Molecular genetic classification in Prader-Willi syndrome: a multisite cohort study

Butler, Merlin G.; Hartin, Samantha N.; Hossain, Waheeda A.; Manzardo, Ann M.; Kimonis, Virginia; Dykens, Elisabeth M.; Gold, June Anne; Kim, Soo-Jeong; Weisensel, Nicolette; Tamura, Roy; Miller, Jennifer; Driscoll, Daniel J.

doi:10.1136/jmedgenet-2018-105301

Cited by 119 publications

(133 citation statements)

References 20 publications

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“…It was anticipated that the larger areas of LOH (involving more genes), the higher the risk of carrying a second genetic disorder or atypical features in UPD patients. 4 Because of limited case numbers in our study, we were unable to identify the phenotypic differences between different subtypes of UPD. However, it is rational for clinicians to cautiously observe the atypical features from PWS patients with larger LOH.…”

Section: Discussionmentioning

confidence: 90%

“…Total isodisomy resulted from nondisjunction events in meiosis II and total heterodisomy from meiosis I nondisjunction error, whereas various numbers of crossing-over events could lead to segmental isodisomy. 7 Among 60 cases of PWS with segmental isodisomy, Butler et al 4 identified 25 cases with two segments and three cases with three segments of LOH, suggesting more than one crossing-over event in those cases. The most common LOH sites were proximal 15q12 and distal 15q26.1.…”

Section: Discussionmentioning

confidence: 99%

“…3 Bulter et al described a subclassification using single nucleotide polymorphism (SNP) array results and reported that 58% (60/ 104) of their UPD patients had segmental isodisomy. 4 There were currently no Taiwanese data regarding the subclassification of UPD patients in PWS. We analyzed our previously diagnosed PWS patients who were assumed to be caused by maternal UPD 15 and arranged a high-resolution SNP array for further categorization.…”

Section: Introductionmentioning

confidence: 99%

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Segmental isodisomy in Prader–Willi syndrome patients: The experience of a single diagnostic center

Pan

Chang

Jong³

et al. 2020

Pediatrics & Neonatology

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Section: Discussionmentioning

confidence: 90%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Segmental isodisomy in Prader–Willi syndrome patients: The experience of a single diagnostic center

Pan

Chang

Jong³

et al. 2020

Pediatrics & Neonatology

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“…Since the markers we studied are from the pericentromeric regions of the respective chromosomes of origin, where cross‐overs are not expected to occur, this finding indicates either a previous maternal meiosis II (mat‐MII) nondisjunction or a postzygotic event. Indeed, in a number of cases of trisomy rescue (Butler et al., ; Chantot‐Bastaraud et al., ) a mat‐MII error has been documented. Similarly, the mechanism leading to the formation of the supernumerary i(12p), associated with Pallister‐Killian syndrome, has been proven to be prezygotic and of maternal origin, presumably occurring at MII as demonstrated by the presence of three genotypes at the distal 12p region and only two at the pericentromeric one (Blyth et al., ; Conlin et al., ).…”

Section: Reconstruction and Formation Mechanisms Of Ssmcmentioning

confidence: 99%

Small supernumerary marker chromosomes: A legacy of trisomy rescue?

et al. 2018

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We studied by a whole genomic approach and trios genotyping, 12 de novo, nonrecurrent small supernumerary marker chromosomes (sSMC), detected as mosaics during pre‐ or postnatal diagnosis and associated with increased maternal age. Four sSMCs contained pericentromeric portions only, whereas eight had additional non‐contiguous portions of the same chromosome, assembled together in a disordered fashion by repair‐based mechanisms in a chromothriptic event. Maternal hetero/isodisomy was detected with a paternal origin of the sSMC in some cases, whereas in others two maternal alleles in the sSMC region and biparental haplotypes of the homologs were detected. In other cases, the homologs were biparental while the sSMC had the same haplotype of the maternally inherited chromosome. These findings strongly suggest that most sSMCs are the result of a multiple‐step mechanism, initiated by maternal meiotic nondisjunction followed by postzygotic anaphase lagging of the supernumerary chromosome and its subsequent chromothripsis.

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“…PWS is the most common syndromic cause of life‐threatening obesity with an estimated incidence of 1/10 000 to 1/25 000 live births, occurring equally in both males and females, and across all ethnicities . The errors in genomic imprinting that are causative for PWS (determined by a DNA methylation analysis) are classified as paternal deletion , which represents the majority of all cases of PWS (60%); maternal uniparental disomy ( UPD ) 15 , found in about 36%; and imprinting centre defect ( ID ), in 4% …”

Section: Introductionmentioning

confidence: 99%

Current and emerging therapies for managing hyperphagia and obesity in Prader‐Willi syndrome: A narrative review

et al. 2019

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Summary In early childhood, individuals with Prader‐Willi syndrome (PWS) experience excess weight gain and severe hyperphagia with food compulsivity, which often leads to early onset morbid obesity. Effective treatments for appetite suppression and weight control are currently unavailable for PWS. Our aim to further understand the pathogenesis of PWS led us to carry out a comprehensive search of the current and emerging therapies for managing hyperphagia and extreme weight gain in PWS. A literature search was performed using PubMed and the following keywords: “PWS” AND “therapy” OR “[drug name]”; reference lists, pharmaceutical websites, and the ClinicalTrials.gov registry were also reviewed. Articles presenting data from current standard treatments in PWS and also clinical trials of pharmacological agents in the pipeline were selected. Current standard treatments include dietary restriction/modifications, exercise, and growth hormone replacement, which appear to have limited efficacy for appetite and weight control in patients with PWS. The long‐term safety and effectiveness of bariatric surgery in PWS remains unknown. However, many promising pharmacotherapies are in development and, if approved, will bring much needed choices into the PWS pharmacological armamentarium. With the progress that is currently being made in our understanding of PWS, an effective treatment may not be far off.

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Molecular genetic classification in Prader-Willi syndrome: a multisite cohort study

Cited by 119 publications

References 20 publications

Segmental isodisomy in Prader–Willi syndrome patients: The experience of a single diagnostic center

Segmental isodisomy in Prader–Willi syndrome patients: The experience of a single diagnostic center

Small supernumerary marker chromosomes: A legacy of trisomy rescue?

Current and emerging therapies for managing hyperphagia and obesity in Prader‐Willi syndrome: A narrative review

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