Bi-allelic variants in NAE1 cause intellectual disability, ischiopubic hypoplasia, stress-mediated lymphopenia and neurodegeneration

Irena J.J. Muffels; Imre F. Schene; Holger Rehmann; Maarten P.G. Massink; Maria M. van der Wal; Corinna Bauder; Martha Labeur; Natalia G. Armando; Maarten H. Lequin; Michiel L. Houben; Jaques C. Giltay; Saskia Haitjema; Albert Huisman; Fleur Vansenne; Judith Bluvstein; John Pappas; Lala V. Shailee; Yuri A. Zarate; Michal Mokry; Gijs W. van Haaften; Edward E.S. Nieuwenhuis; Damian Refojo; Femke van Wijk; Sabine A. Fuchs; Peter M. van Hasselt

doi:10.1016/j.ajhg.2022.12.003

Bi-allelic variants in NAE1 cause intellectual disability, ischiopubic hypoplasia, stress-mediated lymphopenia and neurodegeneration

Irena J.J. Muffels
, Imre F. Schene
, Holger Rehmann
, Maarten P.G. Massink
, Maria M. van der Wal
, Corinna Bauder
, Martha Labeur
, Natalia G. Armando
, Maarten H. Lequin
, Michiel L. Houben
, Jaques C. Giltay
, Saskia Haitjema
, Albert Huisman
, Fleur Vansenne
, Judith Bluvstein
, John Pappas
, Lala V. Shailee
, Yuri A. Zarate
, Michal Mokry
, Gijs W. van Haaften

Edward E.S. Nieuwenhuis, Damian Refojo, Femke van Wijk, Sabine A. Fuchs, Peter M. van Hasselt

Pediatrics

Producción científica: Article › revisión exhaustiva

5 Citas (Scopus)

Resumen

Neddylation has been implicated in various cellular pathways and in the pathophysiology of numerous diseases. We identified four individuals with bi-allelic variants in NAE1, which encodes the neddylation E1 enzyme. Pathogenicity was supported by decreased NAE1 abundance and overlapping clinical and cellular phenotypes. To delineate how cellular consequences of NAE1 deficiency would lead to the clinical phenotype, we focused primarily on the rarest phenotypic features, based on the assumption that these would best reflect the pathophysiology at stake. Two of the rarest features, neuronal loss and lymphopenia worsening during infections, suggest that NAE1 is required during cellular stress caused by infections to protect against cell death. In support, we found that stressing the proteasome system with MG132—requiring upregulation of neddylation to restore proteasomal function and proteasomal stress—led to increased cell death in fibroblasts of individuals with NAE1 genetic variants. Additionally, we found decreased lymphocyte counts after CD3/CD28 stimulation and decreased NF-κB translocation in individuals with NAE1 variants. The rarest phenotypic feature—delayed closure of the ischiopubic rami—correlated with significant downregulation of RUN2X and SOX9 expression in transcriptomic data of fibroblasts. Both genes are involved in the pathophysiology of ischiopubic hypoplasia. Thus, we show that NAE1 plays a major role in (skeletal) development and cellular homeostasis during stress. Our approach suggests that a focus on rare phenotypic features is able to provide significant pathophysiological insights in diseases caused by mutations in genes with pleiotropic effects.

Idioma original	English
Páginas (desde-hasta)	146-160
Número de páginas	15
Publicación	American Journal of Human Genetics
Volumen	110
N.º	1
DOI	https://doi.org/10.1016/j.ajhg.2022.12.003
Estado	Published - ene 5 2023

Nota bibliográfica

Publisher Copyright:
© 2022 American Society of Human Genetics

Financiación

This work was supported by the Max Planck Society (D.R.), the VolkswagenStiftung (D.R.), the Agencia Nacional de Promoción Científica y Tecnológica , Argentina (D.R.) and the Fondo para la convergencia estructural del mercosur -FOCEM ( COF 03/11 ) (D.R.). We would like to thank the parents of individual 1 for drafting Figure 6A. This work was supported by the Max Planck Society (D.R.), the VolkswagenStiftung (D.R.), the Agencia Nacional de Promoción Científica y Tecnológica, Argentina (D.R.) and the Fondo para la convergencia estructural del mercosur-FOCEM (COF 03/11) (D.R.). We would like to thank the parents of individual 1 for drafting Figure 6A. Concept: P.M.v.H. and I.J.J.M. Designing experiments: I.J.J.M. I.F.S. M.M.v.d.W. C.B. M.L. D.R. F.v.W. S.A.F. E.E.S.N. and P.M.v.H. Conducting experiments: I.J.J.M. I.F.S. M.M.v.d.W. C.B. M.L. N.G.A. Acquiring (medical) data of study participants and cells: I.J.J.M. Y.A.Z. L.V.S. J.B. J.P. M.L.H. J.C.G. S.H. A.H. F.V. M.P.G.M. M.L. P.M.v.H. Analyzing data: I.J.J.M. I.F.S. M.P.G.M. M.M.v.d.W. Genetic testing and interpretation of variants: M.P.G.M. G.v.H. Molecular predictions: M.P.G.M. H.R. Writing the manuscript: I.J.J.M. and P.M.v.H. Supervision of experiments and writing process: P.M.v.H. S.A.F. F.v.W. E.E.S.N. D.R. S.A.F. D.R. and F.v.W. spent equal time and effort on supervision of the manuscript. The authors declare no competing interests.

