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Series GSE108515 Query DataSets for GSE108515
Status Public on Nov 01, 2018
Title Disruption of the TFAP2A regulatory domain causes Branchio-Oculo-Facial Syndrome (BOFS) and illuminates pathomechanisms for other human neurocristopathies [4C-seq data set 1]
Organisms Gallus gallus; Homo sapiens
Experiment type Other
Summary BOFS is a rare congenital syndrome that arises due to defects during neural crest (NC) development and is thus considered as a human neurocristopathy. All reported BOFS cases are caused by heterozygous mutations within TFAP2A. Here we describe a unique BOFS patient carrying a de novo heterozygous inversion in which one of the breakpoints is located 40 kb downstream of TFAP2A. Using in vitro and in vivo NC developmental models, we uncovered that TFAP2A is located within a large Topologically Associating Domain (TAD) containing enhancers essential for TFAP2A expression in NC cells (NCC). Importantly, using patient-specific hiPSC lines, we showed that the inversion causes a loss of physical interactions between the inverted TFAP2A allele and its cognate enhancers, leading to TFAP2A monoallelic and haploinsufficient expression in human NCC. More generally, our results highlight potential etiological mechanisms for other human neurocristopathies and illustrate how TAD disruption can lead to a loss of enhancer gene-interactions and, consequently, to pathological changes in gene expression.
 
Overall design 4C-seq interaction profiles were generated in human cells (WT hiPSC, WT hNCC and BOFS patient hNCC) and chicken embryonic tissue (Frontonasal prominences (FNP)) using as viewpoints the TFAP2A promoters or different enhancers located within the TFAP2A regulatory domain (Enh100, Enh480).
 
Contributor(s) Bartusel M, Laugsch M, Rada-Iglesias A
Citation(s) 30982769
Submission date Dec 26, 2017
Last update date Oct 05, 2020
Contact name Milos Nikolic
E-mail(s) milosn@gmail.com
Organization name Center for Molecular Medicine Cologne
Street address Robert Koch Str. 21
City Koeln
State/province Nordrhein-Westfalen
ZIP/Postal code 50674
Country Germany
 
Platforms (2)
GPL16791 Illumina HiSeq 2500 (Homo sapiens)
GPL19005 Illumina HiSeq 2500 (Gallus gallus)
Samples (13)
GSM2902644 WT_hiPSC_TFAP2A_Prom_1
GSM2902645 WT_hiPSC_TFAP2A_Prom_2
GSM2902646 WT_hiPSC_TFAP2A_Enh480_1
This SubSeries is part of SuperSeries:
GSE108522 Disruption of the TFAP2A regulatory domain causes Branchio-Oculo-Facial Syndrome (BOFS) and illuminates pathomechanisms for other human neurocristopathies
Relations
BioProject PRJNA427534
SRA SRP127544

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Supplementary file Size Download File type/resource
GSE108515_RAW.tar 519.1 Mb (http)(custom) TAR (of BEDGRAPH)
GSE108515_WT_hiPSC_TFAP2A_Enh100.bedgraph.gz 82.1 Mb (ftp)(http) BEDGRAPH
GSE108515_WT_hiPSC_TFAP2A_Enh480.bedgraph.gz 81.9 Mb (ftp)(http) BEDGRAPH
GSE108515_WT_hiPSC_TFAP2A_Prom.bedgraph.gz 81.9 Mb (ftp)(http) BEDGRAPH
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Raw data are available in SRA
Processed data provided as supplementary file
Processed data are available on Series record
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