INSTITUTIONAL DIGITAL REPOSITORY

Epithelial to mesenchymal transition induces stem cell like phenotype in renal cell carcinoma cells

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dc.contributor.author Singla, M.
dc.contributor.author Kumar, A.
dc.contributor.author Bal, A.
dc.contributor.author Sarkar, S.
dc.contributor.author Bhattacharyya, S.
dc.date.accessioned 2019-05-16T16:02:03Z
dc.date.available 2019-05-16T16:02:03Z
dc.date.issued 2019-05-16
dc.identifier.uri http://localhost:8080/xmlui/handle/123456789/1252
dc.description.abstract Background: Metastatic dissemination of solid tumors is often initiated by reactivation of an embryonic development program, epithelial-to-mesenchymal-transition (EMT). EMT has been associated with acquiring invasiveness and resistance to conventional therapies. However, the precise role of EMT during renal cell carcinoma is still debatable and is under investigation. In this context, our study is designed to evaluate the role of cyclosporine (CsA) and transforming growth factor-β (TGFβ) administration in inducing EMT-like state in renal carcinoma cells. We also studied the associated phenotypic changes which may lead to tumor metastasis. Methods: The morphological changes in renal cell carcinoma cells (A498) treated with TGF-β/CsA were observed by microscopy. Atomic force microscope was used to evaluate the changes in elasticity of cells treated with TGF-β/CsA. The expression of mesenchymal and chemoresistance genes were checked by RT-PCR. Assays for migration, invasion, sphere formation ability and expression of cancer stem cell-like phenotypes were done to evaluate the metastatic potential of these cells. Lineage specific differentiations were also done to determine the acquisition of stem-cell like phenotype. Results: Our results showed that treatment with TGF-β/CsA led to loss of epithelial characteristics and gain of mesenchymal phenotype in vitro. Changes in shape and elastic properties of the cancer cells favoured metastatic progression, increased tumorisphere formation and invasiveness post treatment. We also observed higher expression of chemoresistance and stemness markers in EMT-induced cells. These cells also differentiated to various lineages like osteoblasts, adipocytes, neural and hepatic cells when induced with the respective differentiation media. Conclusion: We concluded that TGF-β/CsA treatment led to acquisition of EMT-like cancer stem cells phenotype that enhanced local invasion and dissemination of renal carcinoma cells. This subpopulation of cells with EMT-like phenotype a can provide a better perception of the metastatic process. This can provide an in vitro system for testing pharmaceuticals for modulating EMT as a viable strategy within the therapeutic armamentarium for RCC patients. The results of our findings also suggest that CsA directly induced EMT like changes in epithelial cell which may be responsible for the potential risk of malignancy in transplant patients. en_US
dc.language.iso en_US en_US
dc.subject Renal cell carcinoma en_US
dc.subject Cyclosporine A en_US
dc.subject Transforming growth factor-beta en_US
dc.subject Epithelial to mesenchymal transition en_US
dc.subject Chemoresistant gene en_US
dc.subject Cancer stem cells en_US
dc.title Epithelial to mesenchymal transition induces stem cell like phenotype in renal cell carcinoma cells en_US
dc.type Article en_US


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