Third-Generation Single-Molecule Sequencing for Preimplantation Genetic Testing of Aneuploidy and Segmental Imbalances

纳米孔测序 仆从 非整倍体 纳米孔 生物 遗传学 DNA测序 分子生物学 基因 材料科学 纳米技术 染色体
作者
Vivienne J. Tan,Timing Liu,Zainul Arifin,Beatrice Pak,Arnold S.C. Tan,S. M. Wong,Chiea Chuen Khor,Henry Yang,Caroline Lee,Zhongwei Huang,Mahesh Choolani,Samuel S. Chong
出处
期刊:Clinical Chemistry [American Association for Clinical Chemistry]
卷期号:69 (8): 881-889 被引量:6
标识
DOI:10.1093/clinchem/hvad062
摘要

Abstract Background Current strategies for preimplantation genetic testing for aneuploidy or structural rearrangements (PGT-A/SR) rely mainly on next-generation sequencing (NGS) and microarray platforms, which are robust but require expensive instrumentation. We explored the suitability of third-generation single-molecule sequencing as a PGT-A/SR screening platform for both aneuploidy and segmental imbalance. Methods Single-cell and multicell replicates from aneuploid or segmentally unbalanced cell lines (n = 208) were SurePlex-amplified, randomized, and subjected to (a) Nanopore-based single-molecule sequencing (Oxford Nanopore Technologies) and (b) NGS using a leading commercial PGT-A solution (Illumina VeriSeq PGS). Archival SurePlex-amplified trophectoderm biopsy samples (n = 96) previously analyzed using the commercial kit were blinded and reanalyzed using Nanopore. Results Nanopore-based PGT-A identified the specific aberration in 95.45% (84/88) and 97.78% (88/90) of single-/multicells with an aneuploidy or segmental imbalance (10–30.5 Mb), respectively. Comparison against the commercial kit’s results revealed concordances of 98.86% (87/88) and 98.89% (89/90) for the aneuploid and segmentally unbalanced (10–30.5 Mb aberration) samples, respectively. Detection sensitivity for smaller segmental imbalances (5–5.8 Mb aberration, n = 30) decreased markedly on both platforms. Nanopore-based PGT-A reanalysis of trophectoderm biopsy samples was 97.92% (94/96) concordant with the commercial kit results. Conclusion Up to 24 SurePlex-amplified single-cell, multicell, or trophectoderm samples could be sequenced in a single MinION flow-cell for subsequent preimplantation genetic testing for aneuploidy or structural rearrangements (PGT-A/SR) analysis, with results obtainable in ≤3 days and at per-sample costs that are competitive with commercial offerings. Nanopore’s third-generation single-molecule sequencing represents a viable alternative to current commercial NGS-based PGT-A solutions for aneuploidy and segmental imbalance (≥10 Mb) screening of single-/multicell or trophectoderm biopsy samples.

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