Copy-number changes in prenatal diagnosis

Strassberg, Melissa; Fruhman, Gary; Veyver, Ignatia B. Van den

doi:10.1586/erm.11.43

Cited by 26 publications

(38 citation statements)

References 101 publications

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“…However, the challenge of counseling couples about unpredictable outcomes is not new. 26 We observed a recurrent variant of unknown significance in a telomeric region of chromosome 19p13.3 (ranging in size from 632 to 930 kb) in eight stillbirths. This region is known to contain multiple benign variants as well as five loci in the OMIM database that have been associated with disease but not with stillbirth or developmental disorders.…”

Section: Discussionmentioning

confidence: 86%

“…However, inherited pathogenic variants should not be discounted as a cause of stillbirth because of their variable expressivity and incomplete penetrance. 8,26 Our ability to assess confined placental mosaicism, in which the fetus is genetically normal but the placenta is genetically abnormal, was limited.…”

Section: Discussionmentioning

confidence: 99%

“…Microarray analysis is more expensive than standard karyotype analysis, although its cost is expected to decrease 26 and may be offset by the higher yield of genomic abnormalities.…”

Section: Discussionmentioning

confidence: 99%

See 2 more Smart Citations

Karyotype Versus Microarray Testing for Genetic Abnormalities After Stillbirth

Reddy

Page

Saade

et al. 2013

Obstetrical &Amp; Gynecological Survey

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Section: Discussionmentioning

confidence: 86%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Karyotype Versus Microarray Testing for Genetic Abnormalities After Stillbirth

Reddy

Page

Saade

et al. 2013

Obstetrical &Amp; Gynecological Survey

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show abstract

“…Thus, one might argue that the use of genome-wide array in prenatal diagnostics should not be restricted to pregnancies with ultrasound abnormalities [Strassberg et al, 2011]. On the other hand, the interpretation of array results is challenging, especially in the absence of ultrasound abnormalities, as pathogenic CNVs that do not result in a phenotype detectable by ultrasound may sometimes be hard to distinguish from benign CNVs.…”

Section: Introductionmentioning

confidence: 99%

The introduction of arrays in prenatal diagnosis: A special challenge

et al. 2012

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“…However, the fact that only a minority of the submicroscopic abnormalities that are detected in postnatal patients with developmental delay/intellectual disability are accompanied by congenital abnormalities detectable by prenatal ultrasound, suggests the use of CMA in prenatal diagnostics not only for pregnancies with ultrasound abnormalities. 32 In the absence of specific guidelines and large-scale studies for different categories of indications, it has been suggested that CMA should be offered as an adjunction tool to selected groups of high-risk pregnancies (eg abnormal ultrasound findings and a normal conventional karyotype), using the technique as a second-line test only, after a standard karyotype. 25 Recently, the Canadian College of Medical Geneticists (CCMG) has discouraged the use of CMA in pregnancies at low risk for a structural chromosomal abnormality (eg advanced maternal age, positive maternal serum screen, previous pregnancy with a chromosomal abnormality or the presence of 'soft markers' on fetal ultrasound), motivating their position with the fact that CMA performed for the above categories of pregnancies would likely be associated with a low positive predictive value, since the vast majority of fetuses in these situations would be clinically unaffected.…”

Section: Introductionmentioning

confidence: 99%

Chromosomal microarray analysis as a first-line test in pregnancies with a priori low risk for the detection of submicroscopic chromosomal abnormalities

Fiorentino¹,

Napoletano²,

Caiazzo³

et al. 2012

Eur J Hum Genet

105

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In this study, we aimed to explore the utility of chromosomal microarray analysis (CMA) in groups of pregnancies with a priori low risk for detection of submicroscopic chromosome abnormalities, usually not considered an indication for testing, in order to assess whether CMA improves the detection rate of prenatal chromosomal aberrations. A total of 3000 prenatal samples were processed in parallel using both whole-genome CMA and conventional karyotyping. The indications for prenatal testing included: advanced maternal age, maternal serum screening test abnormality, abnormal ultrasound findings, known abnormal fetal karyotype, parental anxiety, family history of a genetic condition and cell culture failure. The use of CMA resulted in an increased detection rate regardless of the indication for analysis. This was evident in high risk groups (abnormal ultrasound findings and abnormal fetal karyotype), in which the percentage of detection was 5.8% (7/120), and also in low risk groups, such as advanced maternal age (6/1118, 0.5%), and parental anxiety (11/1674, 0.7%). A total of 24 (0.8%) fetal conditions would have remained undiagnosed if only a standard karyotype had been performed. Importantly, 17 (0.6%) of such findings would have otherwise been overlooked if CMA was offered only to high risk pregnancies.The results of this study suggest that more widespread CMA testing of fetuses would result in a higher detection of clinically relevant chromosome abnormalities, even in low risk pregnancies. Our findings provide substantial evidence for the introduction of CMA as a first-line diagnostic test for all pregnant women undergoing invasive prenatal testing, regardless of risk factors.

show abstract

Copy-number changes in prenatal diagnosis

Cited by 26 publications

References 101 publications

Karyotype Versus Microarray Testing for Genetic Abnormalities After Stillbirth

Karyotype Versus Microarray Testing for Genetic Abnormalities After Stillbirth

The introduction of arrays in prenatal diagnosis: A special challenge

Chromosomal microarray analysis as a first-line test in pregnancies with a priori low risk for the detection of submicroscopic chromosomal abnormalities

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