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and
IFN-
1 Division of Nephrology-Hypertension and 2 Program in Molecular Pathology, Department of Medicine, University of California, San Diego, and Veterans Affairs Medical Center, La Jolla, California 92161
Nitric oxide (NO)
has been described to exert cytostatic effects on cellular
proliferation; however the mechanisms responsible for these effects
have yet to be fully resolved. Polyamines, conversely, are required
components of cellular proliferation. In experimental models of
inflammation, a relationship between these two pathways has been
suggested by the temporal regulation of a common precursor, arginine.
This study was undertaken to determine the effects NO and the NO
synthase (NOS)-inducing cytokines, tumor necrosis factor-
(TNF-)
and interferon-
(IFN-), exert on polyamine regulation. The
transformed kidney proximal tubule cell line, MCT, maintains high
constitutive levels of the first polyamine biosynthetic enzyme, ornithine decarboxylase (ODC). NO donors markedly suppressed ODC activity in MCT and all other cell lines examined. TNF- and IFN- induction of NO generation resulted in suppressed ODC activity, an
effect prevented by the inducible NOS inhibitor
L-N6-(1-iminoethyl)lysine
(L-NIL). Dithiothreitol reversal
of NO-mediated ODC suppression supports nitrosylation as the mechanism
of inactivation. We also evaluated polyamine uptake, inasmuch as
inhibition of ODC can result in a compensatory induction of polyamine
transporters. Administration of NO donors, or TNF- and IFN-,
suppressed
[3H]putrescine uptake,
thereby preventing transport-mediated reestablishment of intracellular
polyamine levels. This study demonstrates the capacity of NO and
inflammatory cytokines to regulate both polyamine biosynthesis and transport.
antizyme; inflammation; nitrosylation; ornithine decarboxylase; proliferation; tumor necrosis factor-; interferon-
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