通过无细胞DNA基因分型,有反复流产史和父母一方平衡重排史的夫妇中有多大比例可以被识别?

IF 1.3 4区 生物学 Q4 GENETICS & HEREDITY
Laura J C M van Zutven, Jona Mijalkovic, Monique van Veghel-Plandsoen, Margaret Goense, Marike Polak, Maarten F C M Knapen, Sabina de Weerd, Marieke Joosten, Karin E M Diderich, Lies H Hoefsloot, Diane Van Opstal, Malgorzata I Srebniak
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引用次数: 0

摘要

背景:据报道,约有1:30对反复妊娠丢失(RPL)夫妇出现平衡染色体畸变。父母双方的核型分析对于识别这些畸变是必要的。在复发性流产的情况下,全基因组无创产前检测(NIPT)可能是一种更有效的方法,可以识别携带平衡染色体重排风险增加的夫妇。本研究的目的是评估在我们中心检测到的由父母平衡畸变引起的潜在胎儿失衡是否足够大,可以通过全基因组无创产前检测(NIPT)检测到。材料和方法:从1970年1月到2020年5月,我们的实验室收到了30863份因RPL引起的独特的核型分析请求。我们已经鉴定了16045对夫妇,并评估了所有异常的细胞遗传学结果,以评估潜在不平衡重排产物中涉及的染色体片段的最小大小。结果:在所提出的队列中,我们在16045对RPL夫妇中检测到277对女性和185对男性的异常平衡易位/倒置,其风险为1:35(2.9%,95%CI 2.6-3.2%)。我们的研究表明,这些平衡畸变中的绝大多数(98.7%,95%CI 97.1-9.5%)可能会导致胎儿失衡 > 10Mb,如果在流产期间进行全基因组NIPT,则可以检测到。结论:我们的研究表明,全基因组NIPT能够揭示RPL夫妇携带的平衡染色体重排的大多数不平衡产物,因此可以潜在地识别平衡染色体畸变携带者。此外,我们的数据表明,这些夫妇可以接受NIPT,以防他们在未来的妊娠中拒绝侵入性检测。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

What proportion of couples with a history of recurrent pregnancy loss and with a balanced rearrangement in one parent can potentially be identified through cell-free DNA genotyping?

What proportion of couples with a history of recurrent pregnancy loss and with a balanced rearrangement in one parent can potentially be identified through cell-free DNA genotyping?

What proportion of couples with a history of recurrent pregnancy loss and with a balanced rearrangement in one parent can potentially be identified through cell-free DNA genotyping?

What proportion of couples with a history of recurrent pregnancy loss and with a balanced rearrangement in one parent can potentially be identified through cell-free DNA genotyping?

Background: Balanced chromosome aberrations are reported in about 1:30 couples with recurrent pregnancy loss (RPL). Karyotyping of both parents is necessary to identify these aberrations. Genome-wide non-invasive prenatal testing (NIPT) in case of recurrent pregnancy loss could be a more efficient way to identify couples at increased risk for carrying a balanced chromosome rearrangement. The aim of this study was to evaluate whether the potential fetal imbalances caused by parental balanced aberrations detected in our center are large enough to be detectable by genome-wide non-invasive prenatal testing (NIPT).

Material and methods: From January 1970 until May 2020 our laboratory received 30,863 unique requests for karyotyping due to RPL. We have identified 16,045 couples and evaluated all abnormal cytogenetic results to assess the minimal size of the involved chromosomal segments in potential unbalanced products of the rearrangements.

Results: In the presented cohort we detected 277 aberrant balanced translocations/inversions in females and 185 in males amongst 16,045 couples with RPL, which can be translated to a risk of 1:35 (2.9%, 95% CI 2.6-3.2%). Our study showed that the vast majority (98.7%, 95% CI 97.1-99.5%) of these balanced aberrations will potentially cause a fetal imbalance > 10 Mb, which is detectable with genome-wide NIPT if it was performed during one of the miscarriages.

Conclusions: Our study suggests that genome-wide NIPT is able to reveal most unbalanced products of balanced chromosomal rearrangements carried by couples with RPL and therefore can potentially identify balanced chromosomal aberration carriers. Moreover, our data suggest that these couples can be offered NIPT in case they decline invasive testing in future pregnancies.

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来源期刊
Molecular Cytogenetics
Molecular Cytogenetics GENETICS & HEREDITY-
CiteScore
2.60
自引率
7.70%
发文量
49
审稿时长
>12 weeks
期刊介绍: Molecular Cytogenetics encompasses all aspects of chromosome biology and the application of molecular cytogenetic techniques in all areas of biology and medicine, including structural and functional organization of the chromosome and nucleus, genome variation, expression and evolution, chromosome abnormalities and genomic variations in medical genetics and tumor genetics. Molecular Cytogenetics primarily defines a large set of the techniques that operate either with the entire genome or with specific targeted DNA sequences. Topical areas include, but are not limited to: -Structural and functional organization of chromosome and nucleus- Genome variation, expression and evolution- Animal and plant molecular cytogenetics and genomics- Chromosome abnormalities and genomic variations in clinical genetics- Applications in preimplantation, pre- and post-natal diagnosis- Applications in the central nervous system, cancer and haematology research- Previously unreported applications of molecular cytogenetic techniques- Development of new techniques or significant enhancements to established techniques. This journal is a source for numerous scientists all over the world, who wish to improve or introduce molecular cytogenetic techniques into their practice.
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