Characterization of ferroportin disease and SLC40A1-related hemochromatosis – Results from the EASL non-HFE registry

Maria Rosina Troppmair; Andrea Ricci; Stefania Scarlini; Sara Pelucchi; Graça Porto; Fabiana Busti; Mayka Sanchez; Hansi Weissensteiner; Sebastian Schönherr; Lukas Forer; Florian Kronenberg; Lorenz Michael Pammer; Christian Kremser; Benjamin Henninger; Paulo Caleb Junior Lima Santos; Peng An; Fudi Wang; Marco De Gobbi; Sule Unal; Yamakawa Noriyuki; Tetsuya Ishikawa; Hal Drakesmith; Herbert Tilg; Edouard Bardou-Jacquet; Domenico Girelli; Alberto Piperno; Antonello Pietrangelo; Elena Corradini; Benedikt Schaefer; Heinz Zoller

doi:10.1016/j.jhep.2025.10.016

Characterization of ferroportin disease and SLC40A1-related hemochromatosis – Results from the EASL non-HFE registry

Maria Rosina Troppmair
, Andrea Ricci
, Stefania Scarlini
, Sara Pelucchi
, Graça Porto
, Fabiana Busti
, Mayka Sanchez
, Hansi Weissensteiner
, Sebastian Schönherr
, Lukas Forer
, Florian Kronenberg
, Lorenz Michael Pammer
, Christian Kremser
, Benjamin Henninger
, Paulo Caleb Junior Lima Santos
, Peng An
, Fudi Wang
, Marco De Gobbi
, Sule Unal
, Yamakawa Noriyuki

Tetsuya Ishikawa, Hal Drakesmith, Herbert Tilg, Edouard Bardou-Jacquet, Domenico Girelli, Alberto Piperno, Antonello Pietrangelo, Elena Corradini, Benedikt Schaefer, Heinz Zoller

Division of Pediatrics

Innsbruck Medical University
University of Modena and Reggio Emilia
University of Milan - Bicocca
University Hospital Center of Santo António
A.O. Universitaria Integrata di Verona
UIC Barcelona
Universidade Federal de São Paulo
China Agricultural University
Zhejiang University School of Public Health
University of Turin
Kyoto University
Nagoya University
University of Oxford
Hôpital Pontchaillou
Azienda Ospedaliera San Gerardo Monza

Research output: Contribution to journal › Article › peer-review

Abstract

Background & Aims Pathogenic variants in the cellular iron exporter ferroportin (SLC40A1) cause hepatic and splenic iron overload. Low to normal transferrin saturation (TSAT) and iron accumulation in Kupffer cells with high splenic iron distinguish ferroportin disease (FD) from SLC40A1 -related hemochromatosis (SLC40A1-HC), which are both caused by variants in SLC40A1 . The aim of our study was to describe pathogenic mutations in SLC40A1 , phenotypic variability in affected patients and compare outcomes with HFE -related hemochromatosis (HFE-HC). Methods The international EASL non- HFE hemochromatosis patient registry prospectively collected clinical, radiological, biochemical, and genetic data for 95 patients with SLC40A1 variants from six centers. Additionally, 363 patients were identified by a systematic literature review. As a comparator, 603 patients diagnosed with HFE-HC were included. Results The FD phenotype presented in 65.5% of affected individuals. Patients with FD were younger at diagnosis and more often female than those with SLC40A1-HC. SLC40A1 variants were associated with higher hepatic and splenic iron concentrations compared to the HFE-HC group. Variability in phenotypic presentation was high among patients with SLC40A1 variants, and a genotype-to-phenotype correlation could only explain a small proportion of this variation. Variants that directly affect the metal binding site in ferroportin more likely presented with high TSAT. Patients with the SLC40A1-HC phenotype (TSAT '45%) had a higher risk of fibrosis. Life expectancy was similar between patients with SLC40A1 variants and matched patients with HFE-HC. Most individuals with SLC40A1 variants (73.2%) received regular phlebotomies, which were not associated with differences in life expectancy. Conclusions Mutations in SLC40A1 cause a highly variable disease spectrum with hepatic and splenic iron overload. Fibrosis risk is higher in patients with elevated TSAT. Impact and implications Clinical management of individuals with SLC40A1 variants has largely been extrapolated from HFE-related hemochromatosis despite fundamental pathophysiological differences. Our study provides detailed phenotypic characterization that supports diagnosis and distinction of these rare iron overload disorders. Long-term follow-up shows preserved life expectancy, unaffected by phlebotomy, underscoring the need to critically assess phlebotomy on an individualized basis. Patients with SLC40A1-related hemochromatosis (transferrin saturation '45%) had a higher prevalence of chronic liver disease than those with ferroportin disease, suggesting that elevated transferrin saturation and hepatic iron drive disease progression, which can guide risk stratification and clinical decision making. Clinical Trial number Not applicable.

