Familial SYNGAP1 variants define the boundaries of a complex neurodevelopmental disorder with epilepsy.

Authors

Alicia G Harrison
Jan H Magielski
Ian McSalley
Shiva Ganesan
Anna J Prentice
Kristin G Cunningham
Samuel R Pierce
Michael J Boland
Benjamin L Prosser
Ingo Helbig
Jillian L McKee

Publication/Presentation Date

5-23-2025

Abstract

OBJECTIVE: SYNGAP1-related disorders are common neurodevelopmental conditions characterized by autism spectrum disorder, developmental delay, intellectual disability, and a range of generalized seizure types. Disease-causing variants in SYNGAP1 typically occur de novo. This study aims to characterize inherited cases of SYNGAP1-related disorders.

METHODS: Here we report three families including eight total individuals with inherited, protein-truncating variants in SYNGAP1, recruited through a natural history study. In two of the families, the proband inherited their pathogenic variant from a heterozygous parent. In the remaining family, the variant was inherited from a mosaic parent. This study additionally reports two families with inherited missense variants classified as variants of uncertain significance, which are not clearly diagnostic at this time.

RESULTS: Phenotypes in affected children and parents included both typical and attenuated SYNGAP1 presentations, including a single individual with a mosaic SYNGAP1 variant who was clinically unaffected. Among the individuals with protein-truncating variants, generalized epilepsy was observed in six individuals, autism spectrum disorder in two individuals, and developmental delay or intellectual disability in all individuals with germline variants.

SIGNIFICANCE: We demonstrate that SYNGAP1-related disorder can occur in families and that clinical presentations of familial cases are not limited to milder phenotypes. We estimate that 3% of cases of SYNGAP1-related disorder are inherited. Recognition of familial SYNGAP1-related disorders delineates edge cases of a relatively common neurodevelopmental disorder and has implications for variant interpretation and clinical practice.

ISSN

1528-1167

Published In/Presented At

Harrison, A. G., Magielski, J. H., McSalley, I., Ganesan, S., Prentice, A. J., Cunningham, K. G., Pierce, S. R., Boland, M. J., Prosser, B. L., Helbig, I., & McKee, J. L. (2025). Familial SYNGAP1 variants define the boundaries of a complex neurodevelopmental disorder with epilepsy. Epilepsia, 10.1111/epi.18469. Advance online publication. https://doi.org/10.1111/epi.18469

Disciplines

Medicine and Health Sciences | Pediatrics

PubMedID

40407699

Department(s)

Department of Pediatrics

Document Type

Article