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GMS 6006 - Fundamentals of Immunology & Microbiology Spring 2006
February 15, 2006February 15, 2006
Introduction to ImmunityIntroduction to ImmunityAntibody Function & Antibody Function & DiversityDiversity
Wayne T. McCormack, Ph.D.R1-102, 392-7413, mccormac@pathology.ufl.edu
Introduction: The goal of these two lectures is to provide an overview of the immune system and how it operates.
Antibody Gene Rearrangement
Why in the world are we considering antibodies now?
I thought this section was about molecular biology . . .
For further reading: “Immunobiology - The Immune System in Health & Disease”, Janeway et al., 6th edition, 2005.
For the basics: GMS 6006 – Fundamentals of Immunology & Microbiology
For the whole story: GMS 6140 “Principles of Immunology” = GMS 6031/6032/6033 immunology advanced modules
September 30, 2005
Wayne T. McCormack, Ph.D.
All textbook figures herein identified by Fig. number
© Garland Science
“Immunobiology - The Immune System in Health & Disease”, Janeway et al., 6th edition, 2005
Monday, October 29, 2001
West Nile virus spreads throughout Florida, here to stay
By MIRANDA LEITSINGERAssociated Press Writer
MIAMI (AP) - Chevy could hardly stand on his own. He didn'teat, he wasn't responding to his owners and he was dragging hishind quarters. The 9-year-old horse, a Palomino Appaloosa thathas won medals for sliding stops and spins in equestriancompetitions, could barely walk.
''It was so hard to watch ... to see one reduced to this,'' saidowner Sheila Anderson, of Coral Springs. ''I just cried and cried.''
Chevy, a golden-colored horse with a white mane and tail, wasthe first confirmed case in Broward County of the West Nilevirus. As of last week, 51 of Florida's 67 counties from thePanhandle to the Keys were under a medical alert for theHealth experts expected the number to keep increasing …...
Thursday, October 18, 2001
More than 30 on Capitol Hill test positive for anthrax
By TODD S. PURDUM and ALISON MITCHELLThe New York Times
WASHINGTON - Concern about biological terrorism heightenedWednesday as preliminary tests showed that more than 30workers on Capitol Hill were exposed to anthrax spores from thecontaminated letter sent to the office of the Senate majorityleader. Officials also disclosed that early testing has shown thatthe anthrax samples found in media offices in New York andFlorida were of the same strain.
While there was no evidence that anyone has yet been infectedwith what Attorney General John Ashcroft called a ''virulent,strong, very serious'' form of powdery anthrax that was found ina letter Monday in the office of Sen. Tom Daschle, D-S.D., wordthat more than half the workers in his suite were exposedprompted the closure of all six House and Senate office buildingsfor further screening …...
What disease does this man have?
December 29. 2002
UF scientists: Hold off on smallpox vaccine
By DIANE CHUNSun Staff Writer
The UF researchers say mass vaccinations present more risks than benefits.
Beginning in January, county and state public health officials will begin to carry out the Bush administration's plan to vaccinate 10.5 million medical personnel and emergency responders against smallpox.
Should the federal government decide to proceed with the final stage of those plans, scheduled for sometime in 2004, as many as 10 million Floridians might be eligible for voluntary vaccination against smallpox.
The question will then become: Should they get vaccinated? ……
February 28. 2003
3 have reaction to smallpox shot
By DIANE CHUNSun Staff Writer
Officials with the state Department of Health reported that three additional health care workers have apparently had adverse reactions to the smallpox vaccine they received as part of Operation Vaccination.
Thursday's announcement came slightly more than a week after the focus of the state's effort shifted from health department workers to groups drawn from hospitals throughout Florida. A total of 1,186 people had received the vaccine as of Monday. One earlier reaction had been reported. ……
Are there any other medical conditions in which something “foreign” resides in your body?
Is an immune response always
beneficial?c.2000 G.Caviness, BioGrafix
What does “immunity” mean to you? What are the key features of an “immune
response”? How old is the concept of “immunity”?
