Immune system

ANATOMY AND PHYSIOLOGY
IMMUNITY
Maria Carmela L. Domocmat, RN, MSN
Instructor
School of Nursing
Northern Luzon Adventist College

2
To protect the body against pathogens, the
immune system relies on a multilevel network of
physical barriers, immunologically active cells,
and a variety of chemicals.
first line of defense – any barrier that blocks invasion
at the portal of entry – nonspecific
second line of defense – protective cells and fluids;
inflammation and phagocytosis – nonspecific
third line of defense – acquired with exposure to
foreign substance; produces protective antibodies and
creates memory cells – specific

Nonspecific and Specific responses of the
Immune System

Physical or Anatomical Barriers

5
Skin and mucous membranes of respiratory,
urogenital, eyes and digestive tracts
outermost layer of skin is composed of epithelial cells
compacted, cemented together and impregnated with
keratin; few pathogens can penetrate if intact
flushing effect of sweat glands
damaged cells are rapidly replaced
mucous coat impedes attachment and entry of bacteria
blinking and tear production
stomach acid
nasal hair traps larger particles

Sebaceous secretions
Lysozyme, an enzyme that hydrolyzes the cell wall
of bacteria, in tears
High lactic acid and electrolyte concentration in
sweat
Skin’s acidic pH
Hydrochloric acid in stomach
Digestive juices and bile of intestines
Semen contains antimicrobial chemical.
Vagina has acidic pH.
6

7

8
Some hosts are genetically immune to the
diseases of other hosts.
Some pathogens have great specificity.
Some genetic differences exist in
susceptibility.

9
The study of the body’s second and third
lines of defense is called immunology.
Functions of a healthy immune system:
1.Constant surveillance of the body
2.Recognition of foreign material
3.Destruction of entities deemed to be foreign

10

11
Large, complex, and diffuse network of
cells and fluids that penetrate into every
organ and tissue
Four major subdivisions of immune
system are:
1.Reticuloendothelial system (RES)
2.Extracellular fluid (ECF)
3.Bloodstream
4.Lymphatic system

12

13
Network of connective tissue fibers that
interconnects other cells and meshes with the
connective tissue network surrounding organs
Inhabited by phagocytic cells – mononuclear
phagocyte system – macrophages ready to
attack and ingest microbes that passed the
first line of defense

14
Whole blood consists of plasma and blood
cells – red blood cells and white blood
cells.
Serum is the liquid portion of the blood after a
clot has formed-minus clotting factors.
Plasma – 92% water, metabolic proteins,
globulins, clotting factors, hormones and
all other chemicals and gases to support
normal physiological functions

15
Neutrophils- 55-90% - lobed nuclei with lavender
granules; phagocytes
Eosinophils – 1-3% - orange granules and bilobed
nucleus; destroy eucaryotic pathogens
Basophils, mast cells – 0.5% - constricted nuclei,
dark blue granules; release potent chemical
mediators
Lymphocytes – 20-35% - large nucleus B (humoral
immunity) and T cells (cell-mediated immunity)
involved in the specific immune response
Monocytes, macrophages – 3-7%- large nucleus;
phagocytic

18
1.Provides an auxiliary route for return of
extracellular fluid to the circulatory
system
2.Acts as a drain-off system for the
inflammatory response
3.Renders surveillance, recognition, and
protection against foreign material

19

20
Lymph is a plasma-like liquid carried by
lymphatic circulation
Formed when blood components move
out of blood vessels into extracellular
spaces
Made up of water, dissolved salts, 2-5%
proteins
Transports white blood cells, fats, cellular
debris and infectious agents

21
Lymphatic capillaries permeate all parts of
the body except the CNS.
Thin walls easily permeated by
extracellular fluid which is then moved
through contraction of skeletal muscles
Functions to return lymph to circulation;
flow is one-direction-toward the heart-
eventually returning to blood stream

22
Classified as primary and secondary
Primary lymphoid organs – sites of lymphocytic
origin and maturation – thymus and bone
marrow
Secondary lymphoid organs and tissues –
circulatory-based locations such as spleen and
lymph nodes; collections of cells distributed
throughout body tissues – skin and mucous
membranes – SALT, GALT, MALT

