| Literature DB >> 33368194 |
Diego Lopergolo1,2, Flavia Privitera1, Giuseppe Castello1, Caterina Lo Rizzo2, Maria Antonietta Mencarelli2, Anna Maria Pinto2, Francesca Ariani1,2, Aurora Currò1,2, Vittoria Lamacchia1,2, Roberto Canitano3, Elisabetta Vaghi4, Alessandra Ferrarini5, Gerardo Mejia Baltodano6, Damien Lederer7, Lionel Van Maldergem8, Mercedes Serrano9,10, Mercè Pineda11, Maria Del Carmen Fons-Estupina10,12, Hilde Van Esch13, Jeroen Breckpot13, Candy Kumps14, Bert Callewaert14, Sabrina Mueller15, Gian Paolo Ramelli15, Judith Armstrong16, Alessandra Renieri1,2, Francesca Mari1,2.
Abstract
IQSEC2 mutations are associated with IQSEC2-related intellectual disability (ID). Phenotypic spectrum has been better defined in the last few years by the increasing number of reported cases although the genotype-phenotype relationship for IQSEC2 remains overall complex. As for IQSEC2-related ID a wide phenotypic diversity has been described in Rett syndrome (RTT). Several patients harboring IQSEC2 mutations present with clinical symptoms similar to RTT and some cases meet most of the criteria for classic RTT. With the aim of establishing a genotype-phenotype correlation, we collected data of 16 patients harboring IQSEC2 point mutations (15 of them previously unreported) and of five novel patients carrying CNVs encompassing IQSEC2. Most of our patients surprisingly shared a moderate-to-mild phenotype. The similarities in the clinical course between our mild cases and patients with milder forms of atypical RTT reinforce the hypothesis that also IQSEC2 mutated patients may lay under the wide clinical spectrum of RTT and thus IQSEC2 should be considered in the differential diagnosis. Our data confirm that position, type of variant and gender are crucial for IQSEC2-associated phenotype delineation.Entities:
Keywords: IQSEC2; Rett syndrome; intellectual disability; phenotype-genotype
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Year: 2021 PMID: 33368194 DOI: 10.1111/cge.13908
Source DB: PubMed Journal: Clin Genet ISSN: 0009-9163 Impact factor: 4.438