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IKAROS and AIOLOS directly regulate AP-1 transcriptional complexes and are essential for NK cell development.

Wilford GohHarrison SudholzMomeneh ForoutanSebastian ScheerAline PfefferleRebecca B DelconteXiangpeng MengZihan ShenRobert HennesseyIsabella Y KongIona S SchusterChristopher E AndoniouMelissa J DavisSoroor Hediyeh-ZadehFernando Souza-Fonseca GuimaraesIan A ParishPaul A BeavisDaniel ThieleMichael ChopinMariapia A Degli-EspostiJoseph CursonsAxel KalliesJai RautelaStephen L NuttNicholas D Huntington
Published in: Nature immunology (2024)
Ikaros transcription factors are essential for adaptive lymphocyte function, yet their role in innate lymphopoiesis is unknown. Using conditional genetic inactivation, we show that Ikzf1/Ikaros is essential for normal natural killer (NK) cell lymphopoiesis and IKZF1 directly represses Cish, a negative regulator of interleukin-15 receptor resulting in impaired interleukin-15 receptor signaling. Both Bcl2l11 and BIM levels, and intrinsic apoptosis were increased in Ikzf1-null NK cells, which in part accounts for NK lymphopenia as both were restored to normal levels when Ikzf1 and Bcl2l11 were co-deleted. Ikzf1-null NK cells presented extensive transcriptional alterations with reduced AP-1 transcriptional complex expression and increased expression of Ikzf2/Helios and Ikzf3/Aiolos. IKZF1 and IKZF3 directly bound AP-1 family members and deletion of both Ikzf1 and Ikzf3 in NK cells resulted in further reductions in Jun/Fos expression and complete loss of peripheral NK cells. Collectively, we show that Ikaros family members are important regulators of apoptosis, cytokine responsiveness and AP-1 transcriptional activity.
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