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ADAPTIVE IMMUNE RESPONSE

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ADAPTIVE IMMUNE RESPONSE Immune response to infections 1. Innate response Neutrophils, macrophages, NK cells at site of infection 2. Initiation of adaptive response – PowerPoint PPT presentation

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Title: ADAPTIVE IMMUNE RESPONSE


1
ADAPTIVE IMMUNE RESPONSE
  • Immune response to infections
  • 1. Innate response
  • Neutrophils, macrophages, NK cells at site of
    infection
  • 2. Initiation of adaptive response
  • iDCs phagocytose Ag and take to nodes
  • DCs present Ag to T cells
  • Get specific helper (CD4) T cells
  • help B cell activation humoral immunity
  • Activate macrophages CMI
  • Get specific cytotoxic (CD8) T cells
  • Kill virally infected cells CMI

2
ADAPTIVE IMMUNE RESPONSET CELLS
  • Development in thymus
  • Immunogenetic events produce multiple TCRs
  • Similar to B cells
  • TCR gene with multiple V, D, and J segments
  • Recognize 1015 epitopes
  • T cells with TCRs that react with self antigens
    deleted
  • Start with double negative cells no TCR, CD4 or
    CD8
  • Next get double positive cells TCR, CD4, CD8
  • Positive selection weak recognition of MHCI or
    MHCII
  • Negative selection if reaction is strong
    apoptosis
  • 2 of cells survive

3
ADAPTIVE IMMUNE RESPONSET CELLS
4
ADAPTIVE IMMUNE RESPONSET CELLS
  • TCR complex
  • T cell receptor similar to Fab of antibodies
  • Alpha and beta Ig-like chains with variable and
    constant domains
  • Hydrophobic transmembrane regions
  • CD3 proteins
  • Gamma epsilon delta epsilon, each with one
    Ig-like domain
  • Transmembrane segment binds to TCR
  • Cytoplasmic domain of each has one ITAM
  • ITAM immunoreceptor tyrosine-based activation
    notif for signaling
  • Zeta chains disulfide-liked homodimer, each
    protein has 3 ITAM
  • Transmembrane region with aspartate

5
ADAPTIVE IMMUNE RESPONSET CELLS
6
ADAPTIVE IMMUNE RESPONSET CELLS
  • Co-receptors
  • CD4 protein binds to MHC-II on APC
  • CD4 T cells helper T cells
  • MHC-II only on APCs
  • CD8 protein binds to MHC-I on target cells
  • CD8 T cells cytotoxic T cells
  • MHC-I on all nucleated cells

7
ADAPTIVE IMMUNE RESPONSET CELLS
  • Accessory molecules lymphocyte surface molecule
    distinct from Ag receptor complex adhesion or
    signaling
  • CD45R, CD28, CD40L
  • Adhesion molecules tighten interaction with APC
  • LFA (leukocyte function-associated antigen)-1,
    CD2
  • Cytokine receptors IL-1R, IL-2R, others

8
ADAPTIVE IMMUNE RESPONSEantigen presenting cells
  • Antigen Presentation to T cells
  • MHC (major histocompatibility complex) 1
  • all nucleated cells
  • MHC-encoded alpha (hvy) chain and beta 2 (lt)
    microglobulin
  • Polymorphic alpha 1 and alpha 2 domains for
    closed binding cleft
  • agretope
  • Conserved alpha 3 domains binding site for CD8
  • Beta 2 interacts noncovalently with alpha 3

9
ADAPTIVE IMMUNE RESPONSEantigen presenting cells
  • Abbas Fig 4-4

10
ADAPTIVE IMMUNE RESPONSEantigen presenting cells
  • MHC-II dimer of alpha and beta subunits
  • APCs
  • Both chains MHC encoded
  • Alpha 1 and beta 1 domains variable and form open
    binding cleft
  • Most of variability on beta chain
  • Agretope
  • Alpha 2 and beta 2 folded into Ig domains
  • B2 Ig domain binds to CD4

