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dc.contributor.advisorHendry, William J. III
dc.contributor.authorMukherjee, Lipilekha
dc.contributor.authorHendry, I.R.
dc.date.accessioned2017-06-01T20:00:17Z
dc.date.available2017-06-01T20:00:17Z
dc.date.issued2017-04-28
dc.identifier.citationMukherjee, Lipilekha and Hendry, I.R. 2017. Differential regulatory gene expression at the proteomic level in subtypes of human ovarian cancer cell-lines--In Proceedings: 13th Annual Symposium on Graduate Research and Scholarly Projects. Wichita, KS: Wichita State University, p.60
dc.identifier.urihttp://hdl.handle.net/10057/13306
dc.descriptionPresented to the 13th Annual Symposium on Graduate Research and Scholarly Projects (GRASP) held at the Rhatigan Student Center, Wichita State University, April 28, 2017.
dc.descriptionResearch completed in the Department of Biological Sciences
dc.description.abstractOvarian carcinoma is the most lethal neoplasm and the fifth leading cause of mortality in women. Among the different subtypes, widely heterogeneous high-grade serous ovarian cancer (HGSOC) poses a great challenge to modern chemotherapy due to its high recurrence rate and resistance to standard treatments. Recent studies suggest that survival time-line and disease recurrence are linked to the variable expression of biomarkers in cancer cells. Therefore, using Western blot analyses, we assessed the expression of a host of regulatory gene protein products at the wholecell level in extracts from both three HGSOC and five non-HGSOC cell lines. Some of our most distinctive findings from those analyses were that: 1) Nrf2, a key factor in the anti-oxidant response element system, is expressed as a series of protein bands of variable molecular weight in all but the Kuramochi (HGSOC) cell line; 2) Estrogen receptor alpha is expressed in all but the OVSAHO (HGSOC) cell line; and 3) the AUF-1, p120-catenin, and NFKB-p50 proteins are expressed in both HGSOC and non-HGSOC cell types. We will next follow up those findings conducted at the whole-cell level with assessments at the individual cell and subcellular level using immunohistochemical analyses.
dc.description.sponsorshipGraduate School, Academic Affairs, University Libraries, Regional Institute on Aging
dc.language.isoen_US
dc.publisherWichita State University
dc.relation.ispartofseriesGRASP
dc.relation.ispartofseriesv. 13
dc.titleDifferential regulatory gene expression at the proteomic level in subtypes of human ovarian cancer cell-lines
dc.typeAbstract
dc.rights.holderWichita State University


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