IMMUNE NETWORK

  • 제3권1호
  • /
  • Pages.69-77
  • /
  • 2003
  • /
  • 1598-2629(pISSN)
  • /
  • 2092-6685(eISSN)
대한면역학회 (The Korean Association of Immunobiologists)
권호 표지

Cyclooxygenase-2 Specific Inhibitor (SC-58635)가 Lipopolysaccharide로 자극한 대식세포에서 Nitric Oxide와 Prostaglandin E2 생산에 미치는 영향

Effect of Cyclooxygenase-2 Specific Inhibitor (SC-58635) on the Production of Nitric Oxide and Prostaglandin E2 in Lipopolysaccharide-stimulated Macrophage Cells

  • 홍승재 (경희대학교 의과대학 내과학교실) ;
  • 양형인 (경희대학교 의과대학 내과학교실) ;
  • 윤휘중 (경희대학교 의과대학 내과학교실) ;
  • 이명수 (원광대학교 의과대학 내과학교실) ;
  • 강효종 (분당제생병원 내과) ;
  • 김완욱 (가톨릭대학교 의과대학 내과학교실) ;
  • 이상헌 (가톨릭대학교 의과대학 내과학교실) ;
  • 조철수 (가톨릭대학교 의과대학 내과학교실) ;
  • 김호연 (가톨릭대학교 의과대학 내과학교실)
  • Hong, Seung-Jae (Department of Internal Medicine, Kyung-Hee University Medical College) ;
  • Yang, Hyung-In (Department of Internal Medicine, Kyung-Hee University Medical College) ;
  • Yoon, Hwi-Joong (Department of Internal Medicine, Kyung-Hee University Medical College) ;
  • Lee, Myoung-Soo (Department of Internal Medicine, Won-Kwang University Medical College) ;
  • Kang, Hyo-Jong (Department of Internal Medicine, Daejin Medical Center) ;
  • Kim, Wan-Uk (Department of Internal Medicine, Catholic University Medical College) ;
  • Lee, Sang-Heon (Department of Internal Medicine, Catholic University Medical College) ;
  • Cho, Chul-Soo (Department of Internal Medicine, Catholic University Medical College) ;
  • Kim, Ho-Youn (Department of Internal Medicine, Catholic University Medical College)
  • 발행 : 2003.03.30
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초록

Background: Celecoxib, a COX-2 specific inhibitor, has recently been used for the treatment of rheumatoid arthritis. However, the molecular and cellular mechanisms of celecoxib against RA inflammation remain to be defined. To elucidate the action mechanism of celecoxib on inflammatory cells, we investigated the effect of celecoxib on the production of two important mediators of inflammation, nitric oxide and PGE2 Methods: RAW 264.7 cells stimulated with LPS were preincubated with various concentrations of celecoxib (from $10^{-8}$ to $10^{-5}$ M) and $10{\mu}M$ hydrocortisone, respectively. The production of NO and PGE2, the end products of iNOS and COX-2 genes, were estimated in culture supernatants by Greiss method and EIA, respectively. The expression of iNOS gene, COX-2 gene, $NF-{\kappa}B$, and $I-{\kappa}B$ were determined by RT-PCR and western blot analysis. Results: Celecoxib and hydrocortisone inhibited the production of NO and PGE2 in dose dependent manner, when RAW 264.7 cells were stimulated with LPS. The expression of iNOS was also down-regulated by celecoxib and hydrocortisone. Interestingly, COX-2 gene differentially expressed according to the dose of celecoxib, a decrease with lower dose ($10^{-8}$ M) but an increase with higher dose ($10^{-5}$ M). $NF-{\kappa}B$ binding activity was decreased by lower dose of celecoxib, whereas was not affected by higher dose of it. The expression of $I-{\kappa}B$ was suppressed by higher dose of celecoxib. Conclusion: The celecoxib strongly suppressed the production of NO and PGE2 in LPS-stimulated RAW264.7 cells. The decrease of NO seems to be linked to the inhibition of iNOS by celecoxib. The lower and higher dose of celecoxib differentially regulated the COX-2 expression and $NF-{\kappa}B$ activity.

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