Clinical and genetic characterization of a progressive RBL2-associated neurodevelopmental disorder

SYNAPS Study Group

doi:10.1093/brain/awae363

Clinical and genetic characterization of a progressive RBL2-associated neurodevelopmental disorder

SYNAPS Study Group

Department of Biological & Biomedical Sciences, Medical College, Pakistan

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

1 Citation (Scopus)

Abstract

Retinoblastoma (RB) proteins are highly conserved transcriptional regulators that play important roles during development by regulating cell-cycle gene expression. RBL2 dysfunction has been linked to a severe neurodevelopmental disorder. However, to date, clinical features have been described in only six individuals carrying five biallelic predicted loss-of-function (pLOF) variants. To define the phenotypic effects of RBL2 mutations in detail, we identified and clinically characterized a cohort of 35 patients from 20 families carrying pLOF variants in RBL2, including 15 new variants that substantially broaden the molecular spectrum. The clinical presentation of affected individuals is characterized by a range of neurological and developmental abnormalities. Global developmental delay and intellectual disability were observed uniformly, ranging from moderate to profound and involving lack of acquisition of key motor and speech milestones in most patients. Disrupted sleep was also evident in some patients. Frequent features included postnatal microcephaly, infantile hypotonia, aggressive behaviour, stereotypic movements, seizures and non-specific dysmorphic features. Neuroimaging features included cerebral atrophy, white matter volume loss, corpus callosum hypoplasia and cerebellar atrophy. In parallel, we used the fruit fly, Drosophila melanogaster, to investigate how disruption of the conserved RBL2 orthologue Rbf impacts nervous system function and development. We found that Drosophila Rbf LOF mutants recapitulate several features of patients harbouring RBL2 variants, including developmental delay, alterations in head and brain morphology, locomotor defects and perturbed sleep. Surprisingly, in addition to its known role in controlling tissue growth during development, we found that continued Rbf expression is also required in fully differentiated post-mitotic neurons for normal locomotion in Drosophila, and that adult-stage neuronal re-expression of Rbf is sufficient to rescue Rbf mutant locomotor defects. Taken together, our study provides a clinical and experimental basis to understand genotype–phenotype correlations in an RBL2-linked neurodevelopmental disorder and suggests that restoring RBL2 expression through gene therapy approaches might ameliorate some symptoms caused by RBL2 pLOF.

Original language	English (US)
Pages (from-to)	1194-1211
Number of pages	18
Journal	Brain
Volume	148
Issue number	4
DOIs	https://doi.org/10.1093/brain/awae363
Publication status	Published - 1 Apr 2025

Keywords

Drosophila
RBL2
Rbf
cell cycle
neurodevelopmental disorder

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10.1093/brain/awae363

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@article{29a31951350d46369d36d021386334c1,

title = "Clinical and genetic characterization of a progressive RBL2-associated neurodevelopmental disorder",

abstract = "Retinoblastoma (RB) proteins are highly conserved transcriptional regulators that play important roles during development by regulating cell-cycle gene expression. RBL2 dysfunction has been linked to a severe neurodevelopmental disorder. However, to date, clinical features have been described in only six individuals carrying five biallelic predicted loss-of-function (pLOF) variants. To define the phenotypic effects of RBL2 mutations in detail, we identified and clinically characterized a cohort of 35 patients from 20 families carrying pLOF variants in RBL2, including 15 new variants that substantially broaden the molecular spectrum. The clinical presentation of affected individuals is characterized by a range of neurological and developmental abnormalities. Global developmental delay and intellectual disability were observed uniformly, ranging from moderate to profound and involving lack of acquisition of key motor and speech milestones in most patients. Disrupted sleep was also evident in some patients. Frequent features included postnatal microcephaly, infantile hypotonia, aggressive behaviour, stereotypic movements, seizures and non-specific dysmorphic features. Neuroimaging features included cerebral atrophy, white matter volume loss, corpus callosum hypoplasia and cerebellar atrophy. In parallel, we used the fruit fly, Drosophila melanogaster, to investigate how disruption of the conserved RBL2 orthologue Rbf impacts nervous system function and development. We found that Drosophila Rbf LOF mutants recapitulate several features of patients harbouring RBL2 variants, including developmental delay, alterations in head and brain morphology, locomotor defects and perturbed sleep. Surprisingly, in addition to its known role in controlling tissue growth during development, we found that continued Rbf expression is also required in fully differentiated post-mitotic neurons for normal locomotion in Drosophila, and that adult-stage neuronal re-expression of Rbf is sufficient to rescue Rbf mutant locomotor defects. Taken together, our study provides a clinical and experimental basis to understand genotype–phenotype correlations in an RBL2-linked neurodevelopmental disorder and suggests that restoring RBL2 expression through gene therapy approaches might ameliorate some symptoms caused by RBL2 pLOF.",

