Analysis of families with fetal congenital abnormalities but negative prenatal diagnosis by whole exome sequencing

产前诊断 医学 胎儿 外显子组测序 回顾性队列研究 前瞻性队列研究 产科 怀孕 生物 妇科 内科学 遗传学 表型 基因
作者
Fen Fu,L S Li,Kun Du,Rufei Li,Qiuxia Yu,Dingding Wang,Tingying Lei,Qiong Deng,Zhiqiang Nie,W W Zhang,Xin Yang,Jin Han,Zhen Li,Min Pan,L N Zhang,Fangli Li,Y L Zhang,Xiangyi Jing,D-Z. Li,Can Liao
出处
期刊:Chinese Journal of Obstetrics and Gynecology 卷期号:56 (7): 458-466 被引量:1
标识
DOI:10.3760/cma.j.cn112141-20210118-00028
摘要

Objective: To evaluate the value of whole exome sequencing (WES) in prenatal clinical application. Methods: A total of 1 152 cases of congenital abnormal [including structural malformation, nuchal translucency (NT) thickening and intrauterine growth restriction] with traditional prenatal diagnosis [including G-band karyotype analysis and chromosome microarray analysis (CMA)] negative were analyzed. The congenital abnormal fetuses were divided into retrospective group and prospective group according to the time of WES detection, that is whether the pregnancy termination or not. According to the specific location of fetal malformation and their family history, the cohort was divided into subgroups. The clinical prognosis of all fetuses were followed up, and the effect of WES test results on pregnancy decision-making and clinical intervention were analyzed. According to the follow-up results, the data of fetuses with new phenotypes in the third trimester or after birth were re-analyzed. Results: Among 1 152 families who received WES, 5 families were excluded because of nonbiological parents. Among the remaining 1 147 families, 152 fetuses obtained positive diagnosis (13.3%,152/1 147), including 74 fetuses in the retrospective group (16.1%,74/460) and 78 fetuses in the prospective group (11.4%,78/687). In fetuses with negative CMA and G-band karyotype analysis results but new phenotypes in the third trimester or after birth, the positive rate by WES data re-analysis was 4.9% (8/163). A total of 34 (21.3%, 34/160) fetuses were directly affected by the corresponding positive molecular diagnosis. Among 68 cases of live births with diagnostic variation grade 4, 29 cases (42.7%, 29/68) received appropriate medical intervention through rapid review of WES results. Conclusions: WES could increase the detection rate of abnormal fetuses with negative G-banding karyotype analysis and CMA by 13.3%. Prenatal WES could guide pregnancy decision-making and early clinical intervention. It might be an effective strategy to pay attention to the special follow-up of the third trimester and postnatal fetus and to re-analyze the WES data.
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