23

24
Thymus – high rate of growth and activity
until puberty, then begins to shrink; site of T-
cell maturation
Lymph nodes - small, encapsulated, bean-
shaped organs stationed along lymphatic
channels and large blood vessels of the
thoracic and abdominal cavities
Spleen – structurally similar to lymph node;
filters circulating blood to remove worn out
RBCs and pathogens

Nonspecific response

26
•Inflammation
•Fever
•Phagocytosis, NK cells, Interferon
•Complement

27
Classic signs and symptoms characterized by:
Redness – increased circulation and vasodilation in
injured tissue in response to chemical mediators
and cytokines
Warmth – heat given off by the increased blood
flow
Swelling – increased fluid escaping into the tissue
as blood vessels dilate-edema; WBC’s, microbes,
debris and fluid collect to form pus; helping prevent
spread of infection
Pain – stimulation of nerve endings
Possible loss of function

pain (dolor)
heat (calor)
redness (rubor)
swelling (tumor)
loss of function
(functio laesa).

29
Insert figure 14.13
Events in inflammation

30
Diapedesis – migration of cells out of
blood vessels into the tissues
Chemotaxis – migration in response to
specific chemicals at the site of injury or
infection

31

http://images.google.com/imgres?imgurl=http://www.vacadsci.org/jsr/imuneR.jpg&imgrefurl=http://www.vacadsci.org/jsr/tlist2.htm&h=663&w=1009&sz=460&tbnid=w5XN6XPgUBEJ:&tbnh=
97&tbnw=149&hl=en&start=9&prev=/images%3Fq%3Dimmune%2Bresponse%26svnum%3D10%26hl%3Den%26lr%3D%26sa%3DG
Inflammation

Initiated by circulating pyrogens which reset the
hypothalamus to increase body temperature;
signals muscles to increase heat production and
vasoconstriction
exogenous pyrogens – products of infectious agents
endogenous pyrogens – liberated by monocytes,
neutrophils, and macrophages during phagcytosis;
interleukin-1 (IL-1) and tumor necrosis factor (TNF)
Benefits of fever:
inhibits multiplication of temperature-sensitive
microorganisms
impedes nutrition of bacteria by reducing the available
iron
increases metabolism and stimulates immune reactions
and protective physiological processes
34

35
3 main types of phagocytes:
1.Neutrophils – general-purpose; react early to
bacteria and other foreign materials, and to
damaged tissue
2.Eosinophils – attracted to sites of parasitic
infections and antigen-antibody reactions

3. Monocytes
called wandering cells until they enter a tissue where
they become fixed and turn into macrophages
Macrophages
scavenge and process foreign substances to prepare
them for reactions with B and T lymphocytes
▪destroy old, damaged and dead cells in the body
▪macrophages are found in the liver, spleen, lungs,
lymph nodes, skin and intestine

Copyright © 2006 Dr. Salme Taagepera, All rights reserved.
Macrophages in action

38
General activities of phagocytes:
1.To survey tissue compartments and
discover microbes, particulate matter and
dead or injured cells
2.To ingest and eliminate these materials
3.To extract immunogenic information
from foreign matter

39

40
Small protein produced by certain white blood
cells and tissue cells
alpha interferon- lymphocytes and macrophages
beta interferon – fibroblasts and epithelial cells
gamma interferon – T cells
Produced in response to viruses, RNA, immune
products, and various antigens
Bind to cell surfaces and induce expression of
antiviral proteins
Inhibit expression of cancer genes

41

42
Consists of 26 blood proteins that work in concert
to destroy bacteria and viruses
there are only a handful of proteins in the
complement system, and they are floating freely
in your blood.
manufactured in the liver.
activated by and work with (complement) the
antibodies, hence the name.
they cause lysing (bursting) of cells and signal to
phagocytes that a cell needs to be removed

