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• W2897075263 abstract "Prostaglandin E 2 (PGE 2 ) signaling is known to modulate inflammation and vascular resistance. Receptors of PGE 2 [E-type prostanoid receptors (EP)] might be an attractive pharmacological target in immune-mediated diseases such as glomerulonephritis. We hypothesized that selective EP4 antagonism improves nephrotoxic serum nephritis (NTS) by its anti-inflammatory properties. Mice were subjected to NTS and treated with the EP4 antagonist ONO AE3-208 (10 mg·kg body wt −1 ·day −1 ] or vehicle starting from disease initiation. In one set of experiments, treatment was started 4 days after NTS induction. Tubular epithelial cells were evaluated in vitro under starving conditions. EP4 antagonist treatment significantly improved the NTS phenotype without affecting blood pressure levels. Remarkably, the improved NTS phenotype was also observed when treatment was started 4 days after NTS induction. EP4 antagonism decreased tubular chemokine (C-X-C motif) ligand ( Cxcl) 1 and Cxcl-5 expression and thereby subsequently reduced interstitial neutrophil infiltration into the kidney. In vitro, tubular epithelial cells increasingly expressed Cxcl-5 mRNA and Cxcl-5 protein when treated with PGE 2 or an EP4 agonist under starving conditions, which was blunted by EP4 antagonist treatment. Together, EP4 antagonism improves the NTS phenotype, probably by decreasing mainly Cxcl-5 production in tubular cells, thereby reducing renal neutrophil infiltration." @default.
• W2897075263 created "2018-10-26" @default.
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• W2897075263 date "2018-12-01" @default.
• W2897075263 modified "2023-10-17" @default.
• W2897075263 title "Blockade of prostaglandin E₂ receptor 4 ameliorates nephrotoxic serum nephritis" @default.
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• W2897075263 doi "https://doi.org/10.1152/ajprenal.00113.2018" @default.
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