A Germline Heterozygous Dominant Negative IKZF2 Variant Causing Syndromic Primary Immune Regulatory Disorder and ICHAD

Henry Y. Lu; Maryam Vaseghi-Shanjani; Avery J. Lam; Mehul Sharma; Arezoo Mohajeri; Leandro B. R. Silva; Jana Gillies; Gui Xiang Yang; Susan Lin; Maggie P. Fu; Areesha Salman; Ronak Rahmanian; Linlea Armstrong; Jessica Halparin; Connie L. Yang; Mark Chilvers; Erika Henkelman; Wingfield Rehmus; Douglas Morrison; Audi Setiadi; Sara Mostafavi; Michael S. Kobor; Frederick K. Kozak; Catherine M. Biggs; Clara van Karnebeek; Kyla J. Hildebrand; Anna Lehman on behalf of the Care4Rare Canada Consortium

doi:10.1007/s10875-025-01882-2

A Germline Heterozygous Dominant Negative IKZF2 Variant Causing Syndromic Primary Immune Regulatory Disorder and ICHAD

Henry Y. Lu, Maryam Vaseghi-Shanjani, Avery J. Lam, Mehul Sharma, Arezoo Mohajeri, Leandro B. R. Silva, Jana Gillies, Gui Xiang Yang, Susan Lin, Maggie P. Fu, Areesha Salman, Ronak Rahmanian, Linlea Armstrong, Jessica Halparin, Connie L. Yang, Mark Chilvers, Erika Henkelman, Wingfield Rehmus, Douglas Morrison, Audi SetiadiSara Mostafavi, Michael S. Kobor, Frederick K. Kozak, Catherine M. Biggs, Clara van Karnebeek, Kyla J. Hildebrand, Anna Lehman on behalf of the Care4Rare Canada Consortium

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

Abstract

Monogenic defects that impair the control of inflammation and tolerance lead to profound immune dysregulation, including autoimmunity and atopy. Studying these disorders reveals important molecular and cellular factors that regulate human immune homeostasis and identifies potential precision medicine targets. Here, we provide a detailed immunological assessment of a pediatric patient with a recently discovered syndrome causing Immunodysregulation, Craniofacial anomalies, Hearing impairment, Athelia, and Developmental delay (or ICHAD syndrome). The immunodysregulation resulted in autoimmune hemolytic anemia (AIHA) and atopic dermatitis. The patient carried a de novo germline heterozygous c.406+540_574+13477dup;p.Gly136_Ser191dup variant in IKAROS family zinc finger 2 (IKZF2), which encodes HELIOS. This variant led to reduced HELIOS protein expression and dominant interference of wild-type HELIOS-mediated repression of the IL2 promoter. Multi-parameter flow cytometry analyses of patient peripheral blood mononuclear cells revealed strongly impaired natural killer cell differentiation and function, and increased CD8+ T cell activation and cytokine secretion. Strikingly, patient CD4+ T cells were hyperactive, produced elevated levels of nearly all T helper (TH) cytokines, and readily proliferated in response to stimulation. Patient regulatory T cells (Tregs) developed normally but aberrantly produced high levels of many TH cytokines. Single-cell RNA sequencing revealed largely normal Tregs (albeit mostly memory), but naïve CD4+ T cells that were more enriched in genes related to activation, proliferation, metabolism, and TH differentiation. This work describes the immunological phenotype of one of the first reported cases of germline dominant negative HELIOS deficiency, expands our understanding of the pathogenesis of AIHA on a single cell level, and provides valuable insights into HELIOS function in a variety of lymphocyte subsets.

Original language	English
Article number	89
Journal	Journal of clinical immunology
Volume	45
Issue number	1
DOIs	https://doi.org/10.1007/s10875-025-01882-2
Publication status	Published - 1 Dec 2025
Externally published	Yes

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Lu, H. Y., Vaseghi-Shanjani, M., Lam, A. J., Sharma, M., Mohajeri, A., Silva, L. B. R., Gillies, J., Yang, G. X., Lin, S., Fu, M. P., Salman, A., Rahmanian, R., Armstrong, L., Halparin, J., Yang, C. L., Chilvers, M., Henkelman, E., Rehmus, W., Morrison, D., ... Anna Lehman on behalf of the Care4Rare Canada Consortium (2025). A Germline Heterozygous Dominant Negative IKZF2 Variant Causing Syndromic Primary Immune Regulatory Disorder and ICHAD. Journal of clinical immunology, 45(1), Article 89. https://doi.org/10.1007/s10875-025-01882-2

