학술논문
Defining the heterogeneity of unbalanced structural variation underlying breast cancer susceptibility by nanopore genome sequencing
Document Type
Article
Author
Dixon, Katherine; Shen, Yaoqing; O’Neill, Kieran; Mungall, Karen L.; Chan, Simon; Bilobram, Steve; Zhang, Wei; Bezeau, Marjorie; Sharma, Alshanee; Fok, Alexandra; Mungall, Andrew J.; Moore, Richard; Bosdet, Ian; Thibodeau, My Linh; Sun, Sophie; Yip, Stephen; Schrader, Kasmintan A.; Jones, Steven J. M.
Source
European Journal of Human Genetics: EJHG; May 2023, Vol. 31 Issue: 5 p602-606, 5p
Subject
Language
ISSN
10184813; 14765438
Abstract
Germline structural variants (SVs) are challenging to resolve by conventional genetic testing assays. Long-read sequencing has improved the global characterization of SVs, but its sensitivity at cancer susceptibility loci has not been reported. Nanopore long-read genome sequencing was performed for nineteen individuals with pathogenic copy number alterations in BRCA1, BRCA2, CHEK2and PALB2identified by prior clinical testing. Fourteen variants, which spanned single exons to whole genes and included a tandem duplication, were accurately represented. Defining the precise breakpoints of SVs in BRCA1and CHEK2revealed unforeseen allelic heterogeneity and informed the mechanisms underlying the formation of recurrent deletions. Integrating read-based and statistical phasing further helped define extended haplotypes associated with founder alleles. Long-read sequencing is a sensitive method for characterizing private, recurrent and founder SVs underlying breast cancer susceptibility. Our findings demonstrate the potential for nanopore sequencing as a powerful genetic testing assay in the hereditary cancer setting.