Recessive loss of DIAPH1 function causes a progressive neurodevelopmental syndrome with variable immunological involvement
Galassi Deforie V, Maroofian R, Karagoz I, Godwin A, Al Sheikh E, Gestri G, Zaki MS, Woodward BL, Ghorab RM, Alvi JR, Alabdi L, Damseh N, Elshafie RM, Scardamaglia A, Alves C, Shaikh M, Özcan GG, Sadek AA, Issa MY, Striano P, Suri M, Murphy D, Ashhab M, de la Fuente RP, Arteche-López A, Hashem MO, Abdulwahab F, Aboelanine AH, Alkhawaja IA, Ibrahim S, van der Burg M, Berghuis D, Santen GW, Toosi MB, Alerasool M, Eslahi A, Srinivasan VM, Gowda VK, Trollmann R, Vasileiou G, Pauly M, Hashemi-Gorji F, Miryounesi M, Salpietro V, Al-Herz W, Carter SP, Briggs TA, Hussell T, Ruuska-Loewald T, Komulainen-Ebrahim J, Uusimaa J, Hautala T, Potluri S, Shackley F, Mojarrad M, Chung WK, Wilson SW, Sultan T, Gleeson JG, Marafi D, Alkuraya FS, Stewart GS, Efthymiou S, Guille M, Arkwright PD, Houlden H (2026)
Publication Type: Journal article
Publication year: 2026
Journal
Book Volume: 28
Article Number: 102551
Journal Issue: 5
DOI: 10.1016/j.gim.2026.102551
Abstract
Purpose Biallelic DIAPH1 pathogenic variants cause a neurodevelopmental syndrome occasionally associated with immunodeficiency. This study aims to define the clinical and immunological spectrum of DIAPH1 -related neuroimmunological syndrome and explore the gene’s developmental role using vertebrate models. Methods A total of 53 individuals with biallelic DIAPH1 variants, including 33 previously unreported patients, were studied. Clinical features were analyzed, and functional studies were conducted using knockout models in Danio rerio and Xenopus tropicalis . Results Clinical features included developmental delay, intellectual disability, progressive microcephaly, cortical visual impairment or blindness, epilepsy, and frequent occipital-predominant brain abnormalities. Almost half suffered from infections, mainly affecting their respiratory tract related to epilepsy and aspiration. Although the majority had normal lymphocyte subsets and serum immunoglobulins, T cell receptor excision circles and naïve T-lymphocyte counts were consistently low. The Xenopus model mirrored growth and eye defects seen in humans, whereas zebrafish exhibited no overt malformations but showed seizure-like behavior in Phenothiazine assays. Conclusion DIAPH1 is critical for neurodevelopment, immune regulation, and DNA repair. The DNA repair defect may influence susceptibility to infection, lymphoma, or treatment-related toxicity. Although absolute T cell numbers are not consistent with SCID, impaired T cell maturation suggests that these patients could be identified by T cell excision circles newborn screening before neurological symptoms develop.
Authors with CRIS profile
Involved external institutions
University of Portsmouth
United Kingdom (GB)
University of Manchester
United Kingdom (GB)
University College London (UCL)
United Kingdom (GB)
Istituto Giannina Gaslini
Italy (IT)
Nottingham University Hospitals
United Kingdom (GB)
Indira Gandhi Institute of Child Health
India (IN)
Sheffield Children's NHS Foundation Trust
United Kingdom (GB)
National Research Centre (NRC) / المركز القومي للبحوث
Egypt (EG)
Mashhad University of Medical Sciences (MUMS)
Iran, Islamic Republic of (IR)
University of Birmingham
United Kingdom (GB)
Boston Children's Hospital
United States (USA) (US)
University of Child Health Sciences
Pakistan (PK)
University of California, San Diego (UC San Diego, UCSD)
United States (USA) (US)
King Faisal Specialist Hospital & Research Centre
Saudi Arabia (SA)
Ministry of Health
Kuwait (KW)
Al-Quds University / جامعة القدس
Israel (IL)
Harvard University
United States (USA) (US)
Sohag-University
Egypt (EG)
Hospital Universitario 12 de Octubre
Spain (ES)
AlBashir Hospital
Jordan (JO)
Aga Khan University (AKU) / آغا خان یونیورسٹی
Pakistan (PK)
Leiden University Medical Center
Netherlands (NL)
Shahid Beheshti University of Medical Sciences
Iran, Islamic Republic of (IR)
University of L'Aquila / Università degli Studi dell'Aquila
Italy (IT)
Kuwait University
Kuwait (KW)
Oulun Yliopisto / University of Oulo
Finland (FI)
United Kingdom (GB)
University of Manchester
United Kingdom (GB)
University College London (UCL)
United Kingdom (GB)
Istituto Giannina Gaslini
Italy (IT)
Nottingham University Hospitals
United Kingdom (GB)
Indira Gandhi Institute of Child Health
India (IN)
Sheffield Children's NHS Foundation Trust
United Kingdom (GB)
National Research Centre (NRC) / المركز القومي للبحوث
Egypt (EG)
Mashhad University of Medical Sciences (MUMS)
Iran, Islamic Republic of (IR)
University of Birmingham
United Kingdom (GB)
Boston Children's Hospital
United States (USA) (US)
University of Child Health Sciences
Pakistan (PK)
University of California, San Diego (UC San Diego, UCSD)
United States (USA) (US)
King Faisal Specialist Hospital & Research Centre
Saudi Arabia (SA)
Ministry of Health
Kuwait (KW)
Al-Quds University / جامعة القدس
Israel (IL)
Harvard University
United States (USA) (US)
Sohag-University
Egypt (EG)
Hospital Universitario 12 de Octubre
Spain (ES)
AlBashir Hospital
Jordan (JO)
Aga Khan University (AKU) / آغا خان یونیورسٹی
Pakistan (PK)
Leiden University Medical Center
Netherlands (NL)
Shahid Beheshti University of Medical Sciences
Iran, Islamic Republic of (IR)
University of L'Aquila / Università degli Studi dell'Aquila
Italy (IT)
Kuwait University
Kuwait (KW)
Oulun Yliopisto / University of Oulo
Finland (FI)
How to cite
APA:
Galassi Deforie, V., Maroofian, R., Karagoz, I., Godwin, A., Al Sheikh, E., Gestri, G.,... Houlden, H. (2026). Recessive loss of DIAPH1 function causes a progressive neurodevelopmental syndrome with variable immunological involvement. Genetics in Medicine, 28(5). https://doi.org/10.1016/j.gim.2026.102551
MLA:
Galassi Deforie, Valentina, et al. "Recessive loss of DIAPH1 function causes a progressive neurodevelopmental syndrome with variable immunological involvement." Genetics in Medicine 28.5 (2026).
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