FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1915707280> ?p ?o ?g. }

• W1915707280 endingPage "3168" @default.
• W1915707280 startingPage "3156" @default.
• W1915707280 abstract "Abstract IL-1α and IL-1β (in this article referred to as IL-1) play important roles in host defense against infection and inflammatory diseases. IL-1R1 is the receptor for IL-1, and IL-1R2 is suggested to be a decoy receptor, because it lacks the signal-transducing TIR domain in the cytoplasmic part. However, the roles of IL-1R2 in health and disease remain largely unknown. In this study, we generated EGFP-knock-in Il1r2−/− mice and showed that they were highly susceptible to collagen-induced arthritis, an animal model for rheumatoid arthritis in which the expression of IL-1R2 is augmented in inflammatory joints. Il1r2 was highly expressed in neutrophils but had only low expression in other cells, including monocytes and macrophages. Ab production and T cell responses against type II collagen were normal in Il1r2−/− mice. Despite the high expression in neutrophils, no effects of Il1r2 deficiency were observed; however, we found that production of inflammatory mediators in response to IL-1 was greatly enhanced in Il1r2−/− macrophages. These results suggest that IL-1R2 is an important regulator of arthritis by acting specifically on macrophages as a decoy receptor for IL-1." @default.
• W1915707280 created "2016-06-24" @default.
• W1915707280 creator A5009095737 @default.
• W1915707280 creator A5018149450 @default.
• W1915707280 creator A5019623163 @default.
• W1915707280 creator A5029666084 @default.
• W1915707280 creator A5037231222 @default.
• W1915707280 creator A5044756754 @default.
• W1915707280 creator A5059569764 @default.
• W1915707280 creator A5065568071 @default.
• W1915707280 creator A5074919264 @default.
• W1915707280 creator A5089668575 @default.
• W1915707280 date "2015-04-01" @default.
• W1915707280 modified "2023-10-16" @default.
• W1915707280 title "IL-1 Receptor Type 2 Suppresses Collagen-Induced Arthritis by Inhibiting IL-1 Signal on Macrophages" @default.
• W1915707280 cites W1484482114 @default.
• W1915707280 cites W1488576485 @default.
• W1915707280 cites W1491655932 @default.
• W1915707280 cites W1519700871 @default.
• W1915707280 cites W1599213766 @default.
• W1915707280 cites W1910189841 @default.
• W1915707280 cites W1954931145 @default.
• W1915707280 cites W1966000361 @default.
• W1915707280 cites W1966671453 @default.
• W1915707280 cites W1967413976 @default.
• W1915707280 cites W1983881111 @default.
• W1915707280 cites W1993026721 @default.
• W1915707280 cites W1996919490 @default.
• W1915707280 cites W2000581651 @default.
• W1915707280 cites W2006392330 @default.
• W1915707280 cites W2008444492 @default.
• W1915707280 cites W2012430430 @default.
• W1915707280 cites W2025117799 @default.
• W1915707280 cites W2027592271 @default.
• W1915707280 cites W2035445024 @default.
• W1915707280 cites W2038081789 @default.
• W1915707280 cites W2043765645 @default.
• W1915707280 cites W2047711342 @default.
• W1915707280 cites W2055740572 @default.
• W1915707280 cites W2057323778 @default.
• W1915707280 cites W2064888308 @default.
• W1915707280 cites W2064976031 @default.
• W1915707280 cites W2070871300 @default.
• W1915707280 cites W2074395616 @default.
• W1915707280 cites W2078624814 @default.
• W1915707280 cites W2086545085 @default.
• W1915707280 cites W2099596517 @default.
• W1915707280 cites W2111045447 @default.
• W1915707280 cites W2113361721 @default.
• W1915707280 cites W2117439999 @default.
• W1915707280 cites W2121908124 @default.
• W1915707280 cites W2122152368 @default.
• W1915707280 cites W2124335748 @default.
• W1915707280 cites W2133557129 @default.
• W1915707280 cites W2135498543 @default.
• W1915707280 cites W2136434338 @default.
• W1915707280 cites W2140739060 @default.
• W1915707280 cites W2142814906 @default.
• W1915707280 cites W2148361763 @default.
• W1915707280 cites W2150107812 @default.
• W1915707280 cites W2162104177 @default.
• W1915707280 cites W2165275387 @default.
• W1915707280 cites W2166204514 @default.
• W1915707280 cites W2168082890 @default.
• W1915707280 cites W2168194036 @default.
• W1915707280 cites W4313347845 @default.
• W1915707280 doi "https://doi.org/10.4049/jimmunol.1402155" @default.
• W1915707280 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/25725107" @default.
• W1915707280 hasPublicationYear "2015" @default.
• W1915707280 type Work @default.
• W1915707280 sameAs 1915707280 @default.
• W1915707280 citedByCount "54" @default.
• W1915707280 countsByYear W19157072802015 @default.
• W1915707280 countsByYear W19157072802016 @default.
• W1915707280 countsByYear W19157072802017 @default.
• W1915707280 countsByYear W19157072802018 @default.
• W1915707280 countsByYear W19157072802019 @default.
• W1915707280 countsByYear W19157072802020 @default.
• W1915707280 countsByYear W19157072802021 @default.
• W1915707280 countsByYear W19157072802022 @default.
• W1915707280 countsByYear W19157072802023 @default.
• W1915707280 crossrefType "journal-article" @default.
• W1915707280 hasAuthorship W1915707280A5009095737 @default.
• W1915707280 hasAuthorship W1915707280A5018149450 @default.
• W1915707280 hasAuthorship W1915707280A5019623163 @default.
• W1915707280 hasAuthorship W1915707280A5029666084 @default.
• W1915707280 hasAuthorship W1915707280A5037231222 @default.
• W1915707280 hasAuthorship W1915707280A5044756754 @default.
• W1915707280 hasAuthorship W1915707280A5059569764 @default.
• W1915707280 hasAuthorship W1915707280A5065568071 @default.
• W1915707280 hasAuthorship W1915707280A5074919264 @default.
• W1915707280 hasAuthorship W1915707280A5089668575 @default.
• W1915707280 hasBestOaLocation W19157072801 @default.
• W1915707280 hasConcept C10775765 @default.
• W1915707280 hasConcept C119557319 @default.
• W1915707280 hasConcept C126322002 @default.
• W1915707280 hasConcept C170493617 @default.
• W1915707280 hasConcept C181901479 @default.

• next