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CNVs cause autosomal recessive genetic diseases with or without involvement of SNV/indels

Authors :
Wenmiao Zhu
Linyan Meng
Patricia A. Ward
Richard A. Gibbs
Rui Xiao
Lei Wang
Lance Cooper
Bo Yuan
Fan Xia
Weimin Bi
Arthur L. Beaudet
James R. Lupski
Alicia Braxton
Sandra Peacock
Janice L. Smith
Carlos A. Bacino
Stephanie A. Anderson
Yaping Yang
Sau Wai Cheung
Theodore Chiang
Christine M. Eng
Amy M. Breman
Eric S. Schmitt
Chad A. Shaw
Weimin He
Francesco Vetrini
Hongzheng Dai
Yue Wang
Donna M. Muzny
Xia Wang
Pengfei Liu
Source :
Genet Med
Publication Year :
2020
Publisher :
Elsevier BV, 2020.

Abstract

Improved resolution of molecular diagnostic technologies enabled detection of smaller sized exonic level copy-number variants (CNVs). The contribution of CNVs to autosomal recessive (AR) conditions may be better recognized using a large clinical cohort. We retrospectively investigated the CNVs’ contribution to AR conditions in cases subjected to chromosomal microarray analysis (CMA, N = ~70,000) and/or clinical exome sequencing (ES, N = ~12,000) at Baylor Genetics; most had pediatric onset neurodevelopmental disorders. CNVs contributed to biallelic variations in 87 cases, including 81 singletons and three affected sibling pairs. Seventy cases had CNVs affecting both alleles, and 17 had a CNV and a single-nucleotide variant (SNV)/indel in trans. In total, 94.3% of AR-CNVs affected one gene; among these 41.4% were single-exon and 35.0% were multiexon partial-gene events. Sixty-nine percent of homozygous AR-CNVs were embedded in homozygous genomic intervals. Five cases had large deletions unmasking an SNV/indel on the intact allele for a recessive condition, resulting in multiple molecular diagnoses. AR-CNVs are often smaller in size, transmitted through generations, and underrecognized due to limitations in clinical CNV detection methods. Our findings from a large clinical cohort emphasized integrated CNV and SNV/indel analyses for precise clinical and molecular diagnosis especially in the context of genomic disorders.

Details

ISSN :
10983600
Volume :
22
Database :
OpenAIRE
Journal :
Genetics in Medicine
Accession number :
edsair.doi.dedup.....adecc4e3ebbf3e9e4e567545ba6e99c6
Full Text :
https://doi.org/10.1038/s41436-020-0864-8