Identification and validation of differentially expressed proteins in epithelial ovarian cancers using quantitative proteomics

Qu, Hong; Chen, Yuling; Cao, Guangming; Liu, Chongdong; Xu, Jianhong; Deng, Haiteng; Zhang, Zhenyu

doi:10.18632/oncotarget.13077

Cited by 28 publications

(24 citation statements)

References 46 publications

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“…As noted above, possible functional roles in tumor progression are incompletely understood and may differ depending upon the tumor type. In EOC, CLIC1 may be involved in cell cycle regulation and drug resistance 30 , while CLIC4 may have roles in fibroblast activation 29 . While CLIC1 has generally been associated with tumor progression in prior studies 32 , 34 , 38 , there are some contradictions regarding the role of CLIC4 in tumors.…”

Section: Discussionmentioning

confidence: 99%

“…Other studies have indicated that CLIC1 and CLIC4 may play roles in altering the EOC tumor microenvironment and affecting EOC tumor progression. CLIC4 regulated TGFβ-mediated activation of fibroblasts in EOC 29 and knocking down CLIC1 arrested EOC cell division at the G1 phase, inhibited xenograft growth in vivo , and increased susceptibility of the EOC cells to cisplatin and ROS exposure 30 .…”

Section: Introductionmentioning

confidence: 99%

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

Singha

Harper

Goldman

et al. 2018

Sci Rep

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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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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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

Singha

Harper

Goldman

et al. 2018

Sci Rep

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“…CLIC1 is overexpressed in several cancers including liver cancer, gall bladder cancer, pancreatic ductal adenocarcinoma, glioma, breast cancer, nasopharyngeal carcinoma, and gastric cancer to name a few (Wulfkuhle et al, 2002;Petrova et al, 2008;Chang et al, 2009;Wang et al, 2009Wang et al, , 2018Tang et al, 2012;Wei et al, 2015;Jia et al, 2016;Qu et al, 2016). It is known to play a role in cell viability, possibly by modulating mitochondrial function.…”

Section: Clic1mentioning

confidence: 99%

“…Along with CLIC4, CLIC1 is a promising biomarker for epithelial ovarian cancer where its expression predicts patient survival (Singha et al, 2018). CLIC1 is shown to regulate the redox-sensitivity of ovarian cancer cells and is predicted to be a potential marker for lymphoblastic leukemia (Qu et al, 2016;Dehghan-Nayeri et al, 2017;Singha et al, 2018). Modulation of CLIC1 expression by micro RNA, hsa-mir-372 predicts the poor prognosis of patients affected with gall bladder cancers (Zhou et al, 2017) and is important for the migration and invasion of gall bladder cancer cells (He et al, 2018).…”

Section: Clic1mentioning

confidence: 99%

Intracellular Chloride Channels: Novel Biomarkers in Diseases

2020

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“…Other CpG sites located in CPT1A (cg17058475), ABCG1 (cg27243685, cg01881899 and cg10192877) and LGALS3BP (cg25178683, cg11202345, cg14870271, cg17836612 and cg27470213) were also identified in some of the studies. In the literature, the expression of CPT1A, ABCG1, SREBF1 and LGALS3BP has been associated with obesity (50-54) and linked to various cancers (55)(56)(57)(58)(59)(60)(61)(62), including breast cancer (63-69) adding plausibility to the findings. Indeed, CPT1A was recently found to be up-regulated in co-cultured adipocytes isolated from human breast adipose tissue with hormone receptor-positive or -negative breast cancer cells (70).…”

Section: Discussionmentioning

confidence: 97%

Association Between BMI and DNA Methylation in Blood or Normal Adult Breast Tissue: A Systematic Review

et al. 2020

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Background/Aim: Several studies have investigated the influence of obesity on DNA methylation (DNAm) to find biomarkers associated with the detection of chronic diseases, including breast cancer. The aim of the study was to systematically review studies examining the association of body mass index (BMI) and DNAm in blood or normal breast tissue. Materials and Methods: Three scientific literature databases (PubMed, Embase and Web of Science) were screened until May 2018. Results: Twenty-four studies were included along with ours in which we investigated this relation in the normal breast tissue of 40 breast cancer patients. Conclusion: BMIassociated CpG sites were highly variable with few identified in less than half of the studies. Nevertheless, a few genes potentially associated with BMI were highlighted in blood (CPT1A, ABCG1, SREBF1 and LGALS3BP) and in normal breast tissue (PTPRN2 and ABLIM2). The variability of the results could be explained by the tissue and cell-specificity of methylation and differences in methodology.

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Identification and validation of differentially expressed proteins in epithelial ovarian cancers using quantitative proteomics

Cited by 28 publications

References 46 publications

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

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

Intracellular Chloride Channels: Novel Biomarkers in Diseases

Association Between BMI and DNA Methylation in Blood or Normal Adult Breast Tissue: A Systematic Review

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