A Genotype/Phenotype Study of KDM5B-Associated Disorders Suggests a Pathogenic Effect of Dominantly Inherited Missense Variants

Maria Carla Borroto; Coralie Michaud; Chloé Hudon; Pankaj B. Agrawal; Katherine Agre; Carolyn D. Applegate; Alan H. Beggs; Hans Tómas Björnsson; Bert Callewaert; Mei Jan Chen; Cynthia Curry; Orrin Devinsky; Tracy Dudding-Byth; Kelly Fagan; Candice R. Finnila; Ralitza Gavrilova; Casie A. Genetti; Susan M. Hiatt; Friedhelm Hildebrandt; Monica H. Wojcik; Tjitske Kleefstra; Caroline M. Kolvenbach; Bruce R. Korf; Paul Kruszka; Hong Li; Jessica Litwin; Julien Marcadier; Konrad Platzer; Patrick R. Blackburn; Margot R.F. Reijnders; Heiko Reutter; Ina Schanze; Joseph T. Shieh; Cathy A. Stevens; Zaheer Valivullah; Marie José van den Boogaard; Eric W. Klee; Philippe M. Campeau

doi:10.3390/genes15081033

A Genotype/Phenotype Study of KDM5B-Associated Disorders Suggests a Pathogenic Effect of Dominantly Inherited Missense Variants

Maria Carla Borroto, Coralie Michaud, Chloé Hudon, Pankaj B. Agrawal, Katherine Agre, Carolyn D. Applegate, Alan H. Beggs, Hans Tómas Björnsson, Bert Callewaert, Mei Jan Chen, Cynthia Curry, Orrin Devinsky, Tracy Dudding-Byth, Kelly Fagan, Candice R. Finnila, Ralitza Gavrilova, Casie A. Genetti, Susan M. Hiatt, Friedhelm Hildebrandt, Monica H. WojcikTjitske Kleefstra, Caroline M. Kolvenbach, Bruce R. Korf, Paul Kruszka, Hong Li, Jessica Litwin, Julien Marcadier, Konrad Platzer, Patrick R. Blackburn, Margot R.F. Reijnders, Heiko Reutter, Ina Schanze, Joseph T. Shieh, Cathy A. Stevens, Zaheer Valivullah, Marie José van den Boogaard, Eric W. Klee, Philippe M. Campeau

University of Iceland

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

Abstract

Bi-allelic disruptive variants (nonsense, frameshift, and splicing variants) in KDM5B have been identified as causative for autosomal recessive intellectual developmental disorder type 65. In contrast, dominant variants, usually disruptive as well, have been more difficult to implicate in a specific phenotype, since some of them have been found in unaffected controls or relatives. Here, we describe individuals with likely pathogenic variants in KDM5B, including eight individuals with dominant missense variants. This study is a retrospective case series of 21 individuals with variants in KDM5B. We performed deep phenotyping and collected the clinical information and molecular data of these individuals’ family members. We compared the phenotypes according to variant type and to those previously described in the literature. The most common features were developmental delay, impaired intellectual development, behavioral problems, autistic behaviors, sleep disorders, facial dysmorphism, and overgrowth. DD, ASD behaviors, and sleep disorders were more common in individuals with dominant disruptive KDM5B variants, while individuals with dominant missense variants presented more frequently with renal and skin anomalies. This study extends our understanding of the KDM5B-related neurodevelopmental disorder and suggests the pathogenicity of certain dominant KDM5B missense variants.

Original language	English
Article number	1033
Journal	Genes
Volume	15
Issue number	8
DOIs	https://doi.org/10.3390/genes15081033
Publication status	Published - Aug 2024

Bibliographical note

Other keywords

KDM5
epigenetics
genetic syndromes
histone demethylation
intellectual disabilities
neurodevelopmental disorders
polygenetic interactions

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10.3390/genes15081033

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Borroto, M. C., Michaud, C., Hudon, C., Agrawal, P. B., Agre, K., Applegate, C. D., Beggs, A. H., Björnsson, H. T., Callewaert, B., Chen, M. J., Curry, C., Devinsky, O., Dudding-Byth, T., Fagan, K., Finnila, C. R., Gavrilova, R., Genetti, C. A., Hiatt, S. M., Hildebrandt, F., ... Campeau, P. M. (2024). A Genotype/Phenotype Study of KDM5B-Associated Disorders Suggests a Pathogenic Effect of Dominantly Inherited Missense Variants. Genes, 15(8), Article 1033. https://doi.org/10.3390/genes15081033