Original language	English
Pages (from-to)	728-737
Number of pages	10
Journal	Journal of Hepatology
Volume	84
Issue number	4
DOIs	https://doi.org/10.1016/j.jhep.2025.10.016
Publication status	Published - Apr 2026

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

FPN
Ferroportin
HFE4
IREG1
hyperferritinaemia
iron overload
non-HFE
splenic iron

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10.1016/j.jhep.2025.10.016

Cite this

Troppmair, M. R., Ricci, A., Scarlini, S., Pelucchi, S., Porto, G., Busti, F., Sanchez, M., Weissensteiner, H., Schönherr, S., Forer, L., Kronenberg, F., Pammer, L. M., Kremser, C., Henninger, B., Junior Lima Santos, P. C., An, P., Wang, F., De Gobbi, M., Unal, S., ... Zoller, H. (2026). Characterization of ferroportin disease and SLC40A1-related hemochromatosis – Results from the EASL non-HFE registry. Journal of Hepatology, 84(4), 728-737. https://doi.org/10.1016/j.jhep.2025.10.016

@article{c69a82f29c3d4d4486c7b3c5cbc6c24e,

title = "Characterization of ferroportin disease and SLC40A1-related hemochromatosis – Results from the EASL non-HFE registry",

abstract = "Background \& Aims Pathogenic variants in the cellular iron exporter ferroportin (SLC40A1) cause hepatic and splenic iron overload. Low to normal transferrin saturation (TSAT) and iron accumulation in Kupffer cells with high splenic iron distinguish ferroportin disease (FD) from SLC40A1 -related hemochromatosis (SLC40A1-HC), which are both caused by variants in SLC40A1 . The aim of our study was to describe pathogenic mutations in SLC40A1 , phenotypic variability in affected patients and compare outcomes with HFE -related hemochromatosis (HFE-HC). Methods The international EASL non- HFE hemochromatosis patient registry prospectively collected clinical, radiological, biochemical, and genetic data for 95 patients with SLC40A1 variants from six centers. Additionally, 363 patients were identified by a systematic literature review. As a comparator, 603 patients diagnosed with HFE-HC were included. Results The FD phenotype presented in 65.5\% of affected individuals. Patients with FD were younger at diagnosis and more often female than those with SLC40A1-HC. SLC40A1 variants were associated with higher hepatic and splenic iron concentrations compared to the HFE-HC group. Variability in phenotypic presentation was high among patients with SLC40A1 variants, and a genotype-to-phenotype correlation could only explain a small proportion of this variation. Variants that directly affect the metal binding site in ferroportin more likely presented with high TSAT. Patients with the SLC40A1-HC phenotype (TSAT '45\%) had a higher risk of fibrosis. Life expectancy was similar between patients with SLC40A1 variants and matched patients with HFE-HC. Most individuals with SLC40A1 variants (73.2\%) received regular phlebotomies, which were not associated with differences in life expectancy. Conclusions Mutations in SLC40A1 cause a highly variable disease spectrum with hepatic and splenic iron overload. Fibrosis risk is higher in patients with elevated TSAT. Impact and implications Clinical management of individuals with SLC40A1 variants has largely been extrapolated from HFE-related hemochromatosis despite fundamental pathophysiological differences. Our study provides detailed phenotypic characterization that supports diagnosis and distinction of these rare iron overload disorders. Long-term follow-up shows preserved life expectancy, unaffected by phlebotomy, underscoring the need to critically assess phlebotomy on an individualized basis. Patients with SLC40A1-related hemochromatosis (transferrin saturation '45\%) had a higher prevalence of chronic liver disease than those with ferroportin disease, suggesting that elevated transferrin saturation and hepatic iron drive disease progression, which can guide risk stratification and clinical decision making. Clinical Trial number Not applicable.",

keywords = "FPN, Ferroportin, HFE4, IREG1, hyperferritinaemia, iron overload, non-HFE, splenic iron",

