An Alternative Mechanism of Subcellular Iron Uptake Deficiency in Cardiomyocytes

Yuanyuan Dai; Nadezda Ignatyeva; Hang Xu; Ruheen Wali; Karl Toischer; Sören Brandenburg; Christof Lenz; Julius Pronto; Funsho E Fakuade; Samuel Sossalla; Elisabeth M Zeisberg; Andreas Janshoff; Ingo Kutschka; Niels Voigt; Henning Urlaub; Torsten Bloch Rasmussen; Jens Mogensen; Stephan E Lehnart; Gerd Hasenfuss; Antje Ebert

doi:10.1161/CIRCRESAHA.122.321157

An Alternative Mechanism of Subcellular Iron Uptake Deficiency in Cardiomyocytes

Circ Res. 2023 Jul 7;133(2):e19-e46. doi: 10.1161/CIRCRESAHA.122.321157. Epub 2023 Jun 14.

Authors

Yuanyuan Dai^{1

2}, Nadezda Ignatyeva^{1

2}, Hang Xu^{1

2}, Ruheen Wali^{1

2}, Karl Toischer^{1

2

3}, Sören Brandenburg^{1

2

3}, Christof Lenz^{2

4

5

6}, Julius Pronto^{2

7}, Funsho E Fakuade^{2

7

5}, Samuel Sossalla^{1

3

8}, Elisabeth M Zeisberg^{1

2}, Andreas Janshoff⁹, Ingo Kutschka^{2

10}, Niels Voigt^{2

7

5}, Henning Urlaub^{4

6}, Torsten Bloch Rasmussen¹¹, Jens Mogensen¹², Stephan E Lehnart^{1

2

5}, Gerd Hasenfuss^{1

2

3}, Antje Ebert^{1

2}

Affiliations

¹ Heart Research Center Goettingen, Clinic for Cardiology and Pneumology, University Medical Center Goettingen, Georg-August University of Goettingen, Germany (Y.D., N.I., H.X., R.W., K.T., S.B., S.S., E.M.Z., S.E.L., G.H., A.E.).
² DZHK (German Center for Cardiovascular Research), partner site Goettingen, Germany (Y.D., N.I., H.X., R.W., K.T., S.B., C.L., J.P., F.E.F., E.M.Z., I.K., N.V., S.E.L., G.H., A.E.).
³ Heart Center, Clinic for Cardiology and Pneumology, University Medical Center Goettingen (K.T., S.B., S.S., G.H.), University of Goettingen, Germany.
⁴ Department of Clinical Chemistry, University Medical Center Goettingen, (C.L., H.U.), University of Goettingen, Germany.
⁵ Cluster of Excellence "Multiscale Bioimaging: from Molecular Machines to Networks of Excitable Cells" (MBExC; C.L., F.E.F., N.V., S.E.L.), University of Goettingen, Germany.
⁶ Bioanalytical Mass Spectrometry, Max Planck Institute for Multidisciplinary Sciences, Goettingen (C.L., H.U.).
⁷ Institute of Pharmacology and Toxicology, University Medical Center Goettingen, (J.P., F.E.F., N.V.), University of Goettingen, Germany.
⁸ Department for Internal Medicine II, University Medical Center Regensburg (S.S.).
⁹ Institute for Physical Chemistry (A.J.), University of Goettingen, Germany.
¹⁰ Department of Thoracic and Cardiovascular Surgery, University Medical Center Göttingen (I.K.).
¹¹ Department of Cardiology, Aarhus University Hospital, Denmark (T.B.R.).
¹² Department of Cardiology, Aalborg University Hospital, Denmark (J.M.).

PMID: 37313752
DOI: 10.1161/CIRCRESAHA.122.321157

Abstract

Background: Systemic defects in intestinal iron absorption, circulation, and retention cause iron deficiency in 50% of patients with heart failure. Defective subcellular iron uptake mechanisms that are independent of systemic absorption are incompletely understood. The main intracellular route for iron uptake in cardiomyocytes is clathrin-mediated endocytosis.

Methods: We investigated subcellular iron uptake mechanisms in patient-derived and CRISPR/Cas-edited induced pluripotent stem cell-derived cardiomyocytes as well as patient-derived heart tissue. We used an integrated platform of DIA-MA (mass spectrometry data-independent acquisition)-based proteomics and signaling pathway interrogation. We employed a genetic induced pluripotent stem cell model of 2 inherited mutations (TnT [troponin T]-R141W and TPM1 [tropomyosin 1]-L185F) that lead to dilated cardiomyopathy (DCM), a frequent cause of heart failure, to study the underlying molecular dysfunctions of DCM mutations.

Results: We identified a druggable molecular pathomechanism of impaired subcellular iron deficiency that is independent of systemic iron metabolism. Clathrin-mediated endocytosis defects as well as impaired endosome distribution and cargo transfer were identified as a basis for subcellular iron deficiency in DCM-induced pluripotent stem cell-derived cardiomyocytes. The clathrin-mediated endocytosis defects were also confirmed in the hearts of patients with DCM with end-stage heart failure. Correction of the TPM1-L185F mutation in DCM patient-derived induced pluripotent stem cells, treatment with a peptide, Rho activator II, or iron supplementation rescued the molecular disease pathway and recovered contractility. Phenocopying the effects of the TPM1-L185F mutation into WT induced pluripotent stem cell-derived cardiomyocytes could be ameliorated by iron supplementation.

Conclusions: Our findings suggest that impaired endocytosis and cargo transport resulting in subcellular iron deficiency could be a relevant pathomechanism for patients with DCM carrying inherited mutations. Insight into this molecular mechanism may contribute to the development of treatment strategies and risk management in heart failure.

Keywords: cardiomyopathy, dilated; cardiovascular disease; heart failure; iron deficiency; sarcomere.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Cardiomyopathy, Dilated* / genetics
Clathrin / genetics
Clathrin / metabolism
Clathrin / pharmacology
Heart Failure* / genetics
Heart Failure* / metabolism
Humans
Induced Pluripotent Stem Cells* / metabolism
Iron / metabolism
Iron Deficiencies*
Mutation
Myocytes, Cardiac / metabolism

Substances

Iron
Clathrin