FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2888287252> ?p ?o ?g. }

• W2888287252 abstract "pH-sensing ovarian cancer G-protein coupled receptor-1 [OGR1/GPR68] is regulated by key inflammatory cytokines. Patients suffering from inflammatory bowel diseases [IBDs] express increased mucosal levels of OGR1 compared with non-IBD controls. pH-sensing may be relevant for progression of fibrosis, as extracellular acidification leads to fibroblast activation and extracellular matrix remodelling. We aimed to determine OGR1 expression in fibrotic lesions in the intestine of Crohn's disease [CD] patients, and the effect of Ogr1 deficiency in fibrogenesis.Human fibrotic and non-fibrotic terminal ileum was obtained from CD patients undergoing ileocaecal resection due to stenosis. Gene expression of fibrosis markers and pH-sensing receptors was analysed. For the initiation of fibrosis in vivo, spontaneous colitis by Il10-/-, dextran sodium sulfate [DSS]-induced chronic colitis and the heterotopic intestinal transplantation model were used.Increased expression of fibrosis markers was accompanied by an increase in OGR1 [2.71 ± 0.69 vs 1.18 ± 0.03, p = 0.016] in fibrosis-affected human terminal ileum, compared with the non-fibrotic resection margin. Positive correlation between OGR1 expression and pro-fibrotic cytokines [TGFB1 and CTGF] and pro-collagens was observed. The heterotopic animal model for intestinal fibrosis transplanted with terminal ileum from Ogr1-/- mice showed a decrease in mRNA expression of fibrosis markers as well as a decrease in collagen layer thickness and hydroxyproline compared with grafts from wild-type mice.OGR1 expression was correlated with increased expression levels of pro-fibrotic genes and collagen deposition. Ogr1 deficiency was associated with a decrease in fibrosis formation. Targeting OGR1 may be a potential new treatment option for IBD-associated fibrosis." @default.
• W2888287252 created "2018-08-31" @default.
• W2888287252 creator A5001161369 @default.
• W2888287252 creator A5021707048 @default.
• W2888287252 creator A5025638340 @default.
• W2888287252 creator A5030179327 @default.
• W2888287252 creator A5036076144 @default.
• W2888287252 creator A5043492127 @default.
• W2888287252 creator A5044140711 @default.
• W2888287252 creator A5047989406 @default.
• W2888287252 creator A5051900976 @default.
• W2888287252 creator A5053616350 @default.
• W2888287252 creator A5054681942 @default.
• W2888287252 creator A5055934398 @default.
• W2888287252 creator A5058012401 @default.
• W2888287252 creator A5060763473 @default.
• W2888287252 creator A5061091984 @default.
• W2888287252 creator A5065186874 @default.
• W2888287252 creator A5068944242 @default.
• W2888287252 creator A5072937673 @default.
• W2888287252 creator A5075032392 @default.
• W2888287252 date "2018-08-25" @default.
• W2888287252 modified "2023-10-05" @default.
• W2888287252 title "Intestinal Activation of pH-Sensing Receptor OGR1 [GPR68] Contributes to Fibrogenesis" @default.
• W2888287252 cites W1483147211 @default.
• W2888287252 cites W1698593587 @default.
• W2888287252 cites W1717123962 @default.
• W2888287252 cites W1963625450 @default.
• W2888287252 cites W1970613671 @default.
• W2888287252 cites W1973397356 @default.
• W2888287252 cites W1981461721 @default.
• W2888287252 cites W1982910988 @default.
• W2888287252 cites W1984119315 @default.
• W2888287252 cites W1984438195 @default.
• W2888287252 cites W1987778106 @default.
• W2888287252 cites W1989738331 @default.
• W2888287252 cites W1991189920 @default.
• W2888287252 cites W1996406504 @default.
• W2888287252 cites W2013396535 @default.
• W2888287252 cites W2016553429 @default.
• W2888287252 cites W2019851250 @default.
• W2888287252 cites W2028402416 @default.
• W2888287252 cites W2044618021 @default.
• W2888287252 cites W2045402066 @default.
• W2888287252 cites W2049251840 @default.
• W2888287252 cites W2052412395 @default.
• W2888287252 cites W2055769271 @default.
• W2888287252 cites W2069770196 @default.
• W2888287252 cites W2073244778 @default.
• W2888287252 cites W2084074153 @default.
• W2888287252 cites W2086514236 @default.
• W2888287252 cites W2087226541 @default.
• W2888287252 cites W2090438940 @default.
• W2888287252 cites W2093597086 @default.
• W2888287252 cites W2094443518 @default.
• W2888287252 cites W2098733700 @default.
• W2888287252 cites W2106779017 @default.
• W2888287252 cites W2110499503 @default.
• W2888287252 cites W2111880004 @default.
• W2888287252 cites W2113053279 @default.
• W2888287252 cites W2113690494 @default.
• W2888287252 cites W2115865518 @default.
• W2888287252 cites W2118197004 @default.
• W2888287252 cites W2130922818 @default.
• W2888287252 cites W2143625465 @default.
• W2888287252 cites W2152780883 @default.
• W2888287252 cites W2160911117 @default.
• W2888287252 cites W2165581505 @default.
• W2888287252 cites W2170713735 @default.
• W2888287252 cites W2171694485 @default.
• W2888287252 cites W2177537276 @default.
• W2888287252 cites W2181898446 @default.
• W2888287252 cites W2261798779 @default.
• W2888287252 cites W229017931 @default.
• W2888287252 cites W2324795120 @default.
• W2888287252 cites W2418087799 @default.
• W2888287252 cites W2465126356 @default.
• W2888287252 cites W2529401211 @default.
• W2888287252 cites W2610753795 @default.
• W2888287252 cites W2749443843 @default.
• W2888287252 cites W2767709479 @default.
• W2888287252 doi "https://doi.org/10.1093/ecco-jcc/jjy118" @default.
• W2888287252 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30165600" @default.
• W2888287252 hasPublicationYear "2018" @default.
• W2888287252 type Work @default.
• W2888287252 sameAs 2888287252 @default.
• W2888287252 citedByCount "21" @default.
• W2888287252 countsByYear W28882872522019 @default.
• W2888287252 countsByYear W28882872522020 @default.
• W2888287252 countsByYear W28882872522021 @default.
• W2888287252 countsByYear W28882872522022 @default.
• W2888287252 countsByYear W28882872522023 @default.
• W2888287252 crossrefType "journal-article" @default.
• W2888287252 hasAuthorship W2888287252A5001161369 @default.
• W2888287252 hasAuthorship W2888287252A5021707048 @default.
• W2888287252 hasAuthorship W2888287252A5025638340 @default.
• W2888287252 hasAuthorship W2888287252A5030179327 @default.
• W2888287252 hasAuthorship W2888287252A5036076144 @default.
• W2888287252 hasAuthorship W2888287252A5043492127 @default.
• W2888287252 hasAuthorship W2888287252A5044140711 @default.

• next