#6 Inflammation, Apoptosis, Response to Danger Signals Flashcards
How do APCs recognize pathogens?
The PRRs allow APCs to discriminate between self and non-self
They can recognize pathogens and are quiescent until they are activated via a set of PRRs (recognize PAMPs).
Danger Theory (Model)
Immune system detects “danger” (damage) signals from injured tissues, rather than by the recognition of non-self→activate APCs
Humoral response to danger signals
Soluble inflammatory mediators:
Activation of complement, immune cells (releasing chemokines, PG’s, leucotrienes, ROI, NO etc)
Necrosis
Cell gets injured→ necrosis→release danger signals→immune cell is activated→ innate immune response (leukocytes and inflammatory mediators)
Danger signals:
HMGB1
“High mobility group box 1”. Receptor=RAGE
Released during necrosis
-Activates NF-κB pathway (in DC)
Danger signals:
Uric acid
Activates NF-κB pathway (in DC)
Danger signals:
HSPs
Induce NF-κB pathway and release of inflammatory cytokines (TNF-α and IL-1β) (in DC)
Acute Inflammatory Response (common signs)
- ↑ blood supply→redness and heat
- ↑ capillary permeability→ swelling and pain
- ↑ neutrophils
- Arrival of MΦ (16-48 hrs)
- MΦ phagocytosis of debris, restoring homeostasis
Stages of Acute Inflammatory Response
- Detection of danger/damage signal via PRR
- Leukocyte Recruitment and Elimination of Stimuli (release of inflamm. mediators)
- Resolution (Mφ clean up everything via scavenger receptors-type of PRRs)
- Wound healing (Mφ stimulate fibroblasts by releasing TGF-β. (Tissue repair, angiogenesis, re-epithelialization)
Inflammation in Atherosclerosis
- Monocytes recruited via activated endothelium→Mφ
- Several microbial molecules recognized by TLRs→activate cells
- Inflammatory cytokines, chemokines, ROI, NO are released
- Inflammation/tissue damage
- Mφ accumulate lipids and become foam cells
Apoptosis
Apoptotic cells=removed without tissue inflammation (necrosis can cause damage)
- Doesn’t give off danger signals→no immune response
- HMGB1 is not released during apoptosis
- Can render APCs into a tolerant state
- Anti-inflammatory IL-10, TGF-β and regulatory T cells may contribute to the process
What is immunological tolerance?
Process by which the immune system does not respond to Ag (lymph node)
Mechanisms of Apoptosis: Fas
Each cell expresses Fas but only activated lyphocytes express Fas ligand (FasL)
Caspases in Apoptosis
Major executioners, cysteine proteases, orchestrate changes, latent precursors, destroy key components of cell infrastructure
Autoimmune Lymphoproliferative Syndrome (ALPS)
Abnormal lymphocyte survival caused by defective Fas mediated apoptosis
-Majority of patients have heterozygous mutations in gene encoding Fas
Patients have:
- chronic adenopathy and/or splenomegaly in early years of life
- chronic persistence and activation of both T cells that stimulate B-cell maturation (Abs in blood)
- Extended survival of lymphocytes due to defective Fas-mediated apoptosis may allow malignant transformation to occur
