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Touchscreen cognitive deficits, hyperexcitability and hyperactivity in males and females using two models of<i>Cdkl5</i>deficiency

Anna Adhikari, Fiona K B Buchanan, Timothy A. Fenton, David Cameron, Julian Halmai, Nycole A. Copping, Kyle D. Fink, Jill L. Silverman

2022Human Molecular Genetics26 citationsDOIOpen Access PDF

Abstract

Many neurodevelopmental disorders (NDDs) are the result of mutations on the X chromosome. One severe NDD resulting from mutations on the X chromosome is CDKL5 deficiency disorder (CDD). CDD is an epigenetic, X-linked NDD characterized by intellectual disability (ID), pervasive seizures and severe sleep disruption, including recurring hospitalizations. CDD occurs at a 4:1 ratio, with a female bias. CDD is driven by the loss of cyclin-dependent kinase-like 5 (CDKL5), a serine/threonine kinase that is essential for typical brain development, synapse formation and signal transmission. Previous studies focused on male subjects from animal models, likely to avoid the complexity of X mosaicism. For the first time, we report translationally relevant behavioral phenotypes in young adult (8-20 weeks) females and males with robust signal size, including impairments in learning and memory, substantial hyperactivity and increased susceptibility to seizures/reduced seizure thresholds, in both sexes, and in two models of CDD preclinical mice, one with a general loss-of-function mutation and one that is a patient-derived mutation.

Topics & Concepts

BiologyIntellectual disabilityEpilepsyNeuroscienceMutationPhenotypeAutism spectrum disorderCognitionRett syndromeSynapseAutismGeneticsPsychologyDevelopmental psychologyGeneGenetics and Neurodevelopmental DisordersChild Development and Digital Technology
Touchscreen cognitive deficits, hyperexcitability and hyperactivity in males and females using two models of<i>Cdkl5</i>deficiency | Litcius