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IMMUNOGLOBULINS STRUCTURE AND FUNCTION IMMUNOGLOBULINS Definition Glycoprotein molecules that are present on B cells (BCR) or produced by plasma cells (usually referred to as antibodies) in response to an immunogen Antibodies production is the sole function of the B cells Not toxic or destructive, bind the pathogen tightly and target destructive components of the immune system Antibodies are useful in the defense against extracellular pathogens Antibodies are secreted in the secondary lymphoid organs and in bone marrow and find their way to the extracellular spaces During the course of an infection antibody effectiveness improves steadily PHASES OF B CELL RESPONSE ! ! IMMUNOGLOBULIN STRUCTURE • 2x Heavy chain (light blue) • 2x light chain (dark blue) • Variable regions antigen binding disulfide bond • Constant regions carbohydrate CL VL CH VH CH2 1 hinge region CH3 Ribbon structure of IgG BCR (B cell receptor) Associated chains for signaling Antibody !! Transmembrane domain Cytoplasmic domain MEMBRANE BOUND! Antigen recognition and B cell activation SOLUBLE (freely circulating) Antigen recognition and effector functions. Produced by plasma cells ANTIBODY DOMAINS AND THEIR FUNCTIONS !! Antigen recognition antigénkötés s s s s s s VH s s CH1 s s s s Variable domain va riábilis d om ének s s VL s ss ss s konsta ns dom ének CH2 s effektor funkc iók Effector functions CH3 ss s s s s s s s Constant domain s s CL mIg = BCR Associated chains providing signaling capacity ! B CELL ACTIVATION B cell BCR oligomerization results in B cell activation, proliferation and differentiation ! FLEXIBILITY OF ANTIBODIES FEATURES OF ANTIBODY-ANTIGEN INTERACTION Valency: numbers of antigen epitopes an antibody binds Affinity: the strength of interaction between a specific antigen and one binding site of the antibody Avidity: The overall strength of binding at multiple sites in an antibody ANTIGEN BINDING Antigen Binding Fragment (Fab) Complement binding site Constant fragment (Fc) Binding to Fc receptors on phagocytic cells Placental transfer VARIABILITY IN DIFFERENT REGIONS OF THE Ig DETERMINES Ig SPECIFICITY OR CLASS isotype Idiotype Sequence variability of H/Lchain constant regions Sequence variability of H/Lchain variable regions DIFFERENT VARIABLE REGIONS DIFFERENT ANTIGEN-BINDING SITES DIFFERENT SPECIFICITIES ANTIGEN BINDING FRAGMENT (Fab) CONTAINS HYPERVARIABLE REGIONS DNA recombination of gene segments encoding these regions (variable heavy and light polypeptide chains) gives a huge number of variability during B cell development in the bone marrow. Aka. Somatic recombination COMPLEMENTARY DETERMINING REGIONS (CDR) CDR2 CDR1 Light chain CDR3 Epitope CDR1 CDR2 CDR3 Heavy chain VARIABILITY IN DIFFERENT REGIONS OF THE Ig DETERMINES Ig SPECIFICITY OR CLASS Isotype Sequence variability of H/Lchain constant regions Sequence variability of H/Lchain constant regions HUMAN IMMUNOGLOBULIN CLASSES ! ENCODED BY DIFFERENT STRUCTURAL GENE SEGMENTS (ISOTYPES) Heavy chain types: • • • • • IgG - gamma (γ) heavy chains IgM - mu (μ) heavy chains IgA - alpha (α) heavy chains IgD - delta (δ) heavy chains IgE - epsilon (ε) heavy chains Light chain types: • kappa (κ) • lambda (λ) ISOTYPE SWITCHING PHASES OF B CELL RESPONSE ! MAIN CHARACTERISTICS OF ANTIBODY ISOTYPES Ig isotype Serum concentration Characteristics, functions Trace amounts Major isotype of secondary (memory) immune response Complexed with antigen activates effector functions (Fc-receptor binding, complement activation The first isotype in B-lymphocyte membrane Function in serum is not known Trace amounts Major isotype in protection against parasites Mediator of allergic reactions (binds to basophils and mast cells) 3-3,5 mg/ml Major isotype of secretions (saliva, tear, milk) Protection of mucosal surfaces 12-14 mg/ml 1-2 mg/ml Major isotype of primary immune responses Complexed with antigen activates complement Agglutinates microbes The monomeric form is expressed in B-lymphocyte membrane as antigen binding receptor MAIN CHARACTERISTICS OF ANTIBODY ISOTYPES ANTIBODY PRODUCTION DURING THE PRIMARY AND THE SECONDARY IMMUNE RESPONSES Ig. Concentration Level of antibodies secondary response against Szekunder antigen A ’lasyecondary respo Primary response against antigen A primer response IgG IgA IgE IgM IgM primary response against antigen B 5 „A” antig éAn Antigen 10 15 20 25 „A” és „B” Antigen A and antigén 30 B napok Days napok ANTIBODY PRODUCTION DURING THE PRIMARY AND THE SECONDARY IMMUNE RESPONSE ! !! EFFECTOR FUNCTIONS OF ANTIBODIES Antibody-mediated immune responses • NEUTRALIZATION • OPSONIZATION ADCC MAST CELL DEGRANULATION • COMPLEMENT FIXATION NEUTRALIZATION Covering of the pathogen’s surface prevents replication and growth Antigen binding Complement binding site Binding to Fc receptors Placental transfer OPSONIZATION Flagging a pathogen Antigen binding portion (Fab) binds the pathogen, the Fc region binds phagocytic cells Fc-receptors speeding up the process of phagocytosis Antibody Dependent Cellular Cytotoxicity (ADCC) MAST CELL DEGRANULATION FcεRI + IgEs (A) High-affinity FcRs on the surface of the cell bind monomeric Ig before it binds to antigen. (mast cell) (B) Low-affinity FcRs bind multiple Igs that have already bound to a multivalent antigen. (macrophage, NK cell) Antigen binding Complement binding site Binding to Fc receptors Placental transfer COMPLEMENT FIXATION IgM and IgGs activate the classical pathway of the complement system OPSONIZATION BY C3b Bacterium C3b Complement receptor Macrophage IMMUNOGLOBULIN ISOTYPES HAVE EACH THEIR SPECIFIC CAPABILITIES Antigen binding Complement binding site Binding to Fc receptors Placental transfer FcRn on the placenta facilitate the transfer of maternal IgG to the fetus’s circulation PRODUCTION OF IMMUNOGLOBULINS BEFORE BIRTH AFTER BIRTH breast milk IgA 100% (adult) maternal IgG IgM IgG IgA 0 3 month 6 9 1 2 3 4 5 adult year IgG transport is so efficient that at birth babies have as high a level of IgG in their plasma as their mothers These transfers are a form of passive immunization. The babies protection by IgG and IgA is against those pathogen that the mother has mounted At the first year (esp.3-12m) maternal IgGs are catabolized and breast feeding diminishes so babies become most susceptible/vulnerable to infections Pathological consequences of placental transport of IgG (hemolytic disease of the newborn) anti-Rh IgM Passive anti-D IgG DIMERIC IgA (Transcytosis) IgA dimers are in the highly vulnerable mucosal epithelia lining the GI, respiratory, urinary and genital tracts, the eyes, nose and throat