FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2170846620> ?p ?o ?g. }

• W2170846620 endingPage "1383" @default.
• W2170846620 startingPage "1377" @default.
• W2170846620 abstract "We have compared the properties of the novel multidrug resistance modulator, S9788, to a panel of 11 well-known modulators in a model of rat glioblastoma cells resistant to doxorubicin and displaying a P-glycoprotein-mediated multidrug-resistance phenotype complemented by a mechanism of intracellular drug tolerance not yet identified (Br J Cancer 1992, 65, 538-544). S9788, like most modulators, was able to completely restore drug accumulation in the resistant line to the level obtained in the sensitive cells. This was obtained with 10 mumol/l of modulator, which is slightly higher than required for cyclosporine A (3 mumol/l) verapamil and nicardipine (6 mumol/l), but lower than for amiodarone, trifluoperazine and dipyridamole (20 mumol/l), tamoxifen and diltiazem (40 mumol/l), quinine, quinidine and nifedipine (> 100 mumol/l). Complete restoration of drug cytotoxicity was, however, obtained only with amiodarone, and a residual resistance factor of 4 could not be overcome by cyclosporine A or S9788, while other modulators gave residual resistance factors of 5-20 (trifluoperazine, tamoxifen, verapamil, quinine, nicardipine, dipyridamole) or even higher (diltiazem, quinidine, nifedipine). When studying doxorubicin accumulation obtained for an exposure to the IC50 of this drug, it appeared that some modulators were able to decrease this intracellular IC50 independently of their efficiency in resistance reversal (cyclosporine A, S9788, amiodarone, trifluoperazine, quinine, tamoxifen), thus reversing intracellular drug tolerance, whereas other modulators could not reduce this parameter (verapamil, nicardipine, dipyridamole, diltiazem, quinidine). It is suggested that drugs of the first group could be able to segregate doxorubicin in subcellular compartments from which it could not reach its nuclear targets." @default.
• W2170846620 created "2016-06-24" @default.
• W2170846620 creator A5023858440 @default.
• W2170846620 creator A5034156811 @default.
• W2170846620 creator A5060017701 @default.
• W2170846620 date "1993-01-01" @default.
• W2170846620 modified "2023-10-10" @default.
• W2170846620 title "Reversal of multidrug resistance by a new lipophilic cationic molecule, S9788. Comparison with 11 other MDR-modulating agents in a model of doxorubicin-resistant rat glioblastoma cells" @default.
• W2170846620 cites W1474183708 @default.
• W2170846620 cites W1499694712 @default.
• W2170846620 cites W1519177607 @default.
• W2170846620 cites W1572221045 @default.
• W2170846620 cites W1754065147 @default.
• W2170846620 cites W1775749144 @default.
• W2170846620 cites W1981034185 @default.
• W2170846620 cites W1985222126 @default.
• W2170846620 cites W1990918868 @default.
• W2170846620 cites W2001402350 @default.
• W2170846620 cites W2002808451 @default.
• W2170846620 cites W2003464317 @default.
• W2170846620 cites W2009455363 @default.
• W2170846620 cites W2048091892 @default.
• W2170846620 cites W2077361516 @default.
• W2170846620 cites W2081150848 @default.
• W2170846620 cites W2088419541 @default.
• W2170846620 cites W2113250804 @default.
• W2170846620 cites W2140323094 @default.
• W2170846620 doi "https://doi.org/10.1016/0959-8049(93)90005-z" @default.
• W2170846620 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/8398262" @default.
• W2170846620 hasPublicationYear "1993" @default.
• W2170846620 type Work @default.
• W2170846620 sameAs 2170846620 @default.
• W2170846620 citedByCount "28" @default.
• W2170846620 countsByYear W21708466202016 @default.
• W2170846620 countsByYear W21708466202022 @default.
• W2170846620 crossrefType "journal-article" @default.
• W2170846620 hasAuthorship W2170846620A5023858440 @default.
• W2170846620 hasAuthorship W2170846620A5034156811 @default.
• W2170846620 hasAuthorship W2170846620A5060017701 @default.
• W2170846620 hasConcept C114851261 @default.
• W2170846620 hasConcept C126322002 @default.
• W2170846620 hasConcept C133936738 @default.
• W2170846620 hasConcept C185592680 @default.
• W2170846620 hasConcept C2775891158 @default.
• W2170846620 hasConcept C2776694085 @default.
• W2170846620 hasConcept C2776741139 @default.
• W2170846620 hasConcept C2777022698 @default.
• W2170846620 hasConcept C2778707650 @default.
• W2170846620 hasConcept C2780339425 @default.
• W2170846620 hasConcept C2781303535 @default.
• W2170846620 hasConcept C29688787 @default.
• W2170846620 hasConcept C519063684 @default.
• W2170846620 hasConcept C71924100 @default.
• W2170846620 hasConcept C86803240 @default.
• W2170846620 hasConcept C89423630 @default.
• W2170846620 hasConcept C98274493 @default.
• W2170846620 hasConceptScore W2170846620C114851261 @default.
• W2170846620 hasConceptScore W2170846620C126322002 @default.
• W2170846620 hasConceptScore W2170846620C133936738 @default.
• W2170846620 hasConceptScore W2170846620C185592680 @default.
• W2170846620 hasConceptScore W2170846620C2775891158 @default.
• W2170846620 hasConceptScore W2170846620C2776694085 @default.
• W2170846620 hasConceptScore W2170846620C2776741139 @default.
• W2170846620 hasConceptScore W2170846620C2777022698 @default.
• W2170846620 hasConceptScore W2170846620C2778707650 @default.
• W2170846620 hasConceptScore W2170846620C2780339425 @default.
• W2170846620 hasConceptScore W2170846620C2781303535 @default.
• W2170846620 hasConceptScore W2170846620C29688787 @default.
• W2170846620 hasConceptScore W2170846620C519063684 @default.
• W2170846620 hasConceptScore W2170846620C71924100 @default.
• W2170846620 hasConceptScore W2170846620C86803240 @default.
• W2170846620 hasConceptScore W2170846620C89423630 @default.
• W2170846620 hasConceptScore W2170846620C98274493 @default.
• W2170846620 hasIssue "10" @default.
• W2170846620 hasLocation W21708466201 @default.
• W2170846620 hasLocation W21708466202 @default.
• W2170846620 hasOpenAccess W2170846620 @default.
• W2170846620 hasPrimaryLocation W21708466201 @default.
• W2170846620 hasRelatedWork W2002117217 @default.
• W2170846620 hasRelatedWork W2021945543 @default.
• W2170846620 hasRelatedWork W2076875643 @default.
• W2170846620 hasRelatedWork W2128986157 @default.
• W2170846620 hasRelatedWork W2155767001 @default.
• W2170846620 hasRelatedWork W2167758093 @default.
• W2170846620 hasRelatedWork W2322235548 @default.
• W2170846620 hasRelatedWork W2411636280 @default.
• W2170846620 hasRelatedWork W2442693147 @default.
• W2170846620 hasRelatedWork W168537953 @default.
• W2170846620 hasVolume "29" @default.
• W2170846620 isParatext "false" @default.
• W2170846620 isRetracted "false" @default.
• W2170846620 magId "2170846620" @default.
• W2170846620 workType "article" @default.