author = "Troppmair, \{Maria Rosina\} and Andrea Ricci and Stefania Scarlini and Sara Pelucchi and Gra{\c c}a Porto and Fabiana Busti and Mayka Sanchez and Hansi Weissensteiner and Sebastian Sch{\"o}nherr and Lukas Forer and Florian Kronenberg and Pammer, \{Lorenz Michael\} and Christian Kremser and Benjamin Henninger and \{Junior Lima Santos\}, \{Paulo Caleb\} and Peng An and Fudi Wang and \{De Gobbi\}, Marco and Sule Unal and Yamakawa Noriyuki and Tetsuya Ishikawa and Hal Drakesmith and Herbert Tilg and Edouard Bardou-Jacquet and Domenico Girelli and Alberto Piperno and Antonello Pietrangelo and Elena Corradini and Benedikt Schaefer and Heinz Zoller",

note = "Publisher Copyright: {\textcopyright} 2025 The Author(s).",

year = "2026",

month = apr,

doi = "10.1016/j.jhep.2025.10.016",

language = "English",

volume = "84",

pages = "728--737",

journal = "Journal of Hepatology",

issn = "0168-8278",

publisher = "Elsevier B.V.",

number = "4",

}

Troppmair, MR, Ricci, A, Scarlini, S, Pelucchi, S, Porto, G, Busti, F, Sanchez, M, Weissensteiner, H, Schönherr, S, Forer, L, Kronenberg, F, Pammer, LM, Kremser, C, Henninger, B, Junior Lima Santos, PC, An, P, Wang, F, De Gobbi, M, Unal, S, Noriyuki, Y, Ishikawa, T, Drakesmith, H, Tilg, H, Bardou-Jacquet, E, Girelli, D, Piperno, A, Pietrangelo, A, Corradini, E, Schaefer, B & Zoller, H 2026, 'Characterization of ferroportin disease and SLC40A1-related hemochromatosis – Results from the EASL non-HFE registry', Journal of Hepatology, vol. 84, no. 4, pp. 728-737. https://doi.org/10.1016/j.jhep.2025.10.016

TY - JOUR

T1 - Characterization of ferroportin disease and SLC40A1-related hemochromatosis – Results from the EASL non-HFE registry

AU - Troppmair, Maria Rosina

AU - Ricci, Andrea

AU - Scarlini, Stefania

AU - Pelucchi, Sara

AU - Porto, Graça

AU - Busti, Fabiana

AU - Sanchez, Mayka

AU - Weissensteiner, Hansi

AU - Schönherr, Sebastian

AU - Forer, Lukas

AU - Kronenberg, Florian

AU - Pammer, Lorenz Michael

AU - Kremser, Christian

AU - Henninger, Benjamin

AU - Junior Lima Santos, Paulo Caleb

AU - An, Peng

AU - Wang, Fudi

AU - De Gobbi, Marco

AU - Unal, Sule

AU - Noriyuki, Yamakawa

AU - Ishikawa, Tetsuya

AU - Drakesmith, Hal

AU - Tilg, Herbert

AU - Bardou-Jacquet, Edouard

AU - Girelli, Domenico

AU - Piperno, Alberto

AU - Pietrangelo, Antonello

AU - Corradini, Elena

AU - Schaefer, Benedikt

AU - Zoller, Heinz

PY - 2026/4

Y1 - 2026/4

N2 - Background & Aims Pathogenic variants in the cellular iron exporter ferroportin (SLC40A1) cause hepatic and splenic iron overload. Low to normal transferrin saturation (TSAT) and iron accumulation in Kupffer cells with high splenic iron distinguish ferroportin disease (FD) from SLC40A1 -related hemochromatosis (SLC40A1-HC), which are both caused by variants in SLC40A1 . The aim of our study was to describe pathogenic mutations in SLC40A1 , phenotypic variability in affected patients and compare outcomes with HFE -related hemochromatosis (HFE-HC). Methods The international EASL non- HFE hemochromatosis patient registry prospectively collected clinical, radiological, biochemical, and genetic data for 95 patients with SLC40A1 variants from six centers. Additionally, 363 patients were identified by a systematic literature review. As a comparator, 603 patients diagnosed with HFE-HC were included. Results The FD phenotype presented in 65.5% of affected individuals. Patients with FD were younger at diagnosis and more often female than those with SLC40A1-HC. SLC40A1 variants were associated with higher hepatic and splenic iron concentrations compared to the HFE-HC group. Variability in phenotypic presentation was high among patients with SLC40A1 variants, and a genotype-to-phenotype correlation could only explain a small proportion of this variation. Variants that directly affect the metal binding site in ferroportin more likely presented with high TSAT. Patients with the SLC40A1-HC phenotype (TSAT '45%) had a higher risk of fibrosis. Life expectancy was similar between patients with SLC40A1 variants and matched patients with HFE-HC. Most individuals with SLC40A1 variants (73.2%) received regular phlebotomies, which were not associated with differences in life expectancy. Conclusions Mutations in SLC40A1 cause a highly variable disease spectrum with hepatic and splenic iron overload. Fibrosis risk is higher in patients with elevated TSAT. Impact and implications Clinical management of individuals with SLC40A1 variants has largely been extrapolated from HFE-related hemochromatosis despite fundamental pathophysiological differences. Our study provides detailed phenotypic characterization that supports diagnosis and distinction of these rare iron overload disorders. Long-term follow-up shows preserved life expectancy, unaffected by phlebotomy, underscoring the need to critically assess phlebotomy on an individualized basis. Patients with SLC40A1-related hemochromatosis (transferrin saturation '45%) had a higher prevalence of chronic liver disease than those with ferroportin disease, suggesting that elevated transferrin saturation and hepatic iron drive disease progression, which can guide risk stratification and clinical decision making. Clinical Trial number Not applicable.

