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SRX4496705: GSM3316874: AML_P24_Dx_H3K27ac; Homo sapiens; ChIP-Seq
1 ILLUMINA (NextSeq 500) run: 33.3M spots, 2.5G bases, 973.6Mb downloads

Submitted by: NCBI (GEO)
Study: AML subtype is a major determinant of the association between prognostic gene expression signatures and their clinical significance.
show Abstracthide Abstract
Relapse in acute myeloid leukemia (AML) may result from variable genetic origins or convergence on common biological processes. Exploiting the specificity and sensitivity of regulatory DNA, we analyze patient samples of multiple clinical outcomes covering various AML molecular subtypes. We uncover regulatory variation between patients translating into a transcriptional signature that predicts relapse risk. In addition, we find clusters of co-expressed genes within this signature selectively link to relapse risk in distinct patient subgroups defined by molecular subtype or AML maturation. Analyzing these gene clusters and the AML subtypes separately enhances their prognostic value substantially and provides insight in the mechanisms underlying relapse risk across the distinct patient subgroups. We propose that prognostic gene expression signatures in AML are valid only within patient subgroups and do not transcend these subgroups. Overall design: ChIP-sequencing for H3K27ac and RNA-sequencing of pediatric AML patient samples.
Sample: AML_P24_Dx_H3K27ac
SAMN09754251 • SRS3617773 • All experiments • All runs
Organism: Homo sapiens
Library:
Instrument: NextSeq 500
Strategy: ChIP-Seq
Source: GENOMIC
Selection: ChIP
Layout: SINGLE
Construction protocol: TruSeq DNA sample preparation kit (Illumina)
Experiment attributes:
GEO Accession: GSM3316874
Links:
Runs: 1 run, 33.3M spots, 2.5G bases, 973.6Mb
Run# of Spots# of BasesSizePublished
SRR763297433,295,2952.5G973.6Mb2019-09-10

ID:
6092973

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