Figure 2
Figure 2. The developmental relationship of ILCs. The NK cell progenitor (pre-NK) and the ILC progenitor (pre-ILC) evolve from the common lymphoid progenitor (CLP), but the phenotype and developmental requirements of the pre-ILCs have not been defined in humans (dotted lines). ILC3s and ILC2s develop from pre-ILCs under the influence of the transcription factors RORγt and GATA3, respectively. CD127+ ILC1s may derive from pre-ILCs or may be developmentally separated as part of the NK branch together with conventional NK cells (cNK) and CD127low ILC1s. Inset: ILCs have plasticity, as RORγt+ NCR− ILC3 can differentiate in vitro into ILC1s and into NCR+ ILC3s; the latter, in turn, can be induced into a NKp44− cKit− CRTH2− ILC1s, and vice versa, depending on specific activation signals. Whether these ILC1s are similar to the NKp44− cKit− CRTH2− ILC1s that can be found in human tissues and blood remains to be determined. During these processes, these cells downregulate RORγt and upregulate Tbet.

The developmental relationship of ILCs. The NK cell progenitor (pre-NK) and the ILC progenitor (pre-ILC) evolve from the common lymphoid progenitor (CLP), but the phenotype and developmental requirements of the pre-ILCs have not been defined in humans (dotted lines). ILC3s and ILC2s develop from pre-ILCs under the influence of the transcription factors RORγt and GATA3, respectively. CD127+ ILC1s may derive from pre-ILCs or may be developmentally separated as part of the NK branch together with conventional NK cells (cNK) and CD127low ILC1s. Inset: ILCs have plasticity, as RORγt+ NCR ILC3 can differentiate in vitro into ILC1s and into NCR+ ILC3s; the latter, in turn, can be induced into a NKp44 cKit CRTH2 ILC1s, and vice versa, depending on specific activation signals. Whether these ILC1s are similar to the NKp44 cKit CRTH2 ILC1s that can be found in human tissues and blood remains to be determined. During these processes, these cells downregulate RORγt and upregulate Tbet.

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