Adaptive Immune System Flashcards
What are the main cells of the adaptive immune system?
- T lymphocytes
- CD4+ Helper T lymphocytes
- CD8+ Cytotoxic T lymphocytes
- B cells
- Plasma cell
- Memory B cell
Describe the development of the cells of the adaptive immune system?
- Multipotent haematopoietic stem cells found in bone marrow differentiate to form common myeloid and lymphoid progenitor cells
- Lymphoid progenitor cells give rise to T cells, B cells and NK cells
- B cells mature in bone marrow, whereas T cells move and complete maturation within thymus
- Once in thymus T cells are termed thymocytes, where they develop specific T cell markers including the T cell receptor
- Both cells differentiate further within secondary lymphoid organs
- Positive and negative selection occurs here
Where do B cells and T cells mature?
- B cells mature in bone marrow, whereas T cells move and complete maturation within thymus
- Once in thymus T cells are termed thymocytes, where they develop specific T cell markers including the T cell receptor
Where do T cells recieve their TCR?
Thymus
What are T cells in the thymus termed?
Thymocytes
What does TCR stand for?
T cell receptor
Describe the formation of the TCR?
T cell receptor (TCR) formed during T cell development in thymus:
- Composed of alpha and beta chains
- Within these proteins are complementarity determining regions (CDRs)
- Part that binds to antigens
- V(D)J recombination occurs to create diverse selection of antigen binding sites within T cell receptors
What chains is the TCR composed of?
- Composed of alpha and beta chains
What does CDRs stand for?
Comlementarity determining regions
What are CDRs?
- Part that binds to antigens
- V(D)J recombination occurs to create diverse selection of antigen binding sites within T cell receptors
What allows the diversity of the TCR?
- V(D)J recombination occurs to create diverse selection of antigen binding sites within T cell receptors
What does CD refer to?
CD refers to cluster of differentiation:
- All white cells have unique surface markers, named as specific CD markers
- Cells gain and lose these as they mature, so presence or absence allows maturity of cell to be assessed
- CD4+ and CD8+ act as co-receptors with the TCR, to allow TCR to interact with MHC more effectively
What does the presence of CD markers allow to be assessed?
- Cells gain and lose these as they mature, so presence or absence allows maturity of cell to be assessed
What is the function of CD4 and CD8?
- CD4+ and CD8+ act as co-receptors with the TCR, to allow TCR to interact with MHC more effectively
Where does positive and negative selection of T cells occur?
Thymus
Describe the development of T cells in the thymus?
In early stage of development within thymus, neither CD4 nor CD8 is expressed on T cell so they are termed double negative thymocytes (CD4- and CD8-)
They continue to develop and become double positive thymocytes (CD4+CD8+)
They then undergo positive and negative selection:
- Positive selection – identifies T cells capable to interacting with MHC
- If able to interact with MHC survive
- If unable to interact with MHC are destroyed by apoptosis
- Negative selection – identifies T cells that react to strongly to self-antigens
- If react too strongly destroyed by apoptosis
Cells that survive this differentiate into single positive T cells (either CD4 or CD8) depending on whether TCR recognised MHC I or MHC II
Then released from thymus as naïve cells, only differentiating into Th or Tc once they have encountered complementary antigens within secondary lymphoid organs
What is positive and negative selection?
- Positive selection – identifies T cells capable to interacting with MHC
- If able to interact with MHC survive
- If unable to interact with MHC are destroyed by apoptosis
- Negative selection – identifies T cells that react to strongly to self-antigens
- If react too strongly destroyed by apoptosis
What causes T cells to become CD4 or CD8?
Cells that survive this differentiate into single positive T cells (either CD4 or CD8) depending on whether TCR recognised MHC I or MHC II
What are T cells termed when they are released from the thymus?
Naive T cells
When do naive T cells differentiate into T helper or T cytotoxic cells?
