CLIC1 and CLIC4 complement CA125 as a diagnostic biomarker panel for all subtypes of epithelial ovarian cancer

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作者
Bipradeb Singha
Sandra L. Harper
Aaron R. Goldman
Benjamin G. Bitler
Katherine M. Aird
Mark E. Borowsky
Mark G. Cadungog
Qin Liu
Rugang Zhang
Stephanie Jean
Ronny Drapkin
David W. Speicher
机构
[1] The Wistar Institute,Molecular and Cellular Oncogenesis Program
[2] University of Colorado,Department of Obstetrics and Gynecology
[3] Penn State College of Medicine,Department of Cellular and Molecular Physiology
[4] Helen F. Graham Cancer Center & Research Institute,Gene Expression and Regulation Program
[5] The Wistar Institute,Department of Obstetrics and Gynecology, Ovarian Cancer Research Center
[6] University of Pennsylvania Perelman School of Medicine,undefined
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关键词
Cancer Antigen 125 (CA125); Epithelial Ovarian Cancer; Short-term Organ Culture; Chloride Intracellular Channel (CLICs); Normal Ovarian Surface Epithelium;
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摘要
New plasma and tissue biomarkers of epithelial ovarian cancer (EOC) could improve early diagnosis and post-diagnosis clinical management. Here we investigated tissue staining and tissue secretion of CLIC1 and CLIC4 across EOC subtypes. CLIC1 and CLIC4 are two promising biomarkers we previously showed were elevated in EOC patient sera. Individually, CLIC1 or CLIC4 stained larger percentages of malignant tumors across all EOC subtypes compared with CA125, particularly early stage and mucinous tumors. CLIC4 also stained benign tumors but staining was limited to nuclei; whereas malignant tumors showed diffuse cellular staining of stromal and tumor cells. Both proteins were shed by all EOC subtypes tumors in short term organ culture at more consistent levels than CA125, supporting their potential as pan-subtype serum and tissue biomarkers. Elevated CLIC4 expression, but not CLIC1 expression, was a negative indicator of patient survival, and CLIC4 knockdown in cultured cells decreased cell proliferation and migration indicating a potential role in tumor progression. These results suggest CLIC1 and CLIC4 are promising serum and tissue biomarkers as well as potential therapeutic targets for all EOC subtypes. This justifies development of high throughput serum/plasma biomarker assays to evaluate utility of a biomarker panel consisting of CLIC1, CLIC4 and CA125.
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