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Series GSE163771 Query DataSets for GSE163771
Status Public on Sep 06, 2022
Title OCT4-SOX2 dimers reshape the epigenome to promote neural crest multipotency [ATAC-Seq]
Organisms Gallus gallus; Homo sapiens
Experiment type Genome binding/occupancy profiling by high throughput sequencing
Summary The transcription factors OCT4 and SOX2 play an essential role in the establishment and maintenance of pluripotent embryonic stem cells (ESCs). Yet, their function in specialized stem cell populations is still poorly understood. Here, we show that the OCT4 and SOX2 work as dimers to regulate the epigenomic landscape of neural crest cells. By isolating primary neural crest cells at a range of developmental stages, we characterized the transcriptomic and epigenomic changes that take place during specification, migration, and early differentiation. Analysis of these datasets revealed that the OCT4/SOX2 dimer promotes an epigenomic signature inherent to the multipotent neural crest. We found that the emergence of this epigenomic state requires the translocation of OCT4/SOX2 to tissue-specific cis-regulatory regions. By examining genome organization during the induction of hESCs into neural crest cells, we observed that the patterns of genomic occupancy of the dimer are modified during cell fate commitment. Dimer translocation is guided by neural crest-specific pioneer transcription factors, which physically interact with the OCT4/SOX to modify their genomic targets. Our results demonstrate how the ESC pluripotency program is repurposed in specialized stem cells to control chromatin organization and define the developmental potential of embryonic progenitors.
 
Overall design There are three separate experiments in which we performed OMNI-ATAC-Seq. Group #1 - We electroporated chicken embryos with a TFAP2AE1-driven GFP reporter, which marks neural crest. We isolated GFP+ neural crest cells via FACS from various stages across early chicken development, and subjected them to OMNI-ATAC-Seq. Group #2 - We electroporated chicken embryos bilaterally. One side received a control vector (TFAP2AE1-GFP + empty PCI-H2B-RFP) and the other recieved an overexpression vector (TFAP2AE1-GFP + PCI-OCT4-SOX2-H2B-RFP). We isolated GFP+/RFP+ cells from the control and treatment side of the embryos, and performed OMNI-ATAC-Seq on each sample. Group #3 - We generated induced neural crest (iNCCs) from hESC. Along their differentiation, we performed OMNI-ATAC-Seq at multiple timepoints.
 
Contributor(s) Hovland AS, Bhattacharya D, Rothstein M, Simoes-Costa M
Citation(s) 36182685
Submission date Dec 23, 2020
Last update date Oct 28, 2022
Contact name Marcos Simoes-Costa
E-mail(s) [email protected]
Organization name Cornell University
Department Molecular Biology and Genetics
Lab Simoes-Costa Lab
Street address 526 Campus Rd
City Ithaca
State/province New York
ZIP/Postal code 14853
Country USA
 
Platforms (2)
GPL21697 NextSeq 550 (Homo sapiens)
GPL27748 NextSeq 550 (Gallus gallus)
Samples (26)
GSM4986881 11306_10331_109901_HG3JFBGXC_TGGTCA_HH10_1
GSM4986882 11419_10946_112321_HVKM5BGXC_ACAGTGGT_HH10_2
GSM4986883 11419_10946_112321_HVKM5BGXC_CAGATCCA_HH12_1
This SubSeries is part of SuperSeries:
GSE163961 OCT4-SOX2 dimers reshape the epigenome to promote neural crest multipotency
Relations
BioProject PRJNA687499
SRA SRP299102

Download family Format
SOFT formatted family file(s) SOFTHelp
MINiML formatted family file(s) MINiMLHelp
Series Matrix File(s) TXTHelp

Supplementary file Size Download File type/resource
GSE163771_RAW.tar 51.9 Mb (http)(custom) TAR (of NARROWPEAK)
GSE163771_samples_ATAC_400bp.RDS.gz 19.2 Mb (ftp)(http) RDS
GSE163771_samples_ATAC_400bp_counts.txt.gz 2.2 Mb (ftp)(http) TXT
GSE163771_samples_Overexpression_ATAC.RDS.gz 11.6 Mb (ftp)(http) RDS
GSE163771_samples_Overexpression_ATAC_counts.txt.gz 2.0 Mb (ftp)(http) TXT
GSE163771_samples_human_ATAC.RDS.gz 37.7 Mb (ftp)(http) RDS
GSE163771_samples_human_ATAC_counts.txt.gz 4.3 Mb (ftp)(http) TXT
SRA Run SelectorHelp
Raw data are available in SRA
Processed data provided as supplementary file
Processed data are available on Series record

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