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Hepatocyte growth factor/scatter factor and its receptor c-Met are overexpressed and associated with an increased microvessel density in malignant pleural mesothelioma
被引:0
|作者:
Edina Tolnay
Cornelius Kuhnen
Thorsten Wiethege
Jens-Eckehard König
Bruno Voss
Klaus-Michael Müller
机构:
[1] Department of Pulmonology,
[2] Semmelweis Medical School,undefined
[3] Budapest,undefined
[4] Hungary,undefined
[5] Institute of Pathology,undefined
[6] University Clinic Bergmannsheil,undefined
[7] Bürkle-de-la-Camp-Platz 1,undefined
[8] D-44789 Bochum,undefined
[9] Germany Tel.: +49 234 302 6600,undefined
[10] Fax: +49 234 302 6671,undefined
[11] e-mail: patho-bhl@ruhr-uni-bochum.de,undefined
[12] Professional Associations' Research Institute for Occupational Medicine,undefined
[13] Bochum,undefined
[14] Germany,undefined
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关键词:
Key words HGF/SF;
c-Met receptor;
Malignant mesothelioma;
autocrine loop;
angiogenesis;
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摘要:
Hepatocyte growth factor/scatter factor (HGF/SF) stimulates cell proliferation, motility and invasiveness via its receptor c-Met during embryogenesis and repair processes. It induces angiogenesis, promoting endothelial cell migration and capillary-tube formation in vivo. Co-expression of HGF/SF and c-Met receptor results in enhanced tumour growth, invasiveness and a mesenchymal-epithelial transition in some experimental tumours. Since mesothelioma cells have been reported to express c-Met receptor and to migrate in response to HGF/SF, we investigated human malignant pleural mesotheliomas for the demonstration of possible co-expression of the growth factor and its receptor. The microvessel density of the tumours was also analysed in order to assess the influence of HGF/SF expression on tumour angiogenesis. Thirty-nine paraffin-embedded specimens of malignant pleural mesotheliomas were immunostained by anti-HGF/SF and anti-c-Met antibodies and semiquantitatively evaluated. c-Met mRNA expression was visualised in ten tumour samples by a fluorescent in situ hybridisation method. Microvessel density was calculated by counting microvessels with a high-power field (200×) on von-Willebrand-factor-stained slides. We found an increased production of HGF/SF in 33/39 tumours and a corresponding overexpression of c-Met receptor in 29/39 specimens. The FISH method detected increased transcription of c-Met mRNA in malignant cells and in neighbouring vascular endothelial cells. HGF/SF-positive mesotheliomas had significantly higher microvessel densities compared to their HGF/SF-negative counterparts. The observed co-expression of HGF/SF and c-Met in malignant pleural mesotheliomas suggests a possible self-stimulation (autocrine loop) of tumour cells. On the basis of the significantly higher microvessel density values of malignant mesotheliomas overexpressing HGF/SF, we postulate, that HGF/SF may be an additional relevant factor in tumour angiogenesis in malignant pleural mesotheliomas.
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页码:291 / 296
页数:5
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