Screening of congenital heart disease patients using multiplex ligation‐dependent probe amplification: Early diagnosis of syndromic patients

Sørensen, Karina Meden; El-Segaier, Milad; Fernlund, Eva; Errami, Ab; Bouvagnet, Patrice; Nehme, Nancy; Steensberg, Jesper; Hjortdal, Vibeke E.; Soller, Maria; Behjati, Mohaddeseh; Werge, Thomas; Kirchoff, Maria; Schouten, Jan P.; Tommerup, Niels; Andersen, Paal Skytt; Larsen, Lars Allan

doi:10.1002/ajmg.a.35214

Cited by 34 publications

(53 citation statements)

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“…8 Additional MLPA probes were used and family MC061 was found to have a 2q37.3 duplication. 8 Twenty-one families of this series were tested for a panel of 13 sarcomeric genes in a second collaborative study, 7 and disease-causing variants were found only in the alpha cardiac heavy chain myosin gene (MYH6), in three families (MC027 p.(Cys539Arg), MC053 p.(Lys543Arg) and MC081 p.(Arg17His)). These 21 families were selected out of the Registry because at least one affected individual had ASD (for details, see Supplementary Table S1).…”

Section: Discussionmentioning

confidence: 99%

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A systematic variant screening in familial cases of congenital heart defects demonstrates the usefulness of molecular genetics in this field

Malti¹,

Liu²,

Doray³

et al. 2015

Eur J Hum Genet

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The etiology of congenital heart defect (CHD) combines environmental and genetic factors. So far, there were studies reporting on the screening of a single gene on unselected CHD or on familial cases selected for specific CHD types. Our goal was to systematically screen a proband of familial cases of CHD on a set of genetic tests to evaluate the prevalence of disease-causing variant identification. A systematic screening of GATA4, NKX2-5, ZIC3 and Multiplex ligation-dependent probe amplification (MLPA) P311 Kit was setup on the proband of 154 families with at least two cases of non-syndromic CHD. Additionally, ELN screening was performed on families with supravalvular arterial stenosis. Twenty-two variants were found, but segregation analysis confirmed unambiguously the causality of 16 variants: GATA4 (1 × ), NKX2-5 (6 × ), ZIC3 (3 × ), MLPA (2 × ) and ELN (4 × ). Therefore, this approach was able to identify the causal variant in 10.4% of familial CHD cases. This study demonstrated the existence of a de novo variant even in familial CHD cases and the impact of CHD variants on adult cardiac condition even in the absence of CHD. This study showed that the systematic screening of genetic factors is useful in familial CHD cases with up to 10.4% elucidated cases. When successful, it drastically improved genetic counseling by discovering unaffected variant carriers who are at risk of transmitting their variant and are also exposed to develop cardiac complications during adulthood thus prompting long-term cardiac follow-up. This study provides an important baseline at dawning of the next-generation sequencing era.

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Section: Discussionmentioning

confidence: 99%

“…Some families of this cohort were screened for other genes or another MLPA test and are reported elsewhere. 7,8 For details on the enrolled families, see Supplementary Table S1. All variants were submitted to LOVD (www.lovd.nl/3.0/home).…”

Section: Genetic Analysismentioning

confidence: 99%

A systematic variant screening in familial cases of congenital heart defects demonstrates the usefulness of molecular genetics in this field

Malti¹,

Liu²,

Doray³

et al. 2015

Eur J Hum Genet

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“…Recently, Sørensen et al (12) examined 402 CHD patients (378 with isolated CHD and 24 with extra cardiac malformations) with a specific multiplex ligation-dependent probe amplification designed for CHD screening. They identified 14 rare CNVs in 13 (3.2%) patients, with >80% of the detected imbalances found in children younger than 5 y.…”

Section: Discussionmentioning

confidence: 99%

Array comparative genomic hybridization as a clinical diagnostic tool in syndromic and nonsyndromic congenital heart disease

et al. 2013

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Background: Congenital heart diseases (CHDs) are often associated with other congenital anomalies, dysmorphic features, and developmental delay, and only a few cases of chromosomal abnormalities are detected by conventional cytogenetic techniques. The microarray comparative genomic hybridization (CGH) analysis allows the identification of submicroscopic genomic rearrangements. Methods: During the past 3 y, 55 of 330 patients referred for array CGH had CHD of unknown etiology plus at least one additional indication of abnormal chromosomal phenotype. High-resolution 1 × 244K or 4 × 180K Agilent arrays were used in this study (average resolution 7-13 kb). results: Copy-number variations were detected in 37 of 55 patients, and in 29 of 37 patients there were genes that have been associated with CHD. All 37 patients had at least one additional phenotypic abnormality: 30 of 37 had one or more other congenital anomalies, 23 of 37 had dysmorphic features, 16 of 37 had intellectual disability, 13 of 37 had abnormal magnetic resonance imaging, 10 of 37 had hypotonia, and 7 of 37 had seizures. In 9 of 55 patients, unexpected genomic rearrangements in relation to their phenotype were identified. conclusion: In patients with CHD and at least one additional indication of abnormal chromosomal phenotype, array CGH analysis could detect possible submicroscopic chromosomal abnormalities and provide proper genetic counseling.

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“…Although a single biomarker can be used to diagnose a disease, but there are issues where a single biomarker alone cannot accurately predict occurrence of the disease [6]. To address this multi analyte detection various molecular methods have been developed such as; multiplex polymerase chain reaction analysis [7], multiplex ligation-dependent probe amplification [8], DNA microarray for gene expression or SNP detection assays [9], protein microarray [10], phage display [11] etc. These methods, however, are extremely powerful for multianalyte detection but they suffer due to their cost and inability of miniaturization for the onsite analysis.…”

mentioning

confidence: 99%

Miniaturized Multiplex Electrochemical Biosensor in Clinical Bioanalysis

2013

J Bioanal Biomed

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Screening of congenital heart disease patients using multiplex ligation‐dependent probe amplification: Early diagnosis of syndromic patients

Cited by 34 publications

References 20 publications

A systematic variant screening in familial cases of congenital heart defects demonstrates the usefulness of molecular genetics in this field

A systematic variant screening in familial cases of congenital heart defects demonstrates the usefulness of molecular genetics in this field

Array comparative genomic hybridization as a clinical diagnostic tool in syndromic and nonsyndromic congenital heart disease

Miniaturized Multiplex Electrochemical Biosensor in Clinical Bioanalysis

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