Identification of novel candidate gene loci and increased sex chromosome aneuploidy among infants with conotruncal heart defects

Chromosome region 10q22.3-q23.3 contains several low copy repeats (LCRs) and is prone to recombination. Deletions with breakpoints within LCR3 and LCR4 have been described to be associated with intellectual disability and dysmorphic features, while the reciprocal duplications are rarely reported. We present an additional case with multiple congenital anomalies that include microcephaly, cardiac defect, and mild intellectual disability, in which a de novo interstitial 8.2-Mb duplication of 10q22.3-q23.3, including BMPR1A and NGR3, was identified by Illumina SNP array platform. Our study is consistent with the hypothesis that the BMPR1A is a plausible candidate gene for congenital heart disease (CHD) and should contribute to the diagnosis and treatment of these genomic diseases.

Section: Introductionmentioning

confidence: 63%

Duplication of 10q22.3–q23.3 encompassing BMPR1A and NGR3 associated with congenital heart disease, microcephaly, and mild intellectual disability

Tang

Yang

Xie

et al. 2015

“…Schematic representation of the studied 22q11.2 region from the most centromeric 18.2 Mb to the 22.7 Mb position. The figure displays, from top to bottom: scale of locus and assembly, chromosome 22 position by UCSC genome browser hg38, LCR22 blocks, typical and distal deletion intervals, 22q11.2 atypical deletion patients reported in the literature [D'Angelo et al, ; Garcia‐Minaur et al, ; Michaelovsky et al, ; Osoegawa et al, ; Rump et al, ; Verhagen et al, ], LCR22‐C to D/E deletion patients discussed in this report, RefSeq genes, and Segmental Duplications reported by UCSC (a blue shadow remarks the genes included in the deletion detected in our patients and an orange box remarks the duplication blocks included in the distal breakpoint region).…”

Section: Resultsmentioning

confidence: 99%

“…On the other hand, deletions involving any of the two LCRs from D to H, known as distal deletions, are associated with a variable and relatively mild phenotype, with growth delay of prenatal onset [Rauch et al, , ; Ben‐Shachar et al, ; Tan et al, ; Fagerberg et al, ; Mikhail et al, ]. A limited number of patients with deletions involving other LCRs have also been reported and they are frequently called atypical deletions [Garcia‐Minaur et al, ; D'Angelo et al, ; Michaelovsky et al, ; Verhagen et al, ; Molck et al, ; Osoegawa et al, ; Rump et al, ].…”

Section: Introductionmentioning

confidence: 99%

Delineation of a recognizable phenotype for the recurrent LCR22‐C to D/E atypical 22q11.2 deletion

Bengoa-Alonso

Artigas-López

Moreno-Igoa

et al. 2016

The 22q11.2 deletion syndrome is typically caused by haploinsufficiency of a 3 Mb region that extends from LCR22-A until LCR22-D, while the recurrent recombination between any of the LCR22-D to H causes the 22q11.2 distal deletion syndrome. Here, we describe three patients with a de novo atypical ∼1.4 Mb 22q11.2 deletion that involves LCR22-C to a region beyond D (LCR22-C to D/E), encompassing the distal portion of the typical deleted region and the proximal portion of the distal deletion. We also review six previous published patients with the same rearrangement and compare their features with those found in patients with overlapping deletions. Patients with LCR22-C to D/E deletion present a recognizable phenotype characterized by facial dysmorphic features, high frequency of cardiac defects, including conotruncal defects, prematurity, growth restriction, microcephaly, and mild developmental delay. Genotype-phenotype analysis of the patients indicates that CRKL and MAPK1 genes play an important role as causative factors for the main clinical features of the syndrome. In particular, CRKL gene seems to be involved in the occurrence of conotruncal cardiac anomalies, mainly tetralogy of Fallot. © 2016 Wiley Periodicals, Inc.

“…He is non‐syndromic with a complex heart defect including coarctation of the aorta, a VSD, parachute mitral valve and transverse hypoplasia. Duplication of GATA4 is an established cause of conotruncal and septal heart defects with variable penetrance in 8p23.1 DS [Joziasse et al, ; Barber et al, ], and a further infant with isolated Tetralogy of Fallot (TOF) and a full 8p23.1 duplication was recently ascertained among 290 infants with TOF from 974,579 births in the California Study of Birth Defects Causes [Osoegawa et al, , Subject C]. A large microduplication including SOX7 and GATA4 was recently found in another nonsyndromic patient with bicuspid aortic valve and aortic regurgitation (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…The 8p23.1 duplication syndrome (8p23.1DS) is the reciprocal of the 8p23.1 deletion syndrome and a relatively rare genomic condition with an estimated prevalence of 1 in 58,000 [Barber et al, ]. Using molecular cytogenetic methods, the full 8p23.1DS has been confirmed in twenty‐four reported patients of whom nineteen were probands and five were other family members [Barber et al, , , ; Yu et al, , ; Longoni et al, , Patient 3; Barber et al, ; Osoegawa et al, , Subject C]. The 8p23.1 DS has a variable phenotype with the three relatively common features of developmental delay and/or learning difficulties, congenital heart disease (CHD) and a degree of mild dysmorphism that may be minimal [Yu et al, ; Barber et al, ]; other phenotypic features include behavioral problems, cleft lip and/or palate, macrocephaly, seizures, attention deficit hyperactivity disorder (ADHD), ocular anomalies, balance problems, hypotonia, hydrocele [Barber et al, , , ; Yu et al, , ] and, on one occasion, congenital diaphragmatic hernia (CDH) [Longoni et al, , Patient 3].…”

Section: Introductionmentioning

confidence: 99%

Inside the 8p23.1 duplication syndrome; eight microduplications of likely or uncertain clinical significance

Barber

Rosenfeld

Graham

et al. 2015

The 8p23.1 duplication syndrome (8p23.1 DS) is a recurrent genomic condition with an estimated prevalence of 1 in 58,000. The core 3.68 Mb duplication contains 32 genes of which five are currently candidates for the phenotypic features. Here we describe four patients and five families with eight microduplications of 8p23.1 ranging from 187 to 1082 kb in size and one atypical duplication of 4 Mb. These indicate that a minimal region of overlap (MRO) in medial 8p23.1 can give rise to features of 8p23.1 DS including developmental delay, dysmorphism, macrocephaly and otitis media, but not congenital heart disease (CHD). This MRO spans 776 kb (chr8:10,167,881-10,943,836 hg19) and contains SOX7 and seven of the other 32 core 8p23.1 DS genes. In centromeric 8p23.1, microduplications including GATA4 can give rise to non-syndromic CHD but the clinical significance of two smaller centromeric microduplications without GATA4 was uncertain due to severe neurological profiles not usually found in 8p23.1 DS. The clinical significance of three further 8p23.1 microduplications was uncertain due to additional genetic factors without which the probands might not have come to medical attention. Variable expressivity was indicated by the almost entirely unaffected parents in all five families and the mildly affected sibling in one. Intronic interruptions of six genes by microduplication breakpoint intervals had no apparent additional clinical consequences. Our results suggest that 8p23.1 DS is an oligogenetic condition largely caused by the duplication and interactions of the SOX7 and GATA4 transcription factors.