A structural deletion in the 3'UTR of SLC11A2 is associated with altered iron status: Evidence from two large Danish cohorts

Nanna Brøns; Andreas Stribolt Rigas; Kathrine Agergård Kaspersen; Ole Birger Pedersen; Christian Erikstrup; Thomas Folkmann Hansen; Erik Sørensen; Joseph Dowsett; Christina Mikkelsen; Lea Arregui Nordahl Christoffersen; Khoa Manh Dinh; Mie Topholm Bruun; Bitten Aagaard; Ruth Frikke-Schmidt; Henning Bundgaard; Henrik Ullum; Andreas Glenthøj; Sisse Rye Ostrowski; DBDS Genetic Consortium

doi:10.1111/bjh.70210

A structural deletion in the 3'UTR of SLC11A2 is associated with altered iron status: Evidence from two large Danish cohorts

Nanna Brøns^*
, Andreas Stribolt Rigas
, Kathrine Agergård Kaspersen
, Ole Birger Pedersen
, Christian Erikstrup
, Thomas Folkmann Hansen
, Erik Sørensen
, Joseph Dowsett
, Christina Mikkelsen
, Lea Arregui Nordahl Christoffersen
, Khoa Manh Dinh
, Mie Topholm Bruun
, Bitten Aagaard
, Ruth Frikke-Schmidt
, Henning Bundgaard
, Henrik Ullum
, Andreas Glenthøj
, Sisse Rye Ostrowski
, DBDS Genetic Consortium

^*Corresponding author for this work

Clinical Immunology

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

Abstract

The SLC11A2 gene encodes divalent metal transporter 1, a key mediator of cellular and intestinal iron transport. While ultra-rare pathogenic variants in SLC11A2 cause autosomal recessive anaemia with iron overload, the phenotypic consequences of structural variation in this gene remain unexplored. We investigated the impact of a recently identified structural deletion in the 3' untranslated region (SLC11A2-Δ3.5kb) using genetic, biomarker and registry data from two large Danish cohorts: the Danish Blood Donor Study and the Copenhagen Hospital Biobank (CHB). Among 4847 heterozygous carriers and 320 633 non-carriers, SLC11A2-Δ3.5kb was associated with lower ferritin levels in both sexes and increased risk of iron deficiency in women. In female donors, SLC11A2-Δ3.5kb was associated with lower haemoglobin levels, increased risk of donation deferral due to low haemoglobin and increased use of prescribed iron treatment. In male CHB participants carrying HFE variants, concurrent SLC11A2-Δ3.5kb carriage was associated with a 66% reduced risk of iron overload, suggesting a potential disease-modifying role in haemochromatosis. No associations were observed with cardiometabolic, inflammatory, neurological or malignant diseases. These findings suggest that SLC11A2-Δ3.5kb affects iron homeostasis through reduced systemic iron availability and may have clinical relevance for personalised iron deficiency risk assessment and haemochromatosis penetrance.

Original language	English
Pages (from-to)	2123-2134
Number of pages	12
Journal	British Journal of Haematology
Volume	207
Issue number	5
Early online date	17 Oct 2025
DOIs	https://doi.org/10.1111/bjh.70210
Publication status	Published - Nov 2025

Funding

Danmarks Frie Forskningsfond, Grant/Award Number: 0134-00352BThis study was supported by a grant from the Independent Research Fund Denmark (0134-00352B). DBDS is funded by an annual grant from Bio-and Genome Bank Denmark. The initiation of DBDS was supported by the Danish Administrative Regions (02/2611) and the Danish Council for Independent Research (09-069412). Additionally, the DBDS is funded by the Novo Nordisk Foundation (NNF23OC0082015, NNF17OC0027864 and NNF17OC0027594).

Funders	Funder number
Independent Research Fund Denmark	0134-00352B
Bio- and Genome Bank Denmark
Danish Administrative Regions and Bio-and Genome Bank Denmark	02/2611
Independent Research Fund Denmark	09-069412
Novo Nordisk Foundation	NNF23OC0082015, NNF17OC0027864, NNF17OC0027594

Keywords

Blood donors
Haemochromatosis
Iron homeostasis
Structural variation
3' Untranslated Regions/genetics
Sequence Deletion
Anemia, Iron-Deficiency/genetics
Humans
Middle Aged
Male
Iron Overload/genetics
Denmark/epidemiology
Cation Transport Proteins/genetics
Hemochromatosis/genetics
Female
Adult
Iron/metabolism
Aged
Cohort Studies

