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Neuroinflammation, autoinflammation, splenomegaly and anemia caused by bi-allelic mutations in IRAK4

Neuroinflammation, autoinflammation, splenomegaly and anemia caused by bi-allelic mutations in IRAK4
Neuroinflammation, autoinflammation, splenomegaly and anemia caused by bi-allelic mutations in IRAK4
We describe a novel, severe autoinflammatory syndrome characterized by neuroinflammation, systemic autoinflammation, splenomegaly, and anemia (NASA) caused by bi-allelic mutations in IRAK4. IRAK-4 is a serine/threonine kinase with a pivotal role in innate immune signaling from toll-like receptors and production of pro-inflammatory cytokines. In humans, bi-allelic mutations in IRAK4 result in IRAK-4 deficiency and increased susceptibility to pyogenic bacterial infections, but autoinflammation has never been described. We describe 5 affected patients from 2 unrelated families with compound heterozygous mutations in IRAK4 (c.C877T (p.Q293*)/c.G958T (p.D320Y); and c.A86C (p.Q29P)/c.161 + 1G>A) resulting in severe systemic autoinflammation, massive splenomegaly and severe transfusion dependent anemia and, in 3/5 cases, severe neuroinflammation and seizures. IRAK-4 protein expression was reduced in peripheral blood mononuclear cells (PBMC) in affected patients. Immunological analysis demonstrated elevated serum tumor necrosis factor (TNF), interleukin (IL) 1 beta (IL-1β), IL-6, IL-8, interferon α2a (IFN-α2a), and interferon β (IFN-β); and elevated cerebrospinal fluid (CSF) IL-6 without elevation of CSF IFN-α despite perturbed interferon gene signature. Mutations were located within the death domain (DD; p.Q29P and splice site mutation c.161 + 1G>A) and kinase domain (p.Q293*/p.D320Y) of IRAK-4. Structure-based modeling of the DD mutation p.Q29P showed alteration in the alignment of a loop within the DD with loss of contact distance and hydrogen bond interactions with IRAK-1/2 within the myddosome complex. The kinase domain mutation p.D320Y was predicted to stabilize interactions within the kinase active site. While precise mechanisms of autoinflammation in NASA remain uncertain, we speculate that loss of negative regulation of IRAK-4 and IRAK-1; dysregulation of myddosome assembly and disassembly; or kinase active site instability may drive dysregulated IL-6 and TNF production. Blockade of IL-6 resulted in immediate and complete amelioration of systemic autoinflammation and anemia in all 5 patients treated; however, neuroinflammation has, so far proven recalcitrant to IL-6 blockade and the janus kinase (JAK) inhibitor baricitinib, likely due to lack of central nervous system penetration of both drugs. We therefore highlight that bi-allelic mutation in IRAK4 may be associated with a severe and complex autoinflammatory and neuroinflammatory phenotype that we have called NASA (neuroinflammation, autoinflammation, splenomegaly and anemia), in addition to immunodeficiency in humans.
1664-3224
Cooray, Samantha
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Price-Kuehne, Fiona
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Hong, Ying
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Omoyinmi, Ebun
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Burleigh, Alice
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Gilmour, Kimberly C.
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Ahmad, Bilal
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Choi, Sangdun
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Bahar, Mohammad W.
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Torpiano, Paul
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Gagunashvili, Andrey
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Jensen, Barbara
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Bellos, Evangelos
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Sancho-Shimizu, Vanessa
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Herberg, Jethro A.
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Mankad, Kshitij
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Kumar, Atul
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Kaliakatsos, Marios
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Worth, Austen J.J.
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Eleftheriou, Despina
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Whittaker, Elizabeth
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et al.
Cooray, Samantha
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Price-Kuehne, Fiona
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Hong, Ying
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Omoyinmi, Ebun
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Burleigh, Alice
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Gilmour, Kimberly C.
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Ahmad, Bilal
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Choi, Sangdun
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Bahar, Mohammad W.
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Torpiano, Paul
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Gagunashvili, Andrey
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Jensen, Barbara
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Bellos, Evangelos
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Sancho-Shimizu, Vanessa
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Herberg, Jethro A.
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Mankad, Kshitij
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Kumar, Atul
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Kaliakatsos, Marios
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Worth, Austen J.J.
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Eleftheriou, Despina
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Whittaker, Elizabeth
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Brogan, Paul A.
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Cooray, Samantha, Price-Kuehne, Fiona and Hong, Ying , et al. (2023) Neuroinflammation, autoinflammation, splenomegaly and anemia caused by bi-allelic mutations in IRAK4. Frontiers in Immunology, 14, [1231749]. (doi:10.3389/fimmu.2023.1231749).

