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The introduction of arrays in prenatal diagnosis: a special challenge.

机译:在产前诊断中引入阵列:一个特殊的挑战。

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Genome-wide arrays are rapidly replacing conventional karyotyping in postnatal cytogenetic diagnostics and there is a growing request for arrays in the prenatal setting. Several studies have documented 1-3% additional abnormal findings in prenatal diagnosis with arrays compared to conventional karyotyping. A recent meta-analysis demonstrated that 5.2% extra diagnoses can be expected in fetuses with ultrasound abnormalities. However, no consensus exists as to whether the use of genome-wide arrays should be restricted to pregnancies with ultrasound abnormalities, performed in all women undergoing invasive prenatal testing or offered to all pregnant women. Moreover, the interpretation of array results in the prenatal situation is challenging due to the large numbers of copy number variants with no major phenotypic effect. This also raises the question of what, or what not to report, for example, how to deal with unsolicited findings. These issues were discussed at a working group meeting that preceded the European Society of Human Genetics 2011 Conference in Amsterdam. This article is the result of this meeting and explores the introduction of genome-wide arrays into routine prenatal diagnosis. We aim to give some general recommendations on how to develop practical guidelines that can be implemented in the local setting and that are consistent with the emerging international consensus.
机译:全基因组阵列正在迅速取代产后细胞遗传学诊断中的常规核型分析,并且在产前环境中对阵列的需求日益增长。几项研究已证明,与常规核型分析相比,使用阵列进行产前诊断可额外增加1-3%的异常发现。最近的一项荟萃​​分析表明,超声异常胎儿的诊断率有望提高5.2%。但是,关于是否应将全基因组阵列的使用仅限于超声异常妊娠,在所有接受侵入性产前检查的妇女中进行或向所有孕妇提供,尚无共识。此外,由于大量拷贝数变异体没有重大表型效应,因此对产前情况的阵列结果的解释具有挑战性。这也引起了一个问题,例如,什么或不报告什么,如何处理未经请求的发现。在2011年阿姆斯特丹欧洲人类遗传学会会议之前的一个工作组会议上讨论了这些问题。本文是本次会议的结果,并探讨了将全基因组阵列引入常规产前诊断的方法。我们旨在就如何制定可在当地环境中实施并与正在形成的国际共识保持一致的实用指南提供一些一般性建议。

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