keywords = "Drosophila, RBL2, Rbf, cell cycle, neurodevelopmental disorder",

author = "\{SYNAPS Study Group\} and Aughey, \{Gabriel N.\} and Elisa Cali and Reza Maroofian and Zaki, \{Maha S.\} and Pagnamenta, \{Alistair T.\} and Zafar Ali and Uzma Abdulllah and Fatima Rahman and Lara Menzies and Anum Shafique and Mohnish Suri and Emmanuel Roze and Mohammed Aguennouz and Zouiri Ghizlane and Saadi, \{Saadia Maryam\} and Ambrin Fatima and Cheema, \{Huma Arshad\} and Anjum, \{Muhammad Nadeem\} and Godelieve Morel and Stephanie Robin and Robert McFarland and Umut Altunoglu and Verena Kraus and Moneef Shoukier and David Murphy and Kristina Flemming and Hilde Yttervik and Hajar Rhouda and Gaetan Lesca and Nicolas Chatron and Massimiliano Rossi and Murtaza, \{Bibi Nazia\} and Rehman, \{Mujaddad Ur\} and Jenny Lord and Edoardo Giacopuzzi and Azam Hayat and Muhammad Siraj and Consortium, \{Genomics England\} and Badv, \{Reza Shervin\} and Seo, \{Go Hun\} and Christian Beetz and H{\"u}lya Kayserili and Yamna Krioulie and Chung, \{Wendy K.\} and Sadaf Naz and Shazia Maqbool and Chandler, \{Kate E.\} and Kershaw, \{Christopher J.\} and Thomas Wright and Baig, \{Shahid Mahmood\}",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2024. Published by Oxford University Press on behalf of the Guarantors of Brain.",

year = "2025",

month = apr,

day = "1",

doi = "10.1093/brain/awae363",

language = "English (US)",

volume = "148",

pages = "1194--1211",

journal = "Brain",

issn = "0006-8950",

publisher = "Oxford University Press",

number = "4",

}

TY - JOUR

T1 - Clinical and genetic characterization of a progressive RBL2-associated neurodevelopmental disorder

AU - SYNAPS Study Group

AU - Aughey, Gabriel N.

AU - Cali, Elisa

AU - Maroofian, Reza

AU - Zaki, Maha S.

AU - Pagnamenta, Alistair T.

AU - Ali, Zafar

AU - Abdulllah, Uzma

AU - Rahman, Fatima

AU - Menzies, Lara

AU - Shafique, Anum

AU - Suri, Mohnish

AU - Roze, Emmanuel

AU - Aguennouz, Mohammed

AU - Ghizlane, Zouiri

AU - Saadi, Saadia Maryam

AU - Fatima, Ambrin

AU - Cheema, Huma Arshad

AU - Anjum, Muhammad Nadeem

AU - Morel, Godelieve

AU - Robin, Stephanie

AU - McFarland, Robert

AU - Altunoglu, Umut

AU - Kraus, Verena

AU - Shoukier, Moneef

AU - Murphy, David

AU - Flemming, Kristina

AU - Yttervik, Hilde

AU - Rhouda, Hajar

AU - Lesca, Gaetan

AU - Chatron, Nicolas

AU - Rossi, Massimiliano

AU - Murtaza, Bibi Nazia

AU - Rehman, Mujaddad Ur

AU - Lord, Jenny

AU - Giacopuzzi, Edoardo

AU - Hayat, Azam

AU - Siraj, Muhammad

AU - Consortium, Genomics England

AU - Badv, Reza Shervin

AU - Seo, Go Hun

AU - Beetz, Christian

AU - Kayserili, Hülya

AU - Krioulie, Yamna

AU - Chung, Wendy K.

AU - Naz, Sadaf

AU - Maqbool, Shazia

AU - Chandler, Kate E.

AU - Kershaw, Christopher J.

