A fully human anti-BMP6 antibody reduces the need for erythropoietin in rodent models of the anemia of chronic disease

Author:

Petzer Verena12ORCID,Tymoszuk Piotr1ORCID,Asshoff Malte1,Carvalho Joana3,Papworth Jonathan3,Deantonio Cecilia3,Bayliss Luke3,Wake Matthew Stephen3,Seifert Markus14,Brigo Natascha1,Valente de Souza Lara14,Hilbe Richard1,Grubwieser Philipp1,Demetz Egon1ORCID,Dichtl Stefanie1,Volani Chiara1ORCID,Berger Sylvia1,Böhm Felix1,Hoffmann Alexander14,Pfeifhofer-Obermair Christa1,von Raffay Laura1,Sopper Sieghart2ORCID,Arndt Stephanie5,Bosserhoff Anja6ORCID,Kautz Léon7,Perrier Prunelle7,Nairz Manfred1,Wolf Dominik28,Weiss Guenter14ORCID,Germaschewski Volker3,Theurl Igor1

Affiliation:

1. Department of Internal Medicine II (Infectious Diseases, Immunology, Rheumatology, Pneumology) and

2. Department of Internal Medicine V (Hematology and Oncology), Medical University of Innsbruck, Innsbruck, Austria;

3. Kymab Ltd, Cambridge, United Kingdom;

4. Christian Doppler Laboratory for Iron Metabolism and Anemia Research, Medical University of Innsbruck, Innsbruck, Austria;

5. Department of Dermatology, University Medical Center Regensburg, Regensburg, Germany;

6. Institute of Biochemistry, Emil Fischer Center, Friedrich-Alexander University of Erlangen-Nürnberg, Erlangen, Germany;

7. Institut de Recherche en Santé Digestive (IRSD), Université de Toulouse, INSERM U1220, Institut National de la Recherche Agronomique (INRA) U1416, École Nationale Vétérinaire de Toulouse (ENVT), Université Paul Sabatier (UPS), Toulouse, France; and

8. Internal Medicine 3, Oncology, Oncology, Immunooncology and Rheumatology, University Clinic Bonn, Bonn, Germany

Abstract

Abstract Recombinant erythropoietin (EPO) and iron substitution are a standard of care for treatment of anemias associated with chronic inflammation, including anemia of chronic kidney disease. A black box warning for EPO therapy and concerns about negative side effects related to high-dose iron supplementation as well as the significant proportion of patients becoming EPO resistant over time explains the medical need to define novel strategies to ameliorate anemia of chronic disease (ACD). As hepcidin is central to the iron-restrictive phenotype in ACD, therapeutic approaches targeting hepcidin were recently developed. We herein report the therapeutic effects of a fully human anti-BMP6 antibody (KY1070) either as monotherapy or in combination with Darbepoetin alfa on iron metabolism and anemia resolution in 2 different, well-established, and clinically relevant rodent models of ACD. In addition to counteracting hepcidin-driven iron limitation for erythropoiesis, we found that the combination of KY1070 and recombinant human EPO improved the erythroid response compared with either monotherapy in a qualitative and quantitative manner. Consequently, the combination of KY1070 and Darbepoetin alfa resulted in an EPO-sparing effect. Moreover, we found that suppression of hepcidin via KY1070 modulates ferroportin expression on erythroid precursor cells, thereby lowering potentially toxic-free intracellular iron levels and by accelerating erythroid output as reflected by increased maturation of erythrocyte progenitors. In summary, we conclude that treatment of ACD, as a highly complex disease, becomes more effective by a multifactorial therapeutic approach upon mobilization of endogenous iron deposits and stimulation of erythropoiesis.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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