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The Complement
System
By:
Dr. Suzan Yousif
Introduction
• The complement system consists of a group of
serum proteins that act in concert and in an
orderly sequence to exert their effect
• These proteins are not immunoglobulins and
their concentrations in serum do not increase
after immunization
• Complement activation (fixation) leads to lysis
of cells and to the generation of many powerful
biologically active substances
Overview of Complement
Classical Pathway Alternative Pathway
Lectin Pathway
Antibody binds to specific
antigen on pathogen surface
Mannose-binding protein
binds pathogen surface
Pathogen surface creates
environment conducive to
complement activation
Complement Activation
Formation of C3 and C5 convertases
Membrane Attack Pathway
Cytolysis of some pathogens
Opsonization & phagocytosis
of some pathogens
Inflammatory response
Clearance of
Immune complexes
Clearance of
Apoptotic Cells
Complement Activation Pathways
• The Classical Pathway
- Ag- Ab complexes
• The Alternative Pathway
- Aggregated immunoglobulins and microbial
products
• The Mannan - Binding Lectin Pathway
- Microbial products
The Classical Pathway
• Activators: Ag – Ab complexes
• Antibodies involved: IgG and IgM
• Activation in an orderly fashion of nine major
protein components; C1 – C9
• Products of activation are enzymes that
catalyze the subsequent step
The Classical Pathway
• Activation of C1:
 C1 consists of C1q (400.000 Daltons), C1r (95000
Daltons), and C1s (85000 Daltons)
 Subunits are held together by Calcium ions
 C1q is a polymer of 6 identical units
 C1q activation requires binding to a c1q- specific
receptor on the FC region of at least 2 adjacent
molecules of IgG or a single molecule of IgM, a
reaction that requires Calcium ions
Molecular structure of C1
IgA and IgE cannot activate complement
The Classical Pathway
• IgG4, IgA, and IgE do not have complement receptors
• Activated C1q activates C1r which in turn activates
C1s
• Activated C1s has esterolytic and proteolytic
properties which acts on C4 splitting it into two
fragments; C4a and C4b
• C4b complexes with C1s forming an active component
that acts on C2 splitting it into C2a and C2b
• C2a binds to C4b creating a very active complex
called the C3 convertase, where a single molecule can
activate hundreds of C3 molecules
The Classical Pathway
• C3 is split by C4b2a into C3a and C3b
• C3b binds to cells and to C4b2a to generate C5
convertase which splits C5 into C5a and C5b
• C5b binds to cells and activates C6 and C7
• The complex C5b67 activates C8 and C9
forming a giant molecule with a molecular
weight of 106 Daltons called the membrane
attack complex (MAC)
The Classical Pathway
• C5b6789 bound to cells insert themselves into
the cell membrane and produce
transmembrane channels allowing ions to pass
through
• The osmotic equilibrium of the cell is disturbed
with rapid influx of water into the cell which
swells and lyses
The Alternative (properdin) Pathway
• Activators: Bacterial LPS, cell wall of some
bacteria, some yeast cells, aggregated IgA, and
a factor present in cobra venom
• Components: C3 – C9, factor B, factor D, and
Properdin
• C3b present in trace amounts in serum
combines with factor B forming C3bB
Alternative Pathway
Figure 16.14
The Mannan Binding Lectin (MBL)
• Activators: microorganisms and foreign
invaders
• Components: C2 – C9, MASP
• MBL recognizes carbohydrate structures
through its carbohydrate – recognizing domain
(CRD) and then it can interact with an enzyme
called MBL – activated serine protease (MASP)
Lectin Pathway
Figure 16.15
General Functions of Complement
Overview of Complement
Classical Pathway Alternative Pathway
Lectin Pathway
Antibody binds to specific
antigen on pathogen surface
Mannose-binding protein
binds pathogen surface
Pathogen surface creates
environment conducive to
complement activation
Complement Activation
Formation of C3 and C5 convertases
Membrane Attack Pathway
Cytolysis of some pathogens
Opsonization & phagocytosis
of some pathogens
Inflammatory response
Clearance of
Immune complexes
Clearance of
Apoptotic Cells
Complement functions related to
immune defense
• Lysis of cells: This is the original function
identified and causes hypotonic cell death by
making holes. It is not effective against
organisms with rigid cell walls such as fungi
Terminal complement components and the formation of the
membrane attack complex
Before complement After complement treatment
The contents of the cell leak out through the MAC
pore and the cell dies
Opsonization: Antigen coated with C3b binds
to cells bearing complement receptors and
if the cell is a phagocyte, the antigen will
be phagocytosed.