@article{7d2c80db8a9f4631bdd4d3b017138158,

title = "A Genotype/Phenotype Study of KDM5B-Associated Disorders Suggests a Pathogenic Effect of Dominantly Inherited Missense Variants",

abstract = "Bi-allelic disruptive variants (nonsense, frameshift, and splicing variants) in KDM5B have been identified as causative for autosomal recessive intellectual developmental disorder type 65. In contrast, dominant variants, usually disruptive as well, have been more difficult to implicate in a specific phenotype, since some of them have been found in unaffected controls or relatives. Here, we describe individuals with likely pathogenic variants in KDM5B, including eight individuals with dominant missense variants. This study is a retrospective case series of 21 individuals with variants in KDM5B. We performed deep phenotyping and collected the clinical information and molecular data of these individuals{\textquoteright} family members. We compared the phenotypes according to variant type and to those previously described in the literature. The most common features were developmental delay, impaired intellectual development, behavioral problems, autistic behaviors, sleep disorders, facial dysmorphism, and overgrowth. DD, ASD behaviors, and sleep disorders were more common in individuals with dominant disruptive KDM5B variants, while individuals with dominant missense variants presented more frequently with renal and skin anomalies. This study extends our understanding of the KDM5B-related neurodevelopmental disorder and suggests the pathogenicity of certain dominant KDM5B missense variants.",

keywords = "KDM5, epigenetics, genetic syndromes, histone demethylation, intellectual disabilities, neurodevelopmental disorders, polygenetic interactions",

author = "Borroto, \{Maria Carla\} and Coralie Michaud and Chlo{\'e} Hudon and Agrawal, \{Pankaj B.\} and Katherine Agre and Applegate, \{Carolyn D.\} and Beggs, \{Alan H.\} and Bj{\"o}rnsson, \{Hans T{\'o}mas\} and Bert Callewaert and Chen, \{Mei Jan\} and Cynthia Curry and Orrin Devinsky and Tracy Dudding-Byth and Kelly Fagan and Finnila, \{Candice R.\} and Ralitza Gavrilova and Genetti, \{Casie A.\} and Hiatt, \{Susan M.\} and Friedhelm Hildebrandt and Wojcik, \{Monica H.\} and Tjitske Kleefstra and Kolvenbach, \{Caroline M.\} and Korf, \{Bruce R.\} and Paul Kruszka and Hong Li and Jessica Litwin and Julien Marcadier and Konrad Platzer and Blackburn, \{Patrick R.\} and Reijnders, \{Margot R.F.\} and Heiko Reutter and Ina Schanze and Shieh, \{Joseph T.\} and Stevens, \{Cathy A.\} and Zaheer Valivullah and \{van den Boogaard\}, \{Marie Jos{\'e}\} and Klee, \{Eric W.\} and Campeau, \{Philippe M.\}",

note = "Publisher Copyright: {\textcopyright} 2024 by the authors.",

year = "2024",

month = aug,

doi = "10.3390/genes15081033",

language = "English",

volume = "15",

journal = "Genes",

issn = "2073-4425",

publisher = "Multidisciplinary Digital Publishing Institute (MDPI)",

number = "8",

}

Borroto, MC, Michaud, C, Hudon, C, Agrawal, PB, Agre, K, Applegate, CD, Beggs, AH, Björnsson, HT, Callewaert, B, Chen, MJ, Curry, C, Devinsky, O, Dudding-Byth, T, Fagan, K, Finnila, CR, Gavrilova, R, Genetti, CA, Hiatt, SM, Hildebrandt, F, Wojcik, MH, Kleefstra, T, Kolvenbach, CM, Korf, BR, Kruszka, P, Li, H, Litwin, J, Marcadier, J, Platzer, K, Blackburn, PR, Reijnders, MRF, Reutter, H, Schanze, I, Shieh, JT, Stevens, CA, Valivullah, Z, van den Boogaard, MJ, Klee, EW & Campeau, PM 2024, 'A Genotype/Phenotype Study of KDM5B-Associated Disorders Suggests a Pathogenic Effect of Dominantly Inherited Missense Variants', Genes, vol. 15, no. 8, 1033. https://doi.org/10.3390/genes15081033

TY - JOUR

T1 - A Genotype/Phenotype Study of KDM5B-Associated Disorders Suggests a Pathogenic Effect of Dominantly Inherited Missense Variants

AU - Borroto, Maria Carla

AU - Michaud, Coralie

AU - Hudon, Chloé

AU - Agrawal, Pankaj B.

