Loss of DIAPH1 causes SCBMS, combined immunodeficiency, and mitochondrial dysfunction

Meri Kaustio; Naemeh Nayebzadeh; Reetta Hinttala; Terhi Tapiainen; Pirjo Åström; Katariina Mamia; Nora Pernaa; Johanna Lehtonen; Virpi Glumoff; Elisa Rahikkala; Minna Honkila; Päivi Olsén; Antti Hassinen; Minttu Polso; Nashat Al Sukaiti; Jalila Al Shekaili; Mahmood Al Kindi; Nadia Al Hashmi; Henrikki Almusa; Daria Bulanova; Emma Haapaniemi; Pu Chen; Maria Suo-Palosaari; Päivi Vieira; Hannu Tuominen; Hannaleena Kokkonen; Nabil Al Macki; Huda Al Habsi; Tuija Löppönen; Heikki Rantala; Vilja Pietiäinen; Shen Ying Zhang; Marjo Renko; Timo Hautala; Tariq Al Farsi; Johanna Uusimaa; Janna Saarela

doi:10.1016/j.jaci.2020.12.656

Loss of DIAPH1 causes SCBMS, combined immunodeficiency, and mitochondrial dysfunction

Meri Kaustio, Naemeh Nayebzadeh, Reetta Hinttala, Terhi Tapiainen, Pirjo Åström, Katariina Mamia, Nora Pernaa, Johanna Lehtonen, Virpi Glumoff, Elisa Rahikkala, Minna Honkila, Päivi Olsén, Antti Hassinen, Minttu Polso, Nashat Al Sukaiti, Jalila Al Shekaili, Mahmood Al Kindi, Nadia Al Hashmi, Henrikki Almusa, Daria BulanovaEmma Haapaniemi, Pu Chen, Maria Suo-Palosaari, Päivi Vieira, Hannu Tuominen, Hannaleena Kokkonen, Nabil Al Macki, Huda Al Habsi, Tuija Löppönen, Heikki Rantala, Vilja Pietiäinen, Shen Ying Zhang, Marjo Renko, Timo Hautala, Tariq Al Farsi, Johanna Uusimaa, Janna Saarela^*

^*المؤلف المقابل لهذا العمل

Microbiology & Immunology

نتاج البحث: المساهمة في مجلة › Article › مراجعة النظراء

14 اقتباسات (Scopus)

ملخص

Background: Homozygous loss of DIAPH1 results in seizures, cortical blindness, and microcephaly syndrome (SCBMS). We studied 5 Finnish and 2 Omani patients with loss of DIAPH1 presenting with SCBMS, mitochondrial dysfunction, and immunodeficiency. Objective: We sought to further characterize phenotypes and disease mechanisms associated with loss of DIAPH1. Methods: Exome sequencing, genotyping and haplotype analysis, B- and T-cell phenotyping, in vitro lymphocyte stimulation assays, analyses of mitochondrial function, immunofluorescence staining for cytoskeletal proteins and mitochondria, and CRISPR-Cas9 DIAPH1 knockout in heathy donor PBMCs were used. Results: Genetic analyses found all Finnish patients homozygous for a rare DIAPH1 splice-variant (NM_005219:c.684+1G>A) enriched in the Finnish population, and Omani patients homozygous for a previously described pathogenic DIAPH1 frameshift-variant (NM_005219:c.2769delT;p.F923fs). In addition to microcephaly, epilepsy, and cortical blindness characteristic to SCBMS, the patients presented with infection susceptibility due to defective lymphocyte maturation and 3 patients developed B-cell lymphoma. Patients’ immunophenotype was characterized by poor lymphocyte activation and proliferation, defective B-cell maturation, and lack of naive T cells. CRISPR-Cas9 knockout of DIAPH1 in PBMCs from healthy donors replicated the T-cell activation defect. Patient-derived peripheral blood T cells exhibited impaired adhesion and inefficient microtubule-organizing center repositioning to the immunologic synapse. The clinical symptoms and laboratory tests also suggested mitochondrial dysfunction. Experiments with immortalized, patient-derived fibroblasts indicated that DIAPH1 affects the amount of complex IV of the mitochondrial respiratory chain. Conclusions: Our data demonstrate that individuals with SCBMS can have combined immune deficiency and implicate defective cytoskeletal organization and mitochondrial dysfunction in SCBMS pathogenesis.

