Comprehensive Genetic Analysis of 57 Families with Clinically Suspected Cornelia De Lange Syndrome

Overview

Journal J Hum Genet

Specialty Genetics

Date 2019 Jul 25

PMID 31337854

Citations 25

Authors

Hiromi Aoi

Takeshi Mizuguchi

Jose Ricard Ceroni

Veronica Eun Hue Kim

Isabel Furquim

Rachel S Honjo

Takuma Iwaki

Toshifumi Suzuki

Futoshi Sekiguchi

Yuri Uchiyama

Yoshiteru Azuma

Kohei Hamanaka

Eriko Koshimizu

Satoko Miyatake

Satomi Mitsuhashi

Atsushi Takata

Noriko Miyake

Satoru Takeda

Atsuo Itakura

Debora R Bertola

Chong Ae Kim

Naomichi Matsumoto

Affiliations

Soon will be listed here.

Abstract

Cornelia de Lange syndrome (CdLS) is a rare multisystem disorder with specific dysmorphic features. Pathogenic genetic variants encoding cohesion complex subunits and interacting proteins (e.g., NIPBL, SMC1A, SMC3, HDAC8, and RAD21) are the major causes of CdLS. However, there are many clinically diagnosed cases of CdLS without pathogenic variants in these genes. To identify further genetic causes of CdLS, we performed whole-exome sequencing in 57 CdLS families, systematically evaluating both single nucleotides variants (SNVs) and copy number variations (CNVs). We identified pathogenic genetic changes in 36 out of 57 (63.2 %) families, including 32 SNVs and four CNVs. Two known CdLS genes, NIPBL and SMC1A, were mutated in 23 and two cases, respectively. Among the remaining 32 individuals, four genes (ANKRD11, EP300, KMT2A, and SETD5) each harbored a pathogenic variant in a single individual. These variants are known to be involved in CdLS-like. Furthermore, pathogenic CNVs were detected in NIPBL, MED13L, and EHMT1, along with pathogenic SNVs in ZMYND11, MED13L, and PHIP. These three latter genes were involved in diseases other than CdLS and CdLS-like. Systematic clinical evaluation of all patients using a recently proposed clinical scoring system showed that ZMYND11, MED13L, and PHIP abnormality may cause CdLS or CdLS-like.

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