BETting on a Transcriptional Deficit as the Main Cause for Cornelia de Lange Syndrome

García-Gutiérrez, Pablo; García-Domínguez, Mario

Publication:
BETting on a Transcriptional Deficit as the Main Cause for Cornelia de Lange Syndrome

dc.contributor.author	García-Gutiérrez, Pablo
dc.contributor.author	García-Domínguez, Mario
dc.contributor.authoraffiliation	[García-Gutiérrez,P; García-Domínguez,M] Andalusian Centre for Molecular Biology and Regenerative Medicine-CABIMER, CSIC-Universidad de Sevilla-Universidad Pablo de Olavide, Seville, Spain.
dc.contributor.funder	Research at our lab is currently supported by grants PGC 2018-094232-B-I00 from Ministry of Science, Innovation and Universities (MICIU), Spain, and CV20-93141 from regional government from Andalusia (both co-financed by the European regional development fund), to MG-D.
dc.date.accessioned	2022-10-03T06:53:15Z
dc.date.available	2022-10-03T06:53:15Z
dc.date.issued	2021-07-27
dc.description.abstract	Cornelia de Lange Syndrome (CdLS) is a human developmental syndrome with complex multisystem phenotypic features. It has been traditionally considered a cohesinopathy together with other phenotypically related diseases because of their association with mutations in subunits of the cohesin complex. Despite some overlap, the clinical manifestations of cohesinopathies vary considerably and, although their precise molecular mechanisms are not well defined yet, the potential pathomechanisms underlying these diverse developmental defects have been theoretically linked to alterations of the cohesin complex function. The cohesin complex plays a critical role in sister chromatid cohesion, but this function is not affected in CdLS. In the last decades, a non-cohesion-related function of this complex on transcriptional regulation has been well established and CdLS pathoetiology has been recently associated to gene expression deregulation. Up to 70% of CdLS cases are linked to mutations in the cohesin-loading factor NIPBL, which has been shown to play a prominent function on chromatin architecture and transcriptional regulation. Therefore, it has been suggested that CdLS can be considered a transcriptomopathy. Actually, CdLS-like phenotypes have been associated to mutations in chromatin-associated proteins, as KMT2A, AFF4, EP300, TAF6, SETD5, SMARCB1, MAU2, ZMYND11, MED13L, PHIP, ARID1B, NAA10, BRD4 or ANKRD11, most of which have no known direct association with cohesin. In the case of BRD4, a critical highly investigated transcriptional coregulator, an interaction with NIPBL has been recently revealed, providing evidence on their cooperation in transcriptional regulation of developmentally important genes. This new finding reinforces the notion of an altered gene expression program during development as the major etiological basis for CdLS. In this review, we intend to integrate the recent available evidence on the molecular mechanisms underlying the clinical manifestations of CdLS, highlighting data that favors a transcription-centered framework, which support the idea that CdLS could be conceptualized as a transcriptomopathy.	es_ES
dc.description.version	Yes	es_ES
dc.identifier.citation	García-Gutiérrez P, García-Domínguez M. BETting on a Transcriptional Deficit as the Main Cause for Cornelia de Lange Syndrome. Front Mol Biosci. 2021 Jul 27;8:709232	es_ES
dc.identifier.doi	10.3389/fmolb.2021.709232	es_ES
dc.identifier.essn	2296-889X
dc.identifier.pmc	PMC8353280
dc.identifier.pmid	34386522	es_ES
dc.identifier.uri	http://hdl.handle.net/10668/4207
dc.journal.title	Frontiers in Molecular Biosciences
dc.language.iso	en
dc.page.number	18 p.
dc.publisher	Frontiers	es_ES
dc.relation.publisherversion	https://www.frontiersin.org/articles/10.3389/fmolb.2021.709232/full	es_ES
dc.rights	Atribución 4.0 Internacional	*
dc.rights.accessRights	Acceso abierto	es_ES
dc.rights.uri	http://creativecommons.org/licenses/by/4.0/	*
dc.subject	CdLS	es_ES
dc.subject	NIPBL	es_ES
dc.subject	BRD4	es_ES
dc.subject	Transcription	es_ES
dc.subject	Transcriptomopathy	es_ES
dc.subject	Síndrome de De Lange	es_ES
dc.subject	Transcripción genética	es_ES
dc.subject	Proteínas	es_ES
dc.subject	Mutación	es_ES
dc.subject	Expresión génica	es_ES
dc.subject.mesh	Medical Subject Headings::Organisms::Eukaryota::Animals::Chordata::Vertebrates::Mammals::Primates::Haplorhini::Catarrhini::Hominidae::Humans	es_ES
dc.subject.mesh	Medical Subject Headings::Diseases::Nervous System Diseases::Neurologic Manifestations::Neurobehavioral Manifestations::Intellectual Disability::De Lange Syndrome	es_ES
dc.subject.mesh	Medical Subject Headings::Chemicals and Drugs::Amino Acids, Peptides, and Proteins::Proteins::Nuclear Proteins	es_ES
dc.subject.mesh	Medical Subject Headings::Anatomy::Cells::Cellular Structures::Intracellular Space::Cell Nucleus::Cell Nucleus Structures::Intranuclear Space::Chromosomes::Chromosome Structures::Chromatids	es_ES
dc.subject.mesh	Medical Subject Headings::Chemicals and Drugs::Amino Acids, Peptides, and Proteins::Proteins::Transcription Factors	es_ES
dc.subject.mesh	Medical Subject Headings::Anatomy::Cells::Cellular Structures::Intracellular Space::Cell Nucleus::Cell Nucleus Structures::Intranuclear Space::Chromosomes::Chromosome Structures::Chromatin	es_ES
dc.subject.mesh	Medical Subject Headings::Phenomena and Processes::Genetic Phenomena::Phenotype	es_ES
dc.subject.mesh	Medical Subject Headings::Phenomena and Processes::Genetic Phenomena::Genetic Variation::Mutation	es_ES
dc.subject.mesh	Medical Subject Headings::Phenomena and Processes::Genetic Phenomena::Genetic Processes::Gene Expression	es_ES
dc.title	BETting on a Transcriptional Deficit as the Main Cause for Cornelia de Lange Syndrome	es_ES
dc.type	review article
dc.type.hasVersion	VoR
dspace.entity.type	Publication