Juno Genetics-US, Genetic Lab, Basking Ridge, New Jersey.
Juno Genetics-Italy, Reproductive Genetics, Rome, Italy.
Fertil Steril. 2024 Nov;122(5):789-798. doi: 10.1016/j.fertnstert.2024.07.008. Epub 2024 Jul 10.
To evaluate the technical accuracy, inheritance, and pathogenicity of small copy number variants (CNVs) detected by a targeted next-generation sequencing-based preimplantation genetic testing for aneuploidy (PGT-A) platform.
Retrospective observational study performed between 2020 and 2022.
Clinic.
PATIENT(S): A total of 12,157 patients who underwent clinical PGT-A performed by targeted next-generation sequencing for whole chromosome and large segmental aneuploidies.
INTERVENTION(S): An incidental finding was reported when a CNV gain/loss of at least 3 consecutive amplicons appeared in at least 2 embryos from the same in vitro fertilization cycle.
MAIN OUTCOME MEASURE(S): The primary outcome measures were the specificity, incidence, inheritance, and pathogenicity of small CNVs detected by the PGT-A platform. Accuracy of the PGT-A platform CNV calls was assessed via concordance with the CNV calls (size and genomic location) on chromosomal microarray of the gamete provider(s). Parental origin of the CNV and pathogenicity classifications were also reported.
RESULT(S): An incidental finding that met reporting criteria was identified in 75 (0.62%; 95% confidence interval, 0.5%-0.8%) of 12,157 unique PGT-A patients. Chromosomal microarray follow-up was requested for all cases, and results were received for 1 or both members of 65 reproductive couples. In all cases, 1 of the gamete providers was confirmed to have the CNV identified in the embryos (100.0%, N = 65/65; 95% confidence interval, 94.5-100). The identified CNV was of maternal origin in 34 cases (52.3%) and of paternal origin in 31 cases (47.7%). A significant correlation was identified between PGT-A-predicted CNV sizes and chromosomal microarray detected sizes (r = 0.81) and genomic coordinates on parental deoxyribonucleic acid. Twenty-six (40%) of the CNVs were classified as benign/likely benign, 30 (46.2%) as a variant of uncertain significance, and 9 (13.8%) as pathogenic/likely pathogenic.
CONCLUSION(S): Certain PGT-A platforms may enable the detection of inherited, small CNVs with extremely high specificity without prior knowledge of parental status. Most CNVs in this data set were confirmed to be benign/likely benign or a variant of uncertain significance. Pathogenic/likely pathogenic CNVs associated with a broad range of phenotypic features may also be detected, although a reliable negative predictive value for small CNVs with current PGT-A technologies is unknown because of the many technical challenges.
评估基于靶向下一代测序的胚胎植入前非整倍体检测(PGT-A)的技术准确性、遗传和致病性的小拷贝数变异(CNVs)。
2020 年至 2022 年进行的回顾性观察研究。
诊所。
共 12157 名患者接受了靶向全染色体和大片段非整倍性的下一代测序的临床 PGT-A。
当至少 2 个来自同一体外受精周期的胚胎中出现至少 3 个连续扩增子的 CNV 增益/缺失时,报告偶然发现。
PGT-A 平台检测到的小 CNVs 的特异性、发生率、遗传和致病性是主要观察指标。通过与配子提供者的染色体微阵列上的 CNV 调用(大小和基因组位置)的一致性评估 PGT-A 平台 CNV 调用的准确性。还报告了 CNV 的亲本来源和致病性分类。
在 12157 名独特的 PGT-A 患者中,发现了符合报告标准的偶然发现 75 例(0.62%;95%置信区间,0.5%-0.8%)。所有病例均要求进行染色体微阵列随访,并且在 65 对生殖夫妇中的 1 对或 2 对中收到了结果。在所有情况下,1 个配子提供者的 CNV 与胚胎中检测到的 CNV 一致(100.0%,N=65/65;95%置信区间,94.5-100)。在 34 例(52.3%)中,鉴定的 CNV 为母源,在 31 例(47.7%)中为父源。PGT-A 预测的 CNV 大小与染色体微阵列检测到的大小(r=0.81)和父母 DNA 的基因组坐标之间存在显著相关性。26 例(40%)的 CNVs 被归类为良性/可能良性,30 例(46.2%)为意义不明的变异,9 例(13.8%)为致病性/可能致病性。
某些 PGT-A 平台可能能够在没有事先了解父母情况的情况下,以极高的特异性检测到遗传的小 CNVs。本数据集中的大多数 CNVs 被证实为良性/可能良性或意义不明的变异。也可能检测到与广泛表型特征相关的致病性/可能致病性 CNVs,尽管由于存在许多技术挑战,目前 PGT-A 技术中小 CNVs 的可靠阴性预测值尚不清楚。
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