AU - Wright, Thomas

AU - Baig, Shahid Mahmood

PY - 2025/4/1

Y1 - 2025/4/1

N2 - Retinoblastoma (RB) proteins are highly conserved transcriptional regulators that play important roles during development by regulating cell-cycle gene expression. RBL2 dysfunction has been linked to a severe neurodevelopmental disorder. However, to date, clinical features have been described in only six individuals carrying five biallelic predicted loss-of-function (pLOF) variants. To define the phenotypic effects of RBL2 mutations in detail, we identified and clinically characterized a cohort of 35 patients from 20 families carrying pLOF variants in RBL2, including 15 new variants that substantially broaden the molecular spectrum. The clinical presentation of affected individuals is characterized by a range of neurological and developmental abnormalities. Global developmental delay and intellectual disability were observed uniformly, ranging from moderate to profound and involving lack of acquisition of key motor and speech milestones in most patients. Disrupted sleep was also evident in some patients. Frequent features included postnatal microcephaly, infantile hypotonia, aggressive behaviour, stereotypic movements, seizures and non-specific dysmorphic features. Neuroimaging features included cerebral atrophy, white matter volume loss, corpus callosum hypoplasia and cerebellar atrophy. In parallel, we used the fruit fly, Drosophila melanogaster, to investigate how disruption of the conserved RBL2 orthologue Rbf impacts nervous system function and development. We found that Drosophila Rbf LOF mutants recapitulate several features of patients harbouring RBL2 variants, including developmental delay, alterations in head and brain morphology, locomotor defects and perturbed sleep. Surprisingly, in addition to its known role in controlling tissue growth during development, we found that continued Rbf expression is also required in fully differentiated post-mitotic neurons for normal locomotion in Drosophila, and that adult-stage neuronal re-expression of Rbf is sufficient to rescue Rbf mutant locomotor defects. Taken together, our study provides a clinical and experimental basis to understand genotype–phenotype correlations in an RBL2-linked neurodevelopmental disorder and suggests that restoring RBL2 expression through gene therapy approaches might ameliorate some symptoms caused by RBL2 pLOF.

AB - Retinoblastoma (RB) proteins are highly conserved transcriptional regulators that play important roles during development by regulating cell-cycle gene expression. RBL2 dysfunction has been linked to a severe neurodevelopmental disorder. However, to date, clinical features have been described in only six individuals carrying five biallelic predicted loss-of-function (pLOF) variants. To define the phenotypic effects of RBL2 mutations in detail, we identified and clinically characterized a cohort of 35 patients from 20 families carrying pLOF variants in RBL2, including 15 new variants that substantially broaden the molecular spectrum. The clinical presentation of affected individuals is characterized by a range of neurological and developmental abnormalities. Global developmental delay and intellectual disability were observed uniformly, ranging from moderate to profound and involving lack of acquisition of key motor and speech milestones in most patients. Disrupted sleep was also evident in some patients. Frequent features included postnatal microcephaly, infantile hypotonia, aggressive behaviour, stereotypic movements, seizures and non-specific dysmorphic features. Neuroimaging features included cerebral atrophy, white matter volume loss, corpus callosum hypoplasia and cerebellar atrophy. In parallel, we used the fruit fly, Drosophila melanogaster, to investigate how disruption of the conserved RBL2 orthologue Rbf impacts nervous system function and development. We found that Drosophila Rbf LOF mutants recapitulate several features of patients harbouring RBL2 variants, including developmental delay, alterations in head and brain morphology, locomotor defects and perturbed sleep. Surprisingly, in addition to its known role in controlling tissue growth during development, we found that continued Rbf expression is also required in fully differentiated post-mitotic neurons for normal locomotion in Drosophila, and that adult-stage neuronal re-expression of Rbf is sufficient to rescue Rbf mutant locomotor defects. Taken together, our study provides a clinical and experimental basis to understand genotype–phenotype correlations in an RBL2-linked neurodevelopmental disorder and suggests that restoring RBL2 expression through gene therapy approaches might ameliorate some symptoms caused by RBL2 pLOF.

KW - Drosophila

KW - RBL2

KW - Rbf

KW - cell cycle

KW - neurodevelopmental disorder

UR - https://www.scopus.com/pages/publications/105002962168

U2 - 10.1093/brain/awae363

DO - 10.1093/brain/awae363

M3 - Article

C2 - 39692517

AN - SCOPUS:105002962168

SN - 0006-8950

VL - 148

SP - 1194

EP - 1211

JO - Brain

JF - Brain

IS - 4

ER -

Clinical and genetic characterization of a progressive RBL2-associated neurodevelopmental disorder

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Keywords

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