Investigation of copy number variation in children with conotruncal heart defects

Campos, Carla Marques Rondon; Zanardo, Évelin Aline; Dutra, Roberta Lelis; Kulikowski, Leslie Domenici; Kim, Chong

doi:10.5935/abc.20140169

Cited by 16 publications

(20 citation statements)

References 26 publications

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“…Campos et al reported a newborn with severe coarctation of the aorta, patent ductus arteriosus, an atrial septal defect, and several VSDs identified by echocardiography, duodenal atresia, left appendix, constipation, feeding difficulties, failure to thrive, hypertonia, and neuropsychomotor development delay; this child died at the age of 4 months. 31 Case 25 had a 23.5-Kb deletion in chromosome 16p13.3 that contained two OMIM genes, HBA1 and HBA2, which are associated with Hemoglobin H disease. 32 We observed three (5.8%) cases of VOUS.…”

Section: Discussionmentioning

confidence: 99%

Prenatal diagnosis of submicroscopic chromosomal aberrations in fetuses with ventricular septal defects by chromosomal microarray‐based analysis

Xie

Huang

et al. 2016

Prenatal Diagnosis

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Section: Discussionmentioning

confidence: 99%

Prenatal diagnosis of submicroscopic chromosomal aberrations in fetuses with ventricular septal defects by chromosomal microarray‐based analysis

Xie

Huang

et al. 2016

Prenatal Diagnosis

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“…The rates of diagnosis in the various studies are highly variable, from 3.2 to 33.3% [Sørensen et al, 2012;Wang et al, 2013;Campos et al, 2015], which is due to the technique used and the method of selecting patients. In our case, there is a bias towards more severe patients since all of them were syndromic.…”

Section: Discussionmentioning

confidence: 99%

“…Some researchers have investigated the contribution of chromosomal alterations in CHD patients using the MLPA technique; the results ranged from 3.2-33.33% and showed to be highly dependent on the selection of patients and the type of kit used [Sørensen et al, 2012;Wang et al, 2013;Campos et al, 2015].…”

Section: Major Contribution Of Genomic Copy Number Variation In Syndrmentioning

confidence: 99%

Major Contribution of Genomic Copy Number Variation in Syndromic Congenital Heart Disease: The Use of MLPA as the First Genetic Test

et al. 2017

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Congenital heart disease (CHD) is the most common congenital disorder among live births. When associated with extracardiac abnormalities, it is characterized as a syndromic heart disease (syndromic CHD) and corresponds to 25% of all liveborn infants with a heart defect. The etiology in about 65% of the cases still remains unknown, and in about 35% of the patients, it is associated with genetic factors. In the present study, MLPA and SNP-array techniques were used to investigate a group of 47 patients with syndromic CHD. In total, 16 defects (34%) were identified, of which 12 (25.5%) were classified as pathogenic or probably pathogenic. The most frequent abnormalities were 22q11.2 deletion (22q11.2 deletion syndrome) and 7q11.23 deletion (Williams-Beuren syndrome). We also show that rarer malformations may be associated with syndromic CHD, such as 14q32.33 deletion as well as 17q25.3, 15q11.2 (BP1-BP2), 22q13.31, and 12p13.31 (SLC2A3) duplications. The present study demonstrates that CNVs are important causal factors and should be studied in patients with syndromic CHD. Furthermore, the use of MLPA as a first screening test was appropriate, as this less expensive technology detected 11 of the 12 pathogenic abnormalities (91.6%).

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“…The third CNV, a deletion in 8p23.2, did not encompass any genes. In addition to Fakhro et al (2011), another CNV investigation identified a duplication in 8p23.2 in an individual with tetralogy of Fallot (Campos et al 2015). In addition to the deletion in 8p23.2, this case had three exonic heterozygous mutations in DNAH11 (Table 1), all with unknown significance.…”

Section: Discussionmentioning

confidence: 99%

Copy-number variant analysis of classic heterotaxy highlights the importance of body patterning pathways

et al. 2016

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Classic heterotaxy consists of congenital heart defects with abnormally positioned thoracic and abdominal organs. We aimed to uncover novel, genomic copy-number variants (CNVs) in classic heterotaxy cases. A microarray containing 2.5 million single-nucleotide polymorphisms (SNPs) was used to genotype 69 infants (cases) with classic heterotaxy identified from California live births from 1998 to 2009. CNVs were identified using the PennCNV software. We identified 56 rare CNVs encompassing genes in the NODAL (NIPBL, TBX6), BMP (PPP4C), and WNT (FZD3) signaling pathways, not previously linked to classic heterotaxy. We also identified a CNV involving FGF12, a gene previously noted in a classic heterotaxy case. CNVs involving RBFOX1 and near MIR302F were detected in multiple cases. Our findings illustrate the importance of body patterning pathways for cardiac development and left/right axes determination. FGF12, RBFOX1, and MIR302F could be important in human heterotaxy, because they were noted in multiple cases. Further investigation into genes involved in the NODAL, BMP, and WNT body patterning pathways and into the dosage effects of FGF12, RBFOX1, and MIR302F is warranted.

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Investigation of copy number variation in children with conotruncal heart defects

Cited by 16 publications

References 26 publications

Prenatal diagnosis of submicroscopic chromosomal aberrations in fetuses with ventricular septal defects by chromosomal microarray‐based analysis

Prenatal diagnosis of submicroscopic chromosomal aberrations in fetuses with ventricular septal defects by chromosomal microarray‐based analysis

Major Contribution of Genomic Copy Number Variation in Syndromic Congenital Heart Disease: The Use of MLPA as the First Genetic Test

Copy-number variant analysis of classic heterotaxy highlights the importance of body patterning pathways

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