ANO3 and early-onset dyskinetic encephalopathy.

ANO3 and early-onset dyskinetic encephalopathy. Eur J Med Genet. 2020 Oct 09;:104085 Authors: Jiménez de Domingo A, Lopez-Martín S, Albert J, Jiménez de la Peña M, Tirado P, Fernández-Mayoralas DM, Fernández-Perrone AL, Calleja-Pérez B, Martínez-García M, Álvarez S, Fernández-Jaén A Abstract Mutations in the ANO3 gene have been associated with autosomal dominant craniocervical dystonia. However, little else is known about the genotype-phenotype characteristics of this disorder. Here we describe a 3 years-old girl with distal myoclonic dystonia. Whole exome sequencing in trio revealed a de novo missense ANO3 variant not previously described in international databases. A global psychomotor regression was observed once dystonia was present. Brain MRI changes paralleled these findings: whereas MRI at the age of 18 months was normal, mild brain and cerebellar atrophy was observed 18 months later. These results suggest that missense mutations in ANO3 may underlie complex disorders particularly characterized by early psychomotor regression and dystonia. PMID: 33045406 [PubMed - as supplied by publisher]

https://www.ncbi.nlm.nih.gov/pubmed/33045406?dopt=Abstract

Source: European Journal of Medical Genetics - October 9, 2020 Category: Genetics & Stem Cells Authors: Jiménez de Domingo A, Lopez-Martín S, Albert J, Jiménez de la Peña M, Tirado P, Fernández-Mayoralas DM, Fernández-Perrone AL, Calleja-Pérez B, Martínez-García M, Álvarez S, Fernández-Jaén A Tags: Eur J Med Genet Source Type: research