WWOX-related encephalopathies: delineation of the phenotypical spectrum and emerging genotype-phenotype correlation

6533b85afe1ef96bd12b9721

RESEARCH PRODUCT

WWOX-related encephalopathies: delineation of the phenotypical spectrum and emerging genotype-phenotype correlation

Nicolas Lebrun Thierry Bienvenu Stéphane Auvin Aissa Moustaïne Lila Allou Jean-louis Guéant Laurent Pasquier Philippe Jonveaux Andrée Delahaye-duriez Eva Pipiras Anne-isabelle Vermersch Bénédicte Héron Cyril Mignot Laetitia Lambert Aline Saunier Christophe Philippe Marie-laure Moutard Marie-christine Nougues Jeremie Lefranc Virginie Roth Catherine Barrey Boris Keren Mylène Valduga Laurence Olivier-faivre Sandra Chantot-bastaraud Delphine Héron

subject

WWOX Microcephaly [SDV]Life Sciences [q-bio]Nonsense mutation Mutation Missense Biology 03 medical and health sciences 0302 clinical medicine Genetics medicine Humans Spinocerebellar Ataxias Missense mutation Allele Genetics (clinical)infantile 030304 developmental biology Genetics Comparative Genomic Hybridization 0303 health sciences [ SDV ] Life Sciences [q-bio]Tumor Suppressor Proteins Chromosomal fragile site High-Throughput Nucleotide Sequencing genotype/phenotype correlations medicine.disease Null allele 3. Good health Phenotype WW Domain-Containing Oxidoreductase Codon Nonsense intellectual disability Spinocerebellar ataxia Oxidoreductases Spasms Infantile high throughput data mining 030217 neurology & neurosurgery

description

International audience; BACKGROUND:Homozygous mutations in WWOX were reported in eight individuals of two families with autosomal recessive spinocerebellar ataxia type 12 and in two siblings with infantile epileptic encephalopathy (IEE), including one who deceased prior to DNA sampling.METHODS:By combining array comparative genomic hybridisation, targeted Sanger sequencing and next generation sequencing, we identified five further patients from four families with IEE due to biallelic alterations of WWOX.RESULTS:We identified eight deleterious WWOX alleles consisting in four deletions, a four base-pair frameshifting deletion, one missense and two nonsense mutations. Genotype-phenotype correlation emerges from the seven reported families. The phenotype in four patients carrying two predicted null alleles was characterised by (1) little if any psychomotor acquisitions, poor spontaneous motility and absent eye contact from birth, (2) pharmacoresistant epilepsy starting in the 1st weeks of life, (3) possible retinal degeneration, acquired microcephaly and premature death. This contrasted with the less severe autosomal recessive spinocerebellar ataxia type 12 phenotype due to hypomorphic alleles. In line with this correlation, the phenotype in two siblings carrying a null allele and a missense mutation was intermediate.CONCLUSIONS:Our results obtained by a combination of different molecular techniques undoubtedly incriminate WWOX as a gene for recessive IEE and illustrate the usefulness of high throughput data mining for the identification of genes for rare autosomal recessive disorders. The structure of the WWOX locus encompassing the FRA16D fragile site might explain why constitutive deletions are recurrently reported in genetic databases, suggesting that WWOX-related encephalopathies, although likely rare, may not be exceptional.

year	journal	country	edition	language
2014-12-15	Journal of Medical Genetics

https://doi.org/10.1136/jmedgenet-2014-102748