De novo missense variants in HDAC3 leading to epigenetic machinery dysfunction are associated with a variable neurodevelopmental disorder

Jihoon G Yoon; Seong-Kyun Lim; Hoseok Seo; Seungbok Lee; Jaeso Cho; Soo Yeon Kim; Hyun Yong Koh; Annapurna H Poduri; Vijayalakshmi Ramakumaran; Pradeep Vasudevan; Martijn J de Groot; Jung Min Ko; Dohyun Han; Jong-Hee Chae; Chul-Hwan Lee

doi:10.1016/j.ajhg.2024.06.015

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De novo missense variants in HDAC3 leading to epigenetic machinery dysfunction are associated with a variable neurodevelopmental disorder

Authors: Jihoon G Yoon ; Seong-Kyun Lim ; Hoseok Seo ; Seungbok Lee ; Jaeso Cho ; Soo Yeon Kim ; Hyun Yong Koh ; Annapurna H Poduri ; Vijayalakshmi Ramakumaran ; Pradeep Vasudevan ; Martijn J de Groot ; Jung Min Ko ; Dohyun Han ; Jong-Hee Chae ; Chul-Hwan Lee

Citation: AMERICAN JOURNAL OF HUMAN GENETICS, Vol.111(8) : 1588-1604, 2024-08

Journal Title: AMERICAN JOURNAL OF HUMAN GENETICS

ISSN: 0002-9297

Issue Date: 2024-08

MeSH: Adolescent ; Child ; Child, Preschool ; Developmental Disabilities / genetics ; Epigenesis, Genetic* ; Exome Sequencing ; Female ; Histone Deacetylases* / genetics ; Histone Deacetylases* / metabolism ; Humans ; Infant ; Intellectual Disability / genetics ; Male ; Mutation, Missense* / genetics ; Neurodevelopmental Disorders* / genetics ; Nuclear Receptor Co-Repressor 1 / genetics ; Nuclear Receptor Co-Repressor 1 / metabolism ; Phenotype

Keywords: CoREST ; HDAC activity ; NCoR ; cellular mislocalization ; epigenetics ; exome sequencing ; histone deacetylase 3 ; neurodevelopmental disorder ; proteomics

Abstract: Histone deacetylase 3 (HDAC3) is a crucial epigenetic modulator essential for various developmental and physiological functions. Although its dysfunction is increasingly recognized in abnormal phenotypes, to our knowledge, there have been no established reports of human diseases directly linked to HDAC3 dysfunction. Using trio exome sequencing and extensive phenotypic analysis, we correlated heterozygous de novo variants in HDAC3 with a neurodevelopmental disorder having variable clinical presentations, frequently associated with intellectual disability, developmental delay, epilepsy, and musculoskeletal abnormalities. In a cohort of six individuals, we identified missense variants in HDAC3 (c.277G>A [p.Asp93Asn], c.328G>A [p.Ala110Thr], c.601C>T [p.Pro201Ser], c. 797T>C [p.Leu266Ser], c.799G>A [p.Gly267Ser], and c.1075C>T [p.Arg359Cys]), all located in evolutionarily conserved sites and confirmed as de novo. Experimental studies identified defective deacetylation activity in the p.Asp93Asn, p.Pro201Ser, p.Leu266Ser, and p.Gly267Ser variants, positioned near the enzymatic pocket. In addition, proteomic analysis employing co-immunoprecipitation revealed that the disrupted interactions with molecules involved in the CoREST and NCoR complexes, particularly in the p.Ala110Thr variant, consist of a central pathogenic mechanism. Moreover, immunofluorescence analysis showed diminished nuclear to cytoplasmic fluorescence ratio in the p.Ala110Thr, p.Gly267Ser, and p.Arg359Cys variants, indicating impaired nuclear localization. Taken together, our study highlights that de novo missense variants in HDAC3 are associated with a broad spectrum of neurodevelopmental disorders, which emphasizes the complex role of HDAC3 in histone deacetylase activity, multi-protein complex interactions, and nuclear localization for proper physiological functions. These insights open new avenues for understanding the molecular mechanisms of HDAC3-related disorders and may inform future therapeutic strategies.