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title = "A Germline Heterozygous Dominant Negative IKZF2 Variant Causing Syndromic Primary Immune Regulatory Disorder and ICHAD",

abstract = "Monogenic defects that impair the control of inflammation and tolerance lead to profound immune dysregulation, including autoimmunity and atopy. Studying these disorders reveals important molecular and cellular factors that regulate human immune homeostasis and identifies potential precision medicine targets. Here, we provide a detailed immunological assessment of a pediatric patient with a recently discovered syndrome causing Immunodysregulation, Craniofacial anomalies, Hearing impairment, Athelia, and Developmental delay (or ICHAD syndrome). The immunodysregulation resulted in autoimmune hemolytic anemia (AIHA) and atopic dermatitis. The patient carried a de novo germline heterozygous c.406+540\_574+13477dup;p.Gly136\_Ser191dup variant in IKAROS family zinc finger 2 (IKZF2), which encodes HELIOS. This variant led to reduced HELIOS protein expression and dominant interference of wild-type HELIOS-mediated repression of the IL2 promoter. Multi-parameter flow cytometry analyses of patient peripheral blood mononuclear cells revealed strongly impaired natural killer cell differentiation and function, and increased CD8+ T cell activation and cytokine secretion. Strikingly, patient CD4+ T cells were hyperactive, produced elevated levels of nearly all T helper (TH) cytokines, and readily proliferated in response to stimulation. Patient regulatory T cells (Tregs) developed normally but aberrantly produced high levels of many TH cytokines. Single-cell RNA sequencing revealed largely normal Tregs (albeit mostly memory), but na{\"i}ve CD4+ T cells that were more enriched in genes related to activation, proliferation, metabolism, and TH differentiation. This work describes the immunological phenotype of one of the first reported cases of germline dominant negative HELIOS deficiency, expands our understanding of the pathogenesis of AIHA on a single cell level, and provides valuable insights into HELIOS function in a variety of lymphocyte subsets.",

author = "Lu, \{Henry Y.\} and Maryam Vaseghi-Shanjani and Lam, \{Avery J.\} and Mehul Sharma and Arezoo Mohajeri and Silva, \{Leandro B. R.\} and Jana Gillies and Yang, \{Gui Xiang\} and Susan Lin and Fu, \{Maggie P.\} and Areesha Salman and Ronak Rahmanian and Linlea Armstrong and Jessica Halparin and Yang, \{Connie L.\} and Mark Chilvers and Erika Henkelman and Wingfield Rehmus and Douglas Morrison and Audi Setiadi and Sara Mostafavi and Kobor, \{Michael S.\} and Kozak, \{Frederick K.\} and Biggs, \{Catherine M.\} and \{van Karnebeek\}, Clara and Hildebrand, \{Kyla J.\} and \{Anna Lehman on behalf of the Care4Rare Canada Consortium\} and Levings, \{Megan K.\} and Turvey, \{Stuart E.\}",

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

year = "2025",

month = dec,

day = "1",

doi = "10.1007/s10875-025-01882-2",

language = "English",

volume = "45",

journal = "Journal of clinical immunology",

issn = "0271-9142",

publisher = "Springer New York",

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Lu, HY, Vaseghi-Shanjani, M, Lam, AJ, Sharma, M, Mohajeri, A, Silva, LBR, Gillies, J, Yang, GX, Lin, S, Fu, MP, Salman, A, Rahmanian, R, Armstrong, L, Halparin, J, Yang, CL, Chilvers, M, Henkelman, E, Rehmus, W, Morrison, D, Setiadi, A, Mostafavi, S, Kobor, MS, Kozak, FK, Biggs, CM, van Karnebeek, C, Hildebrand, KJ & Anna Lehman on behalf of the Care4Rare Canada Consortium 2025, 'A Germline Heterozygous Dominant Negative IKZF2 Variant Causing Syndromic Primary Immune Regulatory Disorder and ICHAD', Journal of clinical immunology, vol. 45, no. 1, 89. https://doi.org/10.1007/s10875-025-01882-2

TY - JOUR

T1 - A Germline Heterozygous Dominant Negative IKZF2 Variant Causing Syndromic Primary Immune Regulatory Disorder and ICHAD

AU - Lu, Henry Y.

AU - Vaseghi-Shanjani, Maryam

AU - Lam, Avery J.

AU - Sharma, Mehul

AU - Mohajeri, Arezoo

AU - Silva, Leandro B. R.

AU - Gillies, Jana

AU - Yang, Gui Xiang

AU - Lin, Susan

AU - Fu, Maggie P.

AU - Salman, Areesha

AU - Rahmanian, Ronak

AU - Armstrong, Linlea

AU - Halparin, Jessica

AU - Yang, Connie L.

