Autism and intellectual disability due to a novel gain-of-function mutation in UBE3A

Anna M. Gunelson; Kwang Soo Kim; Connolly G. Steigerwald; Devorah Segal; Nicolas J. Abreu; Jason J. Yi

doi:10.1038/s10038-025-01343-z

Autism and intellectual disability due to a novel gain-of-function mutation in UBE3A

Anna M. Gunelson
, Kwang Soo Kim
, Connolly G. Steigerwald
, Devorah Segal
, Nicolas J. Abreu
, Jason J. Yi

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

1 Scopus citations

Abstract

The loss of maternal UBE3A causes Angelman syndrome whereas its duplication is associated with a heterogeneous neurodevelopmental disorder. Here, we describe two affected brothers who possess a novel UBE3A^L734S variant that is not present in two neurotypical siblings. The UBE3A^L734S variant was confirmed to be maternally inherited, and the affected individuals exhibited early global developmental delay, ongoing learning difficulties, and autistic features. Their phenotypes were inconsistent with Angelman syndrome. Biochemical characterization showed the UBE3A^L734S variant causes a dramatic increase in the activity of the UBE3A enzyme, suggesting that a gain in UBE3A activity is the driver of neurodevelopmental disease. Our observations document an emerging class of neurodevelopmental disorders caused by gain-of-function mutations in UBE3A.

Original language	English
Pages (from-to)	439-442
Number of pages	4
Journal	Journal of Human Genetics
Volume	70
Issue number	8
DOIs	https://doi.org/10.1038/s10038-025-01343-z
State	Published - Aug 2025

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title = "Autism and intellectual disability due to a novel gain-of-function mutation in UBE3A",

abstract = "The loss of maternal UBE3A causes Angelman syndrome whereas its duplication is associated with a heterogeneous neurodevelopmental disorder. Here, we describe two affected brothers who possess a novel UBE3AL734S variant that is not present in two neurotypical siblings. The UBE3AL734S variant was confirmed to be maternally inherited, and the affected individuals exhibited early global developmental delay, ongoing learning difficulties, and autistic features. Their phenotypes were inconsistent with Angelman syndrome. Biochemical characterization showed the UBE3AL734S variant causes a dramatic increase in the activity of the UBE3A enzyme, suggesting that a gain in UBE3A activity is the driver of neurodevelopmental disease. Our observations document an emerging class of neurodevelopmental disorders caused by gain-of-function mutations in UBE3A.",

author = "Gunelson, \{Anna M.\} and Kim, \{Kwang Soo\} and Steigerwald, \{Connolly G.\} and Devorah Segal and Abreu, \{Nicolas J.\} and Yi, \{Jason J.\}",

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doi = "10.1038/s10038-025-01343-z",

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AU - Gunelson, Anna M.

AU - Kim, Kwang Soo

AU - Steigerwald, Connolly G.

AU - Segal, Devorah

AU - Abreu, Nicolas J.

AU - Yi, Jason J.

N1 - Publisher Copyright: © The Author(s) 2025.

PY - 2025/8

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N2 - The loss of maternal UBE3A causes Angelman syndrome whereas its duplication is associated with a heterogeneous neurodevelopmental disorder. Here, we describe two affected brothers who possess a novel UBE3AL734S variant that is not present in two neurotypical siblings. The UBE3AL734S variant was confirmed to be maternally inherited, and the affected individuals exhibited early global developmental delay, ongoing learning difficulties, and autistic features. Their phenotypes were inconsistent with Angelman syndrome. Biochemical characterization showed the UBE3AL734S variant causes a dramatic increase in the activity of the UBE3A enzyme, suggesting that a gain in UBE3A activity is the driver of neurodevelopmental disease. Our observations document an emerging class of neurodevelopmental disorders caused by gain-of-function mutations in UBE3A.

AB - The loss of maternal UBE3A causes Angelman syndrome whereas its duplication is associated with a heterogeneous neurodevelopmental disorder. Here, we describe two affected brothers who possess a novel UBE3AL734S variant that is not present in two neurotypical siblings. The UBE3AL734S variant was confirmed to be maternally inherited, and the affected individuals exhibited early global developmental delay, ongoing learning difficulties, and autistic features. Their phenotypes were inconsistent with Angelman syndrome. Biochemical characterization showed the UBE3AL734S variant causes a dramatic increase in the activity of the UBE3A enzyme, suggesting that a gain in UBE3A activity is the driver of neurodevelopmental disease. Our observations document an emerging class of neurodevelopmental disorders caused by gain-of-function mutations in UBE3A.

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JO - Journal of Human Genetics

JF - Journal of Human Genetics

IS - 8

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Autism and intellectual disability due to a novel gain-of-function mutation in UBE3A

Abstract

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