Genes (Jun 2023)

Low-Pass Genome Sequencing-Based Detection of Paternity: Validation in Clinical Cytogenetics

  • Keying Li,
  • Yilin Zhao,
  • Matthew Hoi Kin Chau,
  • Ye Cao,
  • Tak Yeung Leung,
  • Yvonne K. Kwok,
  • Kwong Wai Choy,
  • Zirui Dong

DOI
https://doi.org/10.3390/genes14071357
Journal volume & issue
Vol. 14, no. 7
p. 1357

Abstract

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Submission of a non-biological parent together with a proband for genetic diagnosis would cause a misattributed parentage (MP), possibly leading to misinterpretation of the pathogenicity of genomic variants. Therefore, a rapid and cost-effective paternity/maternity test is warranted before genetic testing. Although low-pass genome sequencing (GS) has been widely used for the clinical diagnosis of germline structural variants, it is limited in paternity/maternity tests due to the inadequate read coverage for genotyping. Herein, we developed rapid paternity/maternity testing based on low-pass GS with trio-based and duo-based analytical modes provided. The optimal read-depth was determined as 1-fold per case regardless of sequencing read lengths, modes, and library construction methods by using 10 trios with confirmed genetic relationships. In addition, low-pass GS with different library construction methods and 1-fold read-depths were performed for 120 prenatal trios prospectively collected, and 1 trio was identified as non-maternity, providing a rate of MP of 0.83% (1/120). All results were further confirmed via quantitative florescent PCR. Overall, we developed a rapid, cost-effective, and sequencing platform-neutral paternity/maternity test based on low-pass GS and demonstrated the feasibility of its clinical use in confirming the parentage for genetic diagnosis.

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