Ovarian cancer cells regulate their mitochondrial content and high mitochondrial content is associated with a poor prognosis

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作者
Jil Weigelt
Mariam Petrosyan
Leticia Oliveira-Ferrer
Barbara Schmalfeldt
Catharina Bartmann
Johannes Dietl
Christine Stürken
Udo Schumacher
机构
[1] University Cancer Center Hamburg,Institute of Anatomy and Experimental Morphology
[2] University Medical Center Hamburg-Eppendorf,Department of Gynecology
[3] University Medical Center Hamburg-Eppendorf,Department of Obstetrics and Gynaecology
[4] University of Wuerzburg,Department of Medicine, Medical School Hamburg
[5] University of Applied Sciences and Medical University,Department of Medicine, Faculty of Science
[6] Medical School of Berlin,undefined
来源
BMC Cancer | / 24卷
关键词
Immunohistochemistry; Intraperitoneal metastases; Mitochondria; Ovarian cancer; Ovarian cancer prognosis; Ovarian cancer xenografts;
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摘要
Most cancer patients ultimately die from the consequences of distant metastases. As metastasis formation consumes energy mitochondria play an important role during this process as they are the most important cellular organelle to synthesise the energy rich substrate ATP, which provides the necessary energy to enable distant metastasis formation. However, mitochondria are also important for the execution of apoptosis, a process which limits metastasis formation. We therefore wanted to investigate the mitochondrial content in ovarian cancer cells and link its presence to the patient’s prognosis in order to analyse which of the two opposing functions of mitochondria dominates during the malignant progression of ovarian cancer. Monoclonal antibodies directed against different mitochondrial specific proteins, namely heat shock proteins 60 (HSP60), fumarase and succinic dehydrogenase, were used in immunohistochemistry in preliminary experiments to identify the antibody most suited to detect mitochondria in ovarian cancer cells in clinical tissue samples. The clearest staining pattern, which even delineated individual mitochondria, was seen with the anti-HSP60 antibody, which was used for the subsequent clinical study staining primary ovarian cancers (n = 155), borderline tumours (n = 24) and recurrent ovarian cancers (n = 26). The staining results were semi-quantitatively scored into three groups according to their mitochondrial content: low (n = 26), intermediate (n = 50) and high (n = 84). Survival analysis showed that high mitochondrial content correlated with a statistically significant overall reduced survival rate In addition to the clinical tissue samples, mitochondrial content was analysed in ovarian cancer cells grown in vitro (cell lines: OVCAR8, SKOV3, OVCAR3 and COV644) and in vivo in severe combined immunodeficiency (SCID) mice.
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