Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UNIPROT:P51532 (
transcriptional activator
)
6,546
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Notch signaling is involved in many cell fate determination events in metazoans. Ligand binding results in proteolytic cleavage to release the signal-transducing Notch intracellular domain (NICD). The nuclear protein RBP-J kappa, when complexed with NICD, acts as a
transcriptional activator
which, in turn, induces a target gene of Notch such as the repressors HES/E(spl) and HERP2. Under physiological stimulation using co-culture with Notch ligand-expressing cells and target cells expressing Notch receptors, the HES1 gene and the HERP2 gene have been shown to be directly up-regulated by Notch ligand binding. However, expression of another member of the HERP family,
HERP1
, was not induced by ligand stimulation in any cells tested, leading to the suggestion that
HERP1
may not be an immediate target of Notch or that Notch pathways can be cell type-specific. Because
HERP1
appears to play a central role in the development of the aorta (Zhong, T. P., Rosenberg, M., Mohideen, M. A., Weinstein, B., and Fishman, M. C. (2000) Science 287, 1820-1824), we re-addressed the issue of its relationship with the Notch pathway by examining its expression in A10 smooth muscle cells derived from thoracic aorta. We show that in these specific cells
HERP1
is also a direct target gene of Notch. NICD activates the
HERP1
promoter in an RBP-J kappa-dependent manner, and induces expression of endogenous
HERP1
mRNA as well as
HERP1
protein in A10 cells. Co-culture with Notch ligand-bearing cells induces endogenous
HERP1
mRNA expression in A10 cells, and these events occur even in the absence of de novo protein synthesis. In addition, RBP-J kappa proved essential for induction of
HERP1
mRNA in Notch signaling because exogenous RBP-J kappa was sufficient to rescue
HERP1
mRNA expression in RBP-J kappa-deficient cells. These findings provide the first solid evidence that
HERP1
is a novel primary target of Notch and underscores the cell-specific complexity of the Notch regulatory pathway. Given that Notch signaling plays a crucial role in vascular development, Notch may derive its function via HERP family members.
...
PMID:HERP1 is a cell type-specific primary target of Notch. 1174 89
