Transcription alterations of KCNQ1 associated with imprinted methylation defects in the Beckwith–Wiedemann locus

Valente, Federica Maria; Sparago, Ángela; Freschi, Andrea; Hill-Harfe, Katherine L.; Maas, Saskia M.; Frints, Suzanna G.M.; Alders, Mariëlle; Pignata, Laura; Franzese, Monica; Angelini, Claudia; Carli, Diana; Mussa, Alessandro; Gazzin, Andrea; Gabbarini, Fulvio; Acurzio, Basilia; Ferrero, Giovanni Battista; Bliek, Jet; Williams, Charles A.; Riccio, Andrea; Cerrato, Flavia

doi:10.1038/s41436-018-0416-7

Cited by 38 publications

(39 citation statements)

References 40 publications

(55 reference statements)

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“…Patient #31 (female) and #32 (male) were siblings. In their family segregates an intragenic inverted microduplication of 160‐kB within KCNQ1 exons 10 responsible for both Long QT syndrome type 1 (LQTS1) (Valente et al, ) and IC2‐LoM (Chiesa et al, ). They physiologically conceived and had children with unrelated partners.…”

Section: Resultsmentioning

confidence: 99%

Phenotype evolution and health issues of adults with Beckwith‐Wiedemann syndrome

Gazzin¹,

Carli²,

Sirchia

et al. 2019

American J of Med Genetics Pt A

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Background: Beckwith-Wiedemann syndrome (BWS) phenotype usually mitigates with age and data on adulthood are limited. Our study aims at reporting phenotype evolution and health issues in adulthood.Methods: 34 patients (16 males), aged 18-58 years (mean 28.5) with BWS were enrolled.Results: 26 patients were molecularly confirmed, 5 tested negative, and 3 were not tested. Final tall stature was present in 44%. Four patients developed Wilms' Tumor (2, 3, 5, and 10 years, respectively); one hepatoblastoma (22 years); one acute lymphoblastic leukemia (21 years); one adrenal adenoma and testicular Sertoli cell tumor (22 and 24 years, respectively); and three benign tumors (hepatic haemangioma, uterine myoma, and mammary fibroepithelioma). Surgery for BWS-related features was required in 85%. Despite surgical correction several patients presented morbidity and sequelae of BWS pediatric issues: pronunciation/swallow difficulties (n = 9) due to macroglossia, painful scoliosis (n = 4) consistent with lateralized overgrowth, recurrent urolithiasis (n = 4), azoospermia (n = 4) likely consequent to cryptorchidism, severe intellectual disability (n = 2) likely related to neonatal asphyxia and diabetes mellitus (n = 1) due to subtotal pancreatectomy for intractable hyperinsulinism. Four patients (two males) had healthy children (three physiologically conceived and one through assisted reproductive technology).Conclusions: Adult health conditions in BWS are mostly consequent to pediatric issues, underlying the preventive role of follow-up strategies in childhood. Malignancy rate observed in early adulthood in this small cohort matches that observed in the first decade of life, cumulatively raising tumor rate in BWS to 20% during the observation period. Further studies are warranted in this direction.

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Section: Resultsmentioning

confidence: 99%

Phenotype evolution and health issues of adults with Beckwith‐Wiedemann syndrome

Gazzin¹,

Carli²,

Sirchia

et al. 2019

American J of Med Genetics Pt A

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“…Approximately 50% of cases are caused by LoM at IC2 (IC2-LoM) leading to reduced expression of CDKN1C, normally expressed by the maternal chromosome only. IC2-LoM is usually a sporadic primary epigenetic defect, however rare familial cases carrying genetic mutations causing secondary hypomethylation have been described (30). An increasingly growing fraction of patients with IC2-LoM also display methylation abnormalities at other imprinted loci leading to additional phenotypes (MLID) (31,32).…”

Section: Chromosome 11mentioning

confidence: 99%

Syndromic Disorders Caused by Disturbed Human Imprinting

Carli

Riberi

Mussa

2020

Jcrpe

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Imprinting disorders are a group of congenital diseases caused by dysregulation of genomic imprinting, affecting prenatal and postnatal growth, neurocognitive development, metabolism and cancer predisposition. Aberrant expression of imprinted genes can be achieved through different mechanisms, classified into epigenetic-if not involving DNA sequence change-or genetic in the case of altered genomic sequence. Despite the underlying mechanism, the phenotype depends on the parental allele affected and opposite phenotypes may result depending on the involvement of the maternal or the paternal chromosome. Imprinting disorders are largely underdiagnosed because of the broad range of clinical signs, the overlap of presentation among different disorders, the presence of mild phenotypes, the mitigation of the phenotype with age and the limited availability of molecular techniques employed for diagnosis. This review briefly illustrates the currently known human imprinting disorders, highlighting endocrinological aspects of pediatric interest.

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“…In addition, increased recurrence risk has been reported in cases with MLID with maternal-effect clinical SNVs (see ref [113] and MLID section). Moreover, high recurrence risk via maternal transmission has been described in rare cases of IC2 LOM with KCNQ1OT1 rearrangements or clinical SNVs [69]. Furthermore, a 50% recurrence risk is also present in the cases with clinical CDKN1C SNVs (only via maternal transmission), and in the cases of inherited chromosomal rearrangements (parental bias depends on the type of mutation).…”

Section: Beckwith-wiedemann Syndrome and Silver-russell Syndromementioning

confidence: 99%

DNA Methylation in the Diagnosis of Monogenic Diseases

Cerrato

Sparago

Ariani

et al. 2020

Genes

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DNA methylation in the human genome is largely programmed and shaped by transcription factor binding and interaction between DNA methyltransferases and histone marks during gamete and embryo development. Normal methylation profiles can be modified at single or multiple loci, more frequently as consequences of genetic variants acting in cis or in trans, or in some cases stochastically or through interaction with environmental factors. For many developmental disorders, specific methylation patterns or signatures can be detected in blood DNA. The recent use of high-throughput assays investigating the whole genome has largely increased the number of diseases for which DNA methylation analysis provides information for their diagnosis. Here, we review the methylation abnormalities that have been associated with mono/oligogenic diseases, their relationship with genotype and phenotype and relevance for diagnosis, as well as the limitations in their use and interpretation of results.

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Transcription alterations of KCNQ1 associated with imprinted methylation defects in the Beckwith–Wiedemann locus

Cited by 38 publications

References 40 publications

Phenotype evolution and health issues of adults with Beckwith‐Wiedemann syndrome

Phenotype evolution and health issues of adults with Beckwith‐Wiedemann syndrome

Syndromic Disorders Caused by Disturbed Human Imprinting

DNA Methylation in the Diagnosis of Monogenic Diseases

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