FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2172127345> ?p ?o ?g. }

• W2172127345 endingPage "1049" @default.
• W2172127345 startingPage "1038" @default.
• W2172127345 abstract "Macrophages act as the primary effector cells during Leishmania infection through production of reactive oxygen species (ROS) and interleukin-1β (IL-1β). However, how macrophage-killing mechanisms are activated during Leishmania-macrophage interactions is poorly understood. Here, we report that the macrophage response against Leishmania infantum in vivo is characterized by an M2b-like phenotype and C-type lectin receptors (CLRs) signature composed of Dectin-1, mannose receptor (MR), and the DC-SIGN homolog SIGNR3 expression. Dectin-1 and MR were crucial for the microbicidal response as indicated by the fact that they activated Syk-p47phox and arachidonic acid (AA)-NADPH oxidase signaling pathways, respectively, needed for ROS production and also triggered Syk-coupled signaling for caspase-1-induced IL-1β secretion. In contrast, SIGNR3 has divergent functions during Leishmania infantum pathogenesis; this CLR favored parasite resilience through inhibition of the LTB4-IL-1β axis. These pathways also operated during infection of primary human macrophages. Therefore, our study promotes CLRs as potential targets for treatment, diagnosis, and prevention of visceral leishmaniasis." @default.
• W2172127345 created "2016-06-24" @default.
• W2172127345 creator A5000811036 @default.
• W2172127345 creator A5003154600 @default.
• W2172127345 creator A5003363793 @default.
• W2172127345 creator A5005747261 @default.
• W2172127345 creator A5016310131 @default.
• W2172127345 creator A5033082298 @default.
• W2172127345 creator A5034548312 @default.
• W2172127345 creator A5034669783 @default.
• W2172127345 creator A5038070846 @default.
• W2172127345 creator A5068459453 @default.
• W2172127345 creator A5076903034 @default.
• W2172127345 creator A5084429684 @default.
• W2172127345 creator A5087422095 @default.
• W2172127345 creator A5088332737 @default.
• W2172127345 date "2013-05-01" @default.
• W2172127345 modified "2023-09-30" @default.
• W2172127345 title "The C-type Lectin Receptors Dectin-1, MR, and SIGNR3 Contribute Both Positively and Negatively to the Macrophage Response to Leishmania infantum" @default.
• W2172127345 cites W1548106543 @default.
• W2172127345 cites W1565755899 @default.
• W2172127345 cites W1884045055 @default.
• W2172127345 cites W1912978047 @default.
• W2172127345 cites W1962869168 @default.
• W2172127345 cites W1965955178 @default.
• W2172127345 cites W1985075809 @default.
• W2172127345 cites W1988822418 @default.
• W2172127345 cites W2020744745 @default.
• W2172127345 cites W2020871710 @default.
• W2172127345 cites W2025355874 @default.
• W2172127345 cites W2036743290 @default.
• W2172127345 cites W2036811549 @default.
• W2172127345 cites W2055229002 @default.
• W2172127345 cites W2057028848 @default.
• W2172127345 cites W2066639757 @default.
• W2172127345 cites W2067736150 @default.
• W2172127345 cites W2073547045 @default.
• W2172127345 cites W2075428144 @default.
• W2172127345 cites W2076251291 @default.
• W2172127345 cites W2086531464 @default.
• W2172127345 cites W2086613620 @default.
• W2172127345 cites W2089229753 @default.
• W2172127345 cites W2093705034 @default.
• W2172127345 cites W2096620140 @default.
• W2172127345 cites W2104475738 @default.
• W2172127345 cites W2113203684 @default.
• W2172127345 cites W2114769428 @default.
• W2172127345 cites W2121073273 @default.
• W2172127345 cites W2122105886 @default.
• W2172127345 cites W2124293643 @default.
• W2172127345 cites W2126924404 @default.
• W2172127345 cites W2132327341 @default.
• W2172127345 cites W2138370786 @default.
• W2172127345 cites W2139243925 @default.
• W2172127345 cites W2141206527 @default.
• W2172127345 cites W2144002025 @default.
• W2172127345 cites W2162303211 @default.
• W2172127345 cites W2162481769 @default.
• W2172127345 doi "https://doi.org/10.1016/j.immuni.2013.04.010" @default.
• W2172127345 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/23684988" @default.
• W2172127345 hasPublicationYear "2013" @default.
• W2172127345 type Work @default.
• W2172127345 sameAs 2172127345 @default.
• W2172127345 citedByCount "118" @default.
• W2172127345 countsByYear W21721273452013 @default.
• W2172127345 countsByYear W21721273452014 @default.
• W2172127345 countsByYear W21721273452015 @default.
• W2172127345 countsByYear W21721273452016 @default.
• W2172127345 countsByYear W21721273452017 @default.
• W2172127345 countsByYear W21721273452018 @default.
• W2172127345 countsByYear W21721273452019 @default.
• W2172127345 countsByYear W21721273452020 @default.
• W2172127345 countsByYear W21721273452021 @default.
• W2172127345 countsByYear W21721273452022 @default.
• W2172127345 countsByYear W21721273452023 @default.
• W2172127345 crossrefType "journal-article" @default.
• W2172127345 hasAuthorship W2172127345A5000811036 @default.
• W2172127345 hasAuthorship W2172127345A5003154600 @default.
• W2172127345 hasAuthorship W2172127345A5003363793 @default.
• W2172127345 hasAuthorship W2172127345A5005747261 @default.
• W2172127345 hasAuthorship W2172127345A5016310131 @default.
• W2172127345 hasAuthorship W2172127345A5033082298 @default.
• W2172127345 hasAuthorship W2172127345A5034548312 @default.
• W2172127345 hasAuthorship W2172127345A5034669783 @default.
• W2172127345 hasAuthorship W2172127345A5038070846 @default.
• W2172127345 hasAuthorship W2172127345A5068459453 @default.
• W2172127345 hasAuthorship W2172127345A5076903034 @default.
• W2172127345 hasAuthorship W2172127345A5084429684 @default.
• W2172127345 hasAuthorship W2172127345A5087422095 @default.
• W2172127345 hasAuthorship W2172127345A5088332737 @default.
• W2172127345 hasBestOaLocation W21721273451 @default.
• W2172127345 hasConcept C106257327 @default.
• W2172127345 hasConcept C136764020 @default.
• W2172127345 hasConcept C170493617 @default.
• W2172127345 hasConcept C189413060 @default.
• W2172127345 hasConcept C202751555 @default.
• W2172127345 hasConcept C203014093 @default.
• W2172127345 hasConcept C2776205754 @default.

• next