Bi‐allelic loss of function variant in the NRCAM gene is associated with motor‐predominant axonal polyneuropathy; the second report

Abstract

AbstractBackgroundThe role of biallelic variants in the NRCAM gene underlying a neurodevelopmental disorder has been defined recently. The phenotype is mainly recognized by varying severity of global developmental delay/intellectual disability, hypotonia, spasticity, and peripheral neuropathy.MethodsHere, we describe a patient with an initial diagnosis of motor‐predominant axonal polyneuropathy or a form of distal SMA. Whole‐exome sequencing (WES), in parallel with WES‐based CNV detection and assessment of homozygosity runs, was performed to identify this patient's possible genetic cause.ResultsWhole exome sequencing revealed a homozygous variant, c.73C > T (p.Gln25*), in the NRCAM gene, while the patient manifests a mild range of phenotypes compared to NRCAM‐related disorder. He presented only motor‐predominant axonal polyneuropathy with no other signs of central nervous system involvement.ConclusionsThis study is the second report of an association between biallelic NRCAM gene variants and a Mendelian disorder. The obtained clinical data, together with the molecular findings in this patient, expands the clinical and molecular spectrum of NRCAM‐related disorder and highlights its phenotypic complexity. Although patients with loss of function variants in this gene have previously presented severe clinical features, we show that type of the pathogenic variant does not necessarily determine the severity of this phenotype.