AI Article Synopsis

  • BRD4 is crucial for loading the cohesin complex onto DNA, which is essential for processes like loop extrusion and the formation of Topologically Associating Domains, and mutations in this complex can lead to conditions known as cohesinopathies, including Cornelia de Lange syndrome.
  • An international study was conducted to analyze clinical and genetic data from 14 new patients with BRD4-related disorders, including two fetuses, combining prenatal findings with information from pediatric and adult cases.
  • The study identifies distinct dysmorphic features associated with BRD4-related disorders and expands the understanding of cohesinopathies, providing a new pattern that differs from existing classifications.

Article Abstract

BRD4 is part of a multiprotein complex involved in loading the cohesin complex onto DNA, a fundamental process required for cohesin-mediated loop extrusion and formation of Topologically Associating Domains. Pathogenic variations in this complex have been associated with a growing number of syndromes, collectively known as cohesinopathies, the most classic being Cornelia de Lange syndrome. However, no cohort study has been conducted to delineate the clinical and molecular spectrum of BRD4-related disorder. We formed an international collaborative study, and collected 14 new patients, including two fetuses. We performed phenotype and genotype analysis, integrated prenatal findings from fetopathological examinations, phenotypes of pediatric patients and adults. We report the first cohort of patients with BRD4-related disorder and delineate the dysmorphic features at different ages. This work extends the phenotypic spectrum of cohesinopathies and characterize a new clinically relevant and recognizable pattern, distinguishable from the other cohesinopathies.

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Source
http://dx.doi.org/10.1111/cge.14141DOI Listing

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