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SRX17794329: GSM6615448: 22Rv1_ATAC_ENZ3w_1nM-DHT_rep1; Homo sapiens; ATAC-seq
1 ILLUMINA (NextSeq 500) run: 47.1M spots, 4G bases, 1.5Gb downloads

External Id: GSM6615448_r1
Submitted by: Biomedicine, School of Medicine, University of Eastern Finland
Study: Chromatin accessibility and pioneer factor FOXA1 restrict glucocorticoid receptor action in prostate cancer (ATAC-Seq)
show Abstracthide Abstract
Treatment of prostate cancer relies predominantly on the inhibition of androgen receptor (AR) signaling. Despite the initial effectiveness of the AR-targeted therapies, the cancer often develops resistance to the AR blockade. One mechanism of the resistance is glucocorticoid receptor (GR)-mediated replacement of AR. Nevertheless, the mechanistic ways and means how the GR-mediated antiandrogen resistance occurs has remained elusive. Here, we have discovered several crucial features of GR action in prostate cancer cells through genome-wide techniques. We detected that the replacement of AR by GR in antiandrogen-exposed prostate cancer cells occurs almost exclusively at pre-accessible chromatin sites displaying FOXA1 occupancy. Counterintuitively to the classical pioneer factor model, silencing of FOXA1 potentiated the chromatin binding and transcriptional activity of GR. This was attributed to FOXA1-mediated repression of the NR3C1 (gene encoding GR) expression via the corepressor TLE3. In comparison to FOXA1, inhibition of coregulator activity efficiently restricted GR-mediated gene regulation and cell proliferation. Overall, we identified chromatin pre-accessibility and FOXA1-mediated repression as important regulators of GR action in prostate cancer, pointing out new avenues to oppose steroid receptor-mediated drug resistance. Overall design: Examination of chromatin accessibility by ATAC-seq from VCaP and 22Rv1 prostate cancer cells grown in the presence or absence of ENZ. All sequencing was done with Illumina NextSeq 500.
Sample: 22Rv1_ATAC_ENZ3w_1nM-DHT_rep1
SAMN31149893 • SRS15320001 • All experiments • All runs
Organism: Homo sapiens
Library:
Name: GSM6615448
Instrument: NextSeq 500
Strategy: ATAC-seq
Source: GENOMIC
Selection: other
Layout: PAIRED
Construction protocol: For ATAC-seq, 100 000 isolated nuclei were treated with 2.5 µl Tn5 Transposase loaded with sequencing adapters. ATAC-seq libraries were prepared with loaded Diagenode Tagmentase (#C01070012) according to instructions.
Runs: 1 run, 47.1M spots, 4G bases, 1.5Gb
Run# of Spots# of BasesSizePublished
SRR2180050047,060,6544G1.5Gb2023-11-07

ID:
24714104

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