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1 Department of Pharmacology and 2 Graduate Institute of Life Sciences, National Defense Medical Center, Taipei, Taiwan, Republic of China
We investigated
whether a complete inhibition of nitric oxide (NO) formation caused by
bacterial endotoxin (lipopolysaccharide, LPS) in vivo prevents the
hypotension and restores the vascular hyporeactivity to normal in vivo
and ex vivo. The combination of dexamethasone (Dex; 3 mg/kg at 30 min
before LPS) plus aminoguanidine (AG; 15 mg/kg at 2 h after LPS)
inhibited the overproduction of nitrate (an indicator of NO) in the
plasma and aortic smooth muscle and also prevented the development of
the delayed hypotension in rats treated with LPS for 6 h. However, the
vascular hyporeactivity to norepinephrine (NE) was only partially
improved either in vivo or ex vivo in endotoxemic rats treated with Dex
plus AG. Pretreatment of aortic rings with
N
-nitro-L-arginine
methyl ester (L-NAME) or
1H-[1,2,4]oxidazolo[4,3-a]quinoxalin-1-one (ODQ) enhanced the contraction to NE in rings obtained from LPS-treated rats, but not in those from Dex plus AG-treated endotoxemic rats. Methylene blue, an inhibitor of soluble guanylyl cyclase (GC), completely restored contractions to NE and aortic cGMP levels to normal
either in LPS-treated rats or in Dex plus AG-treated endotoxemic rats,
whereas the cGMP level was partially inhibited by ODQ in LPS-treated
rats only. These results suggest that non-NO mediator(s) also activates
soluble GC during endotoxemia. Interestingly, we found that in the
presence of tetraethylammonium (an inhibitor of
K+ channels) plus
L-NAME or charybdotoxin [a
specific inhibitor of large-conductance
Ca2+-activated
K+
(KCa) channels] plus ODQ,
the vascular hyporeactivity to NE in the LPS-treated group was also
completely restored to normal. In addition, in the presence of
L-NAME or ODQ, the vascular
hyporeactivity to high K+ was
abolished in rings from the LPