Biochemistry and Molecular Genetics Department, Hospital Clinic of Barcelona, Barcelona, Spain.
CIBER of Rare Diseases (CIBERER), Instituto de Salud Carlos III, Madrid, Spain.
Clin Genet. 2020 Oct;98(4):379-383. doi: 10.1111/cge.13810. Epub 2020 Aug 4.
Chromosomal microarray analysis (CMA) has now replaced karyotyping in the analysis of prenatal cases with a fetal structural anomaly, whereas in those pregnancies undergoing invasive prenatal diagnosis with a normal fetal ultrasound, conventional karyotyping is still performed. The aims of this study were to establish the diagnostic yield of CMA in prenatal diagnosis, and to provide new data that might contribute to reconsider current practices. We reviewed 2905 prenatal samples with a normal rapid aneuploidy detection test referred for evaluation by CMA testing. Our study revealed pathogenic and reported susceptibility copy number variants associated with syndromic disorders in 4.8% (n = 138/2905) of cases, being 2.8% (n = 81/2905) the estimated added diagnostic value of CMA over karyotyping. Clinically significant CMA abnormality was detected in 5.4% (107/1975) of the fetuses with ultrasound anomalies and in 1.4% (5/345) of those considered as low-risk pregnancies. Our series shows that in prenatal samples, CMA increases 2-fold the diagnostic yield achieved by conventional karyotyping.
染色体微阵列分析(CMA)现已取代核型分析,成为胎儿结构异常产前病例的分析方法,而对于那些超声检查正常的接受有创性产前诊断的妊娠,仍进行传统核型分析。本研究旨在确定 CMA 在产前诊断中的诊断效果,并提供可能有助于重新考虑当前实践的新数据。我们回顾了 2905 例经快速非整倍体检测正常的产前样本,这些样本被转诊进行 CMA 检测。我们的研究显示,在 4.8%(n=138/2905)的病例中发现了与综合征疾病相关的致病性和报道的易感性拷贝数变异,CMA 相对于核型分析的额外诊断价值估计为 2.8%(n=81/2905)。在超声异常的胎儿中,有 5.4%(107/1975)的胎儿和在被认为低风险妊娠的胎儿中,有 1.4%(5/345)的胎儿检测到有临床意义的 CMA 异常。我们的系列研究表明,在产前样本中,CMA 将传统核型分析的诊断效果提高了两倍。
