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Attenuation of Forkhead signaling by the retinal determination factor DACH1.


ABSTRACT: The Drosophila Dachshund (Dac) gene, cloned as a dominant inhibitor of the hyperactive growth factor mutant ellipse, encodes a key component of the retinal determination gene network that governs cell fate. Herein, cyclic amplification and selection of targets identified a DACH1 DNA-binding sequence that resembles the FOX (Forkhead box-containing protein) binding site. Genome-wide in silico promoter analysis of DACH1 binding sites identified gene clusters populating cellular pathways associated with the cell cycle and growth factor signaling. ChIP coupled with high-throughput sequencing mapped DACH1 binding sites to corresponding gene clusters predicted in silico and identified as weight matrix resembling the cyclic amplification and selection of targets-defined sequence. DACH1 antagonized FOXM1 target gene expression, promoter occupancy in the context of local chromatin, and contact-independent growth. Attenuation of FOX function by the cell fate determination pathway has broad implications given the diverse role of FOX proteins in cellular biology and tumorigenesis.

SUBMITTER: Zhou J 

PROVIDER: S-EPMC2872468 | biostudies-literature | 2010 Apr

REPOSITORIES: biostudies-literature

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Attenuation of Forkhead signaling by the retinal determination factor DACH1.

Zhou Jie J   Wang Chenguang C   Wang Zhibin Z   Dampier Will W   Wu Kongming K   Casimiro Mathew C MC   Chepelev Iouri I   Popov Vladimir M VM   Quong Andrew A   Tozeren Aydin A   Zhao Keji K   Lisanti Michael P MP   Pestell Richard G RG  

Proceedings of the National Academy of Sciences of the United States of America 20100329 15


The Drosophila Dachshund (Dac) gene, cloned as a dominant inhibitor of the hyperactive growth factor mutant ellipse, encodes a key component of the retinal determination gene network that governs cell fate. Herein, cyclic amplification and selection of targets identified a DACH1 DNA-binding sequence that resembles the FOX (Forkhead box-containing protein) binding site. Genome-wide in silico promoter analysis of DACH1 binding sites identified gene clusters populating cellular pathways associated  ...[more]

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