Inflammation Flashcards
Outline cytokines
Soluble messengers between cells:
• Examples: Interleukins (ILs),Interferons (INFs), Tumour necrosis factors (TNFs), Growth factors (GFs), Colony-stimulating factors, chemokines (chemotactic cytokines)
• Work together- pleiotropism (diff effects on diff cells), redundancy (more than one has same effect), synergism, antagonism
• Peoduced by activated immune cells, epithelium, stromal cells
• Involved in inflammation:
• Induction Phase
- Pro-inflammatory cytokines (TNF-α, IL-6, IL-1β)- local effects and long range- liver, fever
- Interferons (INFα, INFβ)- induces by viral infection and prevent viral replication, activate DC, macrophages, NK, induce chemokines
• Resolution Phase
- Anti-inflammatory cytokines (TGFβ (repair), IL-10)- inhibit synthesis of pro inflammatory cytokines
Outline chemokines
- Large family of small polypeptides (9-15kDa)
- Naming- cysteine-cysteine ligand CCL/CXCL1,2,3etc. Can have more than one name (CCL2=MCP-1). Chemokine receptors identified by numbers but don’t correlate CCR1,2,3
- Redundancies- eg neutrophils attracted by CXCR8, CXCL12
- Produced mainly by activated macrophages and DCs, only during inflammatory episodes
- Cellular distribution of receptors dictates type of leukocyte recruited into tissues- influences selective recruitment together with cellular adhesion molecules
What is Complement?
Set of 30 or more different proteins which act in an enzymic amplification cascade system to generate a number of active Complement components involved in several aspects of the immune response
Outline the Complement activation pathways
Classical:
C1 complex recognises antigen and antibody
Lectin:
Mannose-binding lectin MBL binds bacterial cell walls
Alternative:
Direct recognition of microbial cell surfaces
Key event: cleaving of C3-> C3a+C3b by C3 convertase (C4b2a/C3bBb)
C3b helps form C5 convertases
• Importance of C3&5 cleavage:
- mast cell degranulation (activation- Increases vascular permeability)- C3a, C4a, C5a
- neutrophil chemotaxis- C5a
- microbe opsonization- C3b, C4b
- cell lysis- C5b-C9 (MAC)
- RBC clearance of immune complexes- C3b (to liver and spleen)
Outline the formation of MAC
- C5b binds C6 and C7
- C5b67 complexes bind to membrane via C7
- C8 binds to complex and inserts into membrane
- C9 molecules (10-16) bind to complex and polymerise to form a pore
What’s involved in acute inflammation? Outline it
Complement Adhesion molecules Chemoattractants Mast cells Neutrophils
- Vascular phase- blood flow, vascular permeability, adhesive endothelium
- Cellular phase- leukocytes accumulate in local vasculature and migrate into infected tissue
- Removal of infectious agent
Outline tissue mast cells
• Release mediators
• Respond to C3a, C5a, PAMPs, DAMPs
• Contain granules with preformed histamine
• Degranulation- release of these vasoactive amines, cytokines, chemotactic factors-> vasodilation
• Formation of lipid mediators- use phospholipase A2 to break down arachidonic acid into either leukotrienes (lipoxygenase pathway) or prostaglandins (cyclo-oxygenase pathway)
—> attract neutrophils and increase inflammation
Outline tissue macrophages
• Role in acute inflammation
• Release:
- cytokines- initiate cytokine cascade (TNF-α, IL-6, IL-1β)
- chemokines- recruit more cells
- inflammatory mediators (lipid derived)- leukotrienes and prostaglandins
• Antigen presentation to T cells
What do proinflammatory cytokines do?
Act on the liver to increase secretion of acute phase proteins (APPs)
-C3
-C-reactive protein (activates Complement
-fibrinogen (coagulation)
—> affect site of inflammation but also brain- no appetite during fever
Outline extravasation
Neutrophils entering tissue from blood:
• P-selection is first receptor to be expressed on endothelium during inflammation
• Neutrophils with P-selection ligand (PSGL-1) will slow and interact
• Integrins then expressed on endothelium (ICAM-1, VCAM-1) induced by TNFα, IL-1, LPSs
• Neutrophils have core receptors (LFA-1 for ICAM and VLA for VCAM)- bind and stop neutrophils
• Diapedesis- neutrophil releases enzymes to dissolve junction between cells
• Neutrophils then enter tissue and follow chemokine/complement gradient
Outline resolution phase
End point of acute inflammation
• Neutrophils enter tissue and begin phagocytosis and remove extra mediators
• Monocytes enter some hours later and differentiate into macrophages
• Chemokines promote further recruitment and clearance of infection
• Neutrophils undergo apoptosis and signal to be ingested by macrophages (efferocytosis). They also release phosphatidylserine-> triggers Mφ release of anti-inflammatory cytokines (IL-10, TGFβ)-> macrophages switch from pro-inflammatory to proresolving
Which cellular infiltrates are in acute and chronic inflammation?
Mainly neutrophils in acute
Monocytes, macrophages and lymphocytes in chronic
What causes chronic inflammation?
- Persistent injury/infection- TB, ulcer, viruses
- Prolonged exposure to toxic agent- pulmonary silicosis (silica in lung)
- Autoimmune disease- RA, MS