11
ADAPTIVE IMMUNE RESPONSEantigen presenting cells
  • Abbas Fig 4-6

12
ADAPTIVE IMMUNE RESPONSEantigen presenting cells
  • Peptide presentation by MHC I molecules
  • MHC I molecule synthesized in endoplasmic
    reticulum (ER)
  • Cytoplasmic protein (including microbial)
    degraded by proteosome
  • Usually dealing with degraded (misfolded etc)
    normal proteins
  • Degraded proteins marked by ubiquitin
  • To ER via TAP (transporter assoc w Ag processing)
  • Ag peptide binds to cleft in hvy chain of MHC-I
  • Peptide of 8 or 9 amino acids
  • MHC-I with peptide to cell membrane via golgi and
    exocytic vesicle
  • Uninfected cells usually coated with MHC-I with
    self proteins

13
ADAPTIVE IMMUNE RESPONSEantigen presenting cells
  • Peptide presentation by MHC II molecules
  • Phagocytized proteins degraded in phagolysosomes
    by APCs
  • MHC-II molecule synthesized in ER
  • Invariant chain (Ii) placed in cleft
  • Ii provides stability and prevents MHC-II from
    binding with ER peptides
  • Lysosomal and exocytic vesicles merge
  • Invariant chain replaced with degraded peptide
  • cleft open at ends longer peptides (30 aa)
    presented
  • Fused vesicle migrates to cell membrane

14
ADAPTIVE IMMUNE RESPONSEantigen presenting cells
  • Antigen processing and presentation Abbas Fig
    5-8

15
ADAPTIVE IMMUNE RESPONSEantigen presenting cells
  • Cross-presentation of Ag
  • iDCs phagocytise virally infected cells
  • Some peptides migrate to cytoplasm and processed
    to MHC I
  • Also, some cytoplasmic peptides from phagocytised
    cells processed to MHC II

16
ADAPTIVE IMMUNE RESPONSEantigen presenting cells
  • Cross-presentation of Ag to CD8 T cells. Abbas
    Fig 5-7

17
ADAPTIVE IMMUNE RESPONSEantigen presenting cells
  • Antigen Presenting Cells (APCs) Dendritic cells
    (DCs), B cells, and Macs
  • Dendritic cells only APC that can initiate Ag
    specific response
  • Presumably from myeloid and lineage
  • Precursor DCs in blood differentiate into
    immature DCs (iDC)
  • iDC recognized antigen with TLR and other
    receptors activated
  • Pinocytosis/phagocytosis and cytokine production,
    now DC
  • DCs can no longer phagocytose go to T-cell area
    of lymph nodes where they present Ag to T cells
  • Langerhans cells are skin DC

18
ADAPTIVE IMMUNE RESPONSEantigen presentation to
T cells
  • T Lymphocytes
  • Recognize antigens (on dendritic cells) in
    peripheral lymphoid organs, resulting in
    expansion of Ag-specific lymphocyte pool
  • Differentiate into effector cells and memory
    cells
  • Effector lymphocytes become activated when they
    recognize Ag
  • Activation of T cells requires recognition of Ag
    displayed on APCs, costimulators, and cytokines
    produced by both APC and T cell

19
ADAPTIVE IMMUNE RESPONSE antigen presentation to
T cells
  • Activation of CD4 T Cells
  • MHC II on APC binds with TCR
  • TCR recognizes foreign protein MHC self
    proteins
  • Interaction strengthened by binding of CD4 to MHC
    II molecule
  • Signal transmitted via TCR/CD3 complex zeta
    proteins
  • Adhesion molecule interactions
  • LFA-3 on APC with CD2 on T cell
  • ICAM-1 on APC with LFA-1 on T cell
  • Costimulatory signals also required
  • B7 on APC to CD28 on T cell
  • cytokines
  • Partial activation without adequate costimulatory
    signal Anergy or apoptosis method to eliminate
    self-reacting cells or induce tolerance

20
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21
ADAPTIVE IMMUNE RESPONSEHelper T cell Function
  • TH1 and TH2 CD4 (helper) T cells
  • TH0 cells mature into TH1 or TH 2 depending on
  • Nature and concentration of antigen
  • How antigen presented
  • Type of APC
  • Cytokines
  • TH1 IgM, IgG, activated Macs
  • TH2 humoral response IgA, IgE

22
ADAPTIVE IMMUNE RESPONSECytotoxic T cells
  • Activation of CD8 T cells cytotoxic T cells
    (CTLs)
  • Precursors in nodes bind TCR CD8 to MHC-1 of
    APC costim
  • TCR recognizes foreign protein in self MHC
    molecule
  • Specific clone expands by 100,000
  • Activated CTLs bind with target cell
  • Granulysin, granzymes and perforin released from
    granules apoptosis
  • Also interaction of FasL on CTL with Fas on
    target apoptosis
  • Apoptosis
  • Cell DNA and internal membranes fragment
  • Shrink to apoptotic bodies which are easily
    phagocytosed
  • Clean cell death as apposed to necrosis

