FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2060216716> ?p ?o ?g. }

• W2060216716 endingPage "2084" @default.
• W2060216716 startingPage "2075" @default.
• W2060216716 abstract "Oropharyngeal candidiasis (OPC) is an opportunistic fungal infection caused by Candida albicans. OPC is frequent in HIV/AIDS, implicating adaptive immunity. Mice are naive to Candida, yet IL-17 is induced within 24 h of infection, and susceptibility is strongly dependent on IL-17R signaling. We sought to identify the source of IL-17 during the early innate response to candidiasis. We show that innate responses to Candida require an intact TCR, as SCID, IL-7Rα−/−, and Rag1−/− mice were susceptible to OPC, and blockade of TCR signaling by cyclosporine induced susceptibility. Using fate-tracking IL-17 reporter mice, we found that IL-17 is produced within 1–2 d by tongue-resident populations of γδ T cells and CD3+CD4+CD44hiTCRβ+CCR6+ natural Th17 (nTh17) cells, but not by TCR-deficient innate lymphoid cells (ILCs) or NK cells. These cells function redundantly, as TCR-β−/− and TCR-δ−/− mice were both resistant to OPC. Whereas γδ T cells were previously shown to produce IL-17 during dermal candidiasis and are known to mediate host defense at mucosal surfaces, nTh17 cells are poorly understood. The oral nTh17 population expanded rapidly after OPC, exhibited high TCR-β clonal diversity, and was absent in Rag1−/−, IL-7Rα−/−, and germ-free mice. These findings indicate that nTh17 and γδ T cells, but not ILCs, are key mucosal sentinels that control oral pathogens." @default.
• W2060216716 created "2016-06-24" @default.
• W2060216716 creator A5005500510 @default.
• W2060216716 creator A5009843959 @default.
• W2060216716 creator A5010994218 @default.
• W2060216716 creator A5020370363 @default.
• W2060216716 creator A5023014854 @default.
• W2060216716 creator A5026972754 @default.
• W2060216716 creator A5035200249 @default.
• W2060216716 creator A5036946722 @default.
• W2060216716 creator A5046441344 @default.
• W2060216716 creator A5049895849 @default.
• W2060216716 creator A5062551240 @default.
• W2060216716 creator A5066660712 @default.
• W2060216716 creator A5069742204 @default.
• W2060216716 creator A5080366618 @default.
• W2060216716 creator A5084213389 @default.
• W2060216716 creator A5086035743 @default.
• W2060216716 creator A5086447914 @default.
• W2060216716 creator A5088924932 @default.
• W2060216716 date "2014-09-08" @default.
• W2060216716 modified "2023-10-10" @default.
• W2060216716 title "Oral-resident natural Th17 cells and γδ T cells control opportunistic Candida albicans infections" @default.
• W2060216716 cites W1492322782 @default.
• W2060216716 cites W1505833426 @default.
• W2060216716 cites W1741620332 @default.
• W2060216716 cites W1911254661 @default.
• W2060216716 cites W1960011333 @default.
• W2060216716 cites W1963745142 @default.
• W2060216716 cites W1968683200 @default.
• W2060216716 cites W1981032637 @default.
• W2060216716 cites W1981038069 @default.
• W2060216716 cites W1991036879 @default.
• W2060216716 cites W1991323622 @default.
• W2060216716 cites W1993339415 @default.
• W2060216716 cites W1998541797 @default.
• W2060216716 cites W1998895238 @default.
• W2060216716 cites W2007991617 @default.
• W2060216716 cites W2014913358 @default.
• W2060216716 cites W2017893786 @default.
• W2060216716 cites W2025084949 @default.
• W2060216716 cites W2029393400 @default.
• W2060216716 cites W2029860358 @default.
• W2060216716 cites W2032917789 @default.
• W2060216716 cites W2033289727 @default.
• W2060216716 cites W2034453891 @default.
• W2060216716 cites W2034582472 @default.
• W2060216716 cites W2036743290 @default.
• W2060216716 cites W2037258736 @default.
• W2060216716 cites W2048020246 @default.
• W2060216716 cites W2083382547 @default.
• W2060216716 cites W2085977010 @default.
• W2060216716 cites W2086264253 @default.
• W2060216716 cites W2093897672 @default.
• W2060216716 cites W2095753163 @default.
• W2060216716 cites W2098726188 @default.
• W2060216716 cites W2100105296 @default.
• W2060216716 cites W2101365364 @default.
• W2060216716 cites W2108822061 @default.
• W2060216716 cites W2109666345 @default.
• W2060216716 cites W2109839976 @default.
• W2060216716 cites W2113369941 @default.
• W2060216716 cites W2113561458 @default.
• W2060216716 cites W2116516945 @default.
• W2060216716 cites W2118815108 @default.
• W2060216716 cites W2123093300 @default.
• W2060216716 cites W2132442498 @default.
• W2060216716 cites W2134545706 @default.
• W2060216716 cites W2139643659 @default.
• W2060216716 cites W2144280353 @default.
• W2060216716 cites W2151960040 @default.
• W2060216716 cites W2154942611 @default.
• W2060216716 cites W2157677521 @default.
• W2060216716 cites W2162442785 @default.
• W2060216716 cites W2162721157 @default.
• W2060216716 cites W2169540909 @default.
• W2060216716 cites W2170016098 @default.
• W2060216716 cites W2170908195 @default.
• W2060216716 doi "https://doi.org/10.1084/jem.20130877" @default.
• W2060216716 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4172215" @default.
• W2060216716 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/25200028" @default.
• W2060216716 hasPublicationYear "2014" @default.
• W2060216716 type Work @default.
• W2060216716 sameAs 2060216716 @default.
• W2060216716 citedByCount "208" @default.
• W2060216716 countsByYear W20602167162014 @default.
• W2060216716 countsByYear W20602167162015 @default.
• W2060216716 countsByYear W20602167162016 @default.
• W2060216716 countsByYear W20602167162017 @default.
• W2060216716 countsByYear W20602167162018 @default.
• W2060216716 countsByYear W20602167162019 @default.
• W2060216716 countsByYear W20602167162020 @default.
• W2060216716 countsByYear W20602167162021 @default.
• W2060216716 countsByYear W20602167162022 @default.
• W2060216716 countsByYear W20602167162023 @default.
• W2060216716 crossrefType "journal-article" @default.
• W2060216716 hasAuthorship W2060216716A5005500510 @default.
• W2060216716 hasAuthorship W2060216716A5009843959 @default.

• next