Edward Jenner’s experiment (1796)
material from cowpoxlesion of milkmaid
village boy susceptibleto smallpox
inoculate withcowpox
wait 2 monthsinoculate with
smallpox
child recoversfrom cowpox
child does notdevelop smallpox
GOALS OF THE IMMUNE SYSTEM
Distinguish between “self” and “non-self”
Separate/exclude self from non-self
Remove non-self if self is penetrated
Spaces of the Body That Need to Be Monitored
and Defended
Major classes of pathogens:
bacteria
viruses
protozoa, fungi, parasites
Fig. 10-4
Cells of the Immune System
Hematopoietic stem cells in bone marrow give rise to erythrocytes (red blood cells) and leukocytes (white blood cells):myeloid cells macrophages monocyteslymphocytes B cells T cells
Immunity
Concept Map of “Immunity”
Innate(phagocytes)
Adaptive(lymphocytes)
Surface (skin, mucous membrane)
Subsurface
Humoral(Ab)
Cellular (CMI)
Systemic (IgM, IgG)
Mucosal (IgA)
Cells (PMN; Macrophages; NK)
Proteins (Complement [C′])
Comparison:
Innate Immunity
Adaptive Immunity
“Line of defense”
“first”
“second”
Specificity
general
exquisite
Improved response upon re-exposure
No
Yes
Immunological memory
No
Yes
Cells
Phagocytes NK cells
Lymphocytes (B, T)
What happened that time you cut your finger? What did it feel like & look like?
Did it get infected? What was that yucky stuff that leaked out? Did you have to get a tetanus shot? The next time you got a splinter, did the same thing
happen?
INNATE IMMUNITYInnate immune response: nonspecific, no memory, same
intensity with each response SURFACE PROTECTION anatomic barriers (skin, mucous
membranes)
chemical & enzymatic barriers (stomach acidity, lysozyme in tears)
mechanical: flow & motility (cilia)
commensal organisms
INNATE IMMUNITY
Innate immune response:
SUBSURFACE PROTECTION
Cellsphagocytic monocytes/macrophages dendritic cells (adaptive immunity)
neutrophils (polymorphonuclear leukocytes, PMN)
Fig. 1-4
INNATE IMMUNITYInnate immune response: SUBSURFACE
PROTECTIONCellsProteins complement (C) anti-microbial peptides;
defensins (skin, gut); cryptidins (intestine)
Innate immune responses often trigger INFLAMMATION
Many bacteria activate phagocytosis and trigger inflammation
Principles of Innate and Adaptive Immunity The innate immune system provides first line of defense against many
microorganisms, and is critical for the control of some bacterial pathogens. It also plays a role in initiating the adaptive response, and controls the infection until the adaptive response takes effect in 4-7 days.
The adaptive immune response recognizes pathogens not seen by the innate response, and provides additional effector functions, as well as an improved secondary response upon re-exposure to the same pathogen.
Some phagocytic cells (i.e. macrophages, dendritic cells) act as “antigen-presenting cells” to help promote the specific immune response.
Questions?
also called the specific or acquired immune
response
occurs throughout lifetime as an adaptive response
to infection
often confers life-long immunity (immunological
memory)
enhanced secondary (anamnestic) responses
mediated by lymphocytes (B and T cells)
ADAPTIVE IMMUNITY
The immune response can be divided into 3 phases: Recognition
1. discrimination between various pathogens
(bacteria, viruses, fungi, parasites)
2. discrimination between foreign and self antigen Activation
1. lymphocyte activation requires 2 signals:
antigen recognition & co-stimulation
2. clonal proliferation and differentiation into effector cells
Effector1. Plasma cells produce large amounts of antibody
2. Cytotoxic T cells (CTL) kill virus-infected cells
ADAPTIVE IMMUNITY
ImmunizationPassive
injection/infusion of Ab (“pre-packaged” immunity)
produces temporary immunity
Activeintentional exposure to Ag to elicit and immune response
produces long-lasting immunity
ADAPTIVE IMMUNITY
Antigens & Immunogens
Immunogen: substance that elicits (stimulates) an immune response