اللغة الأصلية	English
الصفحات (من إلى)	599-611
عدد الصفحات	13
دورية	Journal of Allergy and Clinical Immunology
مستوى الصوت	148
رقم الإصدار	2
المعرِّفات الرقمية للأشياء	https://doi.org/10.1016/j.jaci.2020.12.656
حالة النشر	Published - أغسطس 2021

ASJC Scopus subject areas

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الوصول إلى المستند

10.1016/j.jaci.2020.12.656

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قم بذكر هذا

Kaustio, M., Nayebzadeh, N., Hinttala, R., Tapiainen, T., Åström, P., Mamia, K., Pernaa, N., Lehtonen, J., Glumoff, V., Rahikkala, E., Honkila, M., Olsén, P., Hassinen, A., Polso, M., Al Sukaiti, N., Al Shekaili, J., Al Kindi, M., Al Hashmi, N., Almusa, H., ... Saarela, J. (2021). Loss of DIAPH1 causes SCBMS, combined immunodeficiency, and mitochondrial dysfunction. Journal of Allergy and Clinical Immunology, 148(2), 599-611. https://doi.org/10.1016/j.jaci.2020.12.656

Kaustio, M, Nayebzadeh, N, Hinttala, R, Tapiainen, T, Åström, P, Mamia, K, Pernaa, N, Lehtonen, J, Glumoff, V, Rahikkala, E, Honkila, M, Olsén, P, Hassinen, A, Polso, M, Al Sukaiti, N, Al Shekaili, J, Al Kindi, M, Al Hashmi, N, Almusa, H, Bulanova, D, Haapaniemi, E, Chen, P, Suo-Palosaari, M, Vieira, P, Tuominen, H, Kokkonen, H, Al Macki, N, Al Habsi, H, Löppönen, T, Rantala, H, Pietiäinen, V, Zhang, SY, Renko, M, Hautala, T, Al Farsi, T, Uusimaa, J & Saarela, J 2021, 'Loss of DIAPH1 causes SCBMS, combined immunodeficiency, and mitochondrial dysfunction', Journal of Allergy and Clinical Immunology, المجلد 148, رقم 2, الصفحات 599-611. https://doi.org/10.1016/j.jaci.2020.12.656

@article{be2f2bbdc62a4c9182c84746a25377ad,

title = "Loss of DIAPH1 causes SCBMS, combined immunodeficiency, and mitochondrial dysfunction",

abstract = "Background: Homozygous loss of DIAPH1 results in seizures, cortical blindness, and microcephaly syndrome (SCBMS). We studied 5 Finnish and 2 Omani patients with loss of DIAPH1 presenting with SCBMS, mitochondrial dysfunction, and immunodeficiency. Objective: We sought to further characterize phenotypes and disease mechanisms associated with loss of DIAPH1. Methods: Exome sequencing, genotyping and haplotype analysis, B- and T-cell phenotyping, in vitro lymphocyte stimulation assays, analyses of mitochondrial function, immunofluorescence staining for cytoskeletal proteins and mitochondria, and CRISPR-Cas9 DIAPH1 knockout in heathy donor PBMCs were used. Results: Genetic analyses found all Finnish patients homozygous for a rare DIAPH1 splice-variant (NM_005219:c.684+1G>A) enriched in the Finnish population, and Omani patients homozygous for a previously described pathogenic DIAPH1 frameshift-variant (NM_005219:c.2769delT;p.F923fs). In addition to microcephaly, epilepsy, and cortical blindness characteristic to SCBMS, the patients presented with infection susceptibility due to defective lymphocyte maturation and 3 patients developed B-cell lymphoma. Patients{\textquoteright} immunophenotype was characterized by poor lymphocyte activation and proliferation, defective B-cell maturation, and lack of naive T cells. CRISPR-Cas9 knockout of DIAPH1 in PBMCs from healthy donors replicated the T-cell activation defect. Patient-derived peripheral blood T cells exhibited impaired adhesion and inefficient microtubule-organizing center repositioning to the immunologic synapse. The clinical symptoms and laboratory tests also suggested mitochondrial dysfunction. Experiments with immortalized, patient-derived fibroblasts indicated that DIAPH1 affects the amount of complex IV of the mitochondrial respiratory chain. Conclusions: Our data demonstrate that individuals with SCBMS can have combined immune deficiency and implicate defective cytoskeletal organization and mitochondrial dysfunction in SCBMS pathogenesis.",

keywords = "DIAPH1, SCBMS, T cells, immunodeficiency, microcephaly, mitochondrial dysfunction",

