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Their key effector cytokine is IL-10. Their main effector cells are NK cells as well as CD8 T cells, IgG B cells, and IL-10 CD4 T cells. The key THαβ transcription factors are STAT1 and STAT3 as well as IRFs. IL-10 from CD4 T cells activate NK cells' ADCC to apoptose virus-infected cells and to induce host as well as viral DNA fragmentation ...
In immunology, a naive T cell (T h 0 cell) is a T cell that has differentiated in the thymus, and successfully undergone the positive and negative processes of central selection in the thymus. Among these are the naive forms of helper T cells ( CD4 + ) and cytotoxic T cells ( CD8 + ).
A reduced CD4 + /CD8 + ratio is associated with reduced resistance to infection. [9]Patients with tuberculosis show a reduced CD4 + /CD8 + ratio. [9]HIV infection leads to low levels of CD4 + T cells (lowering the CD4 + /CD8 + ratio) through a number of mechanisms, including killing of infected CD4 +.
Priming of naive CD8 T cells generates cytotoxic T cells capable of directly killing pathogen-infected cells. CD4 cells develop into a diverse array of effector cell types depending on the nature of the signals they receive during priming. CD4 effector activity can include cytotoxicity, but more frequently it involves the secretion of a set of ...
The CD8 + T cell response is thought to be important in controlling virus levels, which peak and then decline, as the CD4 + T cell counts rebound. A good CD8 + T cell response has been linked to slower disease progression and a better prognosis, though it does not eliminate the virus. [3] During the acute phase, HIV-induced cell lysis and ...
Optimal CD8 + T cell response relies on CD4 + signalling. [44] CD4 + cells are useful in the initial antigenic activation of naive CD8 T cells, and sustaining memory CD8 + T cells in the aftermath of an acute infection. Therefore, activation of CD4 + T cells can be beneficial to the action of CD8 + T cells. [45] [46] [47]
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