FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W3178941580> ?p ?o ?g. }

• W3178941580 abstract "To date, no study has demonstrated that soluble Fas ligand (sFasL)-mediated inflammation is regulated via interaction with Fas in vivo. We found that FasL interacts specifically with tumor necrosis factor receptor superfamily (TNFRSF)10B, also known as death receptor (DR)5. Autoantibody-induced arthritis (AIA) was attenuated in FasL ( Fasl gld/gld )- and soluble FasL ( Fasl Δs/Δs )-deficient mice, but not in Fas ( Fas lpr/lpr and Fas –/– )- or membrane FasL ( Fasl Δm/Δm )-deficient mice, suggesting sFasL promotes inflammation by binding to a Fas-independent receptor. Affinity purification mass spectrometry analysis using human (h) fibroblast-like synovial cells (FLSCs) identified DR5 as one of several proteins that could be the elusive Fas-independent FasL receptor. Subsequent cellular and biochemical analyses revealed that DR5 interacted specifically with recombinant FasL–Fc protein, although the strength of this interaction was approximately 60-fold lower than the affinity between TRAIL and DR5. A microarray assay using joint tissues from mice with arthritis implied that the chemokine CX3CL1 may play an important downstream role of the interaction. The interaction enhanced Cx3cl1 transcription and increased sCX3CL1 production in FLSCs, possibly in an NF-κB-dependent manner. Moreover, the sFasL–DR5 interaction-mediated CX3CL1–CX3CR1 axis initiated and amplified inflammation by enhancing inflammatory cell influx and aggravating inflammation via secondary chemokine production. Blockade of FasL or CX3CR1 attenuated AIA. Therefore, the sFasL–DR5 interaction promotes inflammation and is a potential therapeutic target." @default.
• W3178941580 created "2021-07-19" @default.
• W3178941580 creator A5006640875 @default.
• W3178941580 creator A5010512463 @default.
• W3178941580 creator A5013714341 @default.
• W3178941580 creator A5023660115 @default.
• W3178941580 creator A5024958150 @default.
• W3178941580 creator A5027316753 @default.
• W3178941580 creator A5027741708 @default.
• W3178941580 creator A5030895412 @default.
• W3178941580 creator A5032091474 @default.
• W3178941580 creator A5038069069 @default.
• W3178941580 creator A5046075146 @default.
• W3178941580 creator A5061306460 @default.
• W3178941580 creator A5063086849 @default.
• W3178941580 creator A5070098382 @default.
• W3178941580 creator A5070181255 @default.
• W3178941580 creator A5085660248 @default.
• W3178941580 date "2021-07-05" @default.
• W3178941580 modified "2023-10-17" @default.
• W3178941580 title "Soluble Fas ligand drives autoantibody-induced arthritis by binding to DR5/TRAIL-R2" @default.
• W3178941580 cites W1496019202 @default.
• W3178941580 cites W1548222555 @default.
• W3178941580 cites W1554892411 @default.
• W3178941580 cites W1568365303 @default.
• W3178941580 cites W1662819364 @default.
• W3178941580 cites W1837819215 @default.
• W3178941580 cites W1967704552 @default.
• W3178941580 cites W1969187681 @default.
• W3178941580 cites W1969945556 @default.
• W3178941580 cites W1971160184 @default.
• W3178941580 cites W1978018492 @default.
• W3178941580 cites W1980396580 @default.
• W3178941580 cites W1984346091 @default.
• W3178941580 cites W1991366673 @default.
• W3178941580 cites W1994253900 @default.
• W3178941580 cites W1998226303 @default.
• W3178941580 cites W2017086893 @default.
• W3178941580 cites W2022508195 @default.
• W3178941580 cites W2029185117 @default.
• W3178941580 cites W2029654543 @default.
• W3178941580 cites W2043814519 @default.
• W3178941580 cites W2053321432 @default.
• W3178941580 cites W2063331298 @default.
• W3178941580 cites W2069075668 @default.
• W3178941580 cites W2076229621 @default.
• W3178941580 cites W2077544595 @default.
• W3178941580 cites W2087339935 @default.
• W3178941580 cites W2088924792 @default.
• W3178941580 cites W2091090735 @default.
• W3178941580 cites W2099903298 @default.
• W3178941580 cites W2105186639 @default.
• W3178941580 cites W2122823330 @default.
• W3178941580 cites W2126972955 @default.
• W3178941580 cites W2137530456 @default.
• W3178941580 cites W2145738273 @default.
• W3178941580 cites W2149103649 @default.
• W3178941580 cites W2152330823 @default.
• W3178941580 cites W2164802863 @default.
• W3178941580 cites W2166254983 @default.
• W3178941580 cites W2166328404 @default.
• W3178941580 cites W2493812037 @default.
• W3178941580 cites W2547223326 @default.
• W3178941580 cites W2763510961 @default.
• W3178941580 cites W2789657762 @default.
• W3178941580 cites W4244156420 @default.
• W3178941580 cites W4313333657 @default.
• W3178941580 cites W4375261546 @default.
• W3178941580 doi "https://doi.org/10.7554/elife.48840" @default.
• W3178941580 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/8257255" @default.
• W3178941580 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/34223817" @default.
• W3178941580 hasPublicationYear "2021" @default.
• W3178941580 type Work @default.
• W3178941580 sameAs 3178941580 @default.
• W3178941580 citedByCount "3" @default.
• W3178941580 countsByYear W31789415802022 @default.
• W3178941580 crossrefType "journal-article" @default.
• W3178941580 hasAuthorship W3178941580A5006640875 @default.
• W3178941580 hasAuthorship W3178941580A5010512463 @default.
• W3178941580 hasAuthorship W3178941580A5013714341 @default.
• W3178941580 hasAuthorship W3178941580A5023660115 @default.
• W3178941580 hasAuthorship W3178941580A5024958150 @default.
• W3178941580 hasAuthorship W3178941580A5027316753 @default.
• W3178941580 hasAuthorship W3178941580A5027741708 @default.
• W3178941580 hasAuthorship W3178941580A5030895412 @default.
• W3178941580 hasAuthorship W3178941580A5032091474 @default.
• W3178941580 hasAuthorship W3178941580A5038069069 @default.
• W3178941580 hasAuthorship W3178941580A5046075146 @default.
• W3178941580 hasAuthorship W3178941580A5061306460 @default.
• W3178941580 hasAuthorship W3178941580A5063086849 @default.
• W3178941580 hasAuthorship W3178941580A5070098382 @default.
• W3178941580 hasAuthorship W3178941580A5070181255 @default.
• W3178941580 hasAuthorship W3178941580A5085660248 @default.
• W3178941580 hasBestOaLocation W31789415801 @default.
• W3178941580 hasConcept C12823836 @default.
• W3178941580 hasConcept C13373296 @default.
• W3178941580 hasConcept C170493617 @default.
• W3178941580 hasConcept C17991360 @default.
• W3178941580 hasConcept C185592680 @default.
• W3178941580 hasConcept C190283241 @default.

• next