This page is "borrowed" from Dr.
John Stevenson at the University of Miami.
Human Host Defense against Infectious
Disease
Resistance factors are present before infection and
nonspecific - i.e., they work all the time and effective
against many different kinds of microbes
External resistance factors - those which act on
body surfaces
- physical
- barriers - skin, mucus, nasal hair
- environmental conditions - dryness
- flushing action - blinking of eyelid, peristalsis,
urination
- chemical - activities carried out by molecules
- salts - secreted by sweat glands in skin
- acids - low pH (HCl in stomach; lactic and other
skin acids produced by normal microbiota)
- lipids - fatty acids secreted by sebaceous glands
and by gall bladder
- enzymes - lysozyme (secretions), digestive enzymes
(stomach, small intestine)
- cellular - activities carried out by cells
- normal microbiota compete with pathogens for
attachment sites and nutrients as well as producing factors
toxic to pathogens
- phagocytes (macrophages; polymorphonuclear
leukocytes [PMN]) are cells that engulf and destroy
particles on mucous membranes by a process known as phagocytosis
Internal resistance factors - those which act within
tissues
- physical - barriers such as connective tissue,
blood-brain barrier
- chemical - activities carried out by molecules
- enzymes - lysozyme and other enzymes in blood and
tissue fluids
- complement - can be nonspecifically activated by
bacterial and fungal polysaccharides or lipopolysaccharides
- triggers inflammation and enhances phagocytosis
(opsonization) by enhancing binding of particles to
phagocytes via receptors
- membrane attack complex (MAC) disrupts (lyses)
enveloped viruses and some bacteria
- cellular - activities carried out by cells
- inflammation - "early-warning" system
- histamine released from mast cells at sites of
tissue damage
- increases permeability of capillaries at these
sites
- capillaries become "leaky" causing accumulation
of complement, enzymes and phagocytes at sites of
infection
- pathogens eliminated (phagocytosis, etc.) and healing
initiated
- cardinal signs of inflammation - erythema
(redness); edema (swelling); fever (heat);
pain (soreness)
- phagocytes (macrophages;
polymorphonuclear leukocytes [PMN]) are cells that
engulf and destroy particles, including pathogens, by a process
known as phagocytosis:
- adhesion (attachment) - phagocyte and pathogen
bind to each other
- ingestion (engulfment) - pseudopodia
surround the pathogen, then fuse to form a vacuole called a
phagosome
- digestion/killing - inside phagolysosomes,
which are formed by fusion of lysosomes with phagosomes:
- hydrogen peroxide and related compounds kill
microbes
- enzymes digest microbes
- egestion - residual (non-digestable) particles
are released from the cell by a process that is essentially
the reverse of ingestion
Immune factors are triggered during infection by
antigens, substances produced by microbes, and is
specific for only those pathogens to which one is exposed
Antibody-Mediated Immunity (AMI)
- antibody
responses - antibody
is produced by B cells (B lymphocytes) stimulated by T
cells (T lymphocytes) in response to antigens made by
infectious agents
- antigen presenting cells (APCs) engulf, process and
present fragments of exogenous antigen molecules on their
surfaces
- Th cells recognize (using antigen receptors on their
surfaces) antigen fragments, then proliferate and differentiate
to form a large population of cytokine-producing Th
cells
- B cells bind exogenous antigen (using antigen
receptors on their surfaces) and bind cytokines (using cytokine
receptors on their surfaces), then proliferate and
differentiate to form a large population of
antibody-producing plasma cells
- mechanisms of action (ways in which AMI functions) -
antibody
binds specifically to the antigen that induced its
formation to carry out these AMI mechanisms:
- neutralization - inhibition of toxin function, viral
infectivity, microbe attachment due to antibody binding to
surface antigens of pathogens
- antibody/complement-mediated lysis - complement is
activated by binding to antibody molecules that have bound to
antigens, and causes lysis of microbes via formation of
a membrane attack complex (MAC)
- opsonization - antibody and complement both
enhance attachment of pathogens to phagocytes via
receptors that bind them
Cell-Mediated
Immunity (CMI)
- cellular responses
- cytotoxic
T lymphocytes (CTLs) are activated by T helper
cells in the presence of viral antigens on virus-infected
cells
- APCs engulf, process and present fragments of
exogenous antigen molecules on their surfaces
- Th cells recognize (using antigen receptors on
their surfaces) antigen fragments, then proliferate and
differentiate to form a large population of
cytokine-producing Th cells
- Tc cells (CTL precursor cells) bind exogenous
antigen (using antigen receptors on their surfaces) and bind
Th cell-produced cytokines (using cytokine receptors on
their surfaces), then proliferate and differentiate to form
a large population of CTLs
- macrophages
are also activated by T helper cells
- APCs engulf, process and present fragments of
exogenous antigen molecules on their surfaces
- Th cells recognize (using antigen receptors on
their surfaces) antigen fragments, then proliferate and
differentiate to form a large population of
cytokine-producing Th cells
- macrophages bind Th cell-produced cytokines
(using cytokine receptors on their surfaces), then
differentiate to form activated macrophages
- mechanisms of action (ways in which CMI functions)
- CTLs kill "target" cells by destroying their
membranes (necrosis) or inducing them to destroy
themselves (apoptosis)
- activated macrophages engulf, kill and digest
intracellular bacteria and fungi much more efficiently than
normal macrophages do, partially because they starve these
microbes (by destroying nutrients the microbes need to
grow)
Immunocompromised people are more susceptible to infectious
diseases than normal people, and this increased susceptibility can be
due to one or more of these:
- genetics - inheritance of defective genes that block
normal development or expression of immune response elements
(cells or molecules)
- immaturity - newborns are highly susceptible because
their immune systems have not yet had a chance to mature and
become fully functional
- infectious diseases - lowered resistance caused by
diseases such as AIDS
- disease treatment - weakened resistance caused by drug
therapy for cancer, etc.
- stress - decreases resistance and immune response
development
