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四个中国家庭中由基因复合杂合变异导致的伴或不伴多指(趾)畸形的短肋胸廓发育不良3型的基因分析及产前诊断

Genetic analysis and prenatal diagnosis of short-rib thoracic dysplasia 3 with or without polydactyly caused by compound heterozygous variants of gene in four Chinese families.

作者信息

Fang Yuying, Li Shuo, Yu Dongyi

机构信息

Center for Medical Genetics and Prenatal Diagnosis, Key Laboratory of Birth Defect Prevention and Genetic, Medicine of Shandong Health Commission, Key Laboratory of Birth Regulation and Control Technology of National Health Commission of China, Shandong Provincial Maternal and Child Health care Hospital affiliated to Qingdao University, Jinan, Shandong, China.

Genetic Testing Center, Qingdao Women and Children hospital, Qingdao, Shandong, China.

出版信息

Front Genet. 2023 Mar 17;14:1075187. doi: 10.3389/fgene.2023.1075187. eCollection 2023.

DOI:10.3389/fgene.2023.1075187
PMID:37007936
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10064095/
Abstract

To describe the genetic variation of dynein cytoplasmic 2 heavy chain 1 () gene in four Chinese families affected with short-rib thoracic dysplasia 3 with or without polydactyly (SRTD3), and to provide evidence for accurate prenatal diagnosis and genetic counseling. The detailed clinical prenatal sonographic features of four fetuses with SRTD3 were carried out. Trio-whole exome sequencing (WES) and proband-WES sequencing was applied to filtrated causative variants in four families. The causative variants of each family were validated in by Sanger sequencing. Bioinformation analysis was applied to predict the harmfulness of these mutations and perform the protein-protein interaction network and Gene Ontology (GO) analysis. A vitro minigene splicing assay was conducted to assess the influence of the splice site variant. Typical characterization of the four fetuses included short long bones, short ribs, narrow chest, hand and foot posture abnormalities, femur short in diameter and slightly bowing, cardiac abnormalities, and so on. Moreover, eight compound heterozygous variants of (NM_001080463.2): c.3842A>C (p.Tyr1281Ser) and c.8833-1G>A, c.8617A>G (p.Met2873Val) and c.7053_7054del (p.Cys2351Ter), c.5984C>T (p.Ala1995Val) and c.10219C>T (p.Arg3407Ter), c.5256del (p.Ala1753GlnfsTer13) and c.9737C>T (p.Thr3246Ile), were identified. Among which, c.10219C>T (p.Arg3407Terp), c.5984C>T (p.Ala1995Val) and c.9737C>T (p.Thr3246Ile) were reported in ClinVar databases, and c.8617A>G (p.Met2873Val), c.10219C>T (p.Arg3407Ter), c.5984C>T (p.Ala1995Val) were found in HGMD databases. Four variants (c.3842A>C (p.Tyr1281Ser), c.8833-1G>A, c.7053_7054del (p.Cys2351Ter) and c.5256del (p.Ala1753GlnfsTer13) were first reported as novel mutations. According to the ACMG guidelines, c.8617A>G (p.Met2873Val), c.7053_7054del (p.Cys2351Ter), c.5984C>T (p.Ala1995Val), c.10219C>T (p.Arg3407Ter) and c.5256del (p.Ala1753GlnfsTer13) were rated as pathogenic or likely pathogenic variants, others variants were predicted to be variants of uncertain significance mutations. The minigene assay results indicated that c.8833-1G>A caused the skipping over exon 56, resulting in exon 56 loss. In our study, we analyzed the genetic mutations in four fetuses with SRTD3 by whole exome sequencing and identified pathogenic variants causing SRTD3. Our results expand the mutation spectrum of in SRTD3, which is helpful for the accurate prenatal diagnosis of SRTD3 fetuses and provide useful strategies for genetic counseling.

摘要

描述四个患有或不患有多指(趾)畸形的短肋胸廓发育不良3型(SRTD3)中国家系中动力蛋白胞质2重链1()基因的遗传变异,为准确的产前诊断和遗传咨询提供依据。对4例SRTD3胎儿进行了详细的临床产前超声特征检查。采用三联体全外显子组测序(WES)和先证者WES测序对4个家系中的致病变异进行筛选。每个家系的致病变异通过桑格测序进行验证。应用生物信息学分析预测这些突变的危害性,并进行蛋白质-蛋白质相互作用网络和基因本体(GO)分析。进行体外小基因剪接试验以评估剪接位点变异的影响。4例胎儿的典型特征包括长骨短、肋骨短、胸廓狭窄、手足姿势异常、股骨直径短且轻度弯曲、心脏异常等。此外,共鉴定出8个(NM_001080463.2)的复合杂合变异:c.3842A>C(p.Tyr1281Ser)和c.8833-1G>A、c.8617A>G(p.Met2873Val)和c.7053_7054del(p.Cys2351Ter)、c.5984C>T(p.Ala1995Val)和c.10219C>T(p.Arg3407Ter)、c.5256del(p.Ala1753GlnfsTer13)和c.9737C>T(p.Thr3246Ile)。其中,c.10219C>T(p.Arg3407Terp)、c.5984C>T(p.Ala1995Val)和c.9737C>T(p.Thr3246Ile)已在ClinVar数据库中报道,c.8617A>G(p.Met2873Val)、c.10219C>T(p.Arg3407Ter)、c.5984C>T(p.Ala1995Val)在HGMD数据库中被发现。4个变异(c.3842A>C(p.Tyr1281Ser)、c.8833-1G>A、c.7053_7054del(p.Cys2351Ter)和c.5256del(p.Ala1753GlnfsTer13))首次作为新突变报道。根据美国医学遗传学与基因组学学会(ACMG)指南,c.8617A>G(p.Met2873Val)、c.7053_7054del(p.Cys2351Ter)、c.5984C>T(p.Ala1995Val)、c.10219C>T(p.Arg3407Ter)和c.5256del(p.Ala1753GlnfsTer13)被评为致病或可能致病变异,其他变异被预测为意义未明的变异。小基因试验结果表明,c.8833-1G>A导致外显子56跳跃,导致外显子56缺失。在本研究中,我们通过全外显子组测序分析了4例SRTD3胎儿的基因突变,并鉴定出导致SRTD3的致病变异。我们的结果扩展了SRTD3中基因的突变谱,有助于SRTD3胎儿的准确产前诊断,并为遗传咨询提供有用的策略。

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