FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2895099230> ?p ?o ?g. }

• W2895099230 abstract "Licorice is an herb extensively used for both culinary and medicinal purposes. Various constituents of licorice have been shown to exhibit anti-tumorigenic effect in diverse cancer types. However, majority of these studies focus on the aspect of their growth-suppressive role. In this study, we systematically analyzed known licorice's constituents on the goal of identifying component(s) that can effectively suppress both cell migration and growth.Effect of licorice's constituents on cell growth was evaluated by MTT assay while cell migration was assessed by both wound-healing and Transwell assays. Cytoskeleton reorganization and focal adhesion assembly were visualized by immunofluorescence staining with labeled phalloidin and anti-paxillin antibody. Activity of Src in cells was judged by western blot using phosphor-Src416 antibody while Src kinase activity was measured using Promega Src kinase assay system. Anti-tumorigenic capabilities of isoliquiritigenin (ISL) and 2, 4, 2', 4'-Tetrahydroxychalcone (THC) were investigated using lung cancer xenograft model.Using a panel of lung cancer cell lines, ISL was identified as the only licorice's constituent capable of inhibiting both cell migration and growth. ISL-led inhibition in cell migration resulted from impaired cytoskeleton reorganization and focal adhesion assembly. Assessing the phosphorylation of 141 cytoskeleton dynamics-associated proteins revealed that ISL reduced the abundance of Tyr421-phosphorylation of cortactin, Tyr925- and Tyr861-phosphorylation of FAK, indicating the involvement of Src because these sites are known to be phosphorylated by Src. Enigmatically, ISL inhibited Src in cells while displayed no effect on Src activity in cell-free system. The discrepancy was explained by the observation that THC, one of the major ISL metabolite identified in lung cancer cells abrogated Src activity both in cells and cell-free system. Similar to ISL, THC deterred cell migration and abolished cytoskeleton reorganization/focal adhesion assembly. Furthermore, we showed both ISL and THC suppressed in vitro lung cancer cell invasion and in vivo tumor progression.Our study suggests that ISL inhibits lung cancer cell migration and tumorigenesis by interfering with Src through its metabolite THC. As licorice is safely used for culinary purposes, our study suggests that ISL or THC may be safely used as a Src inhibitor." @default.
• W2895099230 created "2018-10-12" @default.
• W2895099230 creator A5000095785 @default.
• W2895099230 creator A5010489527 @default.
• W2895099230 creator A5039904642 @default.
• W2895099230 creator A5040136142 @default.
• W2895099230 creator A5041247351 @default.
• W2895099230 creator A5052414538 @default.
• W2895099230 creator A5081288331 @default.
• W2895099230 creator A5089593108 @default.
• W2895099230 date "2018-10-03" @default.
• W2895099230 modified "2023-10-15" @default.
• W2895099230 title "Suppression of lung cancer progression by isoliquiritigenin through its metabolite 2, 4, 2’, 4’-Tetrahydroxychalcone" @default.
• W2895099230 cites W1532635242 @default.
• W2895099230 cites W1912019187 @default.
• W2895099230 cites W1964583793 @default.
• W2895099230 cites W1967394241 @default.
• W2895099230 cites W1971447191 @default.
• W2895099230 cites W1972383046 @default.
• W2895099230 cites W1978265206 @default.
• W2895099230 cites W1982088633 @default.
• W2895099230 cites W1989901669 @default.
• W2895099230 cites W1990915902 @default.
• W2895099230 cites W1992831404 @default.
• W2895099230 cites W1996552917 @default.
• W2895099230 cites W1999816397 @default.
• W2895099230 cites W1999996757 @default.
• W2895099230 cites W2006729275 @default.
• W2895099230 cites W2007349364 @default.
• W2895099230 cites W2007845148 @default.
• W2895099230 cites W2014559586 @default.
• W2895099230 cites W2015098698 @default.
• W2895099230 cites W2020472510 @default.
• W2895099230 cites W2023356119 @default.
• W2895099230 cites W2036988959 @default.
• W2895099230 cites W2041996156 @default.
• W2895099230 cites W2045492296 @default.
• W2895099230 cites W2054429361 @default.
• W2895099230 cites W2058408301 @default.
• W2895099230 cites W2064086605 @default.
• W2895099230 cites W2075758366 @default.
• W2895099230 cites W2077218183 @default.
• W2895099230 cites W2084910248 @default.
• W2895099230 cites W2088388171 @default.
• W2895099230 cites W2101118037 @default.
• W2895099230 cites W2105512558 @default.
• W2895099230 cites W2111378817 @default.
• W2895099230 cites W2114245253 @default.
• W2895099230 cites W2116383371 @default.
• W2895099230 cites W2117692326 @default.
• W2895099230 cites W2131077069 @default.
• W2895099230 cites W2133260711 @default.
• W2895099230 cites W2142351770 @default.
• W2895099230 cites W2145072524 @default.
• W2895099230 cites W2148601288 @default.
• W2895099230 cites W2152261156 @default.
• W2895099230 cites W2158933105 @default.
• W2895099230 cites W2167525778 @default.
• W2895099230 cites W2213854534 @default.
• W2895099230 cites W2282661938 @default.
• W2895099230 cites W2309249759 @default.
• W2895099230 cites W2321550732 @default.
• W2895099230 cites W2519895466 @default.
• W2895099230 cites W2527467615 @default.
• W2895099230 cites W2605132700 @default.
• W2895099230 cites W2758899780 @default.
• W2895099230 cites W2766316939 @default.
• W2895099230 doi "https://doi.org/10.1186/s13046-018-0902-4" @default.
• W2895099230 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6171243" @default.
• W2895099230 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30285892" @default.
• W2895099230 hasPublicationYear "2018" @default.
• W2895099230 type Work @default.
• W2895099230 sameAs 2895099230 @default.
• W2895099230 citedByCount "25" @default.
• W2895099230 countsByYear W28950992302019 @default.
• W2895099230 countsByYear W28950992302020 @default.
• W2895099230 countsByYear W28950992302021 @default.
• W2895099230 countsByYear W28950992302022 @default.
• W2895099230 countsByYear W28950992302023 @default.
• W2895099230 crossrefType "journal-article" @default.
• W2895099230 hasAuthorship W2895099230A5000095785 @default.
• W2895099230 hasAuthorship W2895099230A5010489527 @default.
• W2895099230 hasAuthorship W2895099230A5039904642 @default.
• W2895099230 hasAuthorship W2895099230A5040136142 @default.
• W2895099230 hasAuthorship W2895099230A5041247351 @default.
• W2895099230 hasAuthorship W2895099230A5052414538 @default.
• W2895099230 hasAuthorship W2895099230A5081288331 @default.
• W2895099230 hasAuthorship W2895099230A5089593108 @default.
• W2895099230 hasBestOaLocation W28950992301 @default.
• W2895099230 hasConcept C108636557 @default.
• W2895099230 hasConcept C11960822 @default.
• W2895099230 hasConcept C121608353 @default.
• W2895099230 hasConcept C137738243 @default.
• W2895099230 hasConcept C142669718 @default.
• W2895099230 hasConcept C1491633281 @default.
• W2895099230 hasConcept C151166631 @default.
• W2895099230 hasConcept C185592680 @default.
• W2895099230 hasConcept C2776000893 @default.
• W2895099230 hasConcept C2776974645 @default.
• W2895099230 hasConcept C502942594 @default.

• next