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Selective inhibition of the inducible nitric oxide synthase by aminoguanidine
Thomas P. Misko ,
William M. Moore ,
Thomas P. Kasten ,
G.Allen Nickols ,
John A. Corbett ,
Ronald G. Tilton ,
Michael L. McDaniel ,
Joseph R. Williamson ,
Mark G. Currie
March 1993
March 1993
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Abstract
Overproduction of the free radical nitric oxide (NO) has been implicated in the pathogenesis
of a variety of inflammatory and immunologically mediated diseases as well as complications
of diabetes. In the present study we have demonstrated that aminoguanidine selectively
inhibits the cytokine-inducible isoform of NO synthase which appears to be responsible
for the excess production of NO linked to these disease states. By using organ, cell,
and enzyme-based measurements we have shown that aminoguanidine is equipotent to NG-monomethyl-L-arginine
(L-NMA) as an inhibitor of the cytokine-induced isoform of NO synthase but is 10 to
100-fold less potent as an inhibitor of the constitutive isoform. Thus, aminoguanidine
may be useful as a selective inhibitor of the inducible NO synthase in the treatment
of disease states characterized by the pathological overproduction of NO.