A partial form of AIRE deficiency underlies a mild form of autoimmune polyendocrine syndrome type 1

Bergithe Eikeland Oftedal; Amund Holte Berger; Øyvind Bruserud; Yael Goldfarb; Andre Sulen; Lars Breivik; Alexander Hellesen; Shifra Ben-Dor; Rebecca Haffner-Krausz; Per M. Knappskog; Stefan Johansson; Anette S.B. Wolff; Eirik Bratland; Jakub Abramson; Eystein Sverre Husebye

doi:10.1172/JCI169704

A partial form of AIRE deficiency underlies a mild form of autoimmune polyendocrine syndrome type 1

Bergithe Eikeland Oftedal
, Amund Holte Berger
, Øyvind Bruserud
, Yael Goldfarb
, Andre Sulen
, Lars Breivik
, Alexander Hellesen
, Shifra Ben-Dor
, Rebecca Haffner-Krausz
, Per M. Knappskog
, Stefan Johansson
, Anette S.B. Wolff
, Eirik Bratland
, Jakub Abramson
, Eystein Sverre Husebye

Weizmann Institute of Science

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

Abstract

Autoimmune polyendocrine syndrome type 1 (APS-1) is caused by mutations in the autoimmune regulator (AIRE) gene. Most patients present with severe chronic mucocutaneous candidiasis and organ-specific autoimmunity from early childhood, but the clinical picture is highly variable. AIRE is crucial for negative selection of T cells, and scrutiny of different patient mutations has previously highlighted many of its molecular mechanisms. In patients with a milder adult-onset phenotype sharing a mutation in the canonical donor splice site of intron 7 (c.879+1G>A), both the predicted altered splicing pattern with loss of exon 7 (AireEx7–/–) and normal full-length AIRE mRNA were found, indicating leaky rather than abolished mRNA splicing. Analysis of a corresponding mouse model demonstrated that the AireEx7–/– mutant had dramatically impaired transcriptional capacity of tissue-specific antigens in medullary thymic epithelial cells but still retained some ability to induce gene expression compared with the complete loss-of-function AireC313X–/– mutant. Our data illustrate an association between AIRE activity and the severity of autoimmune disease, with implications for more common autoimmune diseases associated with AIRE variants, such as primary adrenal insufficiency, pernicious anemia, type 1 diabetes, and rheumatoid arthritis.

Original language	English
Article number	e169704
Number of pages	17
Journal	The Journal of Clinical Investigation
Volume	133
Issue number	21
DOIs	https://doi.org/10.1172/JCI169704
State	Published - 1 Nov 2023

ASJC Scopus subject areas

General Medicine

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Oftedal, B. E., Berger, A. H., Bruserud, Ø., Goldfarb, Y., Sulen, A., Breivik, L., Hellesen, A., Ben-Dor, S., Haffner-Krausz, R., Knappskog, P. M., Johansson, S., Wolff, A. S. B., Bratland, E., Abramson, J., & Husebye, E. S. (2023). A partial form of AIRE deficiency underlies a mild form of autoimmune polyendocrine syndrome type 1. The Journal of Clinical Investigation, 133(21), Article e169704. https://doi.org/10.1172/JCI169704

@article{e005dfa103114dfcbedf9326b8a97e9e,

title = "A partial form of AIRE deficiency underlies a mild form of autoimmune polyendocrine syndrome type 1",

abstract = "Autoimmune polyendocrine syndrome type 1 (APS-1) is caused by mutations in the autoimmune regulator (AIRE) gene. Most patients present with severe chronic mucocutaneous candidiasis and organ-specific autoimmunity from early childhood, but the clinical picture is highly variable. AIRE is crucial for negative selection of T cells, and scrutiny of different patient mutations has previously highlighted many of its molecular mechanisms. In patients with a milder adult-onset phenotype sharing a mutation in the canonical donor splice site of intron 7 (c.879+1G>A), both the predicted altered splicing pattern with loss of exon 7 (AireEx7–/–) and normal full-length AIRE mRNA were found, indicating leaky rather than abolished mRNA splicing. Analysis of a corresponding mouse model demonstrated that the AireEx7–/– mutant had dramatically impaired transcriptional capacity of tissue-specific antigens in medullary thymic epithelial cells but still retained some ability to induce gene expression compared with the complete loss-of-function AireC313X–/– mutant. Our data illustrate an association between AIRE activity and the severity of autoimmune disease, with implications for more common autoimmune diseases associated with AIRE variants, such as primary adrenal insufficiency, pernicious anemia, type 1 diabetes, and rheumatoid arthritis.",

