SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2023256140> ?p ?o ?g. }

Showing items 1 to 100 of ±154 with 100 items per page.

W2023256140 endingPage "1732" @default.
W2023256140 startingPage "1720" @default.
W2023256140 abstract "Invariant natural killer T (iNKT) cells are involved in the intrahepatic immune response and in hepatitis. In particular, iNKT lymphocytes are responsible for hepatocyte death in concanavalin A-induced hepatitis in mice. We examined the role of iNKT cells in acute hepatitis induced by a hepatotoxic agent, carbon tetrachloride (CCl(4) ). WT and iNKT cell-deficient (Jα18(-/-) ) mice were challenged with a single dose of 2.4 g/kg CCl(4) and both hepatic physiopathology and immune responses were studied. Plasma alanine and aspartate amino-transferase levels were significantly higher in Jα18(-/-) mice than in WT mice two days after CCl(4) administration. Chemokine CXCL1/keratinocyte-derived chemokine (KC) and MMP-8 were significantly higher in iNKT cell-deficient mice than in control mice. The more severe liver injury in Jα18(-/-) mice was associated with greater leukocyte infiltrate, which was enriched in neutrophils (CD11b(+) CD11c(-) Gr-1(+) cells), in agreement with CXCL1/KC and MMP-8 levels. Complementary experiments with NK-depleted animals indicate a minor role for NK cells in the liver damage found in iNKT-deficient mice. Thus, unlike for ConA-induced hepatitis, we report that iNKT cells protect the liver against acute hepatitis induced by CCl(4) and limit neutrophil infiltration." @default.
W2023256140 created "2016-06-24" @default.
W2023256140 creator A5049544266 @default.
W2023256140 creator A5050027025 @default.
W2023256140 creator A5055348027 @default.
W2023256140 creator A5058822160 @default.
W2023256140 creator A5059824648 @default.
W2023256140 creator A5061635068 @default.
W2023256140 creator A5067667247 @default.
W2023256140 creator A5088788876 @default.
W2023256140 date "2011-05-25" @default.
W2023256140 modified "2023-10-18" @default.
W2023256140 title "Invariant natural killer T-cell-deficient mice display increased CCl4-induced hepatitis associated with CXCL1 over-expression and neutrophil infiltration" @default.
W2023256140 cites W1507189961 @default.
W2023256140 cites W1552424392 @default.
W2023256140 cites W1571951314 @default.
W2023256140 cites W1623305982 @default.
W2023256140 cites W1653749361 @default.
W2023256140 cites W1748261727 @default.
W2023256140 cites W1900386759 @default.
W2023256140 cites W1987344938 @default.
W2023256140 cites W1991709816 @default.
W2023256140 cites W1992523113 @default.
W2023256140 cites W1992893234 @default.
W2023256140 cites W1997994897 @default.
W2023256140 cites W1999241917 @default.
W2023256140 cites W2003478773 @default.
W2023256140 cites W2003747312 @default.
W2023256140 cites W2015194963 @default.
W2023256140 cites W2021608450 @default.
W2023256140 cites W2033185857 @default.
W2023256140 cites W2039401190 @default.
W2023256140 cites W2053954731 @default.
W2023256140 cites W2057368742 @default.
W2023256140 cites W2061372968 @default.
W2023256140 cites W2062362734 @default.
W2023256140 cites W2069556438 @default.
W2023256140 cites W2071276803 @default.
W2023256140 cites W2083851689 @default.
W2023256140 cites W2083988704 @default.
W2023256140 cites W2097139406 @default.
W2023256140 cites W2099465341 @default.
W2023256140 cites W2112942968 @default.
W2023256140 cites W2117985944 @default.
W2023256140 cites W2121477549 @default.
W2023256140 cites W2122953616 @default.
W2023256140 cites W2124491055 @default.
W2023256140 cites W2125961211 @default.
W2023256140 cites W2137597074 @default.
W2023256140 cites W2138453840 @default.
W2023256140 cites W2141131363 @default.
W2023256140 cites W2145379498 @default.
W2023256140 cites W2151164793 @default.
W2023256140 cites W2161307276 @default.
W2023256140 cites W2161817746 @default.
W2023256140 cites W2164209124 @default.
W2023256140 cites W2166835590 @default.
W2023256140 cites W2344344806 @default.
W2023256140 doi "https://doi.org/10.1002/eji.201041006" @default.
W2023256140 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/21469102" @default.
W2023256140 hasPublicationYear "2011" @default.
W2023256140 type Work @default.
W2023256140 sameAs 2023256140 @default.
W2023256140 citedByCount "25" @default.
W2023256140 countsByYear W20232561402012 @default.
W2023256140 countsByYear W20232561402013 @default.
W2023256140 countsByYear W20232561402015 @default.
W2023256140 countsByYear W20232561402016 @default.
W2023256140 countsByYear W20232561402017 @default.
W2023256140 countsByYear W20232561402020 @default.
W2023256140 countsByYear W20232561402021 @default.
W2023256140 countsByYear W20232561402022 @default.
W2023256140 countsByYear W20232561402023 @default.
W2023256140 crossrefType "journal-article" @default.
W2023256140 hasAuthorship W2023256140A5049544266 @default.
W2023256140 hasAuthorship W2023256140A5050027025 @default.
W2023256140 hasAuthorship W2023256140A5055348027 @default.
W2023256140 hasAuthorship W2023256140A5058822160 @default.
W2023256140 hasAuthorship W2023256140A5059824648 @default.
W2023256140 hasAuthorship W2023256140A5061635068 @default.
W2023256140 hasAuthorship W2023256140A5067667247 @default.
W2023256140 hasAuthorship W2023256140A5088788876 @default.
W2023256140 hasBestOaLocation W20232561401 @default.
W2023256140 hasConcept C102124568 @default.
W2023256140 hasConcept C104317684 @default.
W2023256140 hasConcept C109316439 @default.
W2023256140 hasConcept C127716648 @default.
W2023256140 hasConcept C13373296 @default.
W2023256140 hasConcept C134018914 @default.
W2023256140 hasConcept C136449434 @default.
W2023256140 hasConcept C139563560 @default.
W2023256140 hasConcept C178790620 @default.
W2023256140 hasConcept C185592680 @default.
W2023256140 hasConcept C202751555 @default.
W2023256140 hasConcept C203014093 @default.
W2023256140 hasConcept C2776029263 @default.
W2023256140 hasConcept C2776090121 @default.
W2023256140 hasConcept C2776200302 @default.