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Query: UNIPROT:P43146 (
tumour suppressor
)
5,935
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The H-rev107
tumour suppressor
was isolated as a gene specifically expressed in rat fibroblasts resistant toward malignant transformation by the activated HRAS gene (Sers et al., 1997; Hajnal et al., 1994). Here we describe the human homologue of the rat H-rev107 gene. The predicted rat and human proteins are highly conserved exhibiting an overall amino acid identity of 83%. The
H-REV107-1
gene is ubiquitously expressed with the exception of haematopoetic cells and tissues. In contrast,
H-REV107-1
mRNA was found only in eight of 27 cell lines derived from mammary carcinoma, lung carcinoma, gastric carcinoma, kidney carcinoma, melanoma, neuroblastoma and other tumours. The
H-REV107-1
protein was not detectable in any of these tumour cells. Loss of
H-REV107-1
expression was not restricted to cultured human tumour cell lines, but also found in primary squamous cell carcinomas. Gross structural aberrations of the
H-REV107-1
gene were absent in tumorigenic cell lines. Thus, the block to
H-REV107-1
expression is achieved both at the level of transcription and translation. By fluorescence in situ hybridisation the human
H-REV107-1
gene was localised to chromosome 11q11-12.
...
PMID:Transcriptional and translational downregulation of H-REV107, a class II tumour suppressor gene located on human chromosome 11q11-12. 977 74
H-rev107-1 is a growth inhibitory RAS target gene capable of suppressing anchorage independent growth in vitro and in vivo. Using a tumour tissue array with 241 matched tumour and normal tissue cDNA pools, we found down-regulation of
H-REV107-1
in 7 out of 14 ovary-derived cDNAs. RT-PCR analysis and immunohistochemical investigation confirmed expression of
H-REV107-1
in normal ovarian epithelial cells but down-regulation in high grade ovarian carcinomas.
H-REV107-1
is also strongly expressed in immortalized rat and human ovarian epithelial cells in vitro, but suppressed in transformed cells by two different mechanisms. KRAS-transformed rat ovarian cells and PA1 teratocarcinoma cells, reversibly repress
H-REV107-1
via MAP/ERK signaling. In contrast, treatment of A27/80 and OVCAR-3 epithelial ovarian cancer cells with IFNgamma stimulated
H-REV107-1
expression. In NIH3T3 cells harbouring an estrogen-inducible IRF-1, H-rev107-1 is directly induced after activation of IRF-1, indicating that H-rev107-1 is a target of IRF-1. Stimulation of
H-REV107-1
expression was also observed in ovarian epithelial cells suggesting that IRF-1 is involved in
H-REV107-1
regulation in human ovarian epithelium. In the IFNgamma-sensitive cell line A27/80,
H-REV107-1
suppresses colony formation. A27/80 and OVCAR-3 cells overexpressing
H-REV107-1
protein underwent apoptosis. These results demonstrate down-regulation of the class II
tumour suppressor
H-REV107-1
in human ovarian carcinomas and suggest an involvement of
H-REV107-1
in interferon-dependent cell death.
...
PMID:The class II tumour suppressor gene H-REV107-1 is a target of interferon-regulatory factor-1 and is involved in IFNgamma-induced cell death in human ovarian carcinoma cells. 1197 42
