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http://dx.doi.org/10.5734/JGM.2018.15.1.24

A family with X-linked Cornelia de Lange syndrome due to a novel SMC1A missense mutation identified by multi-gene panel sequencing  

Hong, Sungwon (Department of Pediatrics, Nowon Eulji Medical Center, Eulji University)
Lee, Cha Gon (Department of Pediatrics, Nowon Eulji Medical Center, Eulji University)
Publication Information
Journal of Genetic Medicine / v.15, no.1, 2018 , pp. 24-27 More about this Journal
Abstract
Cornelia de Lange syndrome (CdLS) is a rare, clinically and genetically heterogeneous, multi-system developmental disorder caused by mutations in genes that encode components of the cohesin complex. X-linked CdLS caused by an SMC1A mutation is an extremely rare disease characterized by phenotypes milder than those of classic CdLS. In the Republic of Korea, based on a literature review, one family with SMC1A-related CdLS with mild phenotypes has been genetically confirmed to date. In this study, we describe the clinical features of a Korean boy with a hemizygous novel missense mutation and his mother with a heterozygous mutation, i.e., c.2447G>A (p.Arg816His) in SMC1A, identified by multi-gene panel sequencing. The proband had a mild phenotype with typical facial features and his mother exhibited a mild, subclinical phenotype. This study expands the clinical spectrum of patients with X-linked CdLS caused by SMC1A variants. Moreover, these findings reinforce the notion that a dominant negative effect in a carrier female with a heterozygous mutation in SMC1A results in a phenotype milder than that in a male patient with the same mutation.
Keywords
SMC1A; De Lange syndrome; X-Linked genes; High-throughput nucleotide sequencing;
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