宋婷婷; 郑娇; 黎昱; 李佳; 徐盈; 郭芬芬; 杨红

doi:10.3760/cma.j.cn113903-20220816-00770

点赞 0
分享 0
收藏 0
纠错

• 论著 •

22q11.21微缺失与微重复综合征的产前临床表型分析及遗传咨询

中华围产医学杂志, 2023,26(4) : 286-291. DOI: 10.3760/cma.j.cn113903-20220816-00770

摘要

目的

探讨产前诊断22q11.21微缺失与微重复胎儿的不同临床表型、妊娠结局，为临床遗传咨询提供依据。

方法

回顾性分析2015年1月至2022年1月在空军军医大学第一附属医院产前诊断中心因超声检查异常、高龄、血清学筛查高风险等行介入性产前诊断，应用染色体微阵列分析（chromosome microarray analysis，CMA）技术确诊的22q11.21微缺失或微重复病例。对其临床表型及妊娠结局进行描述性分析。

结果

研究期间，共9 141例行CMA检测的病例中，有77例（0.8%）为22q11.21微缺失或微重复胎儿。77例中，62例（80.5%）为22q11.21微缺失，包括58例典型区域缺失和4例非典型区域缺失（均包含与先天性心脏病明确相关的TBX1基因）；15例（19.5%）为22q11.21微重复，包括14例典型区域重复和1例非典型区域重复。62例22q11.21微缺失胎儿中，48例（77.4%）伴有先天性心脏病，其中28例为圆锥动脉干畸形；15例22q11.21微重复胎儿中，5例伴有先天性心脏病。预产期后3~6个月进行电话随访，62例22q11.21微缺失胎儿中，52例终止妊娠，5例失访，5例出生（1例早产出生后1个月死亡，1例生后伴肛门前移及发育迟缓，3例随访未见明显异常）；15例22q11.21微重复胎儿中，4例终止妊娠，2例失访，9例出生（8例随访未见明显异常，1例发育迟缓）。

结论

应用CMA对22q11.21微缺失与微重复胎儿进行产前诊断，并结合超声诊断综合分析其临床表现及妊娠结局，对指导妊娠、患儿出生后的治疗康复均具有重要意义，孕期需结合超声检查进行遗传咨询综合考虑、谨慎处理。

引用本文: 宋婷婷, 郑娇, 黎昱, 等. 22q11.21微缺失与微重复综合征的产前临床表型分析及遗传咨询 [J] . 中华围产医学杂志, 2023, 26(4) : 286-291. DOI: 10.3760/cma.j.cn113903-20220816-00770.

参考文献导出: Endnote NoteExpress RefWorks NoteFirst 医学文献王

扫描看全文

正文

作者信息

基金 0 关键词 0

English Abstract

阅读 0 评论 0

相关资源

引用 | 论文 | 视频

版权归中华医学会所有。

未经授权，不得转载、摘编本刊文章，不得使用本刊的版式设计。

除非特别声明，本刊刊出的所有文章不代表中华医学会和本刊编委会的观点。

22q11.21微缺失微重复是22号染色体上的低拷贝重复序列（low-copy repeats，LCRs）介导的非等位基因同源重组所造成的^［1］。22q11.21微缺失综合征在临床上较为常见，在活产婴儿中发病率为1/4 000，为最常见的染色体微缺失综合征，但该病的临床表现复杂多样，主要表现有心脏畸形、异常面容、胸腺发育不良或缺如、低血钙症、发育迟缓、腭裂、智力低下等^{［2, 3, 4］}。22q11.21微重复的发病率及报道相对较少，临床表现多样，从正常或轻微异常到严重畸形伴智力发育迟缓、行为异常、多发性先天异常、生长发育迟缓等，部分个体的表型与22q11.21微缺失相重叠，这为临床遗传咨询带来巨大挑战。目前，产前诊断22q11.21微缺失微重复胎儿合并先天性心脏病的具体类型尚不明确，是否合并心外其他类型异常也尚不明确。本研究对62例22q11.21微缺失胎儿及15例22q11.21微重复胎儿的产前诊断指征、超声检查结果、妊娠结局等进行分析，为遗传咨询提供理论依据。

