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A novel chemically modified curcumin reduces severity of experimental periodontal disease in rats: Initial observations

  • Muna S. Elburki
  • , Carlos Rossa
  • , Morgana R. Guimaraes
  • , Mark Goodenough
  • , Hsi Ming Lee
  • , Fabiana A. Curylofo
  • , Yu Zhang
  • , Francis Johnson
  • , Lorne M. Golub
  • Stony Brook University
  • Universidade Estadual Paulista Júlio de Mesquita Filho

Research output: Contribution to journalArticlepeer-review

57 Scopus citations

Abstract

Tetracycline-based matrix metalloproteinase- (MMP-) inhibitors are currently approved for two inflammatory diseases, periodontitis and rosacea. The current study addresses the therapeutic potential of a novel pleiotropic MMP-inhibitor not based on an antibiotic. To induce experimental periodontitis, endotoxin (LPS) was repeatedly injected into the gingiva of rats on one side of the maxilla; the contralateral (control) side received saline injections. Two groups of rats were treated by daily oral intubation with a chemically modified curcumin, CMC 2.24, for two weeks; the control groups received vehicle alone. After sacrifice, gingiva, blood, and maxilla were collected, the jaws were defleshed, and periodontal (alveolar) bone loss was quantified morphometrically and by -CT scan. The gingivae were pooled per experimental group, extracted, and analyzed for MMPs (gelatin zymography; western blot) and for cytokines (e.g., IL-1β; ELISA); serum and plasma samples were analyzed for cytokines and MMP-8. The LPS-induced pathologically excessive bone loss was reduced to normal levels based on either morphometric (P = 0.003) or -CT (P = 0.008) analysis. A similar response was seen for MMPs and cytokines in the gingiva and blood. This initial study, on a novel triketonic zinc-binding CMC, indicates potential efficacy on inflammatory mediators and alveolar bone loss in experimental periodontitis and warrants future therapeutic and pharmacokinetic investigations.

Original languageEnglish
Article number959471
JournalMediators of Inflammation
Volume2014
DOIs
StatePublished - 2014

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