Then released from thymus as naïve cells, only differentiating into Th or Tc once they have encountered complementary antigens within secondary lymphoid organs
Describe the function of cytotoxic T cells?
- Recognise and destroy viral infected host cells, or any host cells showing signs of damage via their MHC I expression
- Kill using 3 different mechanisms once activated
- Release IFN and TNF-a which have anti-viral and anti-tumour effects
- Release cytotoxic granules containing perforin and granzyme proteins in direction of target cells
- Performin produces pore in target membrane allowing entry of granzyme enzymes
- Granzymes are proteases that trigger the caspase cascade which leads to apoptosis of cell
- Induce apoptosis via Fas and FasL interactions with target cell
- Activated Tc cell will express FasL on surface, which binds to the Fas receptor on target cell triggering the caspase cascade and causing apoptosis
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What are the 3 mechanisms cytotoxic T cells can use to kill?
- Release IFN and TNF-a which have anti-viral and anti-tumour effects
- Release cytotoxic granules containing perforin and granzyme proteins in direction of target cells
- Performin produces pore in target membrane allowing entry of granzyme enzymes
- Granzymes are proteases that trigger the caspase cascade which leads to apoptosis of cell
- Induce apoptosis via Fas and FasL interactions with target cell
- Activated Tc cell will express FasL on surface, which binds to the Fas receptor on target cell triggering the caspase cascade and causing apoptosis
What does performin and granzymes do?
- Performin produces pore in target membrane allowing entry of granzyme enzymes
- Granzymes are proteases that trigger the caspase cascade which leads to apoptosis of cell
How do cytotoxic T cells induce apoptosis on the target?
- Activated Tc cell will express FasL on surface, which binds to the Fas receptor on target cell triggering the caspase cascade and causing apoptosis
What are functions of helper T cells?
- Help activate other immune cells by releasing T cell cytokines
- Responsible for B cell antibody class switching, activation and growth of cytotoxic T cells and maximise activity of phagocytes
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What are the different types of helper T cell subsets?
-
Th1
- Releases IFN-gamma to maximise activity of phagocytes and cytotoxic T cells
- Function – cellular immunity, clearance of intracellular pathogens
-
Th2
- Releases – IL4, IL5, IL13 to activate basophils, mast cells and eosinophils, and to promote class switching of antibodies to IgE
- Inhibits activity of Th1, over-activity of Th1 can result in type IV hypersensitivity reactions such as in MS, but over-activity of Th2 can result in type I hypersensitivity such as asthma
- Function – humoral immunity, clearance of certain extracellular pathogens, allergy
-
Th17
- Releases – IL17, IL22, IL21 which are pro-inflammatory and stimulates recruitment of neutrophils and macrophages to infected tissues via CXCL-8
- If Th17 over-active can create a chronic inflammatory state as seen in some autoimmune diseases such as rheumatoid arthritis
- Function – tissue inflammation and autoimmunity, clearance of certain extracellular pathogens
For Th1:
- releases
- function
- Releases IFN-gamma to maximise activity of phagocytes and cytotoxic T cells
- Function – cellular immunity, clearance of intracellular pathogens
For Th2:
- releases
- function
- Releases – IL4, IL5, IL13 to activate basophils, mast cells and eosinophils, and to promote class switching of antibodies to IgE
- Inhibits activity of Th1, over-activity of Th1 can result in type IV hypersensitivity reactions such as in MS, but over-activity of Th2 can result in type I hypersensitivity such as asthma
- Function – humoral immunity, clearance of certain extracellular pathogens, allergy
For Th17:
- releases
- function
- Releases – IL17, IL22, IL21 which are pro-inflammatory and stimulates recruitment of neutrophils and macrophages to infected tissues via CXCL-8
- If Th17 over-active can create a chronic inflammatory state as seen in some autoimmune diseases such as rheumatoid arthritis
- Function – tissue inflammation and autoimmunity, clearance of certain extracellular pathogens
How are T regulatory cells formed?
