Variants in ADD1 cause intellectual disability, corpus callosum dysgenesis, and ventriculomegaly in humans

Variants in ADD1 cause intellectual disability, corpus callosum dysgenesis, and ventriculomegaly in humans

Purpose: Adducins interconnect spectrin and actin filaments to form polygonal scaffolds beneath the cell membranes and form ring-like structures in neuronal axons. Adducins regulate mouse neural development, but their function in the human brain is unknown. Methods: We used exome sequencing to uncov...

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Bibliographic Details
Main Authors: Bhoj, E.J (Author), Brasch-Andersen, C. (Author), Brites, P. (Author), Bupp, C. (Author), Caluseriu, O. (Author), Costa, A.R (Author), Fagerberg, C. (Author), Falk, M.J (Author), Feng, I. (Author), Ganetzky, R.D (Author), Hakonarson, H. (Author), Hansen, L.K (Author), Hill, R.S (Author), Hu, K. (Author), Kahle, K.T (Author), Kang, B. (Author), Li, D. (Author), Muraresku, C.C (Author), Neil, J.E (Author), Pinto-Costa, R. (Author), Qi, C. (Author), Ruan, X. (Author), Sousa, M.M (Author), Walsh, C.A (Author), Zhang, X. (Author), Zhong, R. (Author)
Format: Article
Language:English
Published: Elsevier B.V. 2022
Subjects:
Adducin
Agenesis of Corpus Callosum
Alternative splicing
animal
Animals
Axon degeneration
copy number variation
corpus callosum agenesis
DNA Copy Number Variations
genetics
human
Humans
hydrocephalus
Hydrocephalus
Intellectual Disability
intellectual impairment
Membrane-associated periodic ring-like structure (MPS)
Mice
mouse
pathology
phenotype
Phenotype
Online Access:View Fulltext in Publisher
Description
Summary:Purpose: Adducins interconnect spectrin and actin filaments to form polygonal scaffolds beneath the cell membranes and form ring-like structures in neuronal axons. Adducins regulate mouse neural development, but their function in the human brain is unknown. Methods: We used exome sequencing to uncover ADD1 variants associated with intellectual disability (ID) and brain malformations. We studied ADD1 splice isoforms in mouse and human neocortex development with RNA sequencing, super resolution imaging, and immunoblotting. We investigated 4 variant ADD1 proteins and heterozygous ADD1 cells for protein expression and ADD1–ADD2 dimerization. We studied Add1 functions in vivo using Add1 knockout mice. Results: We uncovered loss-of-function ADD1 variants in 4 unrelated individuals affected by ID and/or structural brain defects. Three additional de novo copy number variations covering the ADD1 locus were associated with ID and brain malformations. ADD1 is highly expressed in the neocortex and the corpus callosum, whereas ADD1 splice isoforms are dynamically expressed between cortical progenitors and postmitotic neurons. Human variants impair ADD1 protein expression and/or dimerization with ADD2. Add1 knockout mice recapitulate corpus callosum dysgenesis and ventriculomegaly phenotypes. Conclusion: Our human and mouse genetics results indicate that pathogenic ADD1 variants cause corpus callosum dysgenesis, ventriculomegaly, and/or ID. © 2021 American College of Medical Genetics and Genomics
Physical Description:13
ISBN:10983600 (ISSN)
DOI:10.1016/j.gim.2021.09.014

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