FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2000558013> ?p ?o ?g. }

• W2000558013 endingPage "247" @default.
• W2000558013 startingPage "235" @default.
• W2000558013 abstract "Background and purpose: Given the crucial role of the skeletal muscle chloride conductance (gCl), supported by the voltage-gated chloride channel CLC-1, in controlling muscle excitability, the availability of ligands modulating CLC-1 are of potential medical as well as toxicological importance. Here, we focused our attention on niflumic acid (NFA), a molecule belonging to the fenamates group of non-steroidal anti-inflammatory drugs (NSAID). Experimental approach: Rat muscle Cl− conductance (gCl) and heterologously expressed CLC-1 currents were evaluated by means of current-clamp (using two-microelectrodes) and patch-clamp techniques, respectively. Fura-2 fluorescence was used to determine intracellular calcium concentration, [Ca2+]i, in native muscle fibres. Key results: NFA inhibited native gCl with an IC50 of 42 μM and blocked CLC-1 by interacting with an intracellular binding site. Additionally, NFA increased basal [Ca2+]i in myofibres by promoting a mitochondrial calcium efflux that was not dependent on cyclooxygenase or CLC-1. A structure-activity study revealed that the molecular conditions that mediate the two effects are different. Pretreatment with the Ca-dependent protein kinase C (PKC) inhibitor chelerythrine partially inhibited the NFA effect. Therefore, in addition to direct channel block, NFA also inhibits gCl indirectly by promoting PKC activation. Conclusions and Implications: These cellular effects of NFA on skeletal muscle demonstrate that it is possible to modify CLC-1 and consequently gCl directly by interacting with channel proteins and indirectly by interfering with the calcium-dependent regulation of the channel. The effect of NFA on mitochondrial calcium stores suggests that NSAIDs, widely used drugs, could have potentially dangerous side-effects. British Journal of Pharmacology (2007) 150, 235–247. doi:10.1038/sj.bjp.0706954" @default.
• W2000558013 created "2016-06-24" @default.
• W2000558013 creator A5004636149 @default.
• W2000558013 creator A5020262838 @default.
• W2000558013 creator A5043399255 @default.
• W2000558013 creator A5051256686 @default.
• W2000558013 creator A5058084680 @default.
• W2000558013 creator A5082992801 @default.
• W2000558013 date "2007-01-01" @default.
• W2000558013 modified "2023-09-30" @default.
• W2000558013 title "Niflumic acid inhibits chloride conductance of rat skeletal muscle by directly inhibiting the CLC-1 channel and by increasing intracellular calcium" @default.
• W2000558013 cites W116341769 @default.
• W2000558013 cites W1894088205 @default.
• W2000558013 cites W194428502 @default.
• W2000558013 cites W1964347799 @default.
• W2000558013 cites W1967557485 @default.
• W2000558013 cites W1967838839 @default.
• W2000558013 cites W1974237962 @default.
• W2000558013 cites W1977831332 @default.
• W2000558013 cites W1978409411 @default.
• W2000558013 cites W1996666212 @default.
• W2000558013 cites W2002697895 @default.
• W2000558013 cites W2012429010 @default.
• W2000558013 cites W2015686095 @default.
• W2000558013 cites W2018632150 @default.
• W2000558013 cites W2018983834 @default.
• W2000558013 cites W2024487247 @default.
• W2000558013 cites W2028088027 @default.
• W2000558013 cites W2034848911 @default.
• W2000558013 cites W2035075678 @default.
• W2000558013 cites W2042389451 @default.
• W2000558013 cites W2063934982 @default.
• W2000558013 cites W2080083594 @default.
• W2000558013 cites W2080156145 @default.
• W2000558013 cites W2080962912 @default.
• W2000558013 cites W2081841421 @default.
• W2000558013 cites W2091553400 @default.
• W2000558013 cites W2093013713 @default.
• W2000558013 cites W2093908361 @default.
• W2000558013 cites W2108425243 @default.
• W2000558013 cites W2110798143 @default.
• W2000558013 cites W2111814865 @default.
• W2000558013 cites W2112543188 @default.
• W2000558013 cites W2114096403 @default.
• W2000558013 cites W2121135722 @default.
• W2000558013 cites W2123832242 @default.
• W2000558013 cites W2133433307 @default.
• W2000558013 cites W2141124826 @default.
• W2000558013 cites W2141260882 @default.
• W2000558013 cites W2149083834 @default.
• W2000558013 cites W2154588303 @default.
• W2000558013 cites W2161424579 @default.
• W2000558013 cites W2168984459 @default.
• W2000558013 cites W2413213959 @default.
• W2000558013 cites W4290217457 @default.
• W2000558013 cites W4376595542 @default.
• W2000558013 doi "https://doi.org/10.1038/sj.bjp.0706954" @default.
• W2000558013 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/2042903" @default.
• W2000558013 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/17128287" @default.
• W2000558013 hasPublicationYear "2007" @default.
• W2000558013 type Work @default.
• W2000558013 sameAs 2000558013 @default.
• W2000558013 citedByCount "51" @default.
• W2000558013 countsByYear W20005580132012 @default.
• W2000558013 countsByYear W20005580132013 @default.
• W2000558013 countsByYear W20005580132014 @default.
• W2000558013 countsByYear W20005580132015 @default.
• W2000558013 countsByYear W20005580132016 @default.
• W2000558013 countsByYear W20005580132017 @default.
• W2000558013 countsByYear W20005580132018 @default.
• W2000558013 countsByYear W20005580132019 @default.
• W2000558013 countsByYear W20005580132020 @default.
• W2000558013 countsByYear W20005580132021 @default.
• W2000558013 countsByYear W20005580132022 @default.
• W2000558013 countsByYear W20005580132023 @default.
• W2000558013 crossrefType "journal-article" @default.
• W2000558013 hasAuthorship W2000558013A5004636149 @default.
• W2000558013 hasAuthorship W2000558013A5020262838 @default.
• W2000558013 hasAuthorship W2000558013A5043399255 @default.
• W2000558013 hasAuthorship W2000558013A5051256686 @default.
• W2000558013 hasAuthorship W2000558013A5058084680 @default.
• W2000558013 hasAuthorship W2000558013A5082992801 @default.
• W2000558013 hasBestOaLocation W20005580131 @default.
• W2000558013 hasConcept C100837961 @default.
• W2000558013 hasConcept C12554922 @default.
• W2000558013 hasConcept C134018914 @default.
• W2000558013 hasConcept C145822097 @default.
• W2000558013 hasConcept C147944092 @default.
• W2000558013 hasConcept C170493617 @default.
• W2000558013 hasConcept C178790620 @default.
• W2000558013 hasConcept C181080969 @default.
• W2000558013 hasConcept C181911157 @default.
• W2000558013 hasConcept C185592680 @default.
• W2000558013 hasConcept C195794163 @default.
• W2000558013 hasConcept C2776108454 @default.
• W2000558013 hasConcept C2779700409 @default.
• W2000558013 hasConcept C2779959927 @default.
• W2000558013 hasConcept C519063684 @default.

• next