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Please use this identifier to cite or link to this item: http://10.9.150.37:8080/dspace//handle/atmiyauni/2025
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dc.contributor.authorWaghela, Bhargav N-
dc.contributor.authorVaidya, Foram U-
dc.contributor.authorPathak, Chandramani-
dc.date.accessioned2024-11-25T09:38:23Z-
dc.date.available2024-11-25T09:38:23Z-
dc.date.issued2020-09-21-
dc.identifier.urihttp://10.9.150.37:8080/dspace//handle/atmiyauni/2025-
dc.description.abstractAltered expression of cellular redox genes and proteins contributes to invasion, metastasis, and drug resistance in cancer. NADPH oxidase (NOX) isoforms are the pro_oxidant enzymes that generate ROS as a primary product. Dysregulation of NOX activity and expression alters ROS generation, which either directly or indirectly modulates cell death and survival signaling during the progression of cancer. Nuclear factor erythroid 2_related factor 2 (Nrf_2) is an inducible transcription factor, which transcribes an array of antioxidant genes and protects cancer cells from the oxidative stress. Both NOXs and Nrf_2 participate in the regulation of cellular redox homeostasis; but their dysregulation promotes oxidative stress, which contributes to the progression of different types of cancer. Indeed, the role of NOX isoforms and Nrf_ 2 in developing the drug resistance in cancer is largely unknown. In the present study, we have explored the association of NOX isoforms and Nrf_2 signaling with the MDR1 gene expression in colon carcinoma cells (HCT_116/R). The MDR1 gene was overexpressed to develop resistant HCT_116/R cells and the NOX activation and ROS generation were monitored. We also assessed the role of NOX isoforms and Nrf_2 in the 5_fluorouracil (5_FU) mediated apoptotic cell death of HCT_116/R cells. The HCT_116/R cells demonstrated higher expression of HIF_1α, Nrf_2, and HO_1 and were highly resistant to 5_ FU; they also displayed upregulated expression and activity of NOX_2, as well as elevated ROS levels. Interestingly, the treatment with HDC, a specific NOX_2 inhibitor, reduced the ROS levels in HCT_116/R cells. The treatment with HDC and ML_385 (specific inhibitor of Nrf_2) augmented the 5_FU_mediated apoptotic cell death of HCT_116/R cells, which suggests that NOX_2 and Nrf_2 are involved in the development of the chemoresistant phenotype of these cells. Taken together, NOX_2 and Nrf_2 are associated with developing drug resistance of colorectal cancer cells and might be potential targets to overcome drug resistance during cancer therapyen_US
dc.language.isoenen_US
dc.subject5 fluorouracilen_US
dc.subjectdrug resistanceen_US
dc.subjectHO 1en_US
dc.subject, MDR1en_US
dc.subjectNOX 2en_US
dc.subjectNrf 2en_US
dc.subjectROSen_US
dc.titleUpregulation of NOX 2 and Nrf 2 Promotes 5 Fluorouracil Resistance of Human Colon Carcinoma (HCT 116) Cellsen_US
dc.typeArticleen_US
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