FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2892660368> ?p ?o ?g. }

• W2892660368 endingPage "4332" @default.
• W2892660368 startingPage "4321" @default.
• W2892660368 abstract "Abstract Interferon‐γ (IFN‐γ) plays an important role in innate and adaptive immunity against intracellular infections and is used clinically for the prevention and control of infections in chronic granulomatous disease (CGD) and inborn defects in the IFN‐γ/interleukin (IL)‐12 axis. Using transcriptome profiling (RNA‐seq), we sought to identify differentially expressed genes, transcripts and exons in Epstein‐Barr virus–transformed B lymphocytes (B‐EBV) cells from CGD patients, IFN‐γ receptor deficiency patients, and normal controls, treated in vitro with IFN‐γ for 48 hours. Our results show that IFN‐γ increased the expression of a diverse array of genes related to different cellular programs. In cells from normal controls and CGD patients, IFN‐γ‐induced expression of genes relevant to oxidative killing, nitric oxide synthase pathway, proteasome‐mediated degradation, antigen presentation, chemoattraction, and cell adhesion. IFN‐γ also upregulated genes involved in diverse stages of messenger RNA (mRNA) processing including pre‐mRNA splicing, as well as others implicated in the folding, transport, and assembly of proteins. In particular, differential exon expression of WARS (encoding tryptophanyl‐transfer RNA synthetase, which has an essential function in protein synthesis) induced by IFN‐γ in normal and CGD cells suggests that this gene may have an important contribution to the benefits of IFN‐γ treatment for CGD. Upregulation of mRNA and protein processing related genes in CGD and IFNRD cells could mediate some of the effects of IFN‐γ treatment. These data support the concept that IFN‐γ treatment may contribute to increased immune responses against pathogens through regulation of genes important for mRNA and protein processing." @default.
• W2892660368 created "2018-10-05" @default.
• W2892660368 creator A5004120907 @default.
• W2892660368 creator A5007839902 @default.
• W2892660368 creator A5011173907 @default.
• W2892660368 creator A5025814275 @default.
• W2892660368 creator A5056629197 @default.
• W2892660368 creator A5065215242 @default.
• W2892660368 creator A5067494403 @default.
• W2892660368 creator A5072123349 @default.
• W2892660368 creator A5084203689 @default.
• W2892660368 creator A5090580248 @default.
• W2892660368 creator A5091298095 @default.
• W2892660368 date "2018-09-27" @default.
• W2892660368 modified "2023-10-14" @default.
• W2892660368 title "Gene expression in chronic granulomatous disease and interferon‐γ receptor‐deficient cells treated in vitro with interferon‐γ" @default.
• W2892660368 cites W1484229756 @default.
• W2892660368 cites W1529450221 @default.
• W2892660368 cites W1601440512 @default.
• W2892660368 cites W1623244368 @default.
• W2892660368 cites W1677082860 @default.
• W2892660368 cites W1957480474 @default.
• W2892660368 cites W1959339997 @default.
• W2892660368 cites W1963605778 @default.
• W2892660368 cites W1966675141 @default.
• W2892660368 cites W1970043986 @default.
• W2892660368 cites W1992110183 @default.
• W2892660368 cites W2007034244 @default.
• W2892660368 cites W2019433949 @default.
• W2892660368 cites W2037720427 @default.
• W2892660368 cites W2038524703 @default.
• W2892660368 cites W2038753879 @default.
• W2892660368 cites W2050480356 @default.
• W2892660368 cites W2052012325 @default.
• W2892660368 cites W2059710782 @default.
• W2892660368 cites W2064389502 @default.
• W2892660368 cites W2064546360 @default.
• W2892660368 cites W2070368152 @default.
• W2892660368 cites W2075195835 @default.
• W2892660368 cites W2081716837 @default.
• W2892660368 cites W2093292604 @default.
• W2892660368 cites W2095466982 @default.
• W2892660368 cites W2105969460 @default.
• W2892660368 cites W2108234281 @default.
• W2892660368 cites W2119204091 @default.
• W2892660368 cites W2122643628 @default.
• W2892660368 cites W2122919633 @default.
• W2892660368 cites W2130940389 @default.
• W2892660368 cites W2134526812 @default.
• W2892660368 cites W2136170412 @default.
• W2892660368 cites W2153719235 @default.
• W2892660368 cites W2160040629 @default.
• W2892660368 cites W2161613567 @default.
• W2892660368 cites W2167017590 @default.
• W2892660368 cites W2169324306 @default.
• W2892660368 cites W2169456326 @default.
• W2892660368 cites W2171251572 @default.
• W2892660368 cites W2179438025 @default.
• W2892660368 cites W2319909879 @default.
• W2892660368 cites W2337344156 @default.
• W2892660368 cites W2417690706 @default.
• W2892660368 cites W2418726670 @default.
• W2892660368 cites W2554500207 @default.
• W2892660368 cites W2591941343 @default.
• W2892660368 cites W338119623 @default.
• W2892660368 cites W4313333648 @default.
• W2892660368 doi "https://doi.org/10.1002/jcb.27718" @default.
• W2892660368 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6336507" @default.
• W2892660368 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30260027" @default.
• W2892660368 hasPublicationYear "2018" @default.
• W2892660368 type Work @default.
• W2892660368 sameAs 2892660368 @default.
• W2892660368 citedByCount "3" @default.
• W2892660368 countsByYear W28926603682020 @default.
• W2892660368 countsByYear W28926603682022 @default.
• W2892660368 crossrefType "journal-article" @default.
• W2892660368 hasAuthorship W2892660368A5004120907 @default.
• W2892660368 hasAuthorship W2892660368A5007839902 @default.
• W2892660368 hasAuthorship W2892660368A5011173907 @default.
• W2892660368 hasAuthorship W2892660368A5025814275 @default.
• W2892660368 hasAuthorship W2892660368A5056629197 @default.
• W2892660368 hasAuthorship W2892660368A5065215242 @default.
• W2892660368 hasAuthorship W2892660368A5067494403 @default.
• W2892660368 hasAuthorship W2892660368A5072123349 @default.
• W2892660368 hasAuthorship W2892660368A5084203689 @default.
• W2892660368 hasAuthorship W2892660368A5090580248 @default.
• W2892660368 hasAuthorship W2892660368A5091298095 @default.
• W2892660368 hasBestOaLocation W28926603682 @default.
• W2892660368 hasConcept C104317684 @default.
• W2892660368 hasConcept C108249834 @default.
• W2892660368 hasConcept C127561419 @default.
• W2892660368 hasConcept C136449434 @default.
• W2892660368 hasConcept C150194340 @default.
• W2892660368 hasConcept C162317418 @default.
• W2892660368 hasConcept C193419808 @default.
• W2892660368 hasConcept C203014093 @default.
• W2892660368 hasConcept C2776090121 @default.
• W2892660368 hasConcept C2776178377 @default.

• next