Autoimmunity Flashcards
Describe and explain the nature of the body’s response to self-antigen
The body’s response to self-antigen, self-tolerance, prevents harmful autoimmune responses, categorised into 2 broad phrases
Central Tolerance:
1) Negative Selection of T cells:
- Within the thymus, the TCR expressed on T cells is tested for its affinity against self-antigens
- Cells with TCR that binds too strongly to self-antigens presented by MHC molecules are eliminated through apoptosis - negative selection
- Cytokines like IL-7 play a crucial role in thymocyte survival during this selection process
2) Negative Selection of B cells:
- B cells undergo a similar process in the bone marrow
- Those with BCRs that bind to self-antigens with high affinity are deleted or undergo receptor edition to change their specificity
- The cytokine BAFF (B cell-activating factor) is involved in survival signals for B cells
Peripheral Tolerance:
1) Anergy:
- Anergy is a state of unresponsiveness
- If a T cell encounters its antigen in the absence of appropriate co-stimulatory signals (typically CD28 on T cells with B7 on APCs), it becomes anergic
- In this state, it won’t respond to its specific antigen in the future, effectively sidelining any potential auto-reactive T cells
- IL-2 is also required for full T-cell activation, their absence can contribute to anergy
2) Regulatory T cells (Tregs):
- Tregs are a subtype of T cells that suppress the immune response
- Tregs can secrete anti-inflammatory cytokines like IL-10 and TGF-β, which inhibit the activation of self-reactive T cells and help maintain peripheral tolerance
3) Activation-induced cell death (AICD):
- Auto-reactive cells in the periphery can be induced to undergo apoptosis upon repeated exposure to self-antigen
- This process often involves Fas-Fas ligand interaction
Immunological Ignorance:
- When self-antigens are hidden from the immune system in immune-privileged sites (like the brain and testes) or simply at low levels that don’t trigger an immune response
Describe characteristics of autoimmune disease (genetics, environmental factors, endocrine factors) and some of the mechanisms involved in the pathology
Genetic Factors:
1) Human leukocyte antigens (HLA):
- Part of the MHC which are crucial for antigen presentation
- Certain HLA alleles have been strongly associated with autoimmune diseases
- HLA-DR2 and HLA-DR3 are linked with systemic lupus erythematosus (SLE) and HLA-DR4 is linked with rheumatoid arthritis
2) Non-HLA genes:
- These include genes involved in immune regulation, such as PTPN22 (for T-cell activation) and CTLA-4 (T cell regulation)
3) Cytokine genes:
- Certain polymorphisms in genes encoding cytokines (interleukin-1, interleukin-10, TNF-ɑ) may influence the severity and course of autoimmune diseases
Environmental Factors:
1) Infections:
- Certain viral and bacterial infections can trigger autoimmune diseases through molecular mimicry
- where microbial antigens resemble self-antigens, or by activating immune cells nonspecifically
2) Diet:
- High intake of salt, sugar and fat can influence inflammation and auto-immunity
3) Stress and Trauma:
- Psychological stress and physical trauma can also trigger an immune response that, in genetically predisposed individuals, may lead to autoimmunity
Hormonal Factors:
- Oestrogen: stimulates the immune response, which might explain why autoimmune diseases are more prevalent in women, especially during reproductive years
- Pregnancy: Changes in hormone levels during pregnancy and postpartum period can trigger or exacerbate autoimmune diseases
Mechanisms Involved in Pathology:
1) Failure of T-cell anergy:
- Under normal circumstances, self-reactive T cells become anergic (non-reactive) in the absence of co-stimulation
- However, if these T cells receive the second activation signal, they can trigger an autoimmune response
2) Tregs Dysfunction:
- Dysfunction or a decrease in the number of these cells can lead to autoimmunity
- secreting anti-inflammatory cytokines like IL-10 and TGF-β, which inhibit the activation of self-reactive T cell
3) Molecular Mimicry and Epitope Spreading:
- Infections can lead to an immune response against antigens that resemble self-antigens, leading to an autoimmune response
- the initial immune response can ‘spread’ to different epitopes on the same
Describe potential therapies for autoimmunity
Immunosuppressive Therapies:
1) Glucocorticoid:
- Prednisone and other corticosteroids have powerful anti-inflammatory and immunosuppressive properties by suppressing activity of T cells, macrophages and the production of pro-inflammatory cytokines
- Often used in autoimmune diseases like lupus and rheumatoid arthritis
2) Cytotoxic Agents:
- Drugs like Cyclophosphamide and Azathioprine inhibits the replication of cells, including immune cells, thereby suppressing the immune response
3) Calcineurin Inhibitors:
- Cyclosporin A and Tacrolimus inhibit T-cell activation by blocking the function of calcineurin (essential for T cell activation)
Biologic Therapies:
1) Tumour Necrosis Factor (TNF) Inhibitors:
- Etanercept, infliximab, and adalimumab block the action of TNF, a cytokine that promotes inflammation
2) Interleukin Inhibitors:
- anakinra (IL-1 inhibitor), tocilizumab (IL-6 inhibitor), and ustekinumab (IL-12 and IL-23 inhibitor)
3) B-cell Depleting Agents:
- Rituximab is a monoclonal antibody that depletes B cells
Immune Modulating Therapies:
- DMARDs (Disease-Modifying Antirheumatic Drugs)
- JAK inhibitors: inhibit Janus Kinases, enzymes involved in the signalling pathway
Cell-based Therapies:
- Stem Cell Transplantation: hematopoietic stem cell transplantation (HSCT) can be used to essentially “reboot” the immune system