Antigen: substance that can be recognized by the immune system
Unfortunately the terms are often used interchangeably
Immunogenicity: protein > CHO > NA & lipids>40 kD +++~10 kD +<2 kD +/-
very small nonimmunogenic molecules (haptens) can be made immunogenic by coupling to a larger molecule (carrier), e.g. DNP-BSA
Lymphocytes - lymphoid organsCentral lymphoid organs sites of lymphocyte
development bone marrow and thymus
Peripheral lymphoid organs
where adaptive immune responses occur
spleen, lymph nodes, Peyer’s patches
organized to trap Ag and facilitate interaction of Ag-presenting cells and T cells, and of T and B cells
Fig. 1-7
B cell-richB cell-rich T cell-richT cell-rich
Lymph node
Fig. 1-8
Spleen
Peyer’s patches
Fig. 1-9,1-10
Lymphocytes
B cells: (humoral immunity) surface receptor for antigen is membrane-
bound immunoglobulin (Ig), or antibody differentiate into plasma cells, which
secrete large amounts of antibody
T cells: (cell-mediated immunity) surface receptor for antigen is called the T
cell receptor (TCR) two major classes: cytotoxic T lymphocytes (CTL): CD8 co-receptor
helper T cells (TH): CD4 co-receptor
Fig. 1-5
Lymphocytes are activated by antigen & Ag-specific cells proliferate in a clonal fashion
Fig. 1-13
B cells respond to native AgT cells respond to “processed & presented” Ag
Burnet’s Clonal Selection Hypothesis
Lymphocytes are activated by Ag & Ag-specific cells proliferate in a clonal fashion each lymphocyte bears a unique receptor self-reactive lymphocytes are removed from the repertoire specific interaction with Ag activation differentiated effector cells express same
receptor
Lymphocyte ActivationLymphocytes proliferate and differentiate in response to (1) antigen and (2) signals from other cells in peripheral lymphoid tissues
T cells: B cells: (1) Ag via TCR (1) Ag via surface Ig(2) costimulatory receptors on (2) costimulatory receptors on
professional APC helper T cellsTH, CTL, memory T cells plasma & memory B cells
Questions?Fig. 1-21
Immunity
Concept Map of “Immunity”
Innate(phagocytes)
Adaptive(lymphocytes)
Surface (skin, mucous membrane)
Subsurface
Humoral(Ab)
Cellular (CMI)
Systemic (IgM, IgG)
Mucosal (IgA)
Cells (PMN; Macrophages; NK)
Proteins (Complement [C’])
Immunity
Concept Map of “Immunity”
Innate(phagocytes)
Adaptive(lymphocytes)
Surface (skin, mucous membrane)
Subsurface
Humoral(Ab)
Cellular (CMI)
Systemic (IgM, IgG)
Mucosal (IgA)
Cells (PMN; Macrophages; NK)
Proteins (Complement [C’])
Immunity to disease results from host production of protective substances
Pasteur had hypothesized that immunity resulted from depletion of key nutrients, the accepted mechanism for immunity
Emil von Behring demonstrated that diphtheria microbes produced a toxic, lethal substance detectable in culture supernatants
This “toxin” could be inactivated by heating, and the inactivated “toxoid” was protective by vaccination
Hypothesis: Transfer of serum from protected animals will protect passively immunized normal animals
Early History
von Behring and Kitasato experiment (1892)
isolate serum from blood
healthy rabbitdiphtheriatoxoid
vaccinated rabbit diphtheria-resistantrabbit
rabbit lives
rabbit dies
x
healthy rabbit
healthy rabbit
virulentdiphtheria
Metchnikoff’s “anti-korperen”
Microorganisms are engulfed & digested by phagocytic cells (macrophages)
Substances in the blood, called or anti-korperen (antibodies) enhanced phagocytosis
Antibody Structure: The Puzzle
solved (mostly) by Porter, Edelman, Nisonoff in 1959-1964
Experimental approach: Break Ab molecules into smaller fragments
Reducing agent (break S-S bonds)
2 heavy chains (55 kD) +2 light chains (25 kD)
Fab: fragment antigen-binding
Fc: fragment crystalizable
ANTIBODY STRUCTUREAn antibody molecule is composed of two identical Ig heavy chains (H) and two identical light chainslight chains (L), each with a variable region (V) & constant region (C).
