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: EC:2.7.11.22 (
cdc2
)
8,319
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Transcriptional function of cyclin D1, whose deregulation is frequently observed in human cancers, has been suggested to contribute to cancer formation. In the present study, we show that cyclin D1 protein inhibits
RUNX3
activity by directly binding to it and interfering with its interaction with p300 interaction in lung cancer cells. Cyclin D1 inhibits p300-dependent
RUNX3
acetylation and negatively regulates cyclin-dependent kinase (cdk) inhibitor p21 expression. These transcriptional effects of cyclin D1 do not require
cdk4
/6 kinase activation. We propose that cyclin D1 provides a transcriptional switch that allows the tumor suppressor activity of
RUNX3
to be repressed in cancer cells. Since
RUNX3
plays tumor suppressive roles in a wide range of cancers, a non-canonical cyclin D1 function may be critical for neoplastic transformation of the epithelial cells in which
RUNX3
regulates proliferation.
...
PMID:Cyclin D1 blocks the anti-proliferative function of RUNX3 by interfering with RUNX3-p300 interaction. 2080 Oct 98
Here we presented that the expression of
RUNX3
was significantly decreased in 75 cases of clear cell renal cell carcinoma (CCRCC) tissues (p<0.05). Enforced
RUNX3
expression mediated 786-O cells to exhibit inhibition of growth, G1 cell-cycle arrest and metastasis in vitro, and to lost tumorigenicity in nude mouse model in vivo.
RUNX3
-induced growth suppression was found partially to regulate various proteins, including inhibition of cyclinD1, cyclinE,
cdk2
,
cdk4
and p-Rb, but increase of p27(Kip1), Rb and TIMP-1. Therefore,
RUNX3
had the function of inhibiting the proliferative and metastatic abilities of CCRCC cells by regulating cyclins and TIMP1.
...
PMID:RUNX3 mediates suppression of tumor growth and metastasis of human CCRCC by regulating cyclin related proteins and TIMP-1. 2245 27
Granulosa cell tumors of the ovary (GCT) are the predominant type of ovarian sex cord/stromal tumor. Although prognosis is generally favorable, the outcome for advanced and recurrent GCT is poor. A better understanding of the molecular pathogenesis of GCT is critical to developing effective therapeutic strategies. Here we have examined the potential role of the runt-related transcription factor
RUNX3
. There are only two GCT cell lines available. While
RUNX3
is silenced in the GCT cell line KGN cells, it is highly expressed in another GCT cell line, COV434 cells. Re-expression of
RUNX3
promotes proliferation, anchorage-independent growth, and motility in KGN cells in vitro and tumor formation in mice in vivo. Furthermore, expression of a dominant negative form of
RUNX3
decreases proliferation of COV434 cells. To address a potential mechanism of action, we examined expression of cyclin D2 and the
CDK
inhibitor p27
Kip1
, two cell cycle regulators known to be critical determinants of GCT cell proliferation. We found that
RUNX3
upregulates the expression of cyclin D2 at the mRNA and protein level, and decreases the level of the p27
Kip1
protein, but not p27
Kip1
mRNA. In conclusion, we demonstrate that RUNX proteins are expressed in GCT cell lines and human GCT specimens, albeit at variable levels, and
RUNX3
may play an oncogenic role in a subset of GCTs.
...
PMID:RUNX3 Promotes the Tumorigenic Phenotype in KGN, a Human Granulosa Cell Tumor-Derived Cell Line. 3131 Nov 13
