Sequential prenatal diagnosis of fetal skeletal dysplasia: A cohort study

IF 3.5 2区医学 Q1 OBSTETRICS & GYNECOLOGY

Acta Obstetricia et Gynecologica Scandinavica Pub Date : 2025-03-04 DOI:10.1111/aogs.15095

Mengting Jiang, Bin Zhang, Jing Wang, Wei Qiao, Xiuzhen Mao, Bin Yu

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引用次数: 0

Abstract

Introduction

Genetic factors are considered to be the main factors leading to fetal skeletal dysplasia (SD), and chromosomal microarray analysis (CMA) has been used clinically for the detection of SD fetuses. At present, whole exome sequencing (WES) has been applied in SD fetuses, but there is still a lack of data accumulation. The aim of this study is to perform sequential prenatal diagnosis for fetuses with SD indicated by ultrasound and to explore the clinical value of CMA followed by WES.

Material and Methods

From January 2019 to May 2024, 147 fetuses with SD were detected by prenatal ultrasound screening. After the collection of amniotic fluid or abortive tissue, CMA was performed first, then WES was performed in the cases with a negative CMA result.

Results

147 cases accepted the prenatal CMA test, and 23 cases were reported to have chromosomal abnormalities, including 9 cases of chromosomal aneuploidies, 11 cases of pathogenic copy number variants, and 3 cases of likely pathogenic copy number variants. The detection rate of chromosomal abnormalities by the prenatal CMA test was 15.6% (23/147). 58 cases with negative results of CMA underwent WES, and 21 genes with pathogenic/likely pathogenic variants were detected in 21 cases, including FGFR3, COL2A1, COL1A1, COL1A2, RUNX2, LMX1B, GLI3, SHOX, ALPL, and DYNC2H1. The rate of abnormal prenatal WES was 36.2% (21/58). In the subgroup analysis of the SD phenotype, the detection rate of chromosomal abnormalities in isolated SD fetuses was 7.7% (7/91), which was significantly lower than that in SD fetuses combined with other system abnormalities (28.6%, 16/56) (p = 0.001). The detection rate of monogenic abnormalities in short long bones with other skeletal abnormalities was 62.5% (10/16), which was higher than that in short long bones with non-skeletal abnormalities 10.5% (2/19), and the difference was statistically significant (p = 0.003).

Conclusions

SD is mostly caused by monogenic abnormalities, and prenatal WES has significantly improved the detection rate of SD fetuses. The prenatal WES can be used as an important molecular genetic testing method combined with CMA in the sequential prenatal diagnosis of SD fetuses.

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胎儿骨骼发育不良的顺序产前诊断：一项队列研究。

遗传因素被认为是导致胎儿骨骼发育不良（SD）的主要因素，染色体微阵列分析（CMA）已在临床上用于检测SD胎儿。目前，全外显子组测序（WES）已应用于SD胎儿，但仍缺乏数据积累。本研究的目的是对超声指示的SD胎儿进行序贯产前诊断，探讨CMA后WES的临床价值。材料与方法：2019年1月至2024年5月，对147例SD胎儿进行产前超声筛查。收集羊水或流产组织后，先行CMA， CMA阴性者再行WES。结果：147例接受产前CMA检查，报告染色体异常23例，其中染色体非整倍体9例，致病性拷贝数变异11例，可能致病性拷贝数变异3例。产前CMA检查染色体异常检出率为15.6%（23/147）。58例CMA阴性患者行WES检测，其中21例检测到致病性/可能致病性变异基因，包括FGFR3、COL2A1、COL1A1、COL1A2、RUNX2、LMX1B、GLI3、SHOX、ALPL和DYNC2H1。产前WES异常率为36.2%（21/58）。在SD表型亚组分析中，分离SD胎儿染色体异常检出率为7.7%(7/91)，显著低于合并其他系统异常的SD胎儿（28.6%,16/56）（p = 0.001）。短长骨合并其他骨骼异常的单基因异常检出率为62.5%(10/16)，高于短长骨合并非骨骼异常的10.5%(2/19)，差异有统计学意义（p = 0.003）。结论：SD多由单基因异常引起，产前WES显著提高了SD胎儿的检出率。产前WES结合CMA可作为一种重要的分子遗传学检测方法用于SD胎儿的产前序贯诊断。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Acta Obstetricia et Gynecologica Scandinavica 医学-妇产科学

CiteScore

8.00

自引率

4.70%

发文量

180

审稿时长

3-6 weeks

期刊介绍： Published monthly, Acta Obstetricia et Gynecologica Scandinavica is an international journal dedicated to providing the very latest information on the results of both clinical, basic and translational research work related to all aspects of women’s health from around the globe. The journal regularly publishes commentaries, reviews, and original articles on a wide variety of topics including: gynecology, pregnancy, birth, female urology, gynecologic oncology, fertility and reproductive biology.