Prenatal findings and epimutations for paternal uniparental disomy for chromosome 14 syndrome

Watanabe, Takafumi; Go, Hayato; Kagami, Masayo; Yasuda, Shun; Nomura, Yasuhisa; Fujimori, Keiya

doi:10.1111/jog.12665

Cited by 12 publications

(7 citation statements)

References 12 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…So far, there has been no definitive evidence of imprinting diseases related to the region of 7q11.23‐q21.11, 2p25.3‐p11.2, and 2q11.1‐q37.3 observed in 2 of our cases, and the pregnancy outcomes of both cases were normal. Imprinting diseases reported in the literature include transient neonatal diabetes mellitus related to 6q24, Russell‐Silver, Beckwith‐Wiedemann syndrome, Temple syndrome, UPD (14) pat syndrome, Angelman syndrome, Prader‐Willi Syndrome, UPD (20) mat syndrome, pseudohypoparathyoridism type Ib, and others. Thus, genetic counseling should take into account UPD when NIPT shows extra copies for chromosomes involved in well‐known imprinted disease loci, like pat6q24, mat7p11.2‐p12 and q32.2, segmental pat11p15.5, mat/pat14q32, mat/pat15q11‐q13, and UPD (20) mat (several loci involved)/pat20q13.3.…”

Section: Discussionmentioning

confidence: 99%

Pregnancy outcome of autosomal aneuploidies other than common trisomies detected by noninvasive prenatal testing in routine clinical practice

Wan

Zhang

et al. 2018

Prenatal Diagnosis

View full text Add to dashboard Cite

show abstract

Section: Discussionmentioning

confidence: 99%

Pregnancy outcome of autosomal aneuploidies other than common trisomies detected by noninvasive prenatal testing in routine clinical practice

Wan

Zhang

et al. 2018

Prenatal Diagnosis

View full text Add to dashboard Cite

show abstract

“…Growth restriction, for example, in patients with upd (14) mat [ 11 , 28 ], polyhydramnion in patients with upd (14) pat [ 7 , 29 ] or orofacial malformations in both. Micrognathia, retrognathia or high arch palate are frequently described in patients either with upd (14) mat [ 28 ] or upd (14) pat [ 30 – 32 ]. Paternal isodisomy of chromosome 14 was described in patients with maxillary and mandibular hypoplasia [ 33 ].…”

Section: Discussionmentioning

confidence: 99%

Haploinsufficiency of BMP4 and OTX2 in the Foetus with an abnormal facial profile detected in the first trimester of pregnancy

et al. 2017

View full text Add to dashboard Cite

BackgroundInterstitial microdeletion 14q22q23 is a rare chromosomal syndrome associated with variable defects: microphthalmia/anophthalmia, pituitary anomalies, polydactyly/syndactyly of hands and feet, micrognathia/retrognathia. The reports of the microdeletion 14q22q23 detected in the prenatal stages are limited and the range of clinical features reveals a quite high variability.Case presentationWe report a detection of the microdeletion 14q22.1q23.1 spanning 7,7 Mb and involving the genes BMP4 and OTX2 in the foetus by multiplex ligation-dependent probe amplification (MLPA) and verified by microarray subsequently. The pregnancy was referred to the genetic counselling for abnormal facial profile observed in the first trimester ultrasound scan and micrognathia (suspicion of Pierre Robin sequence), hypoplasia nasal bone and polydactyly in the second trimester ultrasound scan. The pregnancy was terminated on request of the parents.ConclusionAn abnormal facial profile detected on prenatal scan can provide a clue to the presence of rare chromosomal abnormalities in the first trimester of pregnancy despite the normal result of the first trimester screening test. The patients should be provided with genetic counselling. Usage of quick and sensitive methods (MLPA, microarray) is preferable for discovering a causal aberration because some of the CNVs cannot be detected with conventional karyotyping in these cases. To the best of our knowledge, this is the earliest detection of this microdeletion (occurred de novo), the first case detected by MLPA and confirmed by microarray. Literature review of the genotype-phenotype correlation in similar reports leads us to the conclusion that dosage imbalance of the chromosomal segment 14q22q23 (especially haploinsuffiency of the genes BMP4 and OTX2) contributes significantly to orofacial abnormalities. Association of the region with the Pierre Robin sequence appears to be plausible.

show abstract

“…32,33 Three-dimensional ultrasound, fetal X-ray, or fetal magnetic resonance imaging to look for coat-hanger ribs/bell shaped thorax has been used in the past to aid the diagnosis of KOS. [32][33][34] The coat-hanger sign (usually identified on postnatal chest radiographs) could be visible as early as 23 weeks of gestation by prenatal ultrasound. 35 If KOS is suspected in a fetus, parents should be offered amniocentesis for karyotype, CMA, and methylation analysis.…”

Section: Prenatal Diagnosismentioning

confidence: 99%

Kagami-Ogata Syndrome: Case Series and Review of Literature

Sakaria

Mostafavi

Miller

et al. 2021

AJP Rep

View full text Add to dashboard Cite

Kagami-Ogata syndrome (KOS) (OMIM #608149) is a genetic imprinting disorder affecting chromosome 14 that results in a characteristic phenotype consisting of typical facial features, skeletal abnormalities including rib abnormalities described as “coat hanger ribs,” respiratory distress, abdominal wall defects, polyhydramnios, and developmental delay. First identified by Wang et al in 1991, over 80 cases of KOS have been reported in the literature. KOS, however, continues to remain a rare and potentially underdiagnosed disorder. In this report, we describe two unrelated male infants with differing initial presentations who were both found to have the characteristic “coat hanger” rib appearance on chest X-ray, raising suspicion for KOS. Molecular testing confirmed KOS in each case. In addition to these new cases, we reviewed the existing cases reported in literature. Presence of polyhydramnios, small thorax, curved ribs, and abdominal wall defects must alert the perinatologist toward the possibility of KOS to facilitate appropriate molecular testing. The overall prognosis of KOS remains poor. Early diagnosis allows for counseling by a multidisciplinary team and enables parents to make informed decisions regarding both pregnancy management and postnatal care.

show abstract

Prenatal findings and epimutations for paternal uniparental disomy for chromosome 14 syndrome

Cited by 12 publications

References 12 publications

Pregnancy outcome of autosomal aneuploidies other than common trisomies detected by noninvasive prenatal testing in routine clinical practice

Pregnancy outcome of autosomal aneuploidies other than common trisomies detected by noninvasive prenatal testing in routine clinical practice

Haploinsufficiency of BMP4 and OTX2 in the Foetus with an abnormal facial profile detected in the first trimester of pregnancy

Kagami-Ogata Syndrome: Case Series and Review of Literature

Contact Info

Product

Resources

About