Noninvasive prenatal test for <i>FGFR3</i>‐related skeletal dysplasia based on next‐generation sequencing and plasma cell‐free DNA: Test performance analysis and feasibility exploration

Ren, Yuan; Zhao, Jia; Li, Ruibin; Xie, Yifan; Jiang, Sufei; Zhou, Honghui; Liu, Hongtai; You, Yanqin; Chen, Fang; Wang, Wei; Gao, Ya; Meng, Yuanguang; Lu, Yanping

doi:10.1002/pd.5334

Cited by 11 publications

(10 citation statements)

References 23 publications

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“…This further emphasises the need to involve the clinical geneticist in the prenatal evaluation of these conditions. For achondroplasia, thanatophoric dysplasia, and Apert syndrome, as well as selected other syndromes, definitive molecular diagnosis can be achieved using NIPD and analysis of cell‐free DNA in maternal blood . Of greater potential utility, but requiring invasive testing, is exome sequencing, which has the ability to screen affected pregnancies for multiple mutations in many genes, thereby increasing the possibility of arriving at a definitive diagnosis in a timely fashion in pregnancy.…”

Section: Molecular Diagnosismentioning

confidence: 99%

“…39 Both 2D and 3D ultrasonography have limitations in the presence of a high maternal body mass index, excessive fetal movements and thoracic shadowing, particularly at later gestational ages. These limitations can to some extent be [44][45][46] Of greater potential utility, but requiring invasive testing, is exome sequencing, which has the ability to screen affected pregnancies for multiple mutations in many genes, 47 thereby increasing the possibility of arriving at a definitive diagnosis in a timely fashion in pregnancy. Exome sequencing with variant interpretation focused on a virtual panel of genes known to cause skeletal dysplasias has been shown to have a diagnostic yield as high as 83% in fetuses suspected of having a skeletal dyplasia.…”

Section: Other Imaging Aids To Sonographic Diagnosis Of Skeletal Dymentioning

confidence: 99%

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A sonographic approach to the prenatal diagnosis of skeletal dysplasias

Pajkrt

Chitty

2019

Prenatal Diagnosis

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Skeletal dysplasias are a heterogeneous group of conditions, many of which present unexpectedly in the prenatal period with a variety of ultrasound findings. Accurate prenatal diagnosis can now be facilitated using exome sequencing approaches, but in order to interpret results, accurate and detailed phenotyping is required. Here, we describe the sonographic approach to the prenatal diagnosis of skeletal abnormalities and illustrate how taking a systematic approach can facilitate diagnosis.

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Section: Molecular Diagnosismentioning

confidence: 99%

Section: Other Imaging Aids To Sonographic Diagnosis Of Skeletal Dymentioning

confidence: 99%

A sonographic approach to the prenatal diagnosis of skeletal dysplasias

Pajkrt

Chitty

2019

Prenatal Diagnosis

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“…[4][5][6] Recently, noninvasive detection of the de novo mutations causing certain autosomal dominant disease has been determined to have clinical significance. 7 Meanwhile, several studies have demonstrated the detection of fetal monogenic diseases by analyzing cfDNA using quantitative polymerase chain reaction (qPCR), digital PCR, or haplotype-assisted approaches. [8][9][10][11][12][13] The detection of monogenic diseases with such methods provides the full genotype assessment of fetus, and certain method such as the haplotype-based approaches can even interpret the inheritance of the maternal allele.…”

Section: Introductionmentioning

confidence: 99%

Simultaneous detection of fetal aneuploidy, de novoFGFR3 mutations and paternally derived β‐thalassemia by a novel method of noninvasive prenatal testing

Yang

et al. 2021

Prenatal Diagnosis

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Objective: The aim is to develop a novel noninvasive prenatal testing (NIPT) method that simultaneously performs fetal aneuploidy screening and the detection of de novo and paternally derived mutations. Methods: A total of 68 pregnancies, including 26 normal pregnancies, 7 cases with fetal aneuploidies, 7 cases with fetal achondroplasia or thanatophoric dysplasia, 18 cases with fetal skeletal abnormalities, and 10 cases with β-thalassemia high risk were recruited. Plasma cell-free DNA was amplified by Targeted And Genome-wide simultaneous sequencing (TAGs-seq) to generate around 99% of total reads covering the whole-genome region and around 1% covering the target genes. The reads on the whole-genome region were analyzed for fetal aneuploidy using a binary hypothesis T-score and the reads on target genes were analyzed for point mutations by calculating the minor allelic frequency of loci on FGFR3 and HBB. TAGs-seq results were compared with conventional NIPT and diagnostic results. Results: In each sample, TAGs-seq generated 44.7-54 million sequencing reads covering the whole-genome region of 0.1-3� and the target genes of >1000�depth. All cases of fetal aneuploidy and de novo mutations of achondroplasia/thanatophoric dysplasia were identified with high sensitivities and specificities except for one false-negative paternal mutation of β-thalassemia. Conclusions: TAGs-seq is a novel NIPT method that combines the fetal aneuploidy screening and the detection of de novo FGFR3 mutations and paternal HBB mutations. Lin Yang and Yujing Wu joint first authors. This is an open access article under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non-commercial and no modifications or adaptations are made.

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“…Remarkably, 70% of the tests to date have been done on Chinese women. While the majority of cell‐free DNA tests are performed for the common fetal autosomal and sex chromosome aneuploidies, the test menus have expanded to include microdeletions, copy number variations, and single gene disorders . In an extraordinary study published in October 2018, Liu and colleagues performed a large‐scale population analysis using shallow sequencing data from 141 431 NIPTs performed at the Beijing Genome Institute in Shenzhen .…”

Section: Introductionmentioning

confidence: 99%

In case you missed it: The prenatal diagnosis editors bring you the most significant advances of 2018

et al. 2019

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Noninvasive prenatal test for FGFR3‐related skeletal dysplasia based on next‐generation sequencing and plasma cell‐free DNA: Test performance analysis and feasibility exploration

Abstract: Our method had a favorable performance for noninvasively detecting fetal FGFR3 mutations in maternal plasma, highlighting its promising value in developing a noninvasive prenatal test for de novo and paternally inherited disorders.

Cited by 11 publications

References 23 publications

A sonographic approach to the prenatal diagnosis of skeletal dysplasias

A sonographic approach to the prenatal diagnosis of skeletal dysplasias

Simultaneous detection of fetal aneuploidy, de novoFGFR3 mutations and paternally derived β‐thalassemia by a novel method of noninvasive prenatal testing

In case you missed it: The prenatal diagnosis editors bring you the most significant advances of 2018

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