43

45

Specific defense

47
Third line of defense – acquired
Production of specific antibodies by dual system of
B and T lymphocytes in response to an encounter
with a foreign molecule, called an antigen
Two features that characterize specific immunity:
specificity – antibodies produced, function only against
the antigen that they were produced in response to
memory – lymphocytes are programmed to “recall” their
first encounter with an antigen and respond rapidly to
subsequent encounters

http://images.google.com/imgres?imgurl=http://www.vacadsci.org/jsr/imuneR.jpg&imgrefurl=http://www.vacadsci.org/jsr/tlist2.htm&h=663&w=1009&sz=460&tbnid=w5XN6XPgUBEJ:&tb
nh=97&tbnw=149&hl=en&start=9&prev=/images%3Fq%3Dimmune%2Bresponse%26svnum%3D10%26hl%3Den%26lr%3D%26sa%3DG
Nonspecific and Specific responses of the
Immune System
T cells B cells

Made up of two cellular systems (lymphocytes)
1.humoral or circulating antiBody system - B cells
2.cell mediaTed immunity - T cells

http://www.people.virginia.edu/~rjh9u/gif/irsum.gif
B cells make
antibodies
T cells mount
direct attack on
foreign/infected
cell

Aka: humoral immunity
Involves antigen-antibody interactions to
neutralize, eliminate, or destroy foreign
proteins.

Purpose:
Main function of B-cells: to become sensitized to a
specific protein (antigens) and to produce
antibodies directed specifically against that
protein

B-cells
Macrophages
T-lymphocytes

All these work with B-cells to start and
complete antigen-antibody interactions
Therefore: for optimal AMI, the entire
immune system must function adequately

Start in bone marrow
Released in the blood
Then migrate into secondary lymphoid
tissues where maturation is completed
Spleen
Parts of lymph nodes
Tonsils
Peyer’s patches of GIT

Two main functions:

1) Return tissue fluid
to circulation

2) Fights infection
- both specific and
non-specific
resistance.

Lymph- fluid carried by
lymphatic vessels

- fluid enters lymphatic system by diffusing into dead-
end lymphatic capillaries

- infection-fighting activities occur in the lymph nodes

Lymphocytes (25-35% of WBCs)

T-cells: 70% of lymphocytes
▪Cell mediated immunity

B-cells: 20-25% of lymphocytes
▪Humoral immunity

Body learns to make enough of any specific
antibody to provide long-lasting immunity
against specific organisms or toxins

7 Steps needed to make a specific antibody
against an antigen

1.Exposure (invasion)
2.Antigen recognition
3.Lymphocyte sensitization
4.Antibody production and release
5.Antigen-antibody binding
6.Antibody-binding actions
7.Sustained immunity: Memory

B cell activation occurs in response to
exposure to a specific foreign antigen
Invasion must occur in large #s that some
may evade detection by other lines of
defense

Helper T cells secrete a chemical called
interleukins
Interleukin 6 – induces maturation of B cells and
proliferation of T cells

1.Exposure (invasion)
2.Antigen recognition
3.Lymphocyte sensitization
4.Antibody production and release
5.Antigen-antibody binding
6.Antibody-binding actions
7.Sustained immunity: Memory

“virgin” or “naïve” unsensitized B-cells must
recognize the antigen as non-self
Need help of macrophages and
helper/inducer T-cells

1.Exposure (invasion)
2.Antigen recognition
3.Lymphocyte sensitization
4.Antibody production and release
5.Antigen-antibody binding
6.Antibody-binding actions
7.Sustained immunity: Memory

Virgin B-cell can be sensitized only once
Therefore each B-cell can be sensitized to
only one type of antigen
Immediately after it is sensitized –it divides
and form two types of B-lymphocytes

B cells divide:
1.Plasma cells = synthesize and secrete large
numbers of antibodies with the same antigen
target
▪Can make as much as as 300 molecules of antibody
/sec
2.Memory B cells = remain in reserve for future
attacks by the same antigen

When an antibody binds to the outer coat of a
virus particle or the cell wall of a bacterium it
can stop their movement through cell walls.
Or a large number of antibodies can bind to
an invader and signal to the complement
system that the invader needs to be
removed.

