Clinical exome sequencing for fetuses with ultrasound abnormalities and a suspected Mendelian disorder

Normand, Elizabeth A.; Braxton, Alicia; Nassef, Salma; Ward, Patricia A.; Vetrini, Francesco; He, Weimin; Patel, Vipulkumar; Qu, Chunjing; Westerfield, Lauren; Stover, Samantha; Dharmadhikari, Avinash V.; Muzny, Donna M.; Gibbs, Richard A.; Dai, Hongzheng; Meng, Linyan; Wang, Xia; Xiao, Rui; Liu, Pengfei; Bi, Weimin; Xia, Fan; Walkiewicz, Magdalena; Veyver, Ignatia B. Van den; Eng, Christine M.; Yang, Yaping

doi:10.1186/s13073-018-0582-x

Cited by 119 publications

(176 citation statements)

References 51 publications

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“…The challenges of delivering exome studies in a timely manner in antenatal care also need to be overcome, along with explaining to families the problem of phenotypical variation between individuals with the same mutation, even within a single family. 41,42 Project three looked at children who had IMVM. Most children with this antenatal diagnosis do not show adverse developmental outcomes, so fetal maternal clinicians usually give a favourable prognostic category.…”

Section: Discussionmentioning

confidence: 99%

Accuracy of in-utero MRI to detect fetal brain abnormalities and prognosticate developmental outcome: postnatal follow-up of the MERIDIAN cohort

Hart

Embleton

Bradburn

et al. 2020

The Lancet Child & Adolescent Health

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Background In utero MRI (iuMRI) detects fetal brain abnormalities more accurately than ultrasonography and provides additional clinical information in around half of pregnancies. We aimed to study whether postnatal neuroimaging after age 6 months changes the diagnostic accuracy of iuMRI and its ability to predict developmental outcome. MethodsFamilies enrolled in the MERIDIAN study whose child survived to age 3 years were invited to have a case note review and assessment of developmental outcome with the Bayley Scales of Infant and Toddler Development, the Ages and Stages Questionnaire, or both. A paediatric neuroradiologist, masked to the iuMRI results, reviewed the postnatal neuroimaging if the clinical report differed from iuMRI findings. Diagnostic accuracy was recalculated. A paediatric neurologist and neonatologist categorised participants' development as normal, at risk, or abnormal, and the ability of iuMRI and ultrasonography to predict developmental outcome were assessed.Findings 210 participants had case note review, of whom 81 (39%) had additional investigations after age 6 months. The diagnostic accuracy of iuMRI remained higher than ultrasonography (proportion of correct cases was 529 [92%] of 574 vs 387 [67%] of 574; absolute difference 25%, 95% CI 21 to 29; p<0·0001). Developmental outcome data were analysed in 156 participants, and 111 (71%) were categorised as normal or at risk. Of these 111 participants, prognosis was normal or favourable for 56 (51%) using ultrasonography and for 76 (69%) using iuMRI (difference in specificity 18%, 95% CI 7 to 29; p=0·0008). No statistically significant difference was seen in infants with abnormal outcome (difference in sensitivity 4%, 95% CI -10 to 19; p=0·73).Interpretation iuMRI remains the optimal tool to identify fetal brain abnormalities. It is less accurate when used to predict developmental outcome, although better than ultrasonography for identifying children with normal outcome. Further work is needed to determine how the prognostic abilities of iuMRI can be improved.

