A research group including Kobe University's Professor TAKUMI Toru (also a Senior Visiting Scientist at RIKEN Center for Biosystems Dynamics Research) and Assistant Professor TAMADA Kota, both of the Physiology Division in the Graduate School of Medicine, has revealed a causal gene (Necdin, NDN) in autism model mice that have the chromosomal abnormality called copy number variation.
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onto Genetics - GEG Tech top picks July 30, 2021 6:07 AM
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A research group including Professor TAKUMI Toru of Kobe University and Assistant Professor TAMADA Kota, both from the Division of Physiology at the Graduate School of Medicine, has shown that the NDN (Necdin) gene, which has a chromosomal abnormality called copy number variation, is responsible for autism in mouse models. The research group identified this gene by performing a synaptic expression-based screen in an animal model of the disorder (15q dup mice). The NDN gene regulates synapse development during the developmental phase and the formation and maturation of dendritic spines during development. Using CRISPR-Cas9, the researchers removed the single copy of the NDN gene from the 15q dup mouse model to generate mice with a normalized genomic copy number for this gene (15q dupΔNdn mouse). Using this model, they demonstrated that the abnormalities observed in 15q dup mice with abnormal spine turnover and decreased inhibitory synaptic input could be ameliorated. Furthermore, they showed that in most behavioral test results of 15q dupΔNdn mice, abnormal behaviors related to sociability and perseveration were improved.