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Multisystem disorder associated with a pathogenic variant in CLCN7 in the absence of osteopetrosis.

Chung-Lin LeeYeun-Wen ChangHsiang-Yu LinHung-Chang LeeTing-Chi YehLi-Ching FangNi-Chung LeeJeng-Daw TsaiShuan-Pei Lin
Published in: Molecular genetics & genomic medicine (2024)
Elucidating mechanisms by which CLCN7 variants lead to lysosomal dysfunction will advance understanding of genotype-phenotype correlations. Identifying modifier genes and compensatory pathways may reveal therapeutic targets. Ongoing functional characterization of variants along with longitudinal clinical evaluations will continue advancing knowledge of ClC-7's critical roles and disease mechanisms resulting from its dysfunction. Expanded cohort studies are warranted to delineate the full spectrum of associated phenotypes.
Keyphrases
  • copy number
  • genome wide
  • oxidative stress
  • healthcare
  • dna methylation
  • single cell
  • cross sectional