opsonized bacterium
• Inflammation:
- Anaphylatoxins: C5a, C3a, and C4a of which C5a
is the most potent bind receptors on mast cells and
basophils and cause degranulation with the release
of pharmacologically active mediators which induce
smooth-muscle contraction and increases in
vascular permeability.
- Chemoattractants: C3a, C5a and C5b67 attract
and induce monocytes and neutrophils to adhere to
vascular endothelial cells, extravasate through the
endothelial lining of the capillaries and migrate to the
site of complement activation in the tissue.
Inflammation
C5a—chemoattraction
C3a, C4a----activation
C3a, C4a---increased
vascular permeability
anaphylotoxins
• Immune clearance: Removes immune
complexes from the circulation and deposits
them in the liver where they are degraded.
• Virus neutralization: Complement
mediates viral neutralization by facilitating
viral aggregation and by coating the viral
surface.
CR1
Clearance of Immune Complexes
Clearance of Apoptotic Cells
C3b
phagocyte
CR3, CR4
•Phagocyte recognizes C3b deposited on the surface of apoptotic cell
•Apoptotic cell is ingested and destroyed by phagocyte
• This is an important mechanism for clearing self antigens and preventing
autoimmune responses
• Uptake of apoptotic cell also induces self tolerance, thereby
prevents autoimmune response
(anaphylotoxins)
4_2019_04_08!09_43_22_PM.ppt
4_2019_04_08!09_43_22_PM.ppt
4_2019_04_08!09_43_22_PM.ppt

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4_2019_04_08!09_43_22_PM.ppt

  • 2. Introduction • The complement system consists of a group of serum proteins that act in concert and in an orderly sequence to exert their effect • These proteins are not immunoglobulins and their concentrations in serum do not increase after immunization • Complement activation (fixation) leads to lysis of cells and to the generation of many powerful biologically active substances
  • 3. Overview of Complement Classical Pathway Alternative Pathway Lectin Pathway Antibody binds to specific antigen on pathogen surface Mannose-binding protein binds pathogen surface Pathogen surface creates environment conducive to complement activation Complement Activation Formation of C3 and C5 convertases Membrane Attack Pathway Cytolysis of some pathogens Opsonization & phagocytosis of some pathogens Inflammatory response Clearance of Immune complexes Clearance of Apoptotic Cells
  • 4. Complement Activation Pathways • The Classical Pathway - Ag- Ab complexes • The Alternative Pathway - Aggregated immunoglobulins and microbial products • The Mannan - Binding Lectin Pathway - Microbial products
  • 5.
  • 6. The Classical Pathway • Activators: Ag – Ab complexes • Antibodies involved: IgG and IgM • Activation in an orderly fashion of nine major protein components; C1 – C9 • Products of activation are enzymes that catalyze the subsequent step
  • 7. The Classical Pathway • Activation of C1:  C1 consists of C1q (400.000 Daltons), C1r (95000 Daltons), and C1s (85000 Daltons)  Subunits are held together by Calcium ions  C1q is a polymer of 6 identical units  C1q activation requires binding to a c1q- specific receptor on the FC region of at least 2 adjacent molecules of IgG or a single molecule of IgM, a reaction that requires Calcium ions
  • 8.
