FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2960998041> ?p ?o ?g. }

• W2960998041 endingPage "106346" @default.
• W2960998041 startingPage "106346" @default.
• W2960998041 abstract "The OXE receptor is a GPCR activated by eicosanoids produced by the action of 5-lipoxygenase. We previously found that this membrane receptor participates in the regulation of cAMP-dependent and -independent steroidogenesis in human H295R adrenocortical carcinoma cells. In this study we analyzed the effects of the OXE receptor physiological activator 5-oxo-ETE on the growth and migration of H259R cells. While 5-oxo-ETE did not affect the growth of H295R cells, overexpression of OXE receptor caused an increase in cell proliferation, which was further increased by 5-oxo-ETE and blocked by 5-lipoxygenase inhibition. 5-oxo-ETE increased the migratory capacity of H295R cells in wound healing assays, but it did not induce the production of metalloproteases MMP-1, MMP-2, MMP-9 and MMP-10. The pro-migratory effect of 5-oxo-ETE was reduced by pharmacological inhibition of the MEK/ERK1/2, p38 and PKC pathways. 5-oxo-ETE caused significant activation of ERK and p38. ERK activation by the eicosanoid was reduced by the “pan” PKC inhibitor GF109203X but not by the classical PKC inhibitor Gö6976, suggesting the involvement of novel PKCs in this effect. Although H295R cells display detectable phosphorylation of Ser299 in PKCδ, a readout for the activation of this novel PKC, treatment with 5-oxo-ETE per se was unable to induce additional PKCδ activation. Our results revealed signaling effectors activated by 5-oxo-ETE in H295R cells and may have significant implications for our understanding of OXE receptor in adrenocortical cell pathophysiology." @default.
• W2960998041 created "2019-07-23" @default.
• W2960998041 creator A5018709530 @default.
• W2960998041 creator A5024259315 @default.
• W2960998041 creator A5029548499 @default.
• W2960998041 creator A5055483233 @default.
• W2960998041 creator A5073440215 @default.
• W2960998041 date "2019-10-01" @default.
• W2960998041 modified "2023-10-16" @default.
• W2960998041 title "5-oxo-ETE activates migration of H295R adrenocortical cells via MAPK and PKC pathways" @default.
• W2960998041 cites W1503724433 @default.
• W2960998041 cites W1610204701 @default.
• W2960998041 cites W1654089893 @default.
• W2960998041 cites W1806394871 @default.
• W2960998041 cites W1965781391 @default.
• W2960998041 cites W1967561584 @default.
• W2960998041 cites W1968874083 @default.
• W2960998041 cites W1975995627 @default.
• W2960998041 cites W1978053309 @default.
• W2960998041 cites W1979420492 @default.
• W2960998041 cites W1979815791 @default.
• W2960998041 cites W1987496015 @default.
• W2960998041 cites W1989608005 @default.
• W2960998041 cites W1991337026 @default.
• W2960998041 cites W1993046666 @default.
• W2960998041 cites W1994271130 @default.
• W2960998041 cites W1995333517 @default.
• W2960998041 cites W1996530399 @default.
• W2960998041 cites W1996957147 @default.
• W2960998041 cites W2001293789 @default.
• W2960998041 cites W2011929090 @default.
• W2960998041 cites W2017493172 @default.
• W2960998041 cites W2018666623 @default.
• W2960998041 cites W2034133667 @default.
• W2960998041 cites W2034649274 @default.
• W2960998041 cites W2039207394 @default.
• W2960998041 cites W2039490460 @default.
• W2960998041 cites W2039716262 @default.
• W2960998041 cites W2041445540 @default.
• W2960998041 cites W2044082573 @default.
• W2960998041 cites W2045170807 @default.
• W2960998041 cites W2045436741 @default.
• W2960998041 cites W2047497205 @default.
• W2960998041 cites W2054324993 @default.
• W2960998041 cites W2057609644 @default.
• W2960998041 cites W2060632291 @default.
• W2960998041 cites W2063254564 @default.
• W2960998041 cites W2070199322 @default.
• W2960998041 cites W2073763063 @default.
• W2960998041 cites W2074269446 @default.
• W2960998041 cites W2077221155 @default.
• W2960998041 cites W2078261279 @default.
• W2960998041 cites W2081500836 @default.
• W2960998041 cites W2086178662 @default.
• W2960998041 cites W2088053118 @default.
• W2960998041 cites W2089087441 @default.
• W2960998041 cites W2095321628 @default.
• W2960998041 cites W2099709602 @default.
• W2960998041 cites W2100592123 @default.
• W2960998041 cites W2107150819 @default.
• W2960998041 cites W2110378444 @default.
• W2960998041 cites W2114360817 @default.
• W2960998041 cites W2125166909 @default.
• W2960998041 cites W2129860672 @default.
• W2960998041 cites W2134440280 @default.
• W2960998041 cites W2135178410 @default.
• W2960998041 cites W2148822676 @default.
• W2960998041 cites W2156326987 @default.
• W2960998041 cites W2166596095 @default.
• W2960998041 cites W2167428477 @default.
• W2960998041 cites W2248084827 @default.
• W2960998041 cites W2345752351 @default.
• W2960998041 cites W2346423669 @default.
• W2960998041 cites W2429403923 @default.
• W2960998041 cites W2599797927 @default.
• W2960998041 cites W2607050954 @default.
• W2960998041 cites W270414473 @default.
• W2960998041 cites W2722231853 @default.
• W2960998041 cites W2797683329 @default.
• W2960998041 cites W2885664683 @default.
• W2960998041 cites W2889895850 @default.
• W2960998041 doi "https://doi.org/10.1016/j.prostaglandins.2019.106346" @default.
• W2960998041 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6778002" @default.
• W2960998041 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/31301403" @default.
• W2960998041 hasPublicationYear "2019" @default.
• W2960998041 type Work @default.
• W2960998041 sameAs 2960998041 @default.
• W2960998041 citedByCount "4" @default.
• W2960998041 countsByYear W29609980412021 @default.
• W2960998041 countsByYear W29609980412022 @default.
• W2960998041 countsByYear W29609980412023 @default.
• W2960998041 crossrefType "journal-article" @default.
• W2960998041 hasAuthorship W2960998041A5018709530 @default.
• W2960998041 hasAuthorship W2960998041A5024259315 @default.
• W2960998041 hasAuthorship W2960998041A5029548499 @default.
• W2960998041 hasAuthorship W2960998041A5055483233 @default.
• W2960998041 hasAuthorship W2960998041A5073440215 @default.
• W2960998041 hasBestOaLocation W29609980412 @default.

• next