Record type: Article

Abstract

We describe a novel, severe autoinflammatory syndrome characterized by neuroinflammation, systemic autoinflammation, splenomegaly, and anemia (NASA) caused by bi-allelic mutations in IRAK4. IRAK-4 is a serine/threonine kinase with a pivotal role in innate immune signaling from toll-like receptors and production of pro-inflammatory cytokines. In humans, bi-allelic mutations in IRAK4 result in IRAK-4 deficiency and increased susceptibility to pyogenic bacterial infections, but autoinflammation has never been described. We describe 5 affected patients from 2 unrelated families with compound heterozygous mutations in IRAK4 (c.C877T (p.Q293*)/c.G958T (p.D320Y); and c.A86C (p.Q29P)/c.161 + 1G>A) resulting in severe systemic autoinflammation, massive splenomegaly and severe transfusion dependent anemia and, in 3/5 cases, severe neuroinflammation and seizures. IRAK-4 protein expression was reduced in peripheral blood mononuclear cells (PBMC) in affected patients. Immunological analysis demonstrated elevated serum tumor necrosis factor (TNF), interleukin (IL) 1 beta (IL-1β), IL-6, IL-8, interferon α2a (IFN-α2a), and interferon β (IFN-β); and elevated cerebrospinal fluid (CSF) IL-6 without elevation of CSF IFN-α despite perturbed interferon gene signature. Mutations were located within the death domain (DD; p.Q29P and splice site mutation c.161 + 1G>A) and kinase domain (p.Q293*/p.D320Y) of IRAK-4. Structure-based modeling of the DD mutation p.Q29P showed alteration in the alignment of a loop within the DD with loss of contact distance and hydrogen bond interactions with IRAK-1/2 within the myddosome complex. The kinase domain mutation p.D320Y was predicted to stabilize interactions within the kinase active site. While precise mechanisms of autoinflammation in NASA remain uncertain, we speculate that loss of negative regulation of IRAK-4 and IRAK-1; dysregulation of myddosome assembly and disassembly; or kinase active site instability may drive dysregulated IL-6 and TNF production. Blockade of IL-6 resulted in immediate and complete amelioration of systemic autoinflammation and anemia in all 5 patients treated; however, neuroinflammation has, so far proven recalcitrant to IL-6 blockade and the janus kinase (JAK) inhibitor baricitinib, likely due to lack of central nervous system penetration of both drugs. We therefore highlight that bi-allelic mutation in IRAK4 may be associated with a severe and complex autoinflammatory and neuroinflammatory phenotype that we have called NASA (neuroinflammation, autoinflammation, splenomegaly and anemia), in addition to immunodeficiency in humans.

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Accepted/In Press date: 14 August 2023
Published date: 6 September 2023

Identifiers

Local EPrints ID: 501699
URI: http://eprints.soton.ac.uk/id/eprint/501699
DOI: doi:10.3389/fimmu.2023.1231749
ISSN: 1664-3224
PURE UUID: de4dff9d-c5f3-45a2-aad2-4a248b7870dc
ORCID for Evangelos Bellos: ORCID iD orcid.org/0000-0002-3389-5715

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Date deposited: 06 Jun 2025 16:34
Last modified: 22 Aug 2025 02:45

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Contributors

Author: Samantha Cooray
Author: Fiona Price-Kuehne
Author: Ying Hong
Author: Ebun Omoyinmi
Author: Alice Burleigh
Author: Kimberly C. Gilmour
Author: Bilal Ahmad
Author: Sangdun Choi
Author: Mohammad W. Bahar
Author: Paul Torpiano
Author: Andrey Gagunashvili
Author: Barbara Jensen
Author: Evangelos Bellos ORCID iD
Author: Vanessa Sancho-Shimizu
Author: Jethro A. Herberg
Author: Kshitij Mankad
Author: Atul Kumar
Author: Marios Kaliakatsos
Author: Austen J.J. Worth
Author: Despina Eleftheriou
Author: Elizabeth Whittaker
Author: Paul A. Brogan
Corporate Author: et al.

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