FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2890132114> ?p ?o ?g. }

• W2890132114 endingPage "2531" @default.
• W2890132114 startingPage "2515" @default.
• W2890132114 abstract "Resistance to therapies, recurrence, and metastasis remain challenging issues for breast cancer patients, particularly for triple-negative and breast cancer stem cells. The activation of the epithelial-to-mesenchymal transition (EMT) plays an indispensable role in the poor prognosis of those types. The accumulating proofs indicated that the mevalonate pathway crucially mediates a poor prognosis. Here, the effects of lipophilic 3-hydroxy-3-methyl-glutaryl-coenzyme A inhibitors, atorvastatin, lovastatin, and simvastatin, were investigated on expression and function of a selected profile of EMT-related genes in breast cancer stem-like cells. A nontoxic dose of statins (5 μM for 4 days) significantly (P < 0.05 and >2-fold change) altered expression of 50 of 71 studied genes with a shared cluster of 37 genes that are coding chief operator of signaling pathways in Hippo, Notch, Wnt, proliferation, invasion, angiogenesis, and cell death. They also significantly decreased the levels of Yap/Taz proteins and shifted the expression of vimentin/E-cadherin in favor of induction of differentiation. Statins significantly chemosensitized the treated cells to doxorubicin and also reduced in vitro migration of the cells. Whereas lovastatin and simvastatin significantly decreased the expression of CD44, atorvastatin drastically increased CD24 and caused more wide-ranging impacts. In summary, the statins hold back the process of EMT by the antagonizing of EMT-promoting pathways. High degree of overlapping findings is supportive of the central role of the mevalonate pathway in cancer stem-like cells, but further studies are required to find the optimized chemical structure for the maximum abrogation of orchestrated EMT pathways." @default.
• W2890132114 created "2018-09-27" @default.
• W2890132114 creator A5000734558 @default.
• W2890132114 creator A5005958838 @default.
• W2890132114 creator A5046079710 @default.
• W2890132114 creator A5087494128 @default.
• W2890132114 creator A5032752193 @default.
• W2890132114 date "2018-09-06" @default.
• W2890132114 modified "2023-10-18" @default.
• W2890132114 title "Lipophilic statins antagonistically alter the major epithelial‐to‐mesenchymal transition signaling pathways in breast cancer stem–like cells via inhibition of the mevalonate pathway" @default.
• W2890132114 cites W1933244249 @default.
• W2890132114 cites W1972694890 @default.
• W2890132114 cites W1977291335 @default.
• W2890132114 cites W1987007903 @default.
• W2890132114 cites W1991082385 @default.
• W2890132114 cites W1992367938 @default.
• W2890132114 cites W1996053472 @default.
• W2890132114 cites W1998164580 @default.
• W2890132114 cites W2002427864 @default.
• W2890132114 cites W2005294714 @default.
• W2890132114 cites W2007859564 @default.
• W2890132114 cites W2012306194 @default.
• W2890132114 cites W2021700152 @default.
• W2890132114 cites W2032019813 @default.
• W2890132114 cites W2033360354 @default.
• W2890132114 cites W2035059839 @default.
• W2890132114 cites W2035396934 @default.
• W2890132114 cites W2040430549 @default.
• W2890132114 cites W2046196246 @default.
• W2890132114 cites W2088011239 @default.
• W2890132114 cites W2092533035 @default.
• W2890132114 cites W2094400680 @default.
• W2890132114 cites W2095904711 @default.
• W2890132114 cites W2097466570 @default.
• W2890132114 cites W2097689792 @default.
• W2890132114 cites W2100592123 @default.
• W2890132114 cites W2105150792 @default.
• W2890132114 cites W2107277218 @default.
• W2890132114 cites W2111984765 @default.
• W2890132114 cites W2134130337 @default.
• W2890132114 cites W2136309995 @default.
• W2890132114 cites W2141347342 @default.
• W2890132114 cites W2141570734 @default.
• W2890132114 cites W2149914697 @default.
• W2890132114 cites W2151950281 @default.
• W2890132114 cites W2159038842 @default.
• W2890132114 cites W2164171082 @default.
• W2890132114 cites W2325309162 @default.
• W2890132114 cites W2416868628 @default.
• W2890132114 cites W2556760701 @default.
• W2890132114 cites W2606469175 @default.
• W2890132114 cites W4297821733 @default.
• W2890132114 doi "https://doi.org/10.1002/jcb.27544" @default.
• W2890132114 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30191610" @default.
• W2890132114 hasPublicationYear "2018" @default.
• W2890132114 type Work @default.
• W2890132114 sameAs 2890132114 @default.
• W2890132114 citedByCount "26" @default.
• W2890132114 countsByYear W28901321142019 @default.
• W2890132114 countsByYear W28901321142020 @default.
• W2890132114 countsByYear W28901321142021 @default.
• W2890132114 countsByYear W28901321142022 @default.
• W2890132114 countsByYear W28901321142023 @default.
• W2890132114 crossrefType "journal-article" @default.
• W2890132114 hasAuthorship W2890132114A5000734558 @default.
• W2890132114 hasAuthorship W2890132114A5005958838 @default.
• W2890132114 hasAuthorship W2890132114A5032752193 @default.
• W2890132114 hasAuthorship W2890132114A5046079710 @default.
• W2890132114 hasAuthorship W2890132114A5087494128 @default.
• W2890132114 hasConcept C121608353 @default.
• W2890132114 hasConcept C134018914 @default.
• W2890132114 hasConcept C134651460 @default.
• W2890132114 hasConcept C137620995 @default.
• W2890132114 hasConcept C1491633281 @default.
• W2890132114 hasConcept C181199279 @default.
• W2890132114 hasConcept C185592680 @default.
• W2890132114 hasConcept C2778163477 @default.
• W2890132114 hasConcept C2779013556 @default.
• W2890132114 hasConcept C2779982574 @default.
• W2890132114 hasConcept C2780932548 @default.
• W2890132114 hasConcept C2780940807 @default.
• W2890132114 hasConcept C28328180 @default.
• W2890132114 hasConcept C502942594 @default.
• W2890132114 hasConcept C530470458 @default.
• W2890132114 hasConcept C54355233 @default.
• W2890132114 hasConcept C55427017 @default.
• W2890132114 hasConcept C55493867 @default.
• W2890132114 hasConcept C62478195 @default.
• W2890132114 hasConcept C76419328 @default.
• W2890132114 hasConcept C86803240 @default.
• W2890132114 hasConcept C95444343 @default.
• W2890132114 hasConceptScore W2890132114C121608353 @default.
• W2890132114 hasConceptScore W2890132114C134018914 @default.
• W2890132114 hasConceptScore W2890132114C134651460 @default.
• W2890132114 hasConceptScore W2890132114C137620995 @default.
• W2890132114 hasConceptScore W2890132114C1491633281 @default.
• W2890132114 hasConceptScore W2890132114C181199279 @default.
• W2890132114 hasConceptScore W2890132114C185592680 @default.

• next