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Unique variants in CLCN3, encoding an endosomal anion/proton exchanger, underlie a spectrum of neurodevelopmental disorders. | LitMetric

AI Article Synopsis

  • The genetic causes of global developmental delay (GDD) and intellectual disability (ID) vary widely, including mutations in the CLC family of chloride channels, specifically the CLCN3 gene.
  • Nine variants in CLCN3 were identified in individuals with GDD/ID, with findings suggesting that homozygous variants lead to severe neurological issues, while heterozygous variants cause a range of neurodevelopmental anomalies.
  • Electrophysiological analyses showed that certain CLCN3 variants affect chloride channel function, thereby impacting neurodevelopment and suggesting both forms of genetic variants can contribute to GDD/ID and brain structural abnormalities.

Article Abstract

The genetic causes of global developmental delay (GDD) and intellectual disability (ID) are diverse and include variants in numerous ion channels and transporters. Loss-of-function variants in all five endosomal/lysosomal members of the CLC family of Cl channels and Cl/H exchangers lead to pathology in mice, humans, or both. We have identified nine variants in CLCN3, the gene encoding CIC-3, in 11 individuals with GDD/ID and neurodevelopmental disorders of varying severity. In addition to a homozygous frameshift variant in two siblings, we identified eight different heterozygous de novo missense variants. All have GDD/ID, mood or behavioral disorders, and dysmorphic features; 9/11 have structural brain abnormalities; and 6/11 have seizures. The homozygous variants are predicted to cause loss of ClC-3 function, resulting in severe neurological disease similar to the phenotype observed in Clcn3 mice. Their MRIs show possible neurodegeneration with thin corpora callosa and decreased white matter volumes. Individuals with heterozygous variants had a range of neurodevelopmental anomalies including agenesis of the corpus callosum, pons hypoplasia, and increased gyral folding. To characterize the altered function of the exchanger, electrophysiological analyses were performed in Xenopus oocytes and mammalian cells. Two variants, p.Ile607Thr and p.Thr570Ile, had increased currents at negative cytoplasmic voltages and loss of inhibition by luminal acidic pH. In contrast, two other variants showed no significant difference in the current properties. Overall, our work establishes a role for CLCN3 in human neurodevelopment and shows that both homozygous loss of ClC-3 and heterozygous variants can lead to GDD/ID and neuroanatomical abnormalities.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8387284PMC
http://dx.doi.org/10.1016/j.ajhg.2021.06.003DOI Listing

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