| Literature DB >> 25801035 |
Wei Xu1, Rita G Domingues2, Diogo Fonseca-Pereira2, Manuela Ferreira2, Hélder Ribeiro2, Silvia Lopez-Lastra1, Yasutaka Motomura3, Lara Moreira-Santos2, Franck Bihl4, Véronique Braud4, Barbara Kee5, Hugh Brady6, Mark C Coles7, Christian Vosshenrich1, Masato Kubo8, James P Di Santo9, Henrique Veiga-Fernandes10.
Abstract
Innate lymphoid cells (ILCs) are a family of effectors that originate from a common innate lymphoid cell progenitor. However, the transcriptional program that sets the identity of the ILC lineage remains elusive. Here, we show that NFIL3 is a critical regulator of the common helper-like innate lymphoid cell progenitor (CHILP). Cell-intrinsic Nfil3 ablation led to variably impaired development of fetal and adult ILC subsets. Conditional gene targeting demonstrated that NFIL3 exerted its function prior to ILC subset commitment. Accordingly, NFIL3 ablation resulted in loss of ID2(+) CHILP and PLZF(+) ILC progenitors. Nfil3 expression in lymphoid progenitors was under the control of the mesenchyme-derived hematopoietin IL-7, and NFIL3 exerted its function via direct Id2 regulation in the CHILP. Moreover, ectopic Id2 expression in Nfil3-null precursors rescued defective ILC lineage development in vivo. Our data establish NFIL3 as a key regulator of common helper-like ILC progenitors as they emerge during early lymphopoiesis.Entities:
Mesh:
Substances:
Year: 2015 PMID: 25801035 DOI: 10.1016/j.celrep.2015.02.057
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423