AU - Chilvers, Mark

AU - Henkelman, Erika

AU - Rehmus, Wingfield

AU - Morrison, Douglas

AU - Setiadi, Audi

AU - Mostafavi, Sara

AU - Kobor, Michael S.

AU - Kozak, Frederick K.

AU - Biggs, Catherine M.

AU - van Karnebeek, Clara

AU - Hildebrand, Kyla J.

AU - Anna Lehman on behalf of the Care4Rare Canada Consortium

AU - Levings, Megan K.

AU - Turvey, Stuart E.

PY - 2025/12/1

Y1 - 2025/12/1

N2 - Monogenic defects that impair the control of inflammation and tolerance lead to profound immune dysregulation, including autoimmunity and atopy. Studying these disorders reveals important molecular and cellular factors that regulate human immune homeostasis and identifies potential precision medicine targets. Here, we provide a detailed immunological assessment of a pediatric patient with a recently discovered syndrome causing Immunodysregulation, Craniofacial anomalies, Hearing impairment, Athelia, and Developmental delay (or ICHAD syndrome). The immunodysregulation resulted in autoimmune hemolytic anemia (AIHA) and atopic dermatitis. The patient carried a de novo germline heterozygous c.406+540_574+13477dup;p.Gly136_Ser191dup variant in IKAROS family zinc finger 2 (IKZF2), which encodes HELIOS. This variant led to reduced HELIOS protein expression and dominant interference of wild-type HELIOS-mediated repression of the IL2 promoter. Multi-parameter flow cytometry analyses of patient peripheral blood mononuclear cells revealed strongly impaired natural killer cell differentiation and function, and increased CD8+ T cell activation and cytokine secretion. Strikingly, patient CD4+ T cells were hyperactive, produced elevated levels of nearly all T helper (TH) cytokines, and readily proliferated in response to stimulation. Patient regulatory T cells (Tregs) developed normally but aberrantly produced high levels of many TH cytokines. Single-cell RNA sequencing revealed largely normal Tregs (albeit mostly memory), but naïve CD4+ T cells that were more enriched in genes related to activation, proliferation, metabolism, and TH differentiation. This work describes the immunological phenotype of one of the first reported cases of germline dominant negative HELIOS deficiency, expands our understanding of the pathogenesis of AIHA on a single cell level, and provides valuable insights into HELIOS function in a variety of lymphocyte subsets.

AB - Monogenic defects that impair the control of inflammation and tolerance lead to profound immune dysregulation, including autoimmunity and atopy. Studying these disorders reveals important molecular and cellular factors that regulate human immune homeostasis and identifies potential precision medicine targets. Here, we provide a detailed immunological assessment of a pediatric patient with a recently discovered syndrome causing Immunodysregulation, Craniofacial anomalies, Hearing impairment, Athelia, and Developmental delay (or ICHAD syndrome). The immunodysregulation resulted in autoimmune hemolytic anemia (AIHA) and atopic dermatitis. The patient carried a de novo germline heterozygous c.406+540_574+13477dup;p.Gly136_Ser191dup variant in IKAROS family zinc finger 2 (IKZF2), which encodes HELIOS. This variant led to reduced HELIOS protein expression and dominant interference of wild-type HELIOS-mediated repression of the IL2 promoter. Multi-parameter flow cytometry analyses of patient peripheral blood mononuclear cells revealed strongly impaired natural killer cell differentiation and function, and increased CD8+ T cell activation and cytokine secretion. Strikingly, patient CD4+ T cells were hyperactive, produced elevated levels of nearly all T helper (TH) cytokines, and readily proliferated in response to stimulation. Patient regulatory T cells (Tregs) developed normally but aberrantly produced high levels of many TH cytokines. Single-cell RNA sequencing revealed largely normal Tregs (albeit mostly memory), but naïve CD4+ T cells that were more enriched in genes related to activation, proliferation, metabolism, and TH differentiation. This work describes the immunological phenotype of one of the first reported cases of germline dominant negative HELIOS deficiency, expands our understanding of the pathogenesis of AIHA on a single cell level, and provides valuable insights into HELIOS function in a variety of lymphocyte subsets.

UR - https://www.scopus.com/pages/publications/105004337103

U2 - 10.1007/s10875-025-01882-2

DO - 10.1007/s10875-025-01882-2

M3 - Article

C2 - 40295428

SN - 0271-9142

VL - 45

JO - Journal of clinical immunology

JF - Journal of clinical immunology

IS - 1

M1 - 89

ER -

A Germline Heterozygous Dominant Negative IKZF2 Variant Causing Syndromic Primary Immune Regulatory Disorder and ICHAD

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