Abstract
Cornelia de Lange Syndrome (CdLS) is a rare genetic disorder, which causes a range of physical, cognitive, and medical challenges. To retrospectively analyze the clinical characteristics and genetic variations of Chinese patients, and to provide experience for further diagnosis and treatment of CdLS in Chinese children, we identified 15 unrelated Chinese children who presented with unusual facial features, short stature, developmental delay, limb abnormalities, and a wide range of health conditions. In this study, targeted-next generation sequencing was used to screen for causal variants and the clinically relevant variants were subsequently verified using Sanger sequencing. DNA sequencing identified 15 genetic variations, including 11 NIPBL gene variants, two SMC1A gene variants, one RAD21 gene variant, and one HDAC8 variant. The phenotype of these patients was summarized and differences between this cohort and another four groups were compared. The clinical manifestations of the patients in this cohort were mostly consistent with other ethnicities, but several clinical features in our cohort had different frequencies compared with other groups. We identified 15 deleterious variants of which 11 were novel. Variants in the NIPBL gene were the most common cause in our cohort. Our study not only expands upon the spectrum of genetic variations in CdLS, but also broadens our understanding of the clinical features of CdLS.
Highlights
Cornelia de Lange Syndrome (CdLS) is a rare genetic disorder, which causes a range of physical, cognitive, and medical challenges
Genetic variations leading to CdLS have been identified in the following seven genes: NIPBL, SMC1A, SMC3, RAD21, BRD4, HDAC8, and ANKRD112
The preliminary diagnosis of CdLS was made by pediatricians and based on clinical manifestations and laboratory examinations according to the Diagnostic Criteria for Cornelia de Lange Syndrome by Antonie D
Summary
Cornelia de Lange Syndrome (CdLS) is a rare genetic disorder, which causes a range of physical, cognitive, and medical challenges. DNA sequencing identified 15 genetic variations, including 11 NIPBL gene variants, two SMC1A gene variants, one RAD21 gene variant, and one HDAC8 variant. The phenotype of these patients was summarized and differences between this cohort and another four groups were compared. Our study expands upon the spectrum of genetic variations in CdLS, and broadens our understanding of the clinical features of CdLS. Genetic variations leading to CdLS have been identified in the following seven genes: NIPBL, SMC1A, SMC3, RAD21, BRD4, HDAC8, and ANKRD112. Among these genes, NIPBL is a cohesion loading factor. Other genes were described in patients presenting features of CdLS or CdLS-like phenotype as well (i.e. EP300, AFF4)[2]
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