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[[T cells|T cells]] are long lived and are involved in '''cell mediated immunity'''. Functionally they are divided by the expression of CD4⁺ or CD8⁺ markers. CD4⁺ T helper cells recognise antigens bound to MHC II complexes and are involved with the control of intracellular and extracellular pathogens; they can interact with CD8⁺, NK and dendritic cells or with B cells. Cytotoxic CD8⁺ T cells recognise the MHC I complex and destroy infected or neoplastic cells.  

[[T cells|T cells]] are long lived and are involved in '''cell mediated immunity'''. Functionally they are divided by the expression of CD4⁺ or CD8⁺ markers. CD4⁺ T helper cells recognise antigens bound to MHC II complexes and are involved with the control of intracellular and extracellular pathogens; they can interact with CD8⁺, NK and dendritic cells or with B cells. Cytotoxic CD8⁺ T cells recognise the MHC I complex and destroy infected or neoplastic cells.  

Within the blood and lymphoid organs the majority of T cells are antigen-naive T cells; only a small proportion are memory T cells. Naive T cells have yet to encounter antigen and can only be activated by antigen that is presented by dendritic cells. After initial antigenic activation, naïve T-cells develop into an intermediate stage cell called the TH₀ cell which can then be activated by any antigen-presenting cell, e.g. Dendritic cells, [[Macrophages|macrophages]] or [[B cells]].  

Within the blood and lymphoid organs the majority of T cells are antigen-naive T cells; only a small proportion are memory T cells. Naive T cells have yet to encounter antigen and can only be activated by antigen that is presented by dendritic cells. After initial antigenic activation, naïve T-cells develop into an intermediate stage cell called the T_H0 cell which can then be activated by any antigen-presenting cell, e.g. Dendritic cells, [[Macrophages|macrophages]] or [[B cells]].  

The T_H0 cells have the capacity to differentiate into T_H1, T_H2 cells and a very recently described subtype T_H17 cells. The type of cell that develops depends on the antigen presenting cell type. [[Macrophages|Macrophages]] cause the T_H0 cell to develop into a T_H1 cell induced by IL-12 production following macrophage-antigen interaction. B cells cause the T_H0 cell to develop into a T_H2 cell induced by IL-10 production following B cell-antigen interaction. On antigenic stimulation the T_H1 or T_H2 cells become activated, undergo clonal expansion and secrete a range of different cytokines. The third most recently described subset, T_H17, form in the presence of IL-6 and TGF-β which are produced in the prescence of infection, and by either of the Antigen Presenting Cells (APCs).

The T_H0 cells have the capacity to differentiate into T_H1, T_H2 cells and a very recently described subtype T_H17 cells. The type of cell that develops depends on the antigen presenting cell type. [[Macrophages|Macrophages]] cause the T_H0 cell to develop into a T_H1 cell induced by IL-12 production following macrophage-antigen interaction. B cells cause the T_H0 cell to develop into a T_H2 cell induced by IL-10 production following B cell-antigen interaction. On antigenic stimulation the T_H1 or T_H2 cells become activated, undergo clonal expansion and secrete a range of different cytokines. The third most recently described subset, T_H17, form in the presence of IL-6 and TGF-β which are produced in the prescence of infection, and by either of the Antigen Presenting Cells (APCs). The importance of CD4⁺ T_H cells is very clear in immunity. An example of a disease that targets CD4⁺ T cells is the Human Immunodeficieny Viruses (HIV) and Simian Immunodeficieny Viruses (SIV) which, when the CD4⁺ T cells are overwhelmed, causes Advanced Immunodeficiency Syndrome (AIDS).  

For any one cell the cytokine-secreting activation state is short-lived, lasting between 4 - 40 hours. After this time these cells either die or mature into the long-lived memory cells. The proliferation of [[T cells]] continues until the presentation of antigen ceases.

For any one cell the cytokine-secreting activation state is short-lived, lasting between 4 - 40 hours. After this time these cells either die or mature into the long-lived memory cells. The proliferation of [[T cells]] continues until the presentation of antigen ceases.