贡献者信息

宋婷婷

空军军医大学第一附属医院妇产科，西安　710032

郑娇

空军军医大学第一附属医院妇产科，西安　710032

黎昱

空军军医大学第一附属医院妇产科，西安　710032

李佳

空军军医大学第一附属医院妇产科，西安　710032

徐盈

空军军医大学第一附属医院妇产科，西安　710032

郭芬芬

空军军医大学第一附属医院妇产科，西安　710032

杨红

空军军医大学第一附属医院妇产科，西安　710032

通信作者

杨红

空军军医大学第一附属医院妇产科，西安　710032

Email：yanghongfck@163.com

关键词

染色体，人，22对; 染色体缺失; 染色体重复; 产前诊断; 微阵列分析; 遗传咨询;

基金项目

西安市创新能力强基计划-医学研究项目（21YXYJ0106）

作者声明

作者贡献声明

宋婷婷、郑娇：论文撰写、数据分析、经费支持；黎昱、徐盈、郭芬芬：实验操作、数据整理、统计学分析；李佳、杨红：研究指导、论文修改

利益冲突

利益冲突：

所有作者声明无利益冲突

历史

出版日期：2023-04-16

收稿日期：2022-08-16

本文编辑

夏乐

Original Article

Prenatal phenotypic analysis and genetic counseling for 22q11.21 microdeletion and microduplication syndrome

Tingting Song, Jiao Zheng, Yu Li, Jia Li, Ying Xu, Fenfen Guo, Hong Yang

Published 2023-04-16

Cite as Chin J Perinat Med, 2023, 26(4): 286-291. DOI: 10.3760/cma.j.cn113903-20220816-00770

Abstract

Objective

To analyze the prenatal clinical phenotypes and pregnancy outcomes of fetuses with 22q11.21 microdeletion and microduplication syndrome to provide a basis for clinical genetic counseling.

Methods

This retrospective study involved the cases diagnosed with 22q11.21 microdeletion or microduplication by chromosomal microarray analysis (CMA) due to abnormal ultrasound findings, advanced maternal age, or high-risk pregnancies indicated by serum screening in the Prenatal Diagnosis Center of the First Affiliated Hospital of Air Force Medical University from January 2015 to January 2022. Clinical phenotypes and pregnancy outcomes of the fetuses were analyzed and described.

Results

Among 9 141 cases referred for CMA during the study period, 77 cases (0.8%) were diagnosed as 22q11.21 microdeletion or microduplication, including 62 (80.5%) with 22q11.21 microdeletion and 15 (19.5%) with microduplication. In the 22q11.21 microdeletion cases, 58 had typical deletion, and four had atypical deletions, but all fetuses carried TBX1 gene that was clearly associated with congenital heart disease. The 15 fetuses with 22q11.21 microduplication including 14 in the typical region and one in the atypical region. Forty-eight (77.4%) out of the 62 fetuses with 22q11.21 microdeletion were complicated by congenital heart defects, including 28 with conotruncal defects. Five of the 15 fetuses with 22q11.21 microduplication were complicated by congenital heart defects. The cases were followed up on telephone at three to six months after the expected date of delivery. Among the 62 cases with 22q11.21 microdeletion, 52 terminated pregnancies, five were lost to follow-up, and five were delivered (one died after one month of premature delivery, one was born with anal advancement and growth retardation, and three were followed up without obvious abnormality). Among the 15 cases with 22q11.21 microduplication, four terminated pregnancies, two were lost to follow-up, and nine gave birth (eight were followed up without obvious abnormality, one grew slowly).

Conclusions

The application of CMA in the prenatal diagnosis of 22q11.21 microdeletion and microduplication fetuses, and the comprehensive analysis of clinical manifestations and pregnancy outcome combined with ultrasonic diagnosis are of great significance in guiding the treatment and rehabilitation after birth of an affected child. Genetic counseling for cases with 22q11.21 microdeletion and microduplication syndrome should be cautious and consider ultrasound findings.

Key words:

Chromosomes, human, pair 22; Chromosome deletion; Chromosome duplication; Prenatal diagnosis; Microarray analysis; Genetic counseling

Contributor Information

Tingting Song