23
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24
HUMORAL IMMUNE RESPONSE
  • HIR production of antibodies by plasma (B)
    cells
  • Some Definitions
  • Albumin, globulin serum proteins
  • Gamma-globulin immunoglobulin
  • Immunogen, antigen
  • Epitope (linear, conformational)
  • Hapten carrier
  • Adjuvant (alum, Freunds, liposomes, CW
    components)
  • Immune tolerance (dose, co-stimulators,
    transplants )
  • T (cell) independent antigen T dependent Ag
  • Route of Ag administration
  • Immunoglobulin superfamily on next slide

25
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26
HUMORAL IMMUNE RESPONSE
  • Immunoglobulin (antibody) structure

27
HUMORAL IMMUNE RESPONSE
  • Immunoglobulin structure
  • Heavy chain determines class/subclass IgM, G, A,
    D, E
  • Mu, gamma, alpha, delta, epsilon
  • Light chain (kappa, lambda)
  • Domains constant and variable
  • One variable domain on each lt chain and one
    variable domain on each hvy chain
  • Three constant domains on hvy chain of IgG and
    IgA four on IgM and IgE
  • One constant domain on lt chains
  • Variable domains on hvy/lt chains have 3
    complementary determining regions (CDRs)
    complements epitope structure

28
HUMORAL IMMUNE RESPONSE
  • Immunoglobulin structure
  • Fab portion variable region
  • Fc portion
  • C fixatin
  • bind to Fc receptors on effector cells
  • Fc of IgG and IgA involved with transfer across
    placenta and mucosa
  • Hinge region
  • Papain 2 Fab Fc Pepsin F(ab)2 Fc
  • Membrane-spanning portion
  • Interchain disulfide bonds
  • Isotype IgD, IgM, IgG1, IgG2, IgG3, IgG4, IgA1,
    IgA2, IgE
  • Allotype variation of isotype in different
    individuals
  • Idiotype protein sequences in variable region
  • Interacts with epitope

29
HUMORAL IMMUNE RESPONSE
  • Immunoglobulin Classes

30
HUMORAL IMMUNE RESPONSE
  • Membrane-associated antibodies
  • All isotypes may be membrane-associated on B
    cells
  • All membrane-associated AAs monomeric
  • Last CH region has 26 AAs with hydrophobic side
    chains
  • Membrane spanning region
  • Secreted antibodies
  • Found in blood and other extracellular fluids
  • IgG and IgE are monomeric
  • IgD negligible
  • IgM and IgA are multimeric
  • Have tail pieces on end of hvy chains which are
    bound to J chains

31
HUMORAL IMMUNE RESPONSE
  • Immunoglobulin Isotypes
  • IgD lt1 of serum Ig
  • membrane Ig on early B-cells
  • IgM 5-10 of serum Ig
  • membrane Ig on early B-cells
  • IgD and IgM are only isotypes that can be
    expressed together on same cell
  • 5 day half-life in serum
  • Serum IgM pentameric 10 Ag-binding sites tail
    piece and j chain
  • Complement fixation opsonin bacteriolysis
  • First isotype after immunization then wanes

32
HUMORAL IMMUNE RESPONSE
  • Immunoglobulin Isotypes
  • IgG 85 of serum Ig
  • 4 subclasses all monomeric
  • 23 day half-life
  • T cells required
  • Complement fixation opsonin
  • Maternal IgG transported across placenta and
    neonatal intestinal epithelium
  • Second isotype after immunization persists
  • Also anamnestic (booster) response

33
HUMORAL IMMUNE RESPONSE
  • Immunoglobulin Isotypes
  • IgA 5-15 of serum Ig
  • 2 subclasses both dimer, trimer? with tail piece
    and J chain
  • IgA transported across epithelial cells has
    additional secretory component
  • IgE lt1 of serum Ig
  • Bind to Fc receptors on Mast cells, basophils and
    eosinophils
  • Immediate hypersensitivity
  • Parasite infections

