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An Eco‐Friendly Enantioselective Access to (R)‐Naringenin as Inhibitor of Proinflammatory Cytokine Release
Authors:Raffaella Gaggeri  Daniela Rossi  Maria Daglia  Flavio Leoni  Maria Antonia Avanzini  Melissa Mantelli  Markus Juza  Simona Collina
Institution:1. Department of Drug Sciences, University of Pavia, Viale Taramelli 12, I‐27100 Pavia, (phone: +39‐0382987379;2. fax: +39‐0382422975);3. Italfarmaco Research Center, Viale dei Lavoratori 54, I‐20092 Cinisello Balsamo (MI);4. Pediatric Haematology/Oncology Department, Fondazione IRCCS Policlinico San Matteo, Piazzale Golgi 19, I‐27100 Pavia;5. Analytical Development SIL, DSM Nutritional Products, Hauptstrasse 4, CH‐4334 Sisseln
Abstract:(RS)‐Naringenin is a flavanone well‐known for its beneficial health‐related properties, such as its anti‐inflammatory activity. The preparative enantioselective chromatographic resolution of commercial (RS)‐naringenin was performed on a Chiralpak AD‐H column (500×50 mm i.d., dp 20 μm) using MeOH as eluent. The developed method is in accordance with the principles of green chemistry, since the environmental impact was lowered by recycling of the eluent, and allowed the production of gram amounts of each enantiomer with high purity (chemical purity >99%, enantiomeric excess (ee) >94%). Racemic and enantiomeric naringenin were subjected to an exhaustive in vitro investigation of anti‐inflammatory activity, aimed at evaluating the relevance of chirality. The assay with cultured human peripheral blood mononuclear cells (hPBMC) activated by phytohemagglutinin A revealed that (R)‐naringenin was more effective in inhibiting T‐cell proliferation than the (S)‐enantiomer and the racemate. Moreover, (R)‐naringenin significantly reduced proinflammatory cytokine levels such as those of TNF‐α and, with less potency, IL‐6. These results evidenced the anti‐inflammatory potential of naringenin and the higher capacity of (R)‐naringenin to inhibit both in vitro hPBMC proliferation and cytokine secretion at non toxic doses. Thus, (R)‐naringenin is a promising candidate for in vivo investigation.
Keywords:Naringenin  T‐Cell proliferation  Anti‐inflammatory activity  Cytokines  Inhibitors
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