Affiliation:
1. Fundació per la Recerca Sant Joan de Déu Esplugues de Llobregat Spain
2. Institut de Recerca Sant Joan de Déu Esplugues de Llobregat Spain
3. Institute of Human Genetics Technical University of Munich Munich Germany
4. Institute of Neurogenomics Helmholtz Zentrum München Munich Germany
5. Instituto de Salud Carlos III (ISCIII) CIBER‐ER (Biomedical Network Research Center for Rare Diseases) Madrid Spain
6. Genomic Unit Molecular and Genetic Medicine Section Hospital Sant Joan de Déu Esplugues de Llobregat Spain
Abstract
AbstractMECP2 duplication syndrome (MDS) is an X‐linked neurodevelopmental disorder caused by the gain of dose of at least the genes MECP2 and IRAK1 and is characterised by intellectual disability (ID), developmental delay, hypotonia, epilepsy and recurrent infections. It mainly affects males, and females can be affected or asymptomatic carriers. Rett syndrome (RTT) is mainly triggered by loss of function mutations in MECP2 and is a well described syndrome that presents ID, epilepsy, lack of purposeful hand use and impaired speech, among others. As a result of implementing omics technology, altered biological pathways in human RTT samples have been reported, but such molecular characterisation has not been performed in patients with MDS. We gathered human skin fibroblasts from 17 patients with MDS, 10 MECP2 duplication carrier mothers and 21 patients with RTT, and performed multi‐omics (RNAseq and proteomics) analysis. Here, we provide a thorough description and compare the shared and specific dysregulated biological processes between the cohorts. We also highlight the genes TMOD2, SRGAP1, COPS2, CNPY2, IGF2BP1, MOB2, VASP, FZD7, ECSIT and KIF3B as biomarker and therapeutic target candidates due to their implication in neuronal functions. Defining the RNA and protein profiles has shown that our four cohorts are less alike than expected by their shared phenotypes.
Funder
Instituto de Salud Carlos III
Ministerio de Sanidad, Política Social e Igualdad