have been developed against cholera
  • 61. Problems with vaccines conā€™t Some pathogens parasitize macrophages eg. Myobacterium tuberculosis. Others parasitize T helper cells eg. HIV. These suppress the immune system. ā€¢ Recently, there have been concerns about vaccines influencing the development of autism. There have also been concerns about chemicals used to treat pathogens. Eg. Mercury and chloroform
  • 62. Monoclonal antibodies ā€¢ Since B lymphocytes produce specific antibodies, it would be ideal to be able to produce antibodies outside the body. ā€¢ Until recently it was difficult to produce pure cultures. ā€¢ In 1975 two persons (Cesar Milsten and Georges Kohler) succeeded in producing pure cultures.
  • 63. Monoclonal antibodies conā€™t ā€¢ They did this by fusing antibody secreting cells with tumour cells. ā€¢ The resulting cells are called HYBRIDOMAS. ā€¢ These hybridomas secrete antibodies and are considered ā€˜immortalā€™. ā€¢ These hybridoma cells can be cultured as pure clones and each type of antibody collected.
  • 64. Monoclonal antibodies conā€™t ā€¢ The antibodies collected this way are called monoclonal antibodies.
  • 65. Using monoclonal antibodies 1. They can be used to treat a range of infections. 2. They can be used to separate a particular antigen from a complex mixture ā€“ to do this the monoclonal antibodies for the required antigen are immobilized on resin beads which are then packed in a column. When the mixture is passed over the beads, only the required antigen is removed.
  • 66. Using monoclonal antibodies conā€™t ā€¢ The antigen can then be washed from the beads using a chemical which causes the antibodies to release it. 3. They can be used in immunoassays ā€“ this is the use of monoclonal antibodies to determine the amount of a particular antigen in a mixture. The antibodies are labelled eg. With radioactive or fluorescent material for easy detection.
  • 67. Using monoclonal antibodies conā€™t ā€¢ If they are added to a test sample they will attach to their specific antigen. If the sample is washed in a special solution, the unattached antibodies are removed. The amount of antigens in the sample is revealed by the degree of radioactivity or fluorescence. 4. ELISA (Enzyme Linked Immunosorbant Assay) ā€“ this is used in athletes drugs tests, pregnancy test kits and HIV tests.
  • 68. Using monoclonal antibodies conā€™t ā€¢ The antibodies are immobilized and the test solution passed over them. If the antibody is specific for antigen X and X is present in the test solution, it will bind to the antibody. A second set of antibodies with an enzyme attached is added to the solution. It combines with antibody/antigen X complex. If a substrate is added whose colour the enzyme will change , the amount of chemical X can be
  • 69. Using monoclonal antibodies conā€™t determined. 5. Anticancer drugs are linked to monoclonal antibodies which are attracted to the cancer cells. 6. ADEPT (Antibody Direct Enzyme Prodrug Therapy) ā€“ Monoclonal antibodies are tagged with an enzyme which converts an inactive form of the cytotoxic drug (prodrug) into an active form.
  • 70. Using monoclonal antibodies conā€™t ā€¢ Once injected these antibodies link with the cancer cells. The inactive form of the drug is administered in large doses. It is only effective on the cancer cells. ā€¢ Monoclonal antibodies are used in the cancer treatment Mabthera. The active ingredient is rituximab and is used to treat non-Hodgkins lymphoma which is a cancer affecting B cells.
  • 71. Using monoclonal antibodies conā€™t ā€¢ Rituximab binds to a specific protein on the surface of the affected B lymphocytes stimulating the immune system to get rid of the cancer cells.