FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2077548696> ?p ?o ?g. }

• W2077548696 endingPage "27" @default.
• W2077548696 startingPage "18" @default.
• W2077548696 abstract "Interruption in the brain's blood supply leads to an ischemic condition, which is characterised by a depletion of energy phosphates and related failure of ionic pumps, increased extracellular potassium, neuronal depolarisation and release of excitatory amino acids, e.g. glutamate. The subsequent activation of N-methyl-d-aspartate glutamate receptors triggers a wide range of intracellular signals, including the mitogen-activated protein kinase (MAPK) pathway. Activation and inhibition of the MAPK/extracellular regulated kinases (ERK) pathway are both reported to be neuroprotective in conditions associated with excitotoxic injury. The present study was designed to explore the involvement of this signalling pathway in cultured rat cortical neurons subjected to chemically-induced ischemia obtained by coupling the mitochondrial toxin 3-nitropropionic acid with glucose deprivation. Loss of neuronal viability, reduced neuronal energy state (ATP level and mitochondrial membrane potential) and increased cytoplasmic mitochondrial calcium were all observed. The NMDA antagonist MK-801 counteracted these effects, suggesting a glutamate-dependent ischemic cell death. Addition of U0126, a selective inhibitor of MAPK kinase, exacerbated this neuronal cell death. However, non-significant changes in activated cAMP response element-binding protein were seen. The rise in cytoplasmic calcium under ischemic conditions was associated with neuronal cell swelling. Both swelling and increase in cytoplasmic calcium were exacerbated and prevented by U0126 and MK-801, respectively. These data suggest that in this ischemic model the MAPK/ERK pathway might exert a regulatory effect on calcium entry independent from gene expression." @default.
• W2077548696 created "2016-06-24" @default.
• W2077548696 creator A5006221519 @default.
• W2077548696 creator A5016966644 @default.
• W2077548696 creator A5034378967 @default.
• W2077548696 date "2006-12-01" @default.
• W2077548696 modified "2023-09-23" @default.
• W2077548696 title "MEK inhibition exacerbates ischemic calcium imbalance and neuronal cell death in rat cortical cultures" @default.
• W2077548696 cites W1529774113 @default.
• W2077548696 cites W1533853049 @default.
• W2077548696 cites W1578237109 @default.
• W2077548696 cites W1614322283 @default.
• W2077548696 cites W1824170643 @default.
• W2077548696 cites W1933207236 @default.
• W2077548696 cites W1963092557 @default.
• W2077548696 cites W1973587217 @default.
• W2077548696 cites W1973750046 @default.
• W2077548696 cites W1974252208 @default.
• W2077548696 cites W1979813185 @default.
• W2077548696 cites W1996405087 @default.
• W2077548696 cites W1998470223 @default.
• W2077548696 cites W2002935592 @default.
• W2077548696 cites W2006681786 @default.
• W2077548696 cites W2012016665 @default.
• W2077548696 cites W2012797849 @default.
• W2077548696 cites W2014408809 @default.
• W2077548696 cites W2016916414 @default.
• W2077548696 cites W2022658303 @default.
• W2077548696 cites W2024434386 @default.
• W2077548696 cites W2024835352 @default.
• W2077548696 cites W2025644637 @default.
• W2077548696 cites W2030531291 @default.
• W2077548696 cites W2031272027 @default.
• W2077548696 cites W2033678540 @default.
• W2077548696 cites W2034454128 @default.
• W2077548696 cites W2035750459 @default.
• W2077548696 cites W2038638872 @default.
• W2077548696 cites W2042829586 @default.
• W2077548696 cites W2048127649 @default.
• W2077548696 cites W2049517532 @default.
• W2077548696 cites W2051395367 @default.
• W2077548696 cites W2052750950 @default.
• W2077548696 cites W2062299751 @default.
• W2077548696 cites W2067148272 @default.
• W2077548696 cites W2069198916 @default.
• W2077548696 cites W2069894419 @default.
• W2077548696 cites W2073883806 @default.
• W2077548696 cites W2074792377 @default.
• W2077548696 cites W2078594622 @default.
• W2077548696 cites W2086815559 @default.
• W2077548696 cites W2094563432 @default.
• W2077548696 cites W2099768623 @default.
• W2077548696 cites W2120670195 @default.
• W2077548696 cites W2124697511 @default.
• W2077548696 cites W2126416149 @default.
• W2077548696 cites W2133702956 @default.
• W2077548696 cites W2138795251 @default.
• W2077548696 cites W2139748951 @default.
• W2077548696 cites W2140059872 @default.
• W2077548696 cites W2145413598 @default.
• W2077548696 cites W2155152553 @default.
• W2077548696 cites W2156655462 @default.
• W2077548696 cites W2162264368 @default.
• W2077548696 cites W2163841690 @default.
• W2077548696 cites W2169129605 @default.
• W2077548696 cites W2169294911 @default.
• W2077548696 cites W4327766731 @default.
• W2077548696 doi "https://doi.org/10.1016/j.ejphar.2006.08.043" @default.
• W2077548696 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/17097633" @default.
• W2077548696 hasPublicationYear "2006" @default.
• W2077548696 type Work @default.
• W2077548696 sameAs 2077548696 @default.
• W2077548696 citedByCount "15" @default.
• W2077548696 countsByYear W20775486962012 @default.
• W2077548696 countsByYear W20775486962013 @default.
• W2077548696 countsByYear W20775486962015 @default.
• W2077548696 countsByYear W20775486962017 @default.
• W2077548696 crossrefType "journal-article" @default.
• W2077548696 hasAuthorship W2077548696A5006221519 @default.
• W2077548696 hasAuthorship W2077548696A5016966644 @default.
• W2077548696 hasAuthorship W2077548696A5034378967 @default.
• W2077548696 hasConcept C126322002 @default.
• W2077548696 hasConcept C170493617 @default.
• W2077548696 hasConcept C181080969 @default.
• W2077548696 hasConcept C184235292 @default.
• W2077548696 hasConcept C185592680 @default.
• W2077548696 hasConcept C190283241 @default.
• W2077548696 hasConcept C25498285 @default.
• W2077548696 hasConcept C28406088 @default.
• W2077548696 hasConcept C31573885 @default.
• W2077548696 hasConcept C519063684 @default.
• W2077548696 hasConcept C55493867 @default.
• W2077548696 hasConcept C57074206 @default.
• W2077548696 hasConcept C61174792 @default.
• W2077548696 hasConcept C67018056 @default.
• W2077548696 hasConcept C71924100 @default.
• W2077548696 hasConcept C79879829 @default.
• W2077548696 hasConcept C86803240 @default.

• next