Financiadores
FOCEM
Fritz-Haber-Institut der Max-Planck-Gesellschaft
Volkswagen Foundation
Agencia Nacional de Promoción Científica y Tecnológica

ASJC Scopus subject areas

Genetics
Genetics(clinical)

Acceder al documento

10.1016/j.ajhg.2022.12.003

Otros archivos y enlaces

Citar esto

Muffels, I. J. J., Schene, I. F., Rehmann, H., Massink, M. P. G., van der Wal, M. M., Bauder, C., Labeur, M., Armando, N. G., Lequin, M. H., Houben, M. L., Giltay, J. C., Haitjema, S., Huisman, A., Vansenne, F., Bluvstein, J., Pappas, J., Shailee, L. V., Zarate, Y. A., Mokry, M., ... van Hasselt, P. M. (2023). Bi-allelic variants in NAE1 cause intellectual disability, ischiopubic hypoplasia, stress-mediated lymphopenia and neurodegeneration. American Journal of Human Genetics, 110(1), 146-160. https://doi.org/10.1016/j.ajhg.2022.12.003

@article{be0343dfae0447f5852625ed215ce3c9,

title = "Bi-allelic variants in NAE1 cause intellectual disability, ischiopubic hypoplasia, stress-mediated lymphopenia and neurodegeneration",

abstract = "Neddylation has been implicated in various cellular pathways and in the pathophysiology of numerous diseases. We identified four individuals with bi-allelic variants in NAE1, which encodes the neddylation E1 enzyme. Pathogenicity was supported by decreased NAE1 abundance and overlapping clinical and cellular phenotypes. To delineate how cellular consequences of NAE1 deficiency would lead to the clinical phenotype, we focused primarily on the rarest phenotypic features, based on the assumption that these would best reflect the pathophysiology at stake. Two of the rarest features, neuronal loss and lymphopenia worsening during infections, suggest that NAE1 is required during cellular stress caused by infections to protect against cell death. In support, we found that stressing the proteasome system with MG132—requiring upregulation of neddylation to restore proteasomal function and proteasomal stress—led to increased cell death in fibroblasts of individuals with NAE1 genetic variants. Additionally, we found decreased lymphocyte counts after CD3/CD28 stimulation and decreased NF-κB translocation in individuals with NAE1 variants. The rarest phenotypic feature—delayed closure of the ischiopubic rami—correlated with significant downregulation of RUN2X and SOX9 expression in transcriptomic data of fibroblasts. Both genes are involved in the pathophysiology of ischiopubic hypoplasia. Thus, we show that NAE1 plays a major role in (skeletal) development and cellular homeostasis during stress. Our approach suggests that a focus on rare phenotypic features is able to provide significant pathophysiological insights in diseases caused by mutations in genes with pleiotropic effects.",

keywords = "NAE1, lymphopenia, neddylation, neurodegeneration, ocurrence ratio, phenotypic specificity, post-translational protein modification, proteasome, ubiquitination",

author = "Muffels, \{Irena J.J.\} and Schene, \{Imre F.\} and Holger Rehmann and Massink, \{Maarten P.G.\} and \{van der Wal\}, \{Maria M.\} and Corinna Bauder and Martha Labeur and Armando, \{Natalia G.\} and Lequin, \{Maarten H.\} and Houben, \{Michiel L.\} and Giltay, \{Jaques C.\} and Saskia Haitjema and Albert Huisman and Fleur Vansenne and Judith Bluvstein and John Pappas and Shailee, \{Lala V.\} and Zarate, \{Yuri A.\} and Michal Mokry and \{van Haaften\}, \{Gijs W.\} and Nieuwenhuis, \{Edward E.S.\} and Damian Refojo and \{van Wijk\}, Femke and Fuchs, \{Sabine A.\} and \{van Hasselt\}, \{Peter M.\}",

note = "Publisher Copyright: {\textcopyright} 2022 American Society of Human Genetics",

year = "2023",

month = jan,

day = "5",

doi = "10.1016/j.ajhg.2022.12.003",

language = "English",

volume = "110",

pages = "146--160",

number = "1",

}

Muffels, IJJ, Schene, IF, Rehmann, H, Massink, MPG, van der Wal, MM, Bauder, C, Labeur, M, Armando, NG, Lequin, MH, Houben, ML, Giltay, JC, Haitjema, S, Huisman, A, Vansenne, F, Bluvstein, J, Pappas, J, Shailee, LV, Zarate, YA, Mokry, M, van Haaften, GW, Nieuwenhuis, EES, Refojo, D, van Wijk, F, Fuchs, SA & van Hasselt, PM 2023, 'Bi-allelic variants in NAE1 cause intellectual disability, ischiopubic hypoplasia, stress-mediated lymphopenia and neurodegeneration', American Journal of Human Genetics, vol. 110, n.º 1, pp. 146-160. https://doi.org/10.1016/j.ajhg.2022.12.003

TY - JOUR

T1 - Bi-allelic variants in NAE1 cause intellectual disability, ischiopubic hypoplasia, stress-mediated lymphopenia and neurodegeneration

AU - Muffels, Irena J.J.

