Niche derived netrin-1 regulates hematopoietic stem cell dormancy via its receptor neogenin-1

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Renders, Simon | Svendsen, Arthur Flohr | Panten, Jasper | Rama, Nicolas | Maryanovich, Maria | Sommerkamp, Pia | Ladel, Luisa | Redavid, Anna Rita | Gibert, Benjamin | Lazare, Seka | Ducarouge, Benjamin | Schönberger, Katharina | Narr, Andreas | Tourbez, Manon | Dethmers-Ausema, Bertien | Zwart, Erik | Hotz-Wagenblatt, Agnes | Zhang, Dachuan | Korn, Claudia | Zeisberger, Petra | Przybylla, Adriana | Sohn, Markus | Mendez-Ferrer, Simon | Heikenwälder, Mathias | Brune, Maik | Klimmeck, Daniel | Bystrykh, Leonid | Frenette, Paul, S | Mehlen, Patrick | de Haan, Gerald | Cabezas-Wallscheid, Nina | Trumpp, Andreas

Edité par CCSD ; Nature Publishing Group -

International audience. Abstract Haematopoietic stem cells (HSCs) are characterized by their self-renewal potential associated to dormancy. Here we identify the cell surface receptor neogenin-1 as specifically expressed in dormant HSCs. Loss of neogenin-1 initially leads to increased HSC expansion but subsequently to loss of self-renewal and premature exhaustion in vivo. Its ligand netrin-1 induces Egr1 expression and maintains quiescence and function of cultured HSCs in a Neo1 dependent manner. Produced by arteriolar endothelial and periarteriolar stromal cells, conditional netrin-1 deletion in the bone marrow niche reduces HSC numbers, quiescence and self-renewal, while overexpression increases quiescence in vivo. Ageing associated bone marrow remodelling leads to the decline of netrin-1 expression in niches and a compensatory but reversible upregulation of neogenin-1 on HSCs. Our study suggests that niche produced netrin-1 preserves HSC quiescence and self-renewal via neogenin-1 function. Decline of netrin-1 production during ageing leads to the gradual decrease of Neo1 mediated HSC self-renewal.

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