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Vol. 303, Issue 1, 52-57, October 2002
Central Research Laboratories, SSP Co., Ltd., Chiba, Japan (M.O.,
F.K., H.Ho., T.O., M.I., N.I., K.I., F.I., S.S.), and Department of
Molecular Biology, Toho University School of Medicine, Tokyo, Japan
(H.He.)
Nitric oxide (NO) plays an important role in various physiological
processes. Excessive NO production is closely related to inflammatory
and autoimmune diseases such as septic shock and rheumatoid arthritis.
Suppression of excess NO formation in participating cells may be
helpful in improving disease status. In this study, we examined the
effects of a newly synthesized imidazole derivative, 3-(2,4-difluorophenyl)-6-{2-[4-(1H-imidazol-1-ylmethyl)
phenoxy]ethoxy}-2-phenylpyridine (PPA250), on NO production in vitro
and in vivo, as well as on the dimerization of inducible nitric-oxide
synthase (iNOS). PPA250 at concentrations of 25 nM and higher
inhibited NO production in activated mouse macrophage-like RAW264.7
cells. The IC50 was approximately 82 nM. Western blot
analysis revealed that PPA250 prevents dimerization of iNOS but has no
effect on transcription and translation. In addition, oral
administration of PPA250 (10 mg/kg and higher) reduced the NO
concentration in serum from mice in which sepsis was induced by
bacterial lipopolysaccharide. Since the inhibitory activity was
observed not only in vitro but also in vivo, we examined the
therapeutic potential of PPA250 in two animal models of arthritis,
collagen-induced arthritis in mice and adjuvant arthritis in rats.
PPA250 suppressed the development of a destructive polyarthritis in
both models after the appearance of clinical signs. These results
indicate that inhibitors of iNOS homodimerization, including PPA250,
could be useful therapeutic agents for inflammatory and autoimmune
diseases, such as rheumatoid arthritis, in which NO is involved.
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