SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W3206069802> ?p ?o ?g. }

Showing items 1 to 100 of ±177 with 100 items per page.

W3206069802 endingPage "2735" @default.
W3206069802 startingPage "2719" @default.
W3206069802 abstract "Background: The major hurdles for successful cancer treatment are drug resistance and invasiveness developed by breast cancer stem cells (BCSC). Objective: As these two processes are highly energy-dependent, the identification of the main ATP supplier required for stem cell viability may result advantageous in the design of new therapeutic strategies to deter malignant carcinomas. Methods: The energy metabolism (glycolysis and oxidative phosphorylation, OxPhos) was systematically analyzed by assessing relevant protein contents, enzyme activities, and pathway fluxes in BCSC. Once identified as the main ATP supplier, selective energy inhibitors and canonical breast cancer drugs were used to block stem cell viability and metastatic properties. Results: OxPhos and glycolytic protein contents, as well as HK and LDH activities were several times higher in BCSC than in their parental line, MCF-7 cells. However, CS, GDH, COX activities, and both energy metabolism pathway fluxes were significantly lower (38-86%) in BCSC than in MCF-7 cells. OxPhos was the main ATP provider (>85%) in BCSC. Accordingly, oligomycin (a specific and potent canonical OxPhos inhibitor) and other non-canonical drugs with inhibitory effect on OxPhos (celecoxib, dimethylcelecoxib) significantly decreased BCSC viability, levels of epithelial-mesenchymal transition proteins, invasiveness, and induced ROS over-production, with IC50 values ranging from 1 to 20 μM in 24 h treatment. In contrast, glycolytic inhibitors (gossypol, iodoacetic acid, 3-bromopyruvate, 2-deoxyglucose) and canonical chemotherapeutic drugs (paclitaxel, doxorubicin, cisplatin) were much less effective against BCSC viability (IC50> 100 μM). Conclusion: These results indicated that the use of some NSAIDs may be a promising alternative therapeutic strategy to target BCSC." @default.
W3206069802 created "2021-10-25" @default.
W3206069802 creator A5013209374 @default.
W3206069802 creator A5021751498 @default.
W3206069802 creator A5022974085 @default.
W3206069802 creator A5036114433 @default.
W3206069802 creator A5039197501 @default.
W3206069802 creator A5077780793 @default.
W3206069802 creator A5079887676 @default.
W3206069802 creator A5082077975 @default.
W3206069802 creator A5084670840 @default.
W3206069802 date "2022-05-01" @default.
W3206069802 modified "2023-10-18" @default.
W3206069802 title "Celecoxib and Dimethylcelecoxib Block Oxidative Phosphorylation, Epithelial-Mesenchymal Transition and Invasiveness in Breast Cancer Stem Cells" @default.
W3206069802 cites W1527357181 @default.
W3206069802 cites W1543746024 @default.
W3206069802 cites W1556836946 @default.
W3206069802 cites W1573780709 @default.
W3206069802 cites W1590478199 @default.
W3206069802 cites W1868764935 @default.
W3206069802 cites W1897724420 @default.
W3206069802 cites W1965810575 @default.
W3206069802 cites W1969876120 @default.
W3206069802 cites W1971063609 @default.
W3206069802 cites W1973671455 @default.
W3206069802 cites W1974182237 @default.
W3206069802 cites W1974525908 @default.
W3206069802 cites W1975419073 @default.
W3206069802 cites W1975601342 @default.
W3206069802 cites W1976609865 @default.
W3206069802 cites W1990536342 @default.
W3206069802 cites W1993421498 @default.
W3206069802 cites W1996027069 @default.
W3206069802 cites W2000479440 @default.
W3206069802 cites W2022665276 @default.
W3206069802 cites W2023529679 @default.
W3206069802 cites W2026111411 @default.
W3206069802 cites W2028303721 @default.
W3206069802 cites W2029038426 @default.
W3206069802 cites W2045477445 @default.
W3206069802 cites W2050257939 @default.
W3206069802 cites W2050300062 @default.
W3206069802 cites W2055579579 @default.
W3206069802 cites W2056878267 @default.
W3206069802 cites W2060051234 @default.
W3206069802 cites W2065196942 @default.
W3206069802 cites W2066346185 @default.
W3206069802 cites W2074847845 @default.
W3206069802 cites W2078811557 @default.
W3206069802 cites W2081538536 @default.
W3206069802 cites W2083274861 @default.
W3206069802 cites W2085134335 @default.
W3206069802 cites W2086079357 @default.
W3206069802 cites W2086828029 @default.
W3206069802 cites W2087241953 @default.
W3206069802 cites W2089583460 @default.
W3206069802 cites W2094156327 @default.
W3206069802 cites W2100941957 @default.
W3206069802 cites W2105267564 @default.
W3206069802 cites W2107823533 @default.
W3206069802 cites W2110361622 @default.
W3206069802 cites W2110467543 @default.
W3206069802 cites W2116319147 @default.
W3206069802 cites W2116611292 @default.
W3206069802 cites W2119239003 @default.
W3206069802 cites W2126193786 @default.
W3206069802 cites W2130840692 @default.
W3206069802 cites W2133851884 @default.
W3206069802 cites W2136679918 @default.
W3206069802 cites W2137049140 @default.
W3206069802 cites W2139100782 @default.
W3206069802 cites W2151151320 @default.
W3206069802 cites W2154545410 @default.
W3206069802 cites W2155598285 @default.
W3206069802 cites W2159516503 @default.
W3206069802 cites W2168556155 @default.
W3206069802 cites W2174823906 @default.
W3206069802 cites W2279453021 @default.
W3206069802 cites W2414844657 @default.
W3206069802 cites W2530830796 @default.
W3206069802 cites W2577934600 @default.
W3206069802 cites W2637414492 @default.
W3206069802 cites W2766600652 @default.
W3206069802 cites W2772873089 @default.
W3206069802 cites W2782381615 @default.
W3206069802 cites W2791235391 @default.
W3206069802 cites W2791903162 @default.
W3206069802 cites W2793000301 @default.
W3206069802 cites W2799425529 @default.
W3206069802 cites W2801615706 @default.
W3206069802 cites W2803724578 @default.
W3206069802 cites W2892318358 @default.
W3206069802 cites W2898698347 @default.
W3206069802 cites W2912993657 @default.
W3206069802 cites W2913601537 @default.
W3206069802 cites W2922145505 @default.
W3206069802 cites W2945339304 @default.
W3206069802 cites W2951265455 @default.