34
Transport of IgA through Epithelial Cells
35
HUMORAL IMMUNE RESPONSE
  • Neonatal Immunity Neonates lack ability to
    mount effective immune response. Therefore, use
    maternal IgG and IgA
  • IgG transported across placenta into fetal
    circulation
  • IgG and IgA in breast milk ingested
  • IgG and IgA neutralize organisms in gut
  • IgG transported across gut epithelium into
    circulation
  • Neonatal Fc receptor for IgG on placta and gut
    epithelium cells

36
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37
HUMORAL IMMUNE RESPONSEB cell development
38
HUMORAL IMMUNE RESPONSE
  • Immunogenetics
  • Chromosomes 2, 22, 14 have genes for kappa,
    lambda, hvy chains
  • Variable region genes upstream from constant
    region genes
  • Genetic recombination events to form variable
    region of hvy and lt chains
  • V (variable) and J (joining) segments for light
    chains
  • 300 V gene segments and 5 J segments 1500
    possible
  • V, D (diversity), and J segments for hvy chains
  • 300 - 1000 V genes, 12 D genes, and 6 J genes
    lt100,000 possible
  • Association of hvy and light chain gt 1,000,000
    possible

39
HUMORAL IMMUNE RESPONSE
  • Immunogenetics (continued)
  • Class switching
  • Genes for constant region of hvy chain in set
    order
  • IgM, D, G3, G1, G2, G4, E, A1, A2
  • Different constant region genes deleted in
    response to T cell cytokines

40
HUMORAL IMMUNE RESPONSE
  • Production of antibodies by B cell
  • B cell receptor Ig molecule specific for
    non-self antigens
  • Cells with receptors for self antigens removed
    during development in bone marrow
  • Ig IgD and IgM on naive B cells
  • B cell receptor complex
  • IgM or IgD Ig alpha/Ig beta with immunoreceptor
    tyrosine-based activity motif (ITAM)
  • Signal transducing receptor initiates activation
    signal via Ig ITAM
  • Ultimately activates factors that induce
    transcription of genes

41
B Cell Antigen Receptor Complex
42
HUMORAL IMMUNE RESPONSE
  • Antibody response to T (cell) independent
    antigens
  • Surface Ig receptors recognize repeating sites on
    Ag
  • Long polysaccharides
  • Get cross-linking of many Ig receptors,
    activating signal cascade
  • Clonal expansion and plasma cell development of
    specific B cells
  • Disadvantages of T independent response
  • No T cell cytokines for class switching IgM only
  • Ab has lower affinity for Ag (limited affinity
    maturation?)
  • No response in young (lt2yr) children

43
HUMORAL IMMUNE RESPONSE
  • Antibody response to T (cell) dependent antigens
  • Ig receptors on B cell recognize Ag but
    cross-linking inadequate to activate cell
  • Therefore need second signal from T helper cell
    thus
  • 1) Ag binds to Ig receptor on B cell as above
  • 2) Some bound Ag internalized, processed and
    presented in MHC-II surface molecule to T cell
    (which has receptor for this Ag) i.e., B cell
    functions as APC. T cell, so activated, secretes
    cytokines which are received by and stimulate the
    B cell
  • 3) The two signals stimulate the B cell to
    replicate, clonal expansion
  • A) Plasma cells which produce and secrete the Ig
    of the receptor
  • In nodes and bone marrow
  • B) Memory cells with the same receptor
  • Anamnestic (booster) response

44
HUMORAL IMMUNE RESPONSE
  • Activation of B cells continued
  • A second signal may be provided by C receptor
  • Interaction of B cell with T cell via CD40 (B
    cell) CD40L (T cell)
  • Class switching from influence of helper T cell
    cytokines
  • Initial IgM
  • INFg IgG
  • IL-4 IgA, IgE
  • IL-5 IgA (also induces eosinophil production)
  • Somatic mutation increased affinity
  • Primary and Secondary responses
  • Primary immune response strong IgM
  • Secondary immune response (second exposure to Ag)
    faster, more IgG

45
C in B Cell Activation
46
T Cell - Mediated B Cell Activation
47
HUMORAL IMMUNE RESPONSE
  • Antibodies inactivate microorganisms by
  • Agglutination
  • Neutralization
  • Antibody to toxins
  • Antibody to microbial surface molecules that bind
    to host cells
  • Opsonization
  • Natural killer cells have receptors for IgG
  • Eosinophils have receptors for IgG, IgA, and IgE
  • Complement fixation
  • Neutrophils, macrophages have receptors for C3b
  • Gram negative organisms susceptible to MAC
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