AU - Agre, Katherine

AU - Applegate, Carolyn D.

AU - Beggs, Alan H.

AU - Björnsson, Hans Tómas

AU - Callewaert, Bert

AU - Chen, Mei Jan

AU - Curry, Cynthia

AU - Devinsky, Orrin

AU - Dudding-Byth, Tracy

AU - Fagan, Kelly

AU - Finnila, Candice R.

AU - Gavrilova, Ralitza

AU - Genetti, Casie A.

AU - Hiatt, Susan M.

AU - Hildebrandt, Friedhelm

AU - Wojcik, Monica H.

AU - Kleefstra, Tjitske

AU - Kolvenbach, Caroline M.

AU - Korf, Bruce R.

AU - Kruszka, Paul

AU - Li, Hong

AU - Litwin, Jessica

AU - Marcadier, Julien

AU - Platzer, Konrad

AU - Blackburn, Patrick R.

AU - Reijnders, Margot R.F.

AU - Reutter, Heiko

AU - Schanze, Ina

AU - Shieh, Joseph T.

AU - Stevens, Cathy A.

AU - Valivullah, Zaheer

AU - van den Boogaard, Marie José

AU - Klee, Eric W.

AU - Campeau, Philippe M.

PY - 2024/8

Y1 - 2024/8

N2 - Bi-allelic disruptive variants (nonsense, frameshift, and splicing variants) in KDM5B have been identified as causative for autosomal recessive intellectual developmental disorder type 65. In contrast, dominant variants, usually disruptive as well, have been more difficult to implicate in a specific phenotype, since some of them have been found in unaffected controls or relatives. Here, we describe individuals with likely pathogenic variants in KDM5B, including eight individuals with dominant missense variants. This study is a retrospective case series of 21 individuals with variants in KDM5B. We performed deep phenotyping and collected the clinical information and molecular data of these individuals’ family members. We compared the phenotypes according to variant type and to those previously described in the literature. The most common features were developmental delay, impaired intellectual development, behavioral problems, autistic behaviors, sleep disorders, facial dysmorphism, and overgrowth. DD, ASD behaviors, and sleep disorders were more common in individuals with dominant disruptive KDM5B variants, while individuals with dominant missense variants presented more frequently with renal and skin anomalies. This study extends our understanding of the KDM5B-related neurodevelopmental disorder and suggests the pathogenicity of certain dominant KDM5B missense variants.

AB - Bi-allelic disruptive variants (nonsense, frameshift, and splicing variants) in KDM5B have been identified as causative for autosomal recessive intellectual developmental disorder type 65. In contrast, dominant variants, usually disruptive as well, have been more difficult to implicate in a specific phenotype, since some of them have been found in unaffected controls or relatives. Here, we describe individuals with likely pathogenic variants in KDM5B, including eight individuals with dominant missense variants. This study is a retrospective case series of 21 individuals with variants in KDM5B. We performed deep phenotyping and collected the clinical information and molecular data of these individuals’ family members. We compared the phenotypes according to variant type and to those previously described in the literature. The most common features were developmental delay, impaired intellectual development, behavioral problems, autistic behaviors, sleep disorders, facial dysmorphism, and overgrowth. DD, ASD behaviors, and sleep disorders were more common in individuals with dominant disruptive KDM5B variants, while individuals with dominant missense variants presented more frequently with renal and skin anomalies. This study extends our understanding of the KDM5B-related neurodevelopmental disorder and suggests the pathogenicity of certain dominant KDM5B missense variants.

KW - KDM5

KW - epigenetics

KW - genetic syndromes

KW - histone demethylation

KW - intellectual disabilities

KW - neurodevelopmental disorders

KW - polygenetic interactions

UR - https://www.scopus.com/pages/publications/85202591411

U2 - 10.3390/genes15081033

DO - 10.3390/genes15081033

M3 - Article

SN - 2073-4425

VL - 15

JO - Genes

JF - Genes

IS - 8

M1 - 1033

ER -

A Genotype/Phenotype Study of KDM5B-Associated Disorders Suggests a Pathogenic Effect of Dominantly Inherited Missense Variants

Abstract

Bibliographical note

Other keywords

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