The class II tumour suppressor gene H-REV107-1 is a target of interferon-regulatory factor-1 and is involved in IFNγ-induced cell death in human ovarian carcinoma cells

被引:0
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作者
Christine Sers
Knut Husmann
Irina Nazarenko
Steffen Reich
Kai Wiechen
Bakhyt Zhumabayeva
Punam Adhikari
Katharina Schröder
Artur Gontarewicz
Reinhold Schäfer
机构
[1] Institute of Pathology,Departments of Orthopaedic Surgery and Medicine
[2] University Hospital Charité,undefined
[3] Clontech Laboratories,undefined
[4] 1020 East Meadow Circle,undefined
[5] National Research Center for Biotechnology,undefined
[6] Research Laboratory for Calcium Metabolism,undefined
[7] Klinik Balgrist,undefined
[8] Zürich,undefined
来源
Oncogene | 2002年 / 21卷
关键词
tumour suppressor; H-REV107-1; IRF-1; target gene; IRFγ; apoptosis;
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摘要
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 IFNγ 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 IFNγ-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.
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页码:2829 / 2839
页数:10
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