author = "Meri Kaustio and Naemeh Nayebzadeh and Reetta Hinttala and Terhi Tapiainen and Pirjo {\AA}str{\"o}m and Katariina Mamia and Nora Pernaa and Johanna Lehtonen and Virpi Glumoff and Elisa Rahikkala and Minna Honkila and P{\"a}ivi Ols{\'e}n and Antti Hassinen and Minttu Polso and {Al Sukaiti}, Nashat and {Al Shekaili}, Jalila and {Al Kindi}, Mahmood and {Al Hashmi}, Nadia and Henrikki Almusa and Daria Bulanova and Emma Haapaniemi and Pu Chen and Maria Suo-Palosaari and P{\"a}ivi Vieira and Hannu Tuominen and Hannaleena Kokkonen and {Al Macki}, Nabil and {Al Habsi}, Huda and Tuija L{\"o}pp{\"o}nen and Heikki Rantala and Vilja Pieti{\"a}inen and Zhang, {Shen Ying} and Marjo Renko and Timo Hautala and {Al Farsi}, Tariq and Johanna Uusimaa and Janna Saarela",

note = "Funding Information: This work was supported by the Academy of Finland, Finland (decision nos. RH: 317711 , 266498 , 273790 ), Ester and Uuno Kokki Foundation, Finland ; the Finnish Cultural Foundation, Finland ; The Foundation for Pediatric Research , Finland; the Alma and KA Snellman Foundation, Finland ; and Special State Grants for Health Research at the Oulu University Hospital , Finland (grant no. VTR K56772 ). Funding Information: This work was supported by the Academy of Finland, Finland (decision nos. RH: 317711, 266498, 273790), Ester and Uuno Kokki Foundation, Finland; the Finnish Cultural Foundation, Finland; The Foundation for Pediatric Research, Finland; the Alma and KA Snellman Foundation, Finland; and Special State Grants for Health Research at the Oulu University Hospital, Finland (grant no. VTR K56772). Publisher Copyright: {\textcopyright} 2021 The Authors",

year = "2021",

month = aug,

doi = "10.1016/j.jaci.2020.12.656",

language = "English",

volume = "148",

pages = "599--611",

journal = "Journal of Allergy and Clinical Immunology",

issn = "0091-6749",

publisher = "Mosby Inc.",

number = "2",

}

TY - JOUR

T1 - Loss of DIAPH1 causes SCBMS, combined immunodeficiency, and mitochondrial dysfunction

AU - Kaustio, Meri

AU - Nayebzadeh, Naemeh

AU - Hinttala, Reetta

AU - Tapiainen, Terhi

AU - Åström, Pirjo

AU - Mamia, Katariina

AU - Pernaa, Nora

AU - Lehtonen, Johanna

AU - Glumoff, Virpi

AU - Rahikkala, Elisa

AU - Honkila, Minna

AU - Olsén, Päivi

AU - Hassinen, Antti

AU - Polso, Minttu

AU - Al Sukaiti, Nashat

AU - Al Shekaili, Jalila

AU - Al Kindi, Mahmood

AU - Al Hashmi, Nadia

AU - Almusa, Henrikki

AU - Bulanova, Daria

AU - Haapaniemi, Emma

AU - Chen, Pu

AU - Suo-Palosaari, Maria

AU - Vieira, Päivi

AU - Tuominen, Hannu

AU - Kokkonen, Hannaleena

AU - Al Macki, Nabil

AU - Al Habsi, Huda

AU - Löppönen, Tuija

AU - Rantala, Heikki

AU - Pietiäinen, Vilja

AU - Zhang, Shen Ying

AU - Renko, Marjo

AU - Hautala, Timo

AU - Al Farsi, Tariq

AU - Uusimaa, Johanna

AU - Saarela, Janna

N1 - Funding Information: This work was supported by the Academy of Finland, Finland (decision nos. RH: 317711 , 266498 , 273790 ), Ester and Uuno Kokki Foundation, Finland ; the Finnish Cultural Foundation, Finland ; The Foundation for Pediatric Research , Finland; the Alma and KA Snellman Foundation, Finland ; and Special State Grants for Health Research at the Oulu University Hospital , Finland (grant no. VTR K56772 ). Funding Information: This work was supported by the Academy of Finland, Finland (decision nos. RH: 317711, 266498, 273790), Ester and Uuno Kokki Foundation, Finland; the Finnish Cultural Foundation, Finland; The Foundation for Pediatric Research, Finland; the Alma and KA Snellman Foundation, Finland; and Special State Grants for Health Research at the Oulu University Hospital, Finland (grant no. VTR K56772). Publisher Copyright: © 2021 The Authors

