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Genome-wide identification and characterization of Notch transcription complex-binding sequence-paired sites in leukemia cells.


ABSTRACT: Notch transcription complexes (NTCs) drive target gene expression by binding to two distinct types of genomic response elements, NTC monomer-binding sites and sequence-paired sites (SPSs) that bind NTC dimers. SPSs are conserved and have been linked to the Notch responsiveness of a few genes. To assess the overall contribution of SPSs to Notch-dependent gene regulation, we determined the DNA sequence requirements for NTC dimerization using a fluorescence resonance energy transfer (FRET) assay and applied insights from these in vitro studies to Notch-"addicted" T cell acute lymphoblastic leukemia (T-ALL) cells. We found that SPSs contributed to the regulation of about a third of direct Notch target genes. Although originally described in promoters, SPSs are present mainly in long-range enhancers, including an enhancer containing a newly described SPS that regulates HES5 expression. Our work provides a general method for identifying SPSs in genome-wide data sets and highlights the widespread role of NTC dimerization in Notch-transformed leukemia cells.

SUBMITTER: Severson E 

PROVIDER: S-EPMC5931361 | biostudies-literature | 2017 May

REPOSITORIES: biostudies-literature

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Genome-wide identification and characterization of Notch transcription complex-binding sequence-paired sites in leukemia cells.

Severson Eric E   Arnett Kelly L KL   Wang Hongfang H   Zang Chongzhi C   Taing Len L   Liu Hudan H   Pear Warren S WS   Shirley Liu X X   Blacklow Stephen C SC   Aster Jon C JC  

Science signaling 20170502 477


Notch transcription complexes (NTCs) drive target gene expression by binding to two distinct types of genomic response elements, NTC monomer-binding sites and sequence-paired sites (SPSs) that bind NTC dimers. SPSs are conserved and have been linked to the Notch responsiveness of a few genes. To assess the overall contribution of SPSs to Notch-dependent gene regulation, we determined the DNA sequence requirements for NTC dimerization using a fluorescence resonance energy transfer (FRET) assay an  ...[more]

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