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Series GSE121024 Query DataSets for GSE121024
Status Public on Jan 21, 2020
Title The role of Mediator and Little Elongation Complex in transcription termination
Organism Homo sapiens
Experiment type Genome binding/occupancy profiling by high throughput sequencing
Expression profiling by high throughput sequencing
Summary Mediator is a coregulatory complex involved in regulating the transcription of Pol II-dependent genes. Metazoan Mediator subunit MED26 functions as a docking site for the ELL/EAF-containing Super Elongation Complex (SEC) and L ittle Elongation Complex (LEC), which regulate the expression of distinct genes. MED26 helps to recruit SEC to protein-coding genes including c-Myc and LEC to small nuclear RNA (snRNA) genes. However, why MED26 takes advantage of SEC or LEC to regulate different claases of genes is unclear. Here, we present evidence that MED26 recruits LEC to support optimal transcription termination at non-polyadenylated genes including snRNA and replication-dependent histone (RDH) genes. Our findings indicate that LEC recruited by MED26 promotes efficient transcription termination by Pol II through interaction with CBC-ARS2 and NELF/DSIF, and then LEC promotes 3’-end processing through the recruitment of Integrator or Heat labile factor to snRNA or RDH genes, respectively.
 
Overall design Experiment 1: Rpb1 ChIP-seq HEK293T WT and MED26 mutant cells, using mouse chromatin as spike-in. Experiment 2: MED26 ChIP-seq in HEK293T WT cells. Experiment 3: PRO-seq in HEK293T WT and MED26 mutant cells, using D. melanogastor Kc167 cells as spike-in control. Experiment 4: RNA-seq of polyA-selected libraries prepared from HEK293T cells treated with control, AFF4, KIAA0947/ICE1, or MED26 siRNAs. Experiment 5: RNA-seq of ribo-depleted libraries prepared from HEK293T cells treated with control or MED26 siRNAs. Experiment 6: RNA-seq of ribo-depleted libraries prepared from HEK293T WT or MED26 mutant cells.
 
Contributor(s) Takahashi H, Ranjan A, Chen S, Chen K, Conaway JW, Hatakeyama S
Citation(s) 32102997
Submission date Oct 09, 2018
Last update date Mar 09, 2020
Contact name Shiyuan (Cynthia) Chen
E-mail(s) shc@stowers.org
Organization name Stowers Institute for Medical Research
Department Computational Biology
Street address 1000 E 50th St
City Kansas City
State/province MO
ZIP/Postal code 64110
Country USA
 
Platforms (2)
GPL16791 Illumina HiSeq 2500 (Homo sapiens)
GPL18573 Illumina NextSeq 500 (Homo sapiens)
Samples (54)
GSM3424025 293T-D2G8-MED26-MUT_Rpb1_Input_Rep1
GSM3424026 293T-D2G8-MED26-MUT_Rpb1_Input_Rep2
GSM3424027 293T-D2G8-MED26-MUT_Rpb1-IP_Rep1
Relations
BioProject PRJNA495373
SRA SRP164752

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
GSE121024_293T_Input_MED26_ChIP_Pooled.rpm.bw 1.1 Gb (ftp)(http) BW
GSE121024_293T_Med26_ChIP_Pooled.rpm.bw 465.9 Mb (ftp)(http) BW
GSE121024_RAW.tar 6.3 Gb (http)(custom) TAR (of BW)
GSE121024_RNAseqTPM.csv.gz 1.4 Mb (ftp)(http) CSV
GSE121024_RSEM_TPM_PolyARNA-seq.csv.gz 922.6 Kb (ftp)(http) CSV
GSE121024_RSEM_TPM_RiboDepRNA-seq.csv.gz 1.3 Mb (ftp)(http) CSV
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Raw data are available in SRA
Processed data are available on Series record
Processed data provided as supplementary file
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