Osteocyte-derived erythroferrone regulates liver hepcidin during stress erythropoiesis
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Abstract
Our knowledge of which bone marrow cells affect red cell production is still incomplete. To explore the role of osteocytes in the process we performed bulk RNAseq of osteocytes isolated from control and phlebotomized mice. The top-upregulated gene following phlebotomy was Fam132b , erythroferrone ( Erfe ). Erfe expression in osteocytes was also upregulated after erythropoietin (EPO) treatment and hypoxia in vitro . To explore if osteocytes contribute to the systemic ERFE levels, we generated two mouse models. We first transplanted wild-type BM in Erfe-/- mice creating a model where ERFE is produced in the BM but not by osteocytes. After phlebotomy, liver hepcidin suppression was significantly lower in mice where the osteocytes could not produce ERFE. To confirm that osteocytes are responsible for this difference, we generated mice lacking EPO receptors in osteocytes by crossing Epor flox/flox and Dmp1 -Cre mice. After phlebotomy, these mice showed reduced hepcidin suppression in the liver and higher circulating serum hepcidin levels compared to controls. Our work identified a novel function of osteocytes in suppressing systemic hepcidin levels during stress erythropoiesis.
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