AU - Schene, Imre F.

AU - Rehmann, Holger

AU - Massink, Maarten P.G.

AU - van der Wal, Maria M.

AU - Bauder, Corinna

AU - Labeur, Martha

AU - Armando, Natalia G.

AU - Lequin, Maarten H.

AU - Houben, Michiel L.

AU - Giltay, Jaques C.

AU - Haitjema, Saskia

AU - Huisman, Albert

AU - Vansenne, Fleur

AU - Bluvstein, Judith

AU - Pappas, John

AU - Shailee, Lala V.

AU - Zarate, Yuri A.

AU - Mokry, Michal

AU - van Haaften, Gijs W.

AU - Nieuwenhuis, Edward E.S.

AU - Refojo, Damian

AU - van Wijk, Femke

AU - Fuchs, Sabine A.

AU - van Hasselt, Peter M.

PY - 2023/1/5

Y1 - 2023/1/5

N2 - Neddylation has been implicated in various cellular pathways and in the pathophysiology of numerous diseases. We identified four individuals with bi-allelic variants in NAE1, which encodes the neddylation E1 enzyme. Pathogenicity was supported by decreased NAE1 abundance and overlapping clinical and cellular phenotypes. To delineate how cellular consequences of NAE1 deficiency would lead to the clinical phenotype, we focused primarily on the rarest phenotypic features, based on the assumption that these would best reflect the pathophysiology at stake. Two of the rarest features, neuronal loss and lymphopenia worsening during infections, suggest that NAE1 is required during cellular stress caused by infections to protect against cell death. In support, we found that stressing the proteasome system with MG132—requiring upregulation of neddylation to restore proteasomal function and proteasomal stress—led to increased cell death in fibroblasts of individuals with NAE1 genetic variants. Additionally, we found decreased lymphocyte counts after CD3/CD28 stimulation and decreased NF-κB translocation in individuals with NAE1 variants. The rarest phenotypic feature—delayed closure of the ischiopubic rami—correlated with significant downregulation of RUN2X and SOX9 expression in transcriptomic data of fibroblasts. Both genes are involved in the pathophysiology of ischiopubic hypoplasia. Thus, we show that NAE1 plays a major role in (skeletal) development and cellular homeostasis during stress. Our approach suggests that a focus on rare phenotypic features is able to provide significant pathophysiological insights in diseases caused by mutations in genes with pleiotropic effects.

AB - Neddylation has been implicated in various cellular pathways and in the pathophysiology of numerous diseases. We identified four individuals with bi-allelic variants in NAE1, which encodes the neddylation E1 enzyme. Pathogenicity was supported by decreased NAE1 abundance and overlapping clinical and cellular phenotypes. To delineate how cellular consequences of NAE1 deficiency would lead to the clinical phenotype, we focused primarily on the rarest phenotypic features, based on the assumption that these would best reflect the pathophysiology at stake. Two of the rarest features, neuronal loss and lymphopenia worsening during infections, suggest that NAE1 is required during cellular stress caused by infections to protect against cell death. In support, we found that stressing the proteasome system with MG132—requiring upregulation of neddylation to restore proteasomal function and proteasomal stress—led to increased cell death in fibroblasts of individuals with NAE1 genetic variants. Additionally, we found decreased lymphocyte counts after CD3/CD28 stimulation and decreased NF-κB translocation in individuals with NAE1 variants. The rarest phenotypic feature—delayed closure of the ischiopubic rami—correlated with significant downregulation of RUN2X and SOX9 expression in transcriptomic data of fibroblasts. Both genes are involved in the pathophysiology of ischiopubic hypoplasia. Thus, we show that NAE1 plays a major role in (skeletal) development and cellular homeostasis during stress. Our approach suggests that a focus on rare phenotypic features is able to provide significant pathophysiological insights in diseases caused by mutations in genes with pleiotropic effects.

KW - NAE1

KW - lymphopenia

KW - neddylation

KW - neurodegeneration

KW - ocurrence ratio

KW - phenotypic specificity

KW - post-translational protein modification

KW - proteasome

KW - ubiquitination

UR - https://www.scopus.com/pages/publications/85145272959

UR - https://www.scopus.com/pages/publications/85145272959#tab=citedBy

U2 - 10.1016/j.ajhg.2022.12.003

DO - 10.1016/j.ajhg.2022.12.003

M3 - Article

C2 - 36608681

AN - SCOPUS:85145272959

SN - 0002-9297

VL - 110

SP - 146

EP - 160

JO - American Journal of Human Genetics

JF - American Journal of Human Genetics

IS - 1

ER -

Bi-allelic variants in NAE1 cause intellectual disability, ischiopubic hypoplasia, stress-mediated lymphopenia and neurodegeneration

Resumen

Nota bibliográfica

Financiación

ASJC Scopus subject areas

Acceder al documento

Otros archivos y enlaces

Huella

Citar esto