PY - 2021/8

Y1 - 2021/8

N2 - Background: Homozygous loss of DIAPH1 results in seizures, cortical blindness, and microcephaly syndrome (SCBMS). We studied 5 Finnish and 2 Omani patients with loss of DIAPH1 presenting with SCBMS, mitochondrial dysfunction, and immunodeficiency. Objective: We sought to further characterize phenotypes and disease mechanisms associated with loss of DIAPH1. Methods: Exome sequencing, genotyping and haplotype analysis, B- and T-cell phenotyping, in vitro lymphocyte stimulation assays, analyses of mitochondrial function, immunofluorescence staining for cytoskeletal proteins and mitochondria, and CRISPR-Cas9 DIAPH1 knockout in heathy donor PBMCs were used. Results: Genetic analyses found all Finnish patients homozygous for a rare DIAPH1 splice-variant (NM_005219:c.684+1G>A) enriched in the Finnish population, and Omani patients homozygous for a previously described pathogenic DIAPH1 frameshift-variant (NM_005219:c.2769delT;p.F923fs). In addition to microcephaly, epilepsy, and cortical blindness characteristic to SCBMS, the patients presented with infection susceptibility due to defective lymphocyte maturation and 3 patients developed B-cell lymphoma. Patients’ immunophenotype was characterized by poor lymphocyte activation and proliferation, defective B-cell maturation, and lack of naive T cells. CRISPR-Cas9 knockout of DIAPH1 in PBMCs from healthy donors replicated the T-cell activation defect. Patient-derived peripheral blood T cells exhibited impaired adhesion and inefficient microtubule-organizing center repositioning to the immunologic synapse. The clinical symptoms and laboratory tests also suggested mitochondrial dysfunction. Experiments with immortalized, patient-derived fibroblasts indicated that DIAPH1 affects the amount of complex IV of the mitochondrial respiratory chain. Conclusions: Our data demonstrate that individuals with SCBMS can have combined immune deficiency and implicate defective cytoskeletal organization and mitochondrial dysfunction in SCBMS pathogenesis.

AB - Background: Homozygous loss of DIAPH1 results in seizures, cortical blindness, and microcephaly syndrome (SCBMS). We studied 5 Finnish and 2 Omani patients with loss of DIAPH1 presenting with SCBMS, mitochondrial dysfunction, and immunodeficiency. Objective: We sought to further characterize phenotypes and disease mechanisms associated with loss of DIAPH1. Methods: Exome sequencing, genotyping and haplotype analysis, B- and T-cell phenotyping, in vitro lymphocyte stimulation assays, analyses of mitochondrial function, immunofluorescence staining for cytoskeletal proteins and mitochondria, and CRISPR-Cas9 DIAPH1 knockout in heathy donor PBMCs were used. Results: Genetic analyses found all Finnish patients homozygous for a rare DIAPH1 splice-variant (NM_005219:c.684+1G>A) enriched in the Finnish population, and Omani patients homozygous for a previously described pathogenic DIAPH1 frameshift-variant (NM_005219:c.2769delT;p.F923fs). In addition to microcephaly, epilepsy, and cortical blindness characteristic to SCBMS, the patients presented with infection susceptibility due to defective lymphocyte maturation and 3 patients developed B-cell lymphoma. Patients’ immunophenotype was characterized by poor lymphocyte activation and proliferation, defective B-cell maturation, and lack of naive T cells. CRISPR-Cas9 knockout of DIAPH1 in PBMCs from healthy donors replicated the T-cell activation defect. Patient-derived peripheral blood T cells exhibited impaired adhesion and inefficient microtubule-organizing center repositioning to the immunologic synapse. The clinical symptoms and laboratory tests also suggested mitochondrial dysfunction. Experiments with immortalized, patient-derived fibroblasts indicated that DIAPH1 affects the amount of complex IV of the mitochondrial respiratory chain. Conclusions: Our data demonstrate that individuals with SCBMS can have combined immune deficiency and implicate defective cytoskeletal organization and mitochondrial dysfunction in SCBMS pathogenesis.

KW - DIAPH1

KW - SCBMS

KW - T cells

KW - immunodeficiency

KW - microcephaly

KW - mitochondrial dysfunction

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UR - http://www.scopus.com/inward/citedby.url?scp=85104134872&partnerID=8YFLogxK

U2 - 10.1016/j.jaci.2020.12.656

DO - 10.1016/j.jaci.2020.12.656

M3 - Article

C2 - 33662367

AN - SCOPUS:85104134872

SN - 0091-6749

VL - 148

SP - 599

EP - 611

JO - Journal of Allergy and Clinical Immunology

JF - Journal of Allergy and Clinical Immunology

IS - 2

ER -

Loss of DIAPH1 causes SCBMS, combined immunodeficiency, and mitochondrial dysfunction

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