Programs
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- Clinical Fellowship in Laboratory Genetics & Genomics - Fellowship
Publication Type : Journal Article
Thematic Areas : Biotech
Publisher : BMC cancer
Source : BMC cancer, vol. 15, no. 1, p. 843, 2015
Keywords : Gastrointestinal cancer RNA interference Functional inhibition Suicide substrate MIF
Campus : Amritapuri
School : School of Biotechnology
Center : Cell Biology
Department : biotechnology
Year : 2015
Abstract : BackgroundPoor prognosis in gallbladder cancer is due to late presentation of the disease, lack of reliable biomarkers for early diagnosis and limited targeted therapies. Early diagnostic markers and novel therapeutic targets can significantly improve clinical management of gallbladder cancer.MethodsProteomic analysis of four gallbladder cancer cell lines based on the invasive property (non-invasive to highly invasive) was carried out using the isobaric tags for relative and absolute quantitation labeling-based quantitative proteomic approach. The expression of macrophage migration inhibitory factor was analysed in gallbladder adenocarcinoma tissues using immunohistochemistry.nbsp;In vitronbsp;cellular assays were carried out in a panel of gallbladder cancer cell lines using MIF inhibitors, ISO-1 and 4-IPP or its specific siRNA.ResultsThe quantitative proteomic experiment led to the identification of 3,653 proteins, among which 654 were found to be overexpressed and 387 were downregulated in the invasive cell lines (OCUG-1, NOZ and GB-d1) compared to the non-invasive cell line, TGBC24TKB. Among these, macrophage migration inhibitory factor (MIF) was observed to be highly overexpressed in two of the invasive cell lines. MIF is a pleiotropic proinflammatory cytokine that plays a causative role in multiple diseases, including cancer. MIF has been reported to play a central role in tumor cell proliferation and invasion in several cancers. Immunohistochemical labeling of tumor tissue microarrays for MIF expression revealed that it was overexpressed in 21 of 29 gallbladder adenocarcinoma cases. Silencing/inhibition of MIF using siRNA and/or MIF antagonists resulted in a significant decrease in cell viability, colony forming ability and invasive property of the gallbladder cancer cells.ConclusionsOur findings support the role of MIF in tumor aggressiveness and suggest its potential application as a therapeutic target for gallbladder cancer.
Cite this Research Publication : Tejaswini Subbannayya, Pamela Leal-Rojas, Mustafa A Barbhuiya, Remya Raja, Santosh Renuse, Gajanan Sathe, Sneha M Pinto, Nazia Syed, Vishalakshi Nanjappa, Arun H. Patil, and Dr. Bipin G. Nair, “Macrophage Migration Inhibitory Factor-a Therapeutic Target in Gallbladder Cancer”, BMC cancer, vol. 15, no. 1, p. 843, 2015