Innate lymphoid cells drive interleukin-23-dependent innate intestinal pathology

Abstract: The key role of IL-23 in the pathogenesis of autoimmune and chronic inflammatory disorders is supported by the identification of IL-23R susceptibility alleles associated with IBD, psoriasis and ankylosing spondylitis. IL-23 driven inflammation has primarily been linked to the actions of Th17 cells1. Somewhat overlooked, IL-23 also has inflammatory effects on innate immune cells2 and can drive T cell- independent colitis. However the downstream cellular and molecular pathways involved in this innate intestinal … Show more

“…Thus, whereas during steady state, microbiota, T H 17 and RORγt + ILCs are controlled by a complex regulatory network, during tissue damage and consequent inflammation, both adaptive and innate RORγt + cells add up production of IL-22 to force a return to homeostasis. However, such situations are potentially dangerous to the host, as the pro-inflammatory activity of T H 17 cells and RORγt + ILCs may expand beyond control and induce inflammatory pathology [54][55][56] . …”

RORγt+ innate lymphoid cells regulate intestinal homeostasis by integrating negative signals from the symbiotic microbiota

“…Thus, whereas during steady state, microbiota, T H 17 and RORγt + ILCs are controlled by a complex regulatory network, during tissue damage and consequent inflammation, both adaptive and innate RORγt + cells add up production of IL-22 to force a return to homeostasis. However, such situations are potentially dangerous to the host, as the pro-inflammatory activity of T H 17 cells and RORγt + ILCs may expand beyond control and induce inflammatory pathology [54][55][56] . …”

RORγt+ innate lymphoid cells regulate intestinal homeostasis by integrating negative signals from the symbiotic microbiota

“…However, chronic activation of ILC3 can result in disease due to uncontrolled inflammation. ILC3 drive colitis in an innate anti‐CD40 driven model of colitis and during Helicobacter hepaticus infection in an IL‐23‐dependent manner, which has been associated with production of GM‐CSF and IFN‐ γ by pro‐inflammatory ILC3 71, 118, 128, 129. Neonatal ILC3 can also mediate intestinal pathology in response to transgenic over‐expression of IL‐23 through the release of IL‐17A, IL‐22, IFN‐ γ and GM‐CSF 130.…”

Functional and phenotypic heterogeneity of group 3 innate lymphoid cells

“…There also seems to be some plasticity between ILC1 and ILC3 cells 32, 33. Thus, ILCs secreting both IFN γ and IL‐17 in response to IL‐23, or IFN γ and IL‐22 in response to IL‐12+IL‐18 have been reported 26, 34. It is thought that both NK cells and ILC1s depend on IL‐15 for their development,35, 36, 37, 38 which is in contrast to ILC2s and ILC3s, which rely on IL‐7 and are depleted in IL‐7R α −/− mice 19, 39…”

Innate‐like CD8+ T‐cells and NK cells: converging functions and phenotypes