IκBα controls dormancy in hematopoietic stem cells via retinoic acid during embryonic development

Author:

Thambyrajah RoshanaORCID,Maqueda Maria,Fadlullah Muhammad ZakiORCID,Proffitt Martin,Neo Wen HaoORCID,Guillén Yolanda,Casado-Pelaez MartaORCID,Herrero-Molinero Patricia,Brujas Carla,Castelluccio NoemiORCID,González JessicaORCID,Iglesias Arnau,Marruecos Laura,Ruiz-Herguido Cristina,Esteller ManelORCID,Mereu ElisabettaORCID,Lacaud GeorgesORCID,Espinosa LluisORCID,Bigas AnnaORCID

Abstract

AbstractRecent findings suggest that Hematopoietic Stem Cells (HSC) and progenitors arise simultaneously and independently of each other already in the embryonic aorta-gonad mesonephros region, but it is still unknown how their different features are established. Here, we uncover IκBα (Nfkbia, the inhibitor of NF-κB) as a critical regulator of HSC proliferation throughout development. IκBα balances retinoic acid signaling levels together with the epigenetic silencer, PRC2, specifically in HSCs. Loss of IκBα decreases proliferation of HSC and induces a dormancy related gene expression signature instead. Also, IκBα deficient HSCs respond with superior activation to in vitro culture and in serial transplantation. At the molecular level, chromatin regions harboring binding motifs for retinoic acid signaling are hypo-methylated for the PRC2 dependent H3K27me3 mark in IκBα deficient HSCs. Overall, we show that the proliferation index in the developing HSCs is regulated by a IκBα-PRC2 axis, which controls retinoic acid signaling.

Funder

Ministry of Economy and Competitiveness | Agencia Estatal de Investigación

Departament d'Innovació, Universitats i Empresa, Generalitat de Catalunya

Ministry of Economy and Competitiveness | Instituto de Salud Carlos III

Publisher

Springer Science and Business Media LLC

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