Clinical findings in 39 individuals with Bohring–Opitz syndrome from a global patient‐driven registry with implications for tumor surveillance and recurrence risk

Clinical findings in 39 individuals with Bohring–Opitz syndrome from a global patient‐driven registry with implications for tumor surveillance and recurrence risk

Bohring–Opitz syndrome (BOS) is a rare genetic condition caused by pathogenic variants in ASXL1, which is a gene involved in chromatin regulation. BOS is characterized by severe intellectual disabilities, distinctive facial features, hypertrichosis, facial nevus simplex, severe myopia, a typical pos...

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Veröffentlicht in:American journal of medical genetics. Part A 2023-04, Vol.191 (4), p.1050-1058
Hauptverfasser: Russell, Bianca E., Kianmahd, Rebecca R., Munster, Chelsea, Yu, Anna, Ahad, Leena, Tan, Wen‐Hann
Format: Artikel
Sprache:eng
Schlagworte:
ASXL1
Bohring–Opitz syndrome
Chromatin
Cranial sutures
Craniosynostoses - genetics
Craniosynostosis
Genotypes
hepatoblastoma
Humans
Hypertrichosis
Intellectual disabilities
Intellectual Disability - genetics
Kidney Neoplasms
Liver Neoplasms
mosaicism
Motor skill
Myopia
Nevus
Opitz syndrome
Phenotypes
Repressor Proteins - genetics
Tumors
Wilms Tumor
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container_end_page 1058
container_issue 4
container_start_page 1050
container_title American journal of medical genetics. Part A
container_volume 191
creator Russell, Bianca E.
Kianmahd, Rebecca R.
Munster, Chelsea
Yu, Anna
Ahad, Leena
Tan, Wen‐Hann
description Bohring–Opitz syndrome (BOS) is a rare genetic condition caused by pathogenic variants in ASXL1, which is a gene involved in chromatin regulation. BOS is characterized by severe intellectual disabilities, distinctive facial features, hypertrichosis, facial nevus simplex, severe myopia, a typical posture in infancy, variable anomalies, and feeding issues. Wilms tumor has also been reported in two individuals. We report survey data from the largest known cohort of individuals with BOS with 34 participants from the ASXL Patient‐Driven Registry and data on five additional individuals with notable findings. Important or novel findings include hepatoblastoma (n = 1), an additional individual with Wilms tumor, two families with a parent who is mosaic including a pair of siblings, birth weights within the normal range for the majority of participants, as well as presence of craniosynostosis and hernias. Data also include characterization of communication, motor skills, and care level including hospitalization frequency and surgical interventions. No phenotype–genotype correlation could be identified. The ASXL Registry is also presented as a crucial tool for furthering ASXL research and to support the ASXL community.
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ispartof American journal of medical genetics. Part A, 2023-04, Vol.191 (4), p.1050-1058
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source Wiley Online Library - AutoHoldings Journals; MEDLINE
subjects ASXL1
Bohring–Opitz syndrome
Chromatin
Cranial sutures
Craniosynostoses - genetics
Craniosynostosis
Genotypes
hepatoblastoma
Humans
Hypertrichosis
Intellectual disabilities
Intellectual Disability - genetics
Kidney Neoplasms
Liver Neoplasms
mosaicism
Motor skill
Myopia
Nevus
Opitz syndrome
Phenotypes
Repressor Proteins - genetics
Tumors
Wilms Tumor
title Clinical findings in 39 individuals with Bohring–Opitz syndrome from a global patient‐driven registry with implications for tumor surveillance and recurrence risk
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