Recessive PRDM13 mutations cause fatal perinatal brainstem dysfunction with cerebellar hypoplasia and disrupt Purkinje cell differentiation

Marion Coolen; Nami Altin; Karthyayani Rajamani; Eva Pereira; Karine Siquier-Pernet; Emilia Puig Lombardi; Nadjeda Moreno; Giulia Barcia; Marianne Yvert; Annie Laquerrière; Aurore Pouliet; Patrick Nitschké; Nathalie Boddaert; Antonio Rausell; Féréchté Razavi; Alexandra Afenjar; Thierry Billette de Villemeur; Almundher Al-Maawali; Khalid Al-Thihli; Julia Baptista; Ana Beleza-Meireles; Catherine Garel; Marine Legendre; Antoinette Gelot; Lydie Burglen; Sébastien Moutton; Vincent Cantagrel

doi:10.1016/j.ajhg.2022.03.010

Recessive PRDM13 mutations cause fatal perinatal brainstem dysfunction with cerebellar hypoplasia and disrupt Purkinje cell differentiation

Marion Coolen, Nami Altin, Karthyayani Rajamani, Eva Pereira, Karine Siquier-Pernet, Emilia Puig Lombardi, Nadjeda Moreno, Giulia Barcia, Marianne Yvert, Annie Laquerrière, Aurore Pouliet, Patrick Nitschké, Nathalie Boddaert, Antonio Rausell, Féréchté Razavi, Alexandra Afenjar, Thierry Billette de Villemeur, Almundher Al-Maawali, Khalid Al-Thihli, Julia BaptistaAna Beleza-Meireles, Catherine Garel, Marine Legendre, Antoinette Gelot, Lydie Burglen, Sébastien Moutton, Vincent Cantagrel

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

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Abstract

Pontocerebellar hypoplasias (PCHs) are congenital disorders characterized by hypoplasia or early atrophy of the cerebellum and brainstem, leading to a very limited motor and cognitive development. Although over 20 genes have been shown to be mutated in PCHs, a large proportion of affected individuals remains undiagnosed. We describe four families with children presenting with severe neonatal brainstem dysfunction and pronounced deficits in cognitive and motor development associated with four different bi-allelic mutations in PRDM13, including homozygous truncating variants in the most severely affected individuals. Brain MRI and fetopathological examination revealed a PCH-like phenotype, associated with major hypoplasia of inferior olive nuclei and dysplasia of the dentate nucleus. Notably, histopathological examinations highlighted a sparse and disorganized Purkinje cell layer in the cerebellum. PRDM13 encodes a transcriptional repressor known to be critical for neuronal subtypes specification in the mouse retina and spinal cord but had not been implicated, so far, in hindbrain development. snRNA-seq data mining and in situ hybridization in humans show that PRDM13 is expressed at early stages in the progenitors of the cerebellar ventricular zone, which gives rise to cerebellar GABAergic neurons, including Purkinje cells. We also show that loss of function of prdm13 in zebrafish leads to a reduction in Purkinje cells numbers and a complete absence of the inferior olive nuclei. Altogether our data identified bi-allelic mutations in PRDM13 as causing a olivopontocerebellar hypoplasia syndrome and suggest that early deregulations of the transcriptional control of neuronal fate specification could contribute to a significant number of cases.

Original language	English
Pages (from-to)	909-927
Number of pages	19
Journal	American Journal of Human Genetics
Volume	109
Issue number	5
DOIs	https://doi.org/10.1016/j.ajhg.2022.03.010 https://doi.org/10.1016/j.ajhg.2022.03.010
Publication status	Published - May 1 2022

Keywords

Animals
Brain Diseases/pathology
Brain Stem
Cerebellum/abnormalities
Developmental Disabilities
Histone-Lysine N-Methyltransferase/genetics
Humans
Mice
Mutation/genetics
Nervous System Malformations
Neurogenesis/genetics
Purkinje Cells/metabolism
Transcription Factors/genetics
Zebrafish/metabolism

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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Coolen, M., Altin, N., Rajamani, K., Pereira, E., Siquier-Pernet, K., Puig Lombardi, E., Moreno, N., Barcia, G., Yvert, M., Laquerrière, A., Pouliet, A., Nitschké, P., Boddaert, N., Rausell, A., Razavi, F., Afenjar, A., Billette de Villemeur, T., Al-Maawali, A., Al-Thihli, K., ... Cantagrel, V. (2022). Recessive PRDM13 mutations cause fatal perinatal brainstem dysfunction with cerebellar hypoplasia and disrupt Purkinje cell differentiation. American Journal of Human Genetics, 109(5), 909-927. https://doi.org/10.1016/j.ajhg.2022.03.010, https://doi.org/10.1016/j.ajhg.2022.03.010