Access to Document

10.1111/bjh.70210Licence: CC BY

Cite this

Brøns, N., Rigas, A. S., Kaspersen, K. A., Pedersen, O. B., Erikstrup, C., Hansen, T. F., Sørensen, E., Dowsett, J., Mikkelsen, C., Christoffersen, L. A. N., Dinh, K. M., Bruun, M. T., Aagaard, B., Frikke-Schmidt, R., Bundgaard, H., Ullum, H., Glenthøj, A., Ostrowski, S. R., & DBDS Genetic Consortium (2025). A structural deletion in the 3'UTR of SLC11A2 is associated with altered iron status: Evidence from two large Danish cohorts. British Journal of Haematology, 207(5), 2123-2134. https://doi.org/10.1111/bjh.70210

@article{a47b01133fbe42c483f27740c86dda8a,

title = "A structural deletion in the 3'UTR of SLC11A2 is associated with altered iron status: Evidence from two large Danish cohorts",

abstract = "The SLC11A2 gene encodes divalent metal transporter 1, a key mediator of cellular and intestinal iron transport. While ultra-rare pathogenic variants in SLC11A2 cause autosomal recessive anaemia with iron overload, the phenotypic consequences of structural variation in this gene remain unexplored. We investigated the impact of a recently identified structural deletion in the 3' untranslated region (SLC11A2-Δ3.5kb) using genetic, biomarker and registry data from two large Danish cohorts: the Danish Blood Donor Study and the Copenhagen Hospital Biobank (CHB). Among 4847 heterozygous carriers and 320 633 non-carriers, SLC11A2-Δ3.5kb was associated with lower ferritin levels in both sexes and increased risk of iron deficiency in women. In female donors, SLC11A2-Δ3.5kb was associated with lower haemoglobin levels, increased risk of donation deferral due to low haemoglobin and increased use of prescribed iron treatment. In male CHB participants carrying HFE variants, concurrent SLC11A2-Δ3.5kb carriage was associated with a 66\% reduced risk of iron overload, suggesting a potential disease-modifying role in haemochromatosis. No associations were observed with cardiometabolic, inflammatory, neurological or malignant diseases. These findings suggest that SLC11A2-Δ3.5kb affects iron homeostasis through reduced systemic iron availability and may have clinical relevance for personalised iron deficiency risk assessment and haemochromatosis penetrance.",

keywords = "Blood donors, Haemochromatosis, Iron homeostasis, Structural variation, 3' Untranslated Regions/genetics, Sequence Deletion, Anemia, Iron-Deficiency/genetics, Humans, Middle Aged, Male, Iron Overload/genetics, Denmark/epidemiology, Cation Transport Proteins/genetics, Hemochromatosis/genetics, Female, Adult, Iron/metabolism, Aged, Cohort Studies",

author = "Nanna Br{\o}ns and Rigas, \{Andreas Stribolt\} and Kaspersen, \{Kathrine Agerg{\aa}rd\} and Pedersen, \{Ole Birger\} and Christian Erikstrup and Hansen, \{Thomas Folkmann\} and Erik S{\o}rensen and Joseph Dowsett and Christina Mikkelsen and Christoffersen, \{Lea Arregui Nordahl\} and Dinh, \{Khoa Manh\} and Bruun, \{Mie Topholm\} and Bitten Aagaard and Ruth Frikke-Schmidt and Henning Bundgaard and Henrik Ullum and Andreas Glenth{\o}j and Ostrowski, \{Sisse Rye\} and \{DBDS Genetic Consortium\}",

note = "{\textcopyright} 2025 The Author(s). British Journal of Haematology published by British Society for Haematology and John Wiley \& Sons Ltd.",

year = "2025",

month = nov,

doi = "10.1111/bjh.70210",

language = "English",

volume = "207",

pages = "2123--2134",

journal = "British Journal of Haematology",

issn = "0007-1048",

publisher = "John Wiley \& Sons Inc.",

number = "5",

}

Brøns, N, Rigas, AS, Kaspersen, KA, Pedersen, OB, Erikstrup, C, Hansen, TF, Sørensen, E, Dowsett, J, Mikkelsen, C, Christoffersen, LAN, Dinh, KM, Bruun, MT, Aagaard, B, Frikke-Schmidt, R, Bundgaard, H, Ullum, H, Glenthøj, A, Ostrowski, SR & DBDS Genetic Consortium 2025, 'A structural deletion in the 3'UTR of SLC11A2 is associated with altered iron status: Evidence from two large Danish cohorts', British Journal of Haematology, vol. 207, no. 5, pp. 2123-2134. https://doi.org/10.1111/bjh.70210

TY - JOUR

T1 - A structural deletion in the 3'UTR of SLC11A2 is associated with altered iron status