1.Exposure (invasion)
2.Antigen recognition
3.Lymphocyte sensitization
4.Antibody production and release
5.Antigen-antibody binding
6.Antibody-binding actions
7.Sustained immunity: Memory

Antibody molecules are released in blood and
other body fluids as free antibody
Each remain in the blood for 3 to 30 days

Note: circulating antibodies can be
transferred from one person to another to
provide the receiving person with immediate
immunity of short duration

1.Exposure (invasion)
2.Antigen recognition
3.Lymphocyte sensitization
4.Antibody production and release
5.Antigen-antibody binding
6.Antibody-binding actions
7.Sustained immunity: Memory

When a pathogen enters the
body it stimulates specific
lymphocytes to make
antibodies

These antibodies are
proteins of a very specific
shape and they will attach to
the specific antigens on the
surface of the pathogen

Binding of the antibody to
the pathogen targets the
pathogen for destruction by
macrophages

http://www.blc.arizona.edu/courses/181summer/graphics/gr
aphics%20lect16/Life7e-Fig-18-10-
2%20structure%20of%20antibody%20p2.jpg
http://www.biology.arizona.edu/immunology/
tutorials/antibody/graphics/antibody.gif
Antibodies are protein complexes made of 2 heavy chain and 2 light chain peptides
•Constant region (shown dark blue and dark red) = same in all antibodies
•Variable region (shown light blue and light red)= unique in each antibody

http://www.accessexcellence.org/RC/VL/GG/images/Fig_5.03b.jpg

Type Number of
ag binding
sites
Site of action Functions
IgG 2 •Blood
•Tissue fluid
•CAN CROSS
PLACENTA
•Increase
macrophage activity
•Antitoxins
•Agglutination
IgM 10 •Blood
•Tissue fluid
Agglutination
IgA 2 or 4 •Secretions (saliva,
tears, small intestine,
vaginal, prostate,
nasal, breast milk)
•Stop bacteria
adhering to host
cells
•Prevents bacteria
forming colonies on
mucous membranes
IgE 2 Tissues •Activate mast cells
 HISTAMINE
•Worm response

IgG (75% of Total Immunoglobulin)
• Appears in serum and tissues (interstitial fluid)
• Assumes a major role in bloodborne and tissue infections
• Activates the complement system
• Enhances phagocytosis
• Crosses the placenta

IgA (15% of Total Immunoglobulin)
• Appears in body fluids (blood, saliva, tears, breast milk, and
pulmonary, gastrointestinal, prostatic, and vaginal secretions)
• Protects against respiratory, gastrointestinal, and genitourinary
infections
• Prevents absorption of antigens from food
• Passes to neonate in breast milk for protection

IgM (10% of Total Immunoglobulin)
• Appears mostly in intravascular serum
• Appears as the first immunoglobulin produced in response
to bacterial and viral infections
• Activates the complement system

IgD (0.2% of Total Immunoglobulin)
• Appears in small amounts in serum
• Possibly influences B-lymphocyte differentiation, but role
is unclear

IgE (0.004% of Total Immunoglobulin)
• Appears in serum
• Takes part in allergic and some hypersensitivity reactions
• Combats parasitic infections

IgD
IgG
IgA
IgM
IgE

Actual binding of antibody to antigen is
usually not lethal to the antigen

Instead it starts other actions that neutralize,
eliminate, or destroy antigen

1.Exposure (invasion)
2.Antigen recognition
3.Lymphocyte sensitization
4.Antibody production and release
5.Antigen-antibody binding
6.Antibody-binding actions
7.Sustained immunity: Memory

Agglutination
Lysis
Complement fixation
Precipitation
Inactivation-neutralization

1.Exposure (invasion)
2.Antigen recognition
3.Lymphocyte sensitization
4.Antibody production and release
5.Antigen-antibody binding
6.Antibody-binding actions
7.Sustained immunity: Memory

The first exposure to a
pathogen gives only a
slow and small immune
response
Levels of antibodies in the blood build up slowly when you are first exposed to
a particular pathogen.
•It takes over 5 days for the antibodies to reach a level that will fight off the
infection.
•During this time, you will feel the symptoms of the infection and damage will
be caused to your body tissues.
•In serious diseases, this can be fatal.

•The first exposure to a pathogen gives only a slow and small immune response.
•Repeated exposure to the same pathogen gives a much stronger and quicker memory response.

When your body is first infected with a pathogen, the
main task of the immune system is to combat the
infection. However, it also produces lymphocytes that
remain in your body for many years and remember
the pathogen in case it returns.
Immune memory
If you get infected a second time, your immune system is
already prepared for the pathogen and can quickly make
enough antibodies to kill the infection before any symptoms
are felt.
Vaccination takes advantage of this feature of the immune
system.

