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Exome sequencing of fetal anomaly syndromes: novel phenotype-genotype discoveries

机译:胎儿异常综合征的外壳测序:新型表型 - 基因型发现

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摘要

The monogenic etiology of most severe fetal anomaly syndromes is poorly understood. Our objective was to use exome sequencing (ES) to increase our knowledge on causal variants and novel candidate genes associated with specific fetal phenotypes. We employed ES in a cohort of 19 families with one or more fetuses presenting with a distinctive anomaly pattern and/or phenotype recurrence at increased risk for lethal outcomes. Candidate variants were identified in 12 families (63%); in 6 of them a definite diagnosis was achieved including known or novel variants in recognized disease genes (MKS1, OTX2, FGFR2, and RYR1) and variants in novel disease genes describing new fetal phenotypes (CENPF, KIF14). We identified variants likely causal after clinical and functional review (SMAD3, KIF4A, and PIGW) and propose novel candidate genes (PTK7, DNHD1, and TTC28) for early human developmental disease supported by functional and crossspecies phenotyping evidence. We describe rare and novel fetal anomaly syndromes and highlight the diagnostic utility of ES, but also its contribution to discovery. The diagnostic yield of the future application of prenatal ES will depend on our ability to increase our knowledge on the specific phenotype-genotype correlations during fetal development.
机译:最严重的胎生异常综合征的单一的病因尚未理解。我们的目标是使用Exome测序来增加我们对与特定胎儿表型相关的因果变体和新型候选基因的知识。我们在19个家庭的队列中雇用了eS,其中一种或多种胎儿具有独特的异常模式和/或表型复发,在增加致命结果的风险上。候选变体在12个家庭中鉴定(63%);在其中6中,实现了明确的诊断,包括已知的或新的变体在公认的疾病基因(MKS1,OTX2,FGFR2和RYR1)和描述新的胎儿表型(CENPF,KIF14)中的新型疾病基因中的变体。我们鉴定了临床和功能性审查(SMAD3,KIF4A和PIGW)后可能因果的变体,并提出了一种用于功能性和交叉表型证据的早期人类发育疾病的新型候选基因(PTK7,DNHD1和TTC28)。我们描述了罕见的胎生异常综合征,突出了es的诊断效用,也突出了它对发现的贡献。未来产前申请的诊断产量将取决于我们在胎儿发育过程中提高我们对特定表型基因型相关性的知识的能力。

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