Masters Degrees (Basic Medical Sciences)

Permanent URI for this collection

http://hdl.handle.net/11660/228

Browse

Browsing Masters Degrees (Basic Medical Sciences) by Subject "breast cancer"

Now showing 1 - 1 of 1
  • Thumbnail Image
    ItemOpen Access
    Investigating the potential antiproliferative effect of ๐˜”๐˜ฐ๐˜ณ๐˜ช๐˜ฏ๐˜จ๐˜ข ๐˜ฐ๐˜ญ๐˜ฆ๐˜ช๐˜ง๐˜ฆ๐˜ณ๐˜ข aqueous leaf extract in MCF-7 breast cancer cells
    (University of the Free State, 2023) Moremane, Malebogo M.; Tiloke, Charlette; Abrahams, Beynon
    ๐—•๐—ฎ๐—ฐ๐—ธ๐—ด๐—ฟ๐—ผ๐˜‚๐—ป๐—ฑ: Breast cancer is associated with elevated mortality and morbidity rates in women across the world. Current chemotherapeutic drugs such as Doxorubicin (Dox) display contra-indications, thus expressing the need for alternative treatment methods. Therefore, to reduce the cancer burden, the studyโ€™s objective was to investigate whether an aqueous leaf extract of ๐˜”๐˜ฐ๐˜ณ๐˜ช๐˜ฏ๐˜จ๐˜ข ๐˜ฐ๐˜ญ๐˜ฆ๐˜ช๐˜ง๐˜ฆ๐˜ณ๐˜ข (MO), a medicinal tree native to India and indigenous to Africa, possesses antiproliferative potential against MCF-7 breast cancer cells. ๐— ๐—ฒ๐˜๐—ต๐—ผ๐—ฑ๐—ผ๐—น๐—ผ๐—ด๐˜†: In order to suppress cell growth, MCF-7 cells were treated with MO (2600 ฮผg/ml) for 72 hours. Cells were also co-exposed with Dox (0.978 ฮผM), modelled as a positive control. The unexposed cells served as the control. Biochemical analysis was conducted after 72 hours (MTT, GSH, DCFH-DA, ATP, Caspase 3/7, 8/9, qPCR and western blot assays) to assess the efficacy of MO and Dox. ๐—ฅ๐—ฒ๐˜€๐˜‚๐—น๐˜๐˜€: ๐˜”๐˜ฐ๐˜ณ๐˜ช๐˜ฏ๐˜จ๐˜ข ๐˜ฐ๐˜ญ๐˜ฆ๐˜ช๐˜ง๐˜ฆ๐˜ณ๐˜ข aqueous leaf extract significantly reduced the proliferation of breast cancer cells by inducing oxidative stress through increasing ROS whilst decreasing glutathione content and Nrf2 protein expression. Additionally, MO induced apoptosis by increasing caspases -3/7, -8, -9, metabolic activity and upregulating p53. Similar results were observed in Dox-exposed cells. Furthermore, cell death due to MO was activated with downregulation of Bcl-2, PARP-1 and Bax. Dox decreased the growth of breast cancer cells by increasing ROS. In contrast, Dox induced chemoresistance through increased GSH content and downregulated apoptotic protein Bax and p53 gene. However, the MO + Dox combination induced antiproliferative potential similarly to MO, suggesting a possible synergistic effect. ๐—–๐—ผ๐—ป๐—ฐ๐—น๐˜‚๐˜€๐—ถ๐—ผ๐—ป: MO aqueous leaf extract displayed antiproliferative potential by inducing apoptosis and oxidative damage to the MCF-7 breast cancer cells