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Series GSE193484 Query DataSets for GSE193484
Status Public on May 08, 2024
Title Super-silencer perturbation by EZH2 and REST inhibition leads to large loss of chromatin interactions and reduction in cancer growth [HiChIP]
Organism Homo sapiens
Experiment type Genome binding/occupancy profiling by high throughput sequencing
Summary Human silencers have been shown to exist and regulate developmental gene expression. However, the functional importance of human silencers need to be elucidated such as the working mode and whether they can form “super-silencers”. Here, through interrogating two putative silencer components of FGF18 gene, we found that two silencers can cooperate via compensated chromatin interactions to form the “super-silencer”. Furthermore, double knock-out of two silencers exhibited synergistic upregulation of FGF18 expression and changes of cell identity. To disturb the “super-silencers”, we applied the combinational treatment of GSK343 and X5050 (“GR”). We found that GR led to severe loss of TADs and loops, while any single treatment only had mild changes. Such changes of TADs and loops may due to the decreased CTCF proteins upon the GR treatment. Moreover, GSK343 and X5050 can work synergistically to upregulated the super-silencer controlled apoptotic genes, thus gave rise to antitumor effects including apoptosis, cell cycle arrest and tumor growth inhibition. Overall, our data demonstrated the first example of “super-silencer” and showed that combinational usage of GSK343 and X5050 maybe the potential drug to curing cancers through disruption of “super-silencers”.
 
Overall design Silencer knockout (KO) Hi-C data has two biological replicates for each condition including EV, S1KO, S2KO, and DKO. Drug treatment Hi-C data has two biological replicates for each drug-treated condition, including DMSO, GSK343, X5050, GR 8h, GR 24h, and GR 72h. Drug treatment Hi-C data has two biological replicates for each DMSO- and etoposide-treated K562 cells (72 hr). siRNA Hi-C data has two biological replicates for each siScramble- and siCTCF-treated K562 cells (48 h). Silencer KO 4C has two biological replicates for each condition (EV, S1KO, and DKO). Silencer KO RNA-seq has two biological replicates for different KO cells (EV, S1KO S2KO, and DKO). H3K27me3 and H3K27ac ChIP-seq for silencer KO cells (EV, S1KO, and DKO) have two biological replicates. H3K27me3 HiChIP in wild-type K562 cells has one biological replicate. Cut and Run CTCF has two biological replicates for CTCF antibodies in EV, S1KO, S2KO, and DKO cells. Cut and Run H3K27me3 has two biological replicates for H3K27me3 antibodies (24 h) in THP1 and K562 cells. ATAC-seq has two biological replicates for each EV, S1KO, S2KO, and DKO cells. ATAC-seq has two biological replicates for each DMSO- and GR-treated K562 cells (72 h). Drug-treated K562 cells RNA-seq has two biological replicates including DMSO, GSK343, X5050, GR 8 h, GR 24 h, and GR 72 h.
 
Contributor(s) Zhang Y, Chen K, Tang S, Cai Y, Fullwood MJ
Citation(s) 39304765
Submission date Jan 11, 2022
Last update date Sep 24, 2024
Contact name KAIJING CHEN
E-mail(s) KAIJING001@e.ntu.edu.sg
Phone 98667053
Organization name Nanyang Technological University
Department school of biological science
Lab Melissa Fullwood
Street address 60 Nanyang Drive​​
City Singapore
ZIP/Postal code 637551
Country Singapore
 
Platforms (1)
GPL20301 Illumina HiSeq 4000 (Homo sapiens)
Samples (1)
GSM5808388 K562 H3K27me3 HiChIP
This SubSeries is part of SuperSeries:
GSE193489 Super-silencer perturbation by EZH2 and REST inhibition leads to large loss of chromatin interactions and reduction in cancer growth
Relations
BioProject PRJNA796346
SRA SRP354559

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
GSE193484_RAW.tar 1.1 Gb (http)(custom) TAR (of BED, HIC)
SRA Run SelectorHelp
Raw data are available in SRA
Processed data provided as supplementary file

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