Amino acid sequences were determined from myeloma proteins.Fig. 1-17,1-16
Bence-Jones proteins(myeloma proteins) = Ig light chainsfound in the urine of patients with multiple myeloma
Serum protein electrophoresis
multiple myeloma
normal serum
Clinical terms:hypergammaglobulinemiahypogammaglobulinemiaagammaglobulinemia monoclonal gammopathy
Amino acid sequences of Bence-Jones proteins
XXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXXX-----------XX-------------XX----------XXXX---------------------------------------------------------------X------------XX----------XX-XXX--------------------------------------------------------XXX-XX-------------X-X-----------XXXX-------------------------------------------------- XXXXX---XX-----X^XX-----X-----XXXX---------XXXXX-------------------------------------------------- XXX--XXXX-X---^------XX----X-XX----XXX---XX-XX--------------------------------------------------XX------XXXX—X----XX----XX-X----XXX---XXXX--------------------------------------------------
VARIABLE REGION CONSTANT REGION
***** ***** ****** *hypervariable regions *complementarity-determining regions
Light chains: kappa () and lambda ()Heavy chains: mu () – IgM
gamma () – IgGalpha () – IgAdelta () – IgDepsilon () – IgE
But what was the Ab specificity of the myeloma proteins?
Monoclonal Antibodies & HybridomasKohler & Milstein (1974)
Fig. A-14
Fig. 3-5,3-7
Fig. 3-8,3-9
Fig. 3-10
The problem of antigen receptor diversity
Each lymphocyte has a unique receptor Ig for B cells, TCR for T cells
How are antigen receptors with a virtually infinite range of specificities encoded by a finite number of genes? Germline vs. somatic diversity
Tonegawa discovered in 1976 that antibody genes are encoded as gene segments, and must undergo gene rearrangement during lymphocyte development. During the next ~10 years it was discovered that the V regions of all germline Ig and TCR genes are encoded by families of gene segments.
Fig. 1-18
It is estimated that 108-109 different receptor specificities may be present in an individual at any one time. Receptor diversity is generated by:germline diversity of the V region gene segmentscombinatorial diversity (different combinations of gene segments)junctional diversity (additional diversity generated during sloppy recombination)
The problem of antigen receptor diversity
Questions?Fig. 4-2
Classes
Subclasses
Ig isotypes
Fig. 4-18
IgMcomplement fixation (opsonization)
intravascular except during inflammation
primary Ab response
Fig. 4-23,9-27
IgDtrace amount in serum
on surface of mature, naïve B cells
Fig. 7-6
IgG4 subclasses
intravascular & interstitial space
highest concentration in blood
appears late in primary response, predominates in secondary responses
fixes complement
crosses placenta
Fig. 3-4
Fig. 2-18
IgAmonomer in serum
dimer in secretions
mucosal immunity
Fig. 9-20
IgEtrace amount in serum
bound to mast cells via FcR
type I hypersensitivity, allergy
parasite immunity
Fig. 9-33,9-35 Schistosome larva & mast cells
DISTRIBUTION OF Ig ISOTYPES
Fig. 9-22
Fig. 4-17
FUNCTIONS OF Ig ISOTYPES
Fig. 9-1
Fig. 9-24,9-25
Fig. 9-31,9-32
Course of Typical Acute Infection
Fig. 10-1
Kinetics of Antibody Response
Fig. 1-20
The affinity as well as the amount of antibody
increases with repeated
immunization
Questions?Fig. 10-31
Immunity
Concept Map of “Immunity”
Innate(phagocytes)
Adaptive(lymphocytes)
Surface (skin, mucous membrane)
Subsurface
Humoral(Ab)
Cellular (CMI)
Systemic (IgM, IgG)
Mucosal (IgA)
Cells (PMN; Macrophages; NK)
Proteins (Complement [C’])
Lymphocyte development &
toleranceT cell recognition of Ag
Immunity
Concept Map of “Immunity”
Innate(phagocytes)
Adaptive(lymphocytes)
Surface (skin, mucous membrane)
Subsurface
Humoral(Ab)
Cellular (CMI)
Systemic (IgM, IgG)
Mucosal (IgA)
Cells (PMN; Macrophages; NK)
Proteins (Complement [C’])
Humoral immune response
T cell-mediated immunity
Eric Sobel, M.D., Ph.D.