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Section: Discussionmentioning

confidence: 99%

Accuracy of in-utero MRI to detect fetal brain abnormalities and prognosticate developmental outcome: postnatal follow-up of the MERIDIAN cohort

Hart

Embleton

Bradburn

et al. 2020

The Lancet Child & Adolescent Health

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“…The disadvantages are that panel content may not be up to date with the newest disease gene discoveries because they are typically developed on the basis of information on disease genes for conditions that present after birth and not optimized for prenatal presentations. A potentially more successful strategy that we favor is genome‐wide sequencing, such as diagnostic exome sequencing, which has already shown benefit for prenatal cases with CNS abnormalities, but full investigation of the clinical utility and their place in prenatal genetic testing is still underway …”

Section: Detection Of Aneuploidies Copy Number Gains and Losses Andmentioning

confidence: 99%

Prenatally diagnosed developmental abnormalities of the central nervous system and genetic syndromes: A practical review

Veyver

2019

Prenatal Diagnosis

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Developmental brain abnormalities are complex and can be difficult to diagnose by prenatal imaging because of the ongoing growth and development of the brain throughout pregnancy and the limitations of ultrasound, often requiring fetal magnetic resonance imaging as an additional tool. As for all major structural congenital anomalies, amniocentesis with chromosomal microarray and a karyotype is the first‐line recommended test for the genetic work‐up of prenatally diagnosed central nervous system (CNS) abnormalities. Many CNS defects, especially neuronal migration defects affecting the cerebral and cerebellar cortex, are caused by single‐gene mutations in a large number of different genes. Early data suggest that prenatal diagnostic exome sequencing for fetal CNS defects will have a high diagnostic yield, but interpretation of sequencing results can be complex. Yet a genetic diagnosis is important for prognosis prediction and recurrence risk counseling. The evaluation and management of such patients is best done in a multidisciplinary team approach. Here, we review general principles of the genetic work‐up for fetuses with CNS defects and review categories of genetic causes of prenatally diagnosed CNS phenotypes.

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“…Owing to the breakthrough of molecular technologies such as next-generation sequencing and its reduction of costs over the years, whole-exome sequencing (or exome sequencing, WES) has been applied for both research purposes and clinical use (Drury et al, 2015;Fu et al, 2018;Leung et al, 2018;Normand et al, 2018;Lord et al, 2019;Petrovski et al, 2019). Emerging studies show WES has the ability to provide genetic diagnoses ranging from 9.1% to 32% for the fetuses with a structural anomaly (Drury et al, 2015;Fu et al, 2018;Leung et al, 2018;Normand et al, 2018;Lord et al, 2019;Petrovski et al, 2019), while among these cases, WES yielded diagnoses in 3.2% to 21% of the fetuses with increased NT with/without structural malformations (Drury et al, 2015;Lord et al, 2019;Petrovski et al, 2019). However, most of these studies were conducted on prenatal cohorts after the exclusion of abnormal karyotypes and/or CMA results attributed to the cost and the limited ability of WES in CNV detection (Belkadi et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

Prenatal Diagnosis of Fetuses with Increased Nuchal Translucency by Genome Sequencing Analysis

Choy

Wang

Shi

et al. 2019

Preprint

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1 Background: 2 Increased Nuchal Translucency (NT) is an important biomarker associated with increased 3 risk of fetal structural anomalies. It is known to be contributed by a wide range of genetic 4 etiologies from single nucleotide variants to those affecting millions of base-pairs. 5 Currently, prenatal diagnosis is routinely performed by karyotyping and chromosomal 6 microarray analysis (CMA), however, both of them have limited resolution. The diversity 7 of the genetic etiologies warrants an integrated assay such as genome sequencing (GS) 8for comprehensive detection of genomic variants. Herein, we aim to evaluate the 9 feasibility of applying GS in prenatal diagnosis for the fetuses with increased NT.

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Clinical exome sequencing for fetuses with ultrasound abnormalities and a suspected Mendelian disorder

Cited by 119 publications

References 51 publications

Accuracy of in-utero MRI to detect fetal brain abnormalities and prognosticate developmental outcome: postnatal follow-up of the MERIDIAN cohort

Accuracy of in-utero MRI to detect fetal brain abnormalities and prognosticate developmental outcome: postnatal follow-up of the MERIDIAN cohort

Prenatally diagnosed developmental abnormalities of the central nervous system and genetic syndromes: A practical review

Prenatal Diagnosis of Fetuses with Increased Nuchal Translucency by Genome Sequencing Analysis

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