During selection in thymus, some T cells that recognise self-antigens differentiate into regulatory T cell instead of being deleted
Some of this differentiation is also induced in periphery
Describe the functions of T reg cells?
- Suppressing the activation, proliferation and cytokine production of CD4 and CD8 lymphocytes
- Control the response to self-antigens, and so monitor self-tolerance
- Secretes IL10 and transforming growth factor-beta (TGF-b) which are anti-inflammatory to help suppress immune response
What cytokines do T reg cells secrete?
- Secretes IL10 and transforming growth factor-beta (TGF-b) which are anti-inflammatory to help suppress immune response
Are the cytokines that T reg cells secrete pro or anti-inflammatory?
Anti-inflammatory
What kind of immunity are B lymphocytes responsible for?
Responsible for humoral immunity as part of adaptive immune response:
- Acts through actions of antibodies (or immunoglobulins) directed against specific antigens
What do antibodies do?
Recognise antigen and bind to it via the Fab (fragment antigen binding variable region) of antibody
Once bound communicate with other components of immune system via Fc (constant region) of antibody at the base of the Y
How do antibodies bind to antigen?
Fab region of antibody
What does Fab stand for?
Fragment antigen binding variable region
What is the Fab region of antibody also called?
Variable region
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What are the 2 forms antibodies can be found as?
- Soluble form secreted by plasma cells free-floating in bloodstream
- Fixed form membrane bound on to surface of B cell, membrane bound antibody is also referred to as B cell receptor
What are antibodies fixed to surface of B cells called?
B cell receptor
What does BCR stand for?
B cell receptor
What are the 5 different antibody isotypes?
- IgA
- Dimeric
- Present within secretions such as tears and milk
- IgD
- IgE
- Immune response to parasites, also involved in pathogenesis of allergic reactions
- IgG
- Main component of secondary antibody immune response to antigen
- Only isotype able to cross placenta
- IgM
- Primary antibody response to antigen
- Largest antibody with most binding sites, so more efficient at activating complement
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Which antibody is most prevalent?
IgG
What is the only antibody that can cross the placenta?
IgG
What antibody forms the primary antibody response?
IgM
What antibody is most efficient at activating complement?
- IgM
- Primary antibody response to antigen
- Largest antibody with most binding sites, so more efficient at activating complement
What does the suffix of the immunoglobulin isotypes relate to?
Suffix relates to the heavy chain present on the isotype
What does each antibody differ in?
- Biological properties
- Functional locations
- Ability to deal with different antigens
What are some functions of antibodies?
- Bind to antigens directly to form immune complexes which are cleared through filtration in the blood in organs like liver and spleen
- Act as opsonins for phagocytosis
- Activating complement cascade via the classical pathway
- Bind to target cell and initiate a non-phagocystic cell-mediated destruction of cell, called antibody-dependent cellular cytotoxicity (ADCC)
What does ADCC stand for?
Antibody-dependent cellular cytotoxicity
What is ADCC?
Initiates killing of pathogens or target cells via immune cells from innate system:
- Antibodies bind to antigen receptors on target cell via the Fab region of antibody
- The Fc antibody receptor can then bind to a number of immune cells to activate them
- NK cells, macrophages, neutrophils, eosinophils
- Does not involve complement, and mechanism is not phagocytosis
What is ADCC primariliy mediated by?
Primarily mediated by NK cell activation:
- NK cells bind to FC portion of a cell-bound antibody via their FC receptor, CD16
- Activates NK cell, causing cell mediated destruction of target cell through release of perforin and granzyme, causing apoptosis in target cell
- Binding to FC portion of membrane bound antibody can also activate macrophages, neutrophils and eosinophils causing degranulation and toxic enzymes to facilitate extracellular destruction of target cell
Describe the process of ADCC with NK cells?