Once a T cell is activated by the presentation of the
combined MHC/Ag, it will clone (by mitosis) &
differentiate into:
 cytotoxic T cells
 helper T cells
 memory T cells
 suppressor T cells

T-cell receptor structure similar to antibody

1.Cytotoxic T cells
attack foreign cells
seek out the specific pathogen/infected cell that
contains the targeted Ag & destroys it by secreting
various chemicals

Killer cell Target cell

2.Memory T-cells
remain in reserve
When body sees the same antigen again, these cells
produce a rapid, specific response
these cells can immediately differentiate into cytotoxic &
helper T cells, causing a swift secondary response to the
invasion

3.Suppressor T-cells
depress the response of T and B cells
are slow to activate but effectively “put on the brakes” or
end the immune response
activated more slowly than the other T cells
inhibit the response of the immune cells to prevent
potential “autoimmune” response

4.Helper T cells
orchestrate immune response
necessary for coordination of both specific & non-specific
defenses, as well as for stimulating both cell-mediated &
antibody-mediated immunity.
In cell-mediated immunity they release chemicals
(cytokines) that strengthen the activity of cytotoxic T cells.
In antibody-mediated immunity they release cytokines
that stimulate activated B cell division & differentiation
into plasma cells

Helper T cells
release a variety of compounds called cytokines
cytokines
1.coordinate both specific and non-specific defenses
2.stimulate production of more t cells
3.stimulate production of antibodies by B cells

T lymphocytes (T cells) – they mature in the thymus and
are responsible for cell-mediated immunity
a) Helper T cells – direct the rest of the immune system by
releasing cytokines
b) Cytotoxic T cells – release chemicals that break open
and kill invading organisms
c) Memory T cells – remain afterwards to help the immune
system respond more quickly if the same organism is
encountered again
d) Suppressor T cells – suppress the immune response so
that it does not get out of control and destroy normal cells
once the immune response is no longer needed

Antigens
bacteria
viruses
ANTIGENS
bacteria
viruses
SPECIFIC
DEFENSES
(Immune
response)
CELL MEDIATED IMMUNITY
APC’s phagocytize Ag & activate T
cells
Direct physical &
chemical attack

Activated T cells clone &
differentiate into:
 Cytotoxic T cells
 Helper T cells
 Memory T cells
 Suppressor T cells
Remain in
reserve
B cell
activation
stimulate
Prevent
autoimmune
response

Immunization raises host resistance,
defenses, and immunity

Immunity is the resistance to injuries/disease caused by specific pathogens

Types of immunity:
http://faculty.ircc.edu/faculty/tfischer/images/t
ypes%20of%20immunity.jpg

Overview of Immunity

present at birth
independent of previous exposure to Ag
genetically determined
species dependent

arises throughout life by active or passive
means

Active immunity
Lymphocytes are activated by antigens on
the surface of pathogens

Takes time for enough B and T cells to be
produced to mount an effective response.

Natural active immunity
naturally acquired active immunity
acquired due to infection
natural exposure results in immune response &
development of long term immunity

Artificial active immunity
Vaccination
induced (artificial) active immunity – deliberate “artificial”
exposure to Ag (i.e. vaccine/immunization)

Passive immunity – development of immunity
due to transfer of “pre-made” antibodies
 naturally acquired passive immunity – Ab’s
transferred from mom  baby across placenta or in
breast-milk
 induced (artificial) passive immunity – administration
of Ab’s to fight disease after exposure to pathogen

Passive immunity
B and T cells are not activated and plasma
cells have not produced antibodies.
The antigen doesn’t have to be encountered
for the body to make the antibodies.
Antibodies appear immediately in blood but
protection is only temporary.

 Used when a very rapid immune response
is needed
e.g. after infection with tetanus. Human
antibodies are injected. In the case of tetanus
these are antitoxin antibodies.
Antibodies come from blood donors who have
recently had the tetanus vaccination.

Only provides short term protection as abs
destroyed by phagocytes in spleen and liver.

