Genetic diagnosis of common fetal renal abnormalities detected on prenatal ultrasound

产前诊断 羊水 多囊性发育不良肾 外显子组测序 胎儿 多囊肾病 拷贝数变化 遗传咨询 医学 基因检测 病理 生物 产科 怀孕 表型 内科学 遗传学 基因组 基因
作者
Ling Liu,Juan Li,Ying Li,Haiyu Li,Bo Yang,Hui Fan,Jing Wang,Yan Gu,Hui Yu,Maohuan Bai,Tan‐Tan Yu,Shihong Cui,Genyang Cheng,Chenchen Ren
出处
期刊:Prenatal Diagnosis [Wiley]
卷期号:42 (7): 894-900 被引量:7
标识
DOI:10.1002/pd.6154
摘要

This retrospective study aimed to investigate the correlations between phenotypes of fetal renal abnormalities on prenatal ultrasound and genetic aetiologies detected using chromosomal microarray analysis (CMA) and whole-exome sequencing (WES).Fetuses with renal abnormalities were subjected to CMA and were further analysed by WES when CMA-negative. The detection rates for chromosomal abnormalities and monogenic variants among different types of isolated renal abnormalities and those with extrarenal abnormalities (non-isolated cases) were determined and compared.CMA detected chromosomal abnormalities in 78 of 577 fetuses (13.52%). WES detected monogenic variants in 31 of 160 fetuses (19.38%) that had non-diagnostic CMA results. In cases of isolated hyperechogenic kidney, polycystic kidney disease, and multicystic dysplastic kidney, the detection rates of copy number variants (CNVs) by CMA and monogenic variants by WES were not significantly different (p > 0.05). However, monogenic variants were more frequently detected than CNVs when kidney abnormalities were accompanied by reduced amniotic fluid (p < 0.05). Other renal abnormalities identified on prenatal ultrasound had different detection rates.Our findings contribute to the overall knowledge of genetic variants associated with prenatally identified renal anomalies and may aid in decision making regarding prenatal genetic testing options for affected pregnancies.
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