Induction of Erythroferrone in Healthy Humans by Micro-dose Recombinant Erythropoietin or High-altitude Exposure

Overview

Journal Haematologica

Specialty Hematology

Date 2020 Jan 11

PMID 31919080

Citations 13

Authors

Paul Robach

Elena Gammella

Stefania Recalcati

Domenico Girelli

Annalisa Castagna

Matthieu Roustit

Carsten Lundby

Anne-Kristine Lundby

Pierre Bouzat

Samuel Verges

Guillaume Sechaud

Pierluigi Banco

Mario Uhr

Catherine Cornu

Pierre Sallet

Gaetano Cairo

Affiliations

Soon will be listed here.

Abstract

The erythropoietin (Epo)-erythroferrone (ERFE)-hepcidin axis coordinates erythropoiesis and iron homeostasis. While mouse studies have established that Epo-induced ERFE production represses hepcidin synthesis by inhibiting hepatic BMP/SMAD signaling, evidence for the role of ERFE in humans is limited. To investigate the role of ERFE as a physiological erythroid regulator in humans, we conducted two studies: first, 24 males received six injections of saline (placebo), recombinant Epo (rhEpo) 20 UI kg-1 (micro-dose) or 50 UI kg-1 (low-dose). Second, we quantified ERFE in 22 subjects exposed to high altitude (3800 m) for 15 hours. In the first study, total hemoglobin mass (Hbmass) increased after low- but not after micro-dose injections, when compared to placebo. Serum ERFE levels were enhanced by rhEpo, remaining higher than after placebo for 48 (micro-dose) or 72 hours (low-dose) post-injections. Conversely, hepcidin levels decreased when Epo and ERFE arose, before any changes in serum iron parameters occurred. In the second study, serum Epo and ERFE increased at high altitude. The present results demonstrate that in healthy humans ERFE responds to slightly increased Epo levels not associated with Hbmass expansion and down-regulates hepcidin in an apparently iron-independent way. Notably, ERFE flags micro-dose Epo, thus holding promise as novel anti-doping biomarker.

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