- NK cells bind to FC portion of a cell-bound antibody via their FC receptor, CD16
- Activates NK cell, causing cell mediated destruction of target cell through release of perforin and granzyme, causing apoptosis in target cell
- Binding to FC portion of membrane bound antibody can also activate macrophages, neutrophils and eosinophils causing degranulation and toxic enzymes to facilitate extracellular destruction of target cell
Where does B cell development occur?
- B cells express unique surface receptor called a B cell receptor, which is actually an antibody
- During B cell development, V(D)J recombination occurs within the genes encoding the antigen binding sites of B cell receptor, creating diversity
Where does B cell activation occur?
B cells circulate between secondary lymphoid organs looking for antigens that match B cell receptor, activation occurs within these secondary lymphoid organs through 1 of 3 mechanisms
What are the 3 mechanisms of activating B cells?
- Helper T cell dependent activation
- Helper T cell independent activation
- Memory B cell activation helper T cell dependent activation
When does helper T cell dependent activation of B cell occur?
Helper T cell dependent activation occurs when antigen recognised by B cell and helper T cell
When does helper T cell independent activation of B cell occur?
Helper T cell independent activation occurs when B cells are activated directly by antigens found within secondary lymphoid organs:
- T independent antigens are usually lipids or polysaccharides where T dependent antigens are proteins
What kind of molecules are of T independent and T dependent antigens usually?
- T independent antigens are usually lipids or polysaccharides where T dependent antigens are proteins
What happens when a memory B cell re-encounters an antigen?
When a memory B cell re-encounters an antigen that is able to bind to BCR (B cell receptor), the memory B cell reactivates and initiates differentiation into plasma cells, resulting in rapid release of antigen specific antibodies
What could occur following the activation of a B cell?
- B cell bound to antigen differentiates into short lived plasma cell
- Secretes IgM and IgG antibodies specific for the antigen encountered
- Found primarily in spleen and lymph nodes
- Or go to germinal centre of lymph node to proliferate and develop an ability to bind to antigen with greater affinity and undergo immunoglobulin class switching
- This is process where B cells become able to produce a different class of Ig in response to same antigen
- After this has occurred they exit lymph node and travel to bone marrow where they differentiate into long-lived plasma cell or memory B cell
Where do B cells go to proliferate and develop class switching?
Germinal centre of lymph node
What do B cells do after undergoing immunoglobulin class switching?
- After this has occurred they exit lymph node and travel to bone marrow where they differentiate into long-lived plasma cell or memory B cell
What is immunoglobulin class switching?
Mechanism that changes the isotope of an antibody produced by B cells from one to another, such as IgM to IgG in primary and secondary infections:
- Results in change of heavy chai of an antibody, whilst keeping variable region of antibody unchanged
- Meaning new isotope acts on same antigen but with different effector cells
What does immunoglobulin class switching allow?
- Meaning new isotope acts on same antigen but with different effector cells
Does immunoglobulin class switching change the heavy chain or light chain?
- Results in change of heavy chain of an antibody, whilst keeping variable region of antibody unchanged
Describe the speed of response of B cells when first encountering an antigen, compared to re-encountering it in the future?
When foreign antigen first encountered there is a lag phase whilst activated B cells are differentiating into plasma cells, no antibodies are produced here
Once plasma cells have formed a low number of IgM antibodies released to neutralise initial infection, and small amounts of IgG can also be produced
Memory B cells are produced, so if same antigen is encountered in the future the response is faster, causing quick high amounts of IgG and low amounts of IgM
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What are the typical Ig levels when a B cell first encounters an antigen?
Once plasma cells have formed a low number of IgM antibodies released to neutralise initial infection, and small amounts of IgG can also be produced
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What are the typical Ig levels when a B cell re-encounters an antigen?
Memory B cells are produced, so if same antigen is encountered in the future the response is faster, causing quick high amounts of IgG and low amounts of IgM
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What is immunological memory?
These long lived memory cells that enable a quick response in the future is referred to as immunological memory:
- Memory B cells generate accelerated and more potent antibody-mediated immune response
- Memory T cells can either express CD4 or CD8 and respond rapidly