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Chromosomal Microarray Analysis versus Karyotyping in Fetuses with Increased Nuchal Translucency

机译:染色体微阵列分析与胎儿的核型分析增加,颈部半透明增加

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摘要

We have carried out a retrospective study of chromosome anomalies associated with increased nuchal translucency (NT) in order to compare yield rates of karyotype, chromosome microarray analysis (CMA), and non-invasive prenatal testing (NIPT) in this condition. Presenting with increased NT or cystic hygroma ≥3.5 mm as an isolated sign, 249 fetuses underwent karyotype and/or CMA from 11 to 18 gestational weeks. Karyotype and fluorescence in situ hybridization (FISH) analyses detected 103 chromosomal anomalies including 95 aneuploidies and eight chromosomal rearrangements or derivatives. Further, seven pathogenic copy number variants (CNV), five likely pathogenic CNVs, and 15 variants of unknown significance (VOUS) were detected by CMA in fetuses with normal karyotype. Genetic testing is now facing new challenges due to results with uncertain clinical impacts. Additional investigations will be necessary to interpret these findings. More than 15% of the anomalies that we have diagnosed with invasive techniques could not be detected by NIPT. It is therefore definitely not recommended in the case of ultrasound anomalies. These results, while corroborating the use of CMA in fetuses with increased NT as a second tier after rapid aneuploidy testing, do not suggest a dismissal of karyotype analysis.
机译:我们已经对核心半透明(NT)相关的染色体异常进行了回顾性研究,以比较核型,染色体微阵列分析(CMA)和非侵入性产前试验(NIPT)的产量率。随着NT或囊性酸度升高而≥3.5mm作为分离的标志,249胎儿接受核型和/或CMA,从11到18个妊娠周。核型和荧光原位杂交(鱼)分析检测到103个染色体异常,包括95个非血糖倍增物和八种染色体重排或衍生物。此外,通过正常核型中的CMA检测七种致病拷贝数变体(CNV),五种可能的致病CNV和15个未知意义(VOUS)的变体。由于临床影响不确定,遗传测试现在面临新的挑战。需要额外的调查来解释这些调查结果。 NIPT无法检测到我们诊断出侵入性技巧的异常的15%以上。因此,在超声异常的情况下绝对不推荐。这些结果,同时证实在胎儿中使用CMA的使用随着快速的空转测试后作为第二层的胎儿,并不意味着解雇核型分析。

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