Coolen, M, Altin, N, Rajamani, K, Pereira, E, Siquier-Pernet, K, Puig Lombardi, E, Moreno, N, Barcia, G, Yvert, M, Laquerrière, A, Pouliet, A, Nitschké, P, Boddaert, N, Rausell, A, Razavi, F, Afenjar, A, Billette de Villemeur, T, Al-Maawali, A , Al-Thihli, K, Baptista, J, Beleza-Meireles, A, Garel, C, Legendre, M, Gelot, A, Burglen, L, Moutton, S & Cantagrel, V 2022, 'Recessive PRDM13 mutations cause fatal perinatal brainstem dysfunction with cerebellar hypoplasia and disrupt Purkinje cell differentiation', American Journal of Human Genetics, vol. 109, no. 5, pp. 909-927. https://doi.org/10.1016/j.ajhg.2022.03.010, https://doi.org/10.1016/j.ajhg.2022.03.010

@article{3719ddd5c6734ab28d7b4b25b72ee673,

title = "Recessive PRDM13 mutations cause fatal perinatal brainstem dysfunction with cerebellar hypoplasia and disrupt Purkinje cell differentiation",

abstract = "Pontocerebellar hypoplasias (PCHs) are congenital disorders characterized by hypoplasia or early atrophy of the cerebellum and brainstem, leading to a very limited motor and cognitive development. Although over 20 genes have been shown to be mutated in PCHs, a large proportion of affected individuals remains undiagnosed. We describe four families with children presenting with severe neonatal brainstem dysfunction and pronounced deficits in cognitive and motor development associated with four different bi-allelic mutations in PRDM13, including homozygous truncating variants in the most severely affected individuals. Brain MRI and fetopathological examination revealed a PCH-like phenotype, associated with major hypoplasia of inferior olive nuclei and dysplasia of the dentate nucleus. Notably, histopathological examinations highlighted a sparse and disorganized Purkinje cell layer in the cerebellum. PRDM13 encodes a transcriptional repressor known to be critical for neuronal subtypes specification in the mouse retina and spinal cord but had not been implicated, so far, in hindbrain development. snRNA-seq data mining and in situ hybridization in humans show that PRDM13 is expressed at early stages in the progenitors of the cerebellar ventricular zone, which gives rise to cerebellar GABAergic neurons, including Purkinje cells. We also show that loss of function of prdm13 in zebrafish leads to a reduction in Purkinje cells numbers and a complete absence of the inferior olive nuclei. Altogether our data identified bi-allelic mutations in PRDM13 as causing a olivopontocerebellar hypoplasia syndrome and suggest that early deregulations of the transcriptional control of neuronal fate specification could contribute to a significant number of cases.",

keywords = "Animals, Brain Diseases/pathology, Brain Stem, Cerebellum/abnormalities, Developmental Disabilities, Histone-Lysine N-Methyltransferase/genetics, Humans, Mice, Mutation/genetics, Nervous System Malformations, Neurogenesis/genetics, Purkinje Cells/metabolism, Transcription Factors/genetics, Zebrafish/metabolism",

author = "Marion Coolen and Nami Altin and Karthyayani Rajamani and Eva Pereira and Karine Siquier-Pernet and {Puig Lombardi}, Emilia and Nadjeda Moreno and Giulia Barcia and Marianne Yvert and Annie Laquerri{\`e}re and Aurore Pouliet and Patrick Nitschk{\'e} and Nathalie Boddaert and Antonio Rausell and F{\'e}r{\'e}cht{\'e} Razavi and Alexandra Afenjar and {Billette de Villemeur}, Thierry and Almundher Al-Maawali and Khalid Al-Thihli and Julia Baptista and Ana Beleza-Meireles and Catherine Garel and Marine Legendre and Antoinette Gelot and Lydie Burglen and S{\'e}bastien Moutton and Vincent Cantagrel",

