Low-pass whole genome sequencing is a reliable and cost-effective approach for copy number variant analysis in the clinical setting

Patricia C Mazzonetto; Darine Villela; Silvia Souza da Costa; Ana C V Krepischi; Fernanda Milanezi; Michele P Migliavacca; Paulo M Pierry; Adriano Bonaldi; Luiz Gustavo D Almeida; Camila Alves De Souza; José Eduardo Kroll; Marcelo G Paula; Rodrigo Guarischi-Sousa; Cristovam Scapulatempo-Neto; Carla Rosenberg

doi:10.1111/ahg.12532

Low-pass whole genome sequencing is a reliable and cost-effective approach for copy number variant analysis in the clinical setting

Ann Hum Genet. 2024 Mar;88(2):113-125. doi: 10.1111/ahg.12532. Epub 2023 Oct 9.

Authors

Patricia C Mazzonetto^{1

2}, Darine Villela², Silvia Souza da Costa¹, Ana C V Krepischi¹, Fernanda Milanezi², Michele P Migliavacca², Paulo M Pierry², Adriano Bonaldi², Luiz Gustavo D Almeida², Camila Alves De Souza², José Eduardo Kroll², Marcelo G Paula², Rodrigo Guarischi-Sousa², Cristovam Scapulatempo-Neto², Carla Rosenberg^{1

2}

Affiliations

¹ The Human Genome and Stem Cell Research Center, Department of Genetics and Evolutionary Biology, Institute of Biosciences, University of São Paulo, São Paulo, SP, Brazil.
² Diagnósticos da América S.A., DASA, São Paulo, Brazil.

PMID: 37807935
DOI: 10.1111/ahg.12532

Abstract

Introduction: Next generation sequencing technology has greatly reduced the cost and time required for sequencing a genome. An approach that is rapidly being adopted as an alternative method for CNV analysis is the low-pass whole genome sequencing (LP-WGS). Here, we evaluated the performance of LP-WGS to detect copy number variants (CNVs) in clinical cytogenetics.

Materials and methods: DNA samples with known CNVs detected by chromosomal microarray analyses (CMA) were selected for comparison and used as positive controls; our panel included 44 DNA samples (12 prenatal and 32 postnatal), comprising a total of 55 chromosome imbalances. The selected cases were chosen to provide a wide range of clinically relevant CNVs, the vast majority being associated with intellectual disability or recognizable syndromes. The chromosome imbalances ranged in size from 75 kb to 90.3 Mb, including aneuploidies and two cases of mosaicism.

Results: All CNVs were successfully detected by LP-WGS, showing a high level of consistency and robust performance of the sequencing method. Notably, the size of chromosome imbalances detected by CMA and LP-WGS were compatible between the two different platforms, which indicates that the resolution and sensitivity of the LP-WGS approach are at least similar to those provided by CMA.

Discussion: Our data show the potential use of LP-WGS to detect CNVs in clinical diagnosis and confirm the method as an alternative for chromosome imbalances detection. The diagnostic effectiveness and feasibility of LP-WGS, in this technical validation study, were evidenced by a clinically representative dataset of CNVs that allowed a systematic assessment of the detection power and the accuracy of the sequencing approach. Further, since the software used in this study is commercially available, the method can easily be tested and implemented in a routine diagnostic setting.

Keywords: CNV; copy number variation; cytogenetics; low-pass whole genome sequencing; next-generation sequencing (NGS); postnatal diagnosis; prenatal diagnosis; structural variant.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Aneuploidy*
Cost-Benefit Analysis
DNA
DNA Copy Number Variations*
Female
Humans
Pregnancy
Whole Genome Sequencing / methods

Substances

DNA

Grants and funding

Fundação de Amparo à Pesquisa do Estado de São Paulo