author = "Oftedal, \{Bergithe Eikeland\} and Berger, \{Amund Holte\} and {\O}yvind Bruserud and Yael Goldfarb and Andre Sulen and Lars Breivik and Alexander Hellesen and Shifra Ben-Dor and Rebecca Haffner-Krausz and Knappskog, \{Per M.\} and Stefan Johansson and Wolff, \{Anette S.B.\} and Eirik Bratland and Jakub Abramson and Husebye, \{Eystein Sverre\}",

note = "We highly appreciate the technical assistance of Hajirah Muneer, Elin Theodorsen, Marie Karlsen, and Elisabeth Tombra Halvorsen (all from Haukeland University Hospital, Bergen, Norway); Brith Bergum at the Flow Cytometry Section, Core Facilities, Department of Clinical Science, University of Bergen; and Endy Spriet at the Molecular Imaging Center, Core Facilities, Department of Biomedicine, University of Bergen. The Genomics Core Facility (GCF) at the University of Bergen, which is a part of the NorSeq Consortium, provided RNA-Seq services. GCF is supported in part by major grants from the Research Council of Norway (grant no. 245979/F50), Trond Mohn Stiftelse (grant no. BFS2016-genom), and the Bergen Research Foundation (BFS) (grant no. BFS2017TMT04 and BFS2017TMT08). This study was supported by grants from the University of Bergen, the Bergen Research Foundation, Stiftelsen KG Jebsen, and the Regional Health Authorities of Western Norway. BEO received grant funding from the Research Council of Norway (grant no. 250030), the Regional Health Authorities of Western Norway, and the Novo Nordisk Foundation (grant no. 103302). AHB received a project grant from the Meltzer Research Fund.",

year = "2023",

month = nov,

day = "1",

doi = "10.1172/JCI169704",

language = "الإنجليزيّة",

volume = "133",

journal = "The Journal of Clinical Investigation",

issn = "0021-9738",

publisher = "American Society for Clinical Investigation",

number = "21",

}

Oftedal, BE, Berger, AH, Bruserud, Ø, Goldfarb, Y, Sulen, A, Breivik, L, Hellesen, A, Ben-Dor, S, Haffner-Krausz, R, Knappskog, PM, Johansson, S, Wolff, ASB, Bratland, E, Abramson, J & Husebye, ES 2023, 'A partial form of AIRE deficiency underlies a mild form of autoimmune polyendocrine syndrome type 1', The Journal of Clinical Investigation, vol. 133, no. 21, e169704. https://doi.org/10.1172/JCI169704

TY - JOUR

T1 - A partial form of AIRE deficiency underlies a mild form of autoimmune polyendocrine syndrome type 1

AU - Oftedal, Bergithe Eikeland

AU - Berger, Amund Holte

AU - Bruserud, Øyvind

AU - Goldfarb, Yael

AU - Sulen, Andre

AU - Breivik, Lars

AU - Hellesen, Alexander

AU - Ben-Dor, Shifra

AU - Haffner-Krausz, Rebecca

AU - Knappskog, Per M.

AU - Johansson, Stefan

AU - Wolff, Anette S.B.