A mother’s antibodies pass across the
placenta to the foetus and remain for several
months.
Colostrum (the first breast milk) contains lots
of IgA which remain on surface of the baby’s
gut wall and pass into blood

A preparation containing antigenic
material:
Whole live microorganism
Dead microorganism
Attenuated (harmless) microorganism
Toxoid (harmless form of toxin)
Preparation of harmless ags

Injection into vein or muscle
Oral

117

Why aren’t they always effective?
Natural infections persist within the body for a
long time so the immune system has time to
develop an effective response, vaccinations from
dead m-os do not do this.
Less effective vaccines need booster injections
to stimulate secondary responses
Some people don’t respond well/at all to
vaccinations
Defective immune systems
Malnutrition particularly protein

Antigenic variation caused by mutation
Antigenic drift – small changes (still recognised by
memory cells)
Antigenic shift – large changes (no longer recognised)
No vaccines against protoctists (malaria and sleeping
sickness)
Many stages to Plamodium life cycle with many
antigens so vaccinations would have to be effective
against all stages (or be effective just against infective
stage but given in very small time period).

Sleeping sickness – Trypanosoma has a
thousand different ags and changes them
every 4-5 days
Antigenic concealment parasites live inside
body cells
Plasmodium – liver and blood cells
Parasitic worms – cover themselves in host
proteins
HIV – live inside T-helper cells

http://www.vacadsci.org/jsr/imuneR.jpg
Review of the immune response
Non-
specific
response
Specific
response
NOTE: key role played by Helper T cells!!!

Recommended Adult
Immunization
Schedule
Recommended
pediatric immunization
schedule
•Contraindications

Who should not get the vaccine or should wait?
1. people who have had a life threatening allergic reaction to
gelatin, neomycin, or a previous dose of the vaccine
2. people who are moderately or severely ill should wait
3. pregnant women should wait until after birth, women should
not get pregnant for 1 month after getting the vaccine
4. people with HIV/AIDS, immune system problems, taking any
drugs that affect the immune system, have cancer, or taking
chemotherapy or x-ray therapy for cancer should check with
their doctor before receiving the vaccine
5. people who recently had a blood transfusion should check
with their doctor

Live-microbial vaccines should not be given
simultaneously with blood, plasma, or immune globulin,
which can interfere with development of desired
antibodies; ideally, such vaccines should be given 2 wk
before or 6 to 12 wk after the immune globulins.
Immunocompromised patients should not receive live-
virus vaccines, which could provoke severe or fatal
infections.
In patients receiving short-term (ie, < 14 days)
immunosuppressive therapy (eg, corticosteroids,
antimetabolites, alkylating compounds, radiation), live-
virus vaccines should be withheld until after treatment.

Immunity may or may not be life-long with
vaccines.
To help keep the antibody levels high enough
to keep you protected you sometimes need
to have “booster shots”.

Nutrition and the immune system
Malnutrition impairs immune function
Fish oil: anti inflam
Stress and the immune system
Chronic stress has detrimental effects on immune
system
Ageing and the immune system
Vaccination

About This Presentation

Slide Content

Tags

Categories

Download

Quick Actions

Statistics

Related Slideshows

Immune system

About This Presentation

Slide Content

Slide 1

Slide 2

Slide 3

Slide 4

Slide 5

Slide 6

Slide 7

Slide 8

Slide 9

Slide 10

Slide 11

Slide 12

Slide 13

Slide 14

Slide 15

Slide 18

Slide 19

Slide 20

Slide 21

Slide 22

Slide 23

Slide 24

Slide 25

Slide 26

Slide 27

Slide 28

Slide 29

Slide 30

Slide 31

Slide 32

Slide 34

Slide 35

Slide 36

Slide 37

Slide 38

Slide 39

Slide 40

Slide 41

Slide 42

Slide 43

Slide 45

Slide 46

Slide 47

Slide 48

Slide 49

Slide 50

Slide 52

Slide 53

Slide 54

Slide 56

Slide 57

Slide 58

Slide 59

Slide 60

Slide 61

Slide 62

Slide 63

Slide 64

Slide 66

Slide 67

Slide 68

Slide 69

Slide 70

Slide 71

Slide 72

Slide 73

Slide 74

Slide 75

Slide 77

Slide 78

Slide 79

Slide 80

Slide 82

Slide 83

Slide 84

Slide 85

Slide 87