T2 - Evidence from two large Danish cohorts

AU - Brøns, Nanna

AU - Rigas, Andreas Stribolt

AU - Kaspersen, Kathrine Agergård

AU - Pedersen, Ole Birger

AU - Erikstrup, Christian

AU - Hansen, Thomas Folkmann

AU - Sørensen, Erik

AU - Dowsett, Joseph

AU - Mikkelsen, Christina

AU - Christoffersen, Lea Arregui Nordahl

AU - Dinh, Khoa Manh

AU - Bruun, Mie Topholm

AU - Aagaard, Bitten

AU - Frikke-Schmidt, Ruth

AU - Bundgaard, Henning

AU - Ullum, Henrik

AU - Glenthøj, Andreas

AU - Ostrowski, Sisse Rye

AU - DBDS Genetic Consortium

PY - 2025/11

Y1 - 2025/11

N2 - The SLC11A2 gene encodes divalent metal transporter 1, a key mediator of cellular and intestinal iron transport. While ultra-rare pathogenic variants in SLC11A2 cause autosomal recessive anaemia with iron overload, the phenotypic consequences of structural variation in this gene remain unexplored. We investigated the impact of a recently identified structural deletion in the 3' untranslated region (SLC11A2-Δ3.5kb) using genetic, biomarker and registry data from two large Danish cohorts: the Danish Blood Donor Study and the Copenhagen Hospital Biobank (CHB). Among 4847 heterozygous carriers and 320 633 non-carriers, SLC11A2-Δ3.5kb was associated with lower ferritin levels in both sexes and increased risk of iron deficiency in women. In female donors, SLC11A2-Δ3.5kb was associated with lower haemoglobin levels, increased risk of donation deferral due to low haemoglobin and increased use of prescribed iron treatment. In male CHB participants carrying HFE variants, concurrent SLC11A2-Δ3.5kb carriage was associated with a 66% reduced risk of iron overload, suggesting a potential disease-modifying role in haemochromatosis. No associations were observed with cardiometabolic, inflammatory, neurological or malignant diseases. These findings suggest that SLC11A2-Δ3.5kb affects iron homeostasis through reduced systemic iron availability and may have clinical relevance for personalised iron deficiency risk assessment and haemochromatosis penetrance.

AB - The SLC11A2 gene encodes divalent metal transporter 1, a key mediator of cellular and intestinal iron transport. While ultra-rare pathogenic variants in SLC11A2 cause autosomal recessive anaemia with iron overload, the phenotypic consequences of structural variation in this gene remain unexplored. We investigated the impact of a recently identified structural deletion in the 3' untranslated region (SLC11A2-Δ3.5kb) using genetic, biomarker and registry data from two large Danish cohorts: the Danish Blood Donor Study and the Copenhagen Hospital Biobank (CHB). Among 4847 heterozygous carriers and 320 633 non-carriers, SLC11A2-Δ3.5kb was associated with lower ferritin levels in both sexes and increased risk of iron deficiency in women. In female donors, SLC11A2-Δ3.5kb was associated with lower haemoglobin levels, increased risk of donation deferral due to low haemoglobin and increased use of prescribed iron treatment. In male CHB participants carrying HFE variants, concurrent SLC11A2-Δ3.5kb carriage was associated with a 66% reduced risk of iron overload, suggesting a potential disease-modifying role in haemochromatosis. No associations were observed with cardiometabolic, inflammatory, neurological or malignant diseases. These findings suggest that SLC11A2-Δ3.5kb affects iron homeostasis through reduced systemic iron availability and may have clinical relevance for personalised iron deficiency risk assessment and haemochromatosis penetrance.

KW - Blood donors

KW - Haemochromatosis

KW - Iron homeostasis

KW - Structural variation

KW - 3' Untranslated Regions/genetics

KW - Sequence Deletion

KW - Anemia, Iron-Deficiency/genetics

KW - Humans

KW - Middle Aged

KW - Male

KW - Iron Overload/genetics

KW - Denmark/epidemiology

KW - Cation Transport Proteins/genetics

KW - Hemochromatosis/genetics

KW - Female

KW - Adult

KW - Iron/metabolism

KW - Aged

KW - Cohort Studies

U2 - 10.1111/bjh.70210

DO - 10.1111/bjh.70210

M3 - Article

C2 - 41103144

SN - 0007-1048

VL - 207

SP - 2123

EP - 2134

JO - British Journal of Haematology

JF - British Journal of Haematology

IS - 5

ER -

A structural deletion in the 3'UTR of SLC11A2 is associated with altered iron status: Evidence from two large Danish cohorts

Abstract

Funding

Keywords

Access to Document

Fingerprint

Cite this