AU - Bratland, Eirik

AU - Abramson, Jakub

AU - Husebye, Eystein Sverre

N1 - We highly appreciate the technical assistance of Hajirah Muneer, Elin Theodorsen, Marie Karlsen, and Elisabeth Tombra Halvorsen (all from Haukeland University Hospital, Bergen, Norway); Brith Bergum at the Flow Cytometry Section, Core Facilities, Department of Clinical Science, University of Bergen; and Endy Spriet at the Molecular Imaging Center, Core Facilities, Department of Biomedicine, University of Bergen. The Genomics Core Facility (GCF) at the University of Bergen, which is a part of the NorSeq Consortium, provided RNA-Seq services. GCF is supported in part by major grants from the Research Council of Norway (grant no. 245979/F50), Trond Mohn Stiftelse (grant no. BFS2016-genom), and the Bergen Research Foundation (BFS) (grant no. BFS2017TMT04 and BFS2017TMT08). This study was supported by grants from the University of Bergen, the Bergen Research Foundation, Stiftelsen KG Jebsen, and the Regional Health Authorities of Western Norway. BEO received grant funding from the Research Council of Norway (grant no. 250030), the Regional Health Authorities of Western Norway, and the Novo Nordisk Foundation (grant no. 103302). AHB received a project grant from the Meltzer Research Fund.

PY - 2023/11/1

Y1 - 2023/11/1

N2 - Autoimmune polyendocrine syndrome type 1 (APS-1) is caused by mutations in the autoimmune regulator (AIRE) gene. Most patients present with severe chronic mucocutaneous candidiasis and organ-specific autoimmunity from early childhood, but the clinical picture is highly variable. AIRE is crucial for negative selection of T cells, and scrutiny of different patient mutations has previously highlighted many of its molecular mechanisms. In patients with a milder adult-onset phenotype sharing a mutation in the canonical donor splice site of intron 7 (c.879+1G>A), both the predicted altered splicing pattern with loss of exon 7 (AireEx7–/–) and normal full-length AIRE mRNA were found, indicating leaky rather than abolished mRNA splicing. Analysis of a corresponding mouse model demonstrated that the AireEx7–/– mutant had dramatically impaired transcriptional capacity of tissue-specific antigens in medullary thymic epithelial cells but still retained some ability to induce gene expression compared with the complete loss-of-function AireC313X–/– mutant. Our data illustrate an association between AIRE activity and the severity of autoimmune disease, with implications for more common autoimmune diseases associated with AIRE variants, such as primary adrenal insufficiency, pernicious anemia, type 1 diabetes, and rheumatoid arthritis.

AB - Autoimmune polyendocrine syndrome type 1 (APS-1) is caused by mutations in the autoimmune regulator (AIRE) gene. Most patients present with severe chronic mucocutaneous candidiasis and organ-specific autoimmunity from early childhood, but the clinical picture is highly variable. AIRE is crucial for negative selection of T cells, and scrutiny of different patient mutations has previously highlighted many of its molecular mechanisms. In patients with a milder adult-onset phenotype sharing a mutation in the canonical donor splice site of intron 7 (c.879+1G>A), both the predicted altered splicing pattern with loss of exon 7 (AireEx7–/–) and normal full-length AIRE mRNA were found, indicating leaky rather than abolished mRNA splicing. Analysis of a corresponding mouse model demonstrated that the AireEx7–/– mutant had dramatically impaired transcriptional capacity of tissue-specific antigens in medullary thymic epithelial cells but still retained some ability to induce gene expression compared with the complete loss-of-function AireC313X–/– mutant. Our data illustrate an association between AIRE activity and the severity of autoimmune disease, with implications for more common autoimmune diseases associated with AIRE variants, such as primary adrenal insufficiency, pernicious anemia, type 1 diabetes, and rheumatoid arthritis.

UR - https://www.scopus.com/pages/publications/85175677951

U2 - 10.1172/JCI169704

DO - 10.1172/JCI169704

M3 - مقالة

SN - 0021-9738

VL - 133

JO - The Journal of Clinical Investigation

JF - The Journal of Clinical Investigation

IS - 21

M1 - e169704

ER -

A partial form of AIRE deficiency underlies a mild form of autoimmune polyendocrine syndrome type 1

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