AB - Background & Aims Pathogenic variants in the cellular iron exporter ferroportin (SLC40A1) cause hepatic and splenic iron overload. Low to normal transferrin saturation (TSAT) and iron accumulation in Kupffer cells with high splenic iron distinguish ferroportin disease (FD) from SLC40A1 -related hemochromatosis (SLC40A1-HC), which are both caused by variants in SLC40A1 . The aim of our study was to describe pathogenic mutations in SLC40A1 , phenotypic variability in affected patients and compare outcomes with HFE -related hemochromatosis (HFE-HC). Methods The international EASL non- HFE hemochromatosis patient registry prospectively collected clinical, radiological, biochemical, and genetic data for 95 patients with SLC40A1 variants from six centers. Additionally, 363 patients were identified by a systematic literature review. As a comparator, 603 patients diagnosed with HFE-HC were included. Results The FD phenotype presented in 65.5% of affected individuals. Patients with FD were younger at diagnosis and more often female than those with SLC40A1-HC. SLC40A1 variants were associated with higher hepatic and splenic iron concentrations compared to the HFE-HC group. Variability in phenotypic presentation was high among patients with SLC40A1 variants, and a genotype-to-phenotype correlation could only explain a small proportion of this variation. Variants that directly affect the metal binding site in ferroportin more likely presented with high TSAT. Patients with the SLC40A1-HC phenotype (TSAT '45%) had a higher risk of fibrosis. Life expectancy was similar between patients with SLC40A1 variants and matched patients with HFE-HC. Most individuals with SLC40A1 variants (73.2%) received regular phlebotomies, which were not associated with differences in life expectancy. Conclusions Mutations in SLC40A1 cause a highly variable disease spectrum with hepatic and splenic iron overload. Fibrosis risk is higher in patients with elevated TSAT. Impact and implications Clinical management of individuals with SLC40A1 variants has largely been extrapolated from HFE-related hemochromatosis despite fundamental pathophysiological differences. Our study provides detailed phenotypic characterization that supports diagnosis and distinction of these rare iron overload disorders. Long-term follow-up shows preserved life expectancy, unaffected by phlebotomy, underscoring the need to critically assess phlebotomy on an individualized basis. Patients with SLC40A1-related hemochromatosis (transferrin saturation '45%) had a higher prevalence of chronic liver disease than those with ferroportin disease, suggesting that elevated transferrin saturation and hepatic iron drive disease progression, which can guide risk stratification and clinical decision making. Clinical Trial number Not applicable.

KW - FPN

KW - Ferroportin

KW - HFE4

KW - IREG1

KW - hyperferritinaemia

KW - iron overload

KW - non-HFE

KW - splenic iron

UR - https://www.scopus.com/pages/publications/105025096376

U2 - 10.1016/j.jhep.2025.10.016

DO - 10.1016/j.jhep.2025.10.016

M3 - Article

C2 - 41855270

AN - SCOPUS:105025096376

SN - 0168-8278

VL - 84

SP - 728

EP - 737

JO - Journal of Hepatology

JF - Journal of Hepatology

IS - 4

ER -

Characterization of ferroportin disease and SLC40A1-related hemochromatosis – Results from the EASL non-HFE registry

Abstract

UN SDGs

Keywords

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