Identification of a family of cAMP response element-binding protein coactivators by genome-scale functional analysis in mammalian cells.

نویسندگان

  • Vadim Iourgenko
  • Wenjun Zhang
  • Craig Mickanin
  • Ira Daly
  • Can Jiang
  • Jonathan M Hexham
  • Anthony P Orth
  • Loren Miraglia
  • Jodi Meltzer
  • Dan Garza
  • Gung-Wei Chirn
  • Elizabeth McWhinnie
  • Dalia Cohen
  • Joanne Skelton
  • Robert Terry
  • Yang Yu
  • Dale Bodian
  • Frank P Buxton
  • Jian Zhu
  • Chuanzheng Song
  • Mark A Labow
چکیده

This report describes an unbiased method for systematically determining gene function in mammalian cells. A total of 20,704 predicted human full-length cDNAs were tested for induction of the IL-8 promoter. A number of genes, including those for cytokines, receptors, adapters, kinases, and transcription factors, were identified that induced the IL-8 promoter through known regulatory sites. Proteins that acted through a cooperative interaction between an AP-1 and an unrecognized cAMP response element (CRE)-like site were also identified. A protein, termed transducer of regulated cAMP response element-binding protein (CREB) (TORC1), was identified that activated expression through the variant CRE and consensus CRE sites. TORC1 potently induced known CREB1 target genes, bound CREB1, and activated expression through a potent transcription activation domain. A functional Drosophila TORC gene was also identified. Thus, TORCs represent a family of highly conserved CREB coactivators that may control the potency and specificity of CRE-mediated responses.

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عنوان ژورنال:
  • Proceedings of the National Academy of Sciences of the United States of America

دوره 100 21  شماره 

صفحات  -

تاریخ انتشار 2003