Cognitive Behavioral Phenotyping of DSCAM Heterozygosity As a Model for Autism Spectrum Disorder

Overview

Journal Genes Brain Behav

Specialties Genetics
Neurology
Social Sciences

Date 2024 Sep 18

PMID 39294095

Authors

Ryan C Neff

Katherine A Stangis

Ujjawal Beniwal

Ty Hergenreder

Bing Ye

Geoffrey G Murphy

Affiliations

Soon will be listed here.

Abstract

It is estimated that 1 in 36 children are affected by autism spectrum disorder (ASD) in the United States, which is nearly a twofold increase from a decade ago. Recent genetic studies have identified de novo loss-of-function (dnLoF) mutations in the Down Syndrome Cell Adhesion Molecule (DSCAM) as a strong risk factor for ASD. Previous research has shown that DSCAM ablation confers social interaction deficits and perseverative behaviors in mouse models. However, it remains unknown to what extent DSCAM underexpression captures the full range of behaviors, specifically cognitive phenotypes, presented in ASD. Here, we conducted a comprehensive cognitive behavioral phenotyping which revealed that loss of one copy of DSCAM, as in the DSCAM+/-, that is, DSCAM heterozygous mice, displayed hyperactivity, increased anxiety-like behavior, and motor coordination deficits. Additionally, hippocampal-dependent learning and memory was affected, including impairments in working memory, long-term memory, and contextual fear learning. Interestingly, implicit learning processes remained intact. Therefore, DSCAM LoF produces autistic-like behaviors that are similar to those observed in human cases of ASD. These findings further support a role for DSCAM dnLoF mutations in ASD and suggest DSCAM+/- as a suitable model for ASD research.

Citing Articles

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PMID: 39605537 PMC: 11601461. DOI: 10.1101/2024.03.27.587112.

Cognitive behavioral phenotyping of DSCAM heterozygosity as a model for autism spectrum disorder.

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PMID: 39294095 PMC: 11410459. DOI: 10.1111/gbb.70002.

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