T helper 17 cells (T_h17) are a subset of T helper cells producing interleukin 17. They are considered developmentally distinct from T_h1 and T_h2 cells and are thought to play a key role in autoimmune disease.^[1][2] More specifically, they are thought to play a role in tissue injury in these conditions.^[3]

It remains unclear which cytokines exactly contribute to T_h17 formation, but transforming growth factor beta (TGF-?), interleukin 6 (IL-6), interleukin 21 (IL-21) and interleukin 23 (IL-23) have been implicated in mice and humans.^[4][5] Other proteins involved in their differentiation are signal transducer and activator of transcription 3 (STAT3) and the retinoic-acid-receptor-related orphan receptors alpha (ROR?) and ROR?.^[4] Effector cytokines associated with this cell type are IL-17, IL-21 and IL-22.^[6]

Differentiation

Activation of precursor T helper cells in the presence of TGF-beta and IL-6 is thought to drive differentiation of T_h17 cells in the mouse. Aside from cytokine environment, it is unclear whether any other elements of the initial activation of T_h17 cells differ from those of other T helper cells. It has been suggested that IL-23 is involved in the expansion of established T_h17 populations, but that cytokine alone does not induce differentiation of naive T-cell precursors into that cell type.^[7] IL-21, a cytokine produced by T_h17 cells themselves, has also been shown to initiate an alternative route for the activation of T_h17 populations.^[8] In humans, a combination of TGF-beta, IL-1? and IL-23 induces Th17 differentiation from naive T cells.^[5] Both Interferon gamma (IFN?) and IL-4, the main stimulators of T_h1 and T_h2 differentiation respectively, have been shown to negatively regulate T_h17 differentiation.

Functions

On initial characterisation, T_h17 cells were broadly implicated in autoimmune disease and auto-specific T_h17 were shown to be highly pathogenic. A more natural role for T_h17 cells is suggested by studies which have demonstrated preferential induction of IL-17 in cases of host infection with various bacterial and fungal species. T_h17 primarily produce two main members of the IL-17 family; IL-17A and IL-17F which are involved in the recruitment, activation and migration of neutrophils.

References

External links

There are some open access Network Protocols for studying TH17 cells at Nature Protocols:

• TH17 cells contribute to uveitis and scleritis and are inhibited by IL-27/STAT1 in the retina - Western Blot Analysis
• TH17 cells contribute to uveitis and scleritis and are inhibited by IL-27/STAT1 in the retina - Confocal microscopy
• TH17 cells contribute to uveitis and scleritis and are inhibited by IL-27/STAT1 in the retina - Chromatin immunoprecipitation

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