note = "Funding Information: The project is funded by the Agence Nationale de la Recherche ANR-16-CE12- 0005-01, the Fondation pour la Recherche M{\'e}dicale FRM-DEQ20160334938, and the patient association CSC “Conna{\^i}tre les syndromes C{\'e}r{\'e}belleux.” This work was also supported by state funding from the Agence Nationale de la Recherche under “Investissements d'avenir” program (ANR-10-IAHU-01), the Fondation Bettencourt Schueller, and the MSDAvenir Fund (DEVO-DECODE project). The human embryonic and fetal material was provided by the Joint MRC-Wellcome (MR/R006237/1) Human Developmental Biology Resource (https://www.hdbr.org). We would like to thank S. Amat, F. Pelluard, and I. Deryabin for providing clinical information and material; M. Hibi (Nagoya University) for providing the zebrafish ptf1a probe; B. Crespo for technical help; and L. Colleaux for guidance during the course of the project. The authors declare no competing interests. Funding Information: The project is funded by the Agence Nationale de la Recherche ANR-16-CE12- 0005-01 , the Fondation pour la Recherche M{\'e}dicale FRM-DEQ20160334938 , and the patient association CSC “ Conna{\^i}tre les syndromes C{\'e}r{\'e}belleux .” This work was also supported by state funding from the Agence Nationale de la Recherche under “Investissements d{\textquoteright}avenir” program ( ANR-10-IAHU-01 ), the Fondation Bettencourt Schueller , and the MSDAvenir Fund (DEVO-DECODE project). The human embryonic and fetal material was provided by the Joint MRC-Wellcome (MR/R006237/1) Human Developmental Biology Resource ( https://www.hdbr.org ). We would like to thank S. Amat, F. Pelluard, and I. Deryabin for providing clinical information and material; M. Hibi (Nagoya University) for providing the zebrafish ptf1a probe; B. Crespo for technical help; and L. Colleaux for guidance during the course of the project. Publisher Copyright: {\textcopyright} 2022 American Society of Human Genetics",

year = "2022",

month = may,

day = "1",

doi = "10.1016/j.ajhg.2022.03.010",

language = "English",

volume = "109",

pages = "909--927",

journal = "American Journal of Human Genetics",

issn = "0002-9297",

publisher = "Cell Press",

number = "5",

}

TY - JOUR

T1 - Recessive PRDM13 mutations cause fatal perinatal brainstem dysfunction with cerebellar hypoplasia and disrupt Purkinje cell differentiation

AU - Coolen, Marion

AU - Altin, Nami

AU - Rajamani, Karthyayani

AU - Pereira, Eva

AU - Siquier-Pernet, Karine

AU - Puig Lombardi, Emilia

AU - Moreno, Nadjeda

AU - Barcia, Giulia

AU - Yvert, Marianne

AU - Laquerrière, Annie

AU - Pouliet, Aurore

AU - Nitschké, Patrick

AU - Boddaert, Nathalie

AU - Rausell, Antonio

AU - Razavi, Féréchté

AU - Afenjar, Alexandra

AU - Billette de Villemeur, Thierry

AU - Al-Maawali, Almundher

AU - Al-Thihli, Khalid

AU - Baptista, Julia

AU - Beleza-Meireles, Ana

AU - Garel, Catherine

AU - Legendre, Marine

AU - Gelot, Antoinette

AU - Burglen, Lydie

AU - Moutton, Sébastien

AU - Cantagrel, Vincent

N1 - Funding Information: The project is funded by the Agence Nationale de la Recherche ANR-16-CE12- 0005-01, the Fondation pour la Recherche Médicale FRM-DEQ20160334938, and the patient association CSC “Connaître les syndromes Cérébelleux.” This work was also supported by state funding from the Agence Nationale de la Recherche under “Investissements d'avenir” program (ANR-10-IAHU-01), the Fondation Bettencourt Schueller, and the MSDAvenir Fund (DEVO-DECODE project). The human embryonic and fetal material was provided by the Joint MRC-Wellcome (MR/R006237/1) Human Developmental Biology Resource (https://www.hdbr.org). We would like to thank S. Amat, F. Pelluard, and I. Deryabin for providing clinical information and material; M. Hibi (Nagoya University) for providing the zebrafish ptf1a probe; B. Crespo for technical help; and L. Colleaux for guidance during the course of the project. The authors declare no competing interests. Funding Information: The project is funded by the Agence Nationale de la Recherche ANR-16-CE12- 0005-01 , the Fondation pour la Recherche Médicale FRM-DEQ20160334938 , and the patient association CSC “ Connaître les syndromes Cérébelleux .” This work was also supported by state funding from the Agence Nationale de la Recherche under “Investissements d’avenir” program ( ANR-10-IAHU-01 ), the Fondation Bettencourt Schueller , and the MSDAvenir Fund (DEVO-DECODE project). The human embryonic and fetal material was provided by the Joint MRC-Wellcome (MR/R006237/1) Human Developmental Biology Resource ( https://www.hdbr.org ). We would like to thank S. Amat, F. Pelluard, and I. Deryabin for providing clinical information and material; M. Hibi (Nagoya University) for providing the zebrafish ptf1a probe; B. Crespo for technical help; and L. Colleaux for guidance during the course of the project. Publisher Copyright: © 2022 American Society of Human Genetics

