Chemotherapy-induced transposable elements activate MDA5 to enhance haematopoietic regeneration

Author:

Clapes ThomasORCID,Polyzou Aikaterini,Prater Pia,Sagar ,Morales-Hernández Antonio,Ferrarini Mariana GalvaoORCID,Kehrer NatalieORCID,Lefkopoulos StylianosORCID,Bergo Veronica,Hummel Barbara,Obier Nadine,Maticzka Daniel,Bridgeman Anne,Herman Josip S.ORCID,Ilik Ibrahim,Klaeylé Lhéanna,Rehwinkel JanORCID,McKinney-Freeman ShannonORCID,Backofen RolfORCID,Akhtar AsifaORCID,Cabezas-Wallscheid NinaORCID,Sawarkar Ritwick,Rebollo Rita,Grün DominicORCID,Trompouki EiriniORCID

Abstract

AbstractHaematopoietic stem cells (HSCs) are normally quiescent, but have evolved mechanisms to respond to stress. Here, we evaluate haematopoietic regeneration induced by chemotherapy. We detect robust chromatin reorganization followed by increased transcription of transposable elements (TEs) during early recovery. TE transcripts bind to and activate the innate immune receptor melanoma differentiation-associated protein 5 (MDA5) that generates an inflammatory response that is necessary for HSCs to exit quiescence. HSCs that lack MDA5 exhibit an impaired inflammatory response after chemotherapy and retain their quiescence, with consequent better long-term repopulation capacity. We show that the overexpression of ERV and LINE superfamily TE copies in wild-type HSCs, but not in Mda5−/− HSCs, results in their cycling. By contrast, after knockdown of LINE1 family copies, HSCs retain their quiescence. Our results show that TE transcripts act as ligands that activate MDA5 during haematopoietic regeneration, thereby enabling HSCs to mount an inflammatory response necessary for their exit from quiescence.

Funder

Deutsche Forschungsgemeinschaft

RCUK | Medical Research Council

Max-Planck-Gesellschaft

Fritz Thyssen Stiftung

Publisher

Springer Science and Business Media LLC

Subject

Cell Biology

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