  • 10.
  • 11. IgA and IgE cannot activate complement
  • 12. The Classical Pathway • IgG4, IgA, and IgE do not have complement receptors • Activated C1q activates C1r which in turn activates C1s • Activated C1s has esterolytic and proteolytic properties which acts on C4 splitting it into two fragments; C4a and C4b • C4b complexes with C1s forming an active component that acts on C2 splitting it into C2a and C2b • C2a binds to C4b creating a very active complex called the C3 convertase, where a single molecule can activate hundreds of C3 molecules
  • 13. The Classical Pathway • C3 is split by C4b2a into C3a and C3b • C3b binds to cells and to C4b2a to generate C5 convertase which splits C5 into C5a and C5b • C5b binds to cells and activates C6 and C7 • The complex C5b67 activates C8 and C9 forming a giant molecule with a molecular weight of 106 Daltons called the membrane attack complex (MAC)
  • 14. The Classical Pathway • C5b6789 bound to cells insert themselves into the cell membrane and produce transmembrane channels allowing ions to pass through • The osmotic equilibrium of the cell is disturbed with rapid influx of water into the cell which swells and lyses
  • 15.
  • 16. The Alternative (properdin) Pathway • Activators: Bacterial LPS, cell wall of some bacteria, some yeast cells, aggregated IgA, and a factor present in cobra venom • Components: C3 – C9, factor B, factor D, and Properdin • C3b present in trace amounts in serum combines with factor B forming C3bB
  • 17.
  • 19. The Mannan Binding Lectin (MBL) • Activators: microorganisms and foreign invaders • Components: C2 – C9, MASP • MBL recognizes carbohydrate structures through its carbohydrate – recognizing domain (CRD) and then it can interact with an enzyme called MBL – activated serine protease (MASP)
  • 21.
  • 22. General Functions of Complement
  • 23. Overview of Complement Classical Pathway Alternative Pathway Lectin Pathway Antibody binds to specific antigen on pathogen surface Mannose-binding protein binds pathogen surface Pathogen surface creates environment conducive to complement activation Complement Activation Formation of C3 and C5 convertases Membrane Attack Pathway Cytolysis of some pathogens Opsonization & phagocytosis of some pathogens Inflammatory response Clearance of Immune complexes Clearance of Apoptotic Cells
  • 24. Complement functions related to immune defense • Lysis of cells: This is the original function identified and causes hypotonic cell death by making holes. It is not effective against organisms with rigid cell walls such as fungi
  • 25. Terminal complement components and the formation of the membrane attack complex
  • 26. Before complement After complement treatment The contents of the cell leak out through the MAC pore and the cell dies
  • 27. Opsonization: Antigen coated with C3b binds to cells bearing complement receptors and if the cell is a phagocyte, the antigen will be phagocytosed. opsonized bacterium
  • 28. • Inflammation: - Anaphylatoxins: C5a, C3a, and C4a of which C5a is the most potent bind receptors on mast cells and basophils and cause degranulation with the release of pharmacologically active mediators which induce smooth-muscle contraction and increases in vascular permeability. - Chemoattractants: C3a, C5a and C5b67 attract and induce monocytes and neutrophils to adhere to vascular endothelial cells, extravasate through the endothelial lining of the capillaries and migrate to the site of complement activation in the tissue.
  • 30. • Immune clearance: Removes immune complexes from the circulation and deposits them in the liver where they are degraded. • Virus neutralization: Complement mediates viral neutralization by facilitating viral aggregation and by coating the viral surface.
  • 32. Clearance of Apoptotic Cells C3b phagocyte CR3, CR4 •Phagocyte recognizes C3b deposited on the surface of apoptotic cell •Apoptotic cell is ingested and destroyed by phagocyte • This is an important mechanism for clearing self antigens and preventing autoimmune responses • Uptake of apoptotic cell also induces self tolerance, thereby prevents autoimmune response