PY - 2022/5/1

Y1 - 2022/5/1

N2 - Pontocerebellar hypoplasias (PCHs) are congenital disorders characterized by hypoplasia or early atrophy of the cerebellum and brainstem, leading to a very limited motor and cognitive development. Although over 20 genes have been shown to be mutated in PCHs, a large proportion of affected individuals remains undiagnosed. We describe four families with children presenting with severe neonatal brainstem dysfunction and pronounced deficits in cognitive and motor development associated with four different bi-allelic mutations in PRDM13, including homozygous truncating variants in the most severely affected individuals. Brain MRI and fetopathological examination revealed a PCH-like phenotype, associated with major hypoplasia of inferior olive nuclei and dysplasia of the dentate nucleus. Notably, histopathological examinations highlighted a sparse and disorganized Purkinje cell layer in the cerebellum. PRDM13 encodes a transcriptional repressor known to be critical for neuronal subtypes specification in the mouse retina and spinal cord but had not been implicated, so far, in hindbrain development. snRNA-seq data mining and in situ hybridization in humans show that PRDM13 is expressed at early stages in the progenitors of the cerebellar ventricular zone, which gives rise to cerebellar GABAergic neurons, including Purkinje cells. We also show that loss of function of prdm13 in zebrafish leads to a reduction in Purkinje cells numbers and a complete absence of the inferior olive nuclei. Altogether our data identified bi-allelic mutations in PRDM13 as causing a olivopontocerebellar hypoplasia syndrome and suggest that early deregulations of the transcriptional control of neuronal fate specification could contribute to a significant number of cases.

AB - Pontocerebellar hypoplasias (PCHs) are congenital disorders characterized by hypoplasia or early atrophy of the cerebellum and brainstem, leading to a very limited motor and cognitive development. Although over 20 genes have been shown to be mutated in PCHs, a large proportion of affected individuals remains undiagnosed. We describe four families with children presenting with severe neonatal brainstem dysfunction and pronounced deficits in cognitive and motor development associated with four different bi-allelic mutations in PRDM13, including homozygous truncating variants in the most severely affected individuals. Brain MRI and fetopathological examination revealed a PCH-like phenotype, associated with major hypoplasia of inferior olive nuclei and dysplasia of the dentate nucleus. Notably, histopathological examinations highlighted a sparse and disorganized Purkinje cell layer in the cerebellum. PRDM13 encodes a transcriptional repressor known to be critical for neuronal subtypes specification in the mouse retina and spinal cord but had not been implicated, so far, in hindbrain development. snRNA-seq data mining and in situ hybridization in humans show that PRDM13 is expressed at early stages in the progenitors of the cerebellar ventricular zone, which gives rise to cerebellar GABAergic neurons, including Purkinje cells. We also show that loss of function of prdm13 in zebrafish leads to a reduction in Purkinje cells numbers and a complete absence of the inferior olive nuclei. Altogether our data identified bi-allelic mutations in PRDM13 as causing a olivopontocerebellar hypoplasia syndrome and suggest that early deregulations of the transcriptional control of neuronal fate specification could contribute to a significant number of cases.

KW - Animals

KW - Brain Diseases/pathology

KW - Brain Stem

KW - Cerebellum/abnormalities

KW - Developmental Disabilities

KW - Histone-Lysine N-Methyltransferase/genetics

KW - Humans

KW - Mice

KW - Mutation/genetics

KW - Nervous System Malformations

KW - Neurogenesis/genetics

KW - Purkinje Cells/metabolism

KW - Transcription Factors/genetics

KW - Zebrafish/metabolism

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UR - http://www.scopus.com/inward/citedby.url?scp=85129579312&partnerID=8YFLogxK

U2 - 10.1016/j.ajhg.2022.03.010

DO - 10.1016/j.ajhg.2022.03.010

M3 - Article

C2 - 35390279

AN - SCOPUS:85129579312

SN - 0002-9297

VL - 109

SP - 909

EP - 927

JO - American Journal of Human Genetics

JF - American Journal of Human Genetics

IS - 5

ER -

Recessive PRDM13 mutations cause fatal perinatal brainstem dysfunction with cerebellar hypoplasia and disrupt Purkinje cell differentiation

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