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Profiling beneficial and potential adverse effects of <scp>MeCP2</scp> overexpression in a hypomorphic Rett syndrome mouse model

Sheryl Anne D. Vermudez, Rocco G. Gogliotti, Bright Arthur, Aditi Buch, Clarissa Morales, Yuta Moxley, Hemangi Rajpal, P. Jeffrey Conn, Colleen M. Niswender

2021Genes Brain & Behavior14 citationsDOIOpen Access PDF

Abstract

Abstract De novo loss‐of‐function mutations in methyl‐CpG‐binding protein 2 (MeCP2) lead to the neurodevelopmental disorder Rett syndrome (RTT). Despite promising results from strategies aimed at increasing MeCP2 levels, additional studies exploring how hypomorphic MeCP2 mutations impact the therapeutic window are needed. Here, we investigated the consequences of genetically introducing a wild‐type MECP2 transgene in the Mecp2 R133C mouse model of RTT. The MECP2 transgene reversed the majority of RTT‐like phenotypes exhibited by male and female Mecp2 R133C mice. However, three core symptom domains were adversely affected in female Mecp2 R133C/+ animals; these phenotypes resemble those observed in disease contexts of excess MeCP2. Parallel control experiments in Mecp2 Null/+ mice linked these adverse effects to the hypomorphic R133C mutation. Collectively, these data provide evidence regarding the safety and efficacy of genetically overexpressing functional MeCP2 in Mecp2 R133C mice and suggest that personalized approaches may warrant consideration for the clinical assessment of MeCP2‐targeted therapies.

Topics & Concepts

Rett syndromeMECP2Profiling (computer programming)Adverse effectBiologyComputer scienceGeneticsGenePharmacologyPhenotypeOperating systemGenetics and Neurodevelopmental DisordersAutism Spectrum Disorder ResearchCongenital heart defects research
Profiling beneficial and potential adverse effects of <scp>MeCP2</scp> overexpression in a hypomorphic Rett syndrome mouse model | Litcius