AP-1/jun binding sites mediate serum inducibility of the human vimentin promoter.
AUTOR(ES)
Rittling, S R
RESUMO
The vimentin gene is inducible by serum in quiescent Balb/c 3T3 cells, but the molecular mechanism of this induction is unknown. The results presented here represent a first step towards the elucidation of the pathway of events leading from growth factor-receptor interaction to this induction. A series of Bal 31 deletions of the human vimentin promoter are used to show that a sequence residing at -700 is responsible for the serum, and also TPA inducibility of this gene. This sequence is able to confer serum inducibility upon uninducible constructs regardless of its position and orientation, indicating that it is this element alone which is required for this induction. The isolated sequence is a strong enhancer as well. Further deletions and the use of synthetic oligonucleotides demonstrate that a 24-mer containing two AP-1/jun binding sites confer both serum and TPA inducibility upon the human vimentin gene. Gel retardation analysis confirms that this sequence binds an AP-1 -like protein.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=336896Documentos Relacionados
- Serum, AP-1 and Ets-1 stimulate the human ets-1 promoter.
- Interleukin 1 induction of the c-jun promoter.
- Functional analysis and growth factor regulation of the human vimentin promoter.
- The SIF binding element confers sis/PDGF inducibility onto the c-fos promoter.
- Two AP1 sites binding JunB are essential for human papillomavirus type 18 transcription in keratinocytes.
