Literature DB >> 18682896

Genomic and proteomic characterization of YDOV-157, a newly established human epithelial ovarian cancer cell line.

HanByoul Cho1, Eun Suk Kang, Soon Won Hong, Youn Jin Oh, Sun Mi Choi, Sang Wun Kim, Sung Hoon Kim, Young Tae Kim, Kyoung Sun Lee, Yang Kyu Choi, Jae-Hoon Kim.   

Abstract

The existence of several model systems with which to investigate a particular disease is advantageous for researchers. This is especially true for ovarian cancer, which, due to its complex and heterogeneous nature, inherently requires a large number of model systems. Here, we report a new ovarian serous adenocarcinoma cell line, designated YDOV-157, and characterized via post genomics and post proteomics. In this study, primary culture of tumor cells from ascites was performed and the cells were immortalized up to at least 60 passages in vitro. We studied the morphologies, cell proliferation, BRCA1/2 mutations, tumorigenesis capacity, and chemosensitivity of YDOV-157. Using a cDNA microarray, differentially expressed genes were identified and some of them were validated. Using proteomic analysis, we identified proteins that were differentially expressed in YDOV-157. The newly derived cell line, designated YDOV-157, grew as a monolayer and the doubling time was 102 h. When transplanted into nude mice, it initiated the formation of tumor masses with microscopic findings identical to those of the primary tumor. Chemosensitivity test showed that paclitaxel induced the highest chemosensitivity index. In microarray analysis, 2,520 probes were differently expressed, compared to human ovarian surface epithelial cells (HOSEs). In SYBR Green real-time PCR, the expression of E2F2 (P = 0.040) and CRABP2 genes (P = 0.030) was significantly higher in the ovarian cancer cell lines than in HOSEs. Furthermore, proteomic analysis showed that expression of 28 spots was significantly altered between YDOV-157 and HOSE. In conclusion, the newly derived YDOV-157 cell line may be an important research resource for studying cancer cell biology and should also be very useful for developing new strategies that inhibit cancer cell growth and progression.

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Year:  2008        PMID: 18682896     DOI: 10.1007/s11010-008-9892-4

Source DB:  PubMed          Journal:  Mol Cell Biochem        ISSN: 0300-8177            Impact factor:   3.396


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Journal:  Genes Chromosomes Cancer       Date:  2014-02-01       Impact factor: 5.006

2.  Lipocalin2 expressions correlate significantly with tumor differentiation in epithelial ovarian cancer.

Authors:  HanByoul Cho; Jae-Hoon Kim
Journal:  J Histochem Cytochem       Date:  2009-02-02       Impact factor: 2.479

3.  PLAG1 silencing promotes cell chemosensitivity in ovarian cancer via the IGF2 signaling pathway.

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Journal:  Int J Mol Med       Date:  2020-01-08       Impact factor: 4.101

4.  TOM40 Inhibits Ovarian Cancer Cell Growth by Modulating Mitochondrial Function Including Intracellular ATP and ROS Levels.

Authors:  Wookyeom Yang; Ha-Yeon Shin; Hanbyoul Cho; Joon-Yong Chung; Eun-Ju Lee; Jae-Hoon Kim; Eun-Suk Kang
Journal:  Cancers (Basel)       Date:  2020-05-22       Impact factor: 6.639

5.  The role of S100A14 in epithelial ovarian tumors.

Authors:  Hanbyoul Cho; Ha-Yeon Shin; Sunghoon Kim; Jane Seon-Young Kim; Joon-Yong Chung; Eun Joo Chung; Kyung-Hee Chun; Stephen M Hewitt; Jae-Hoon Kim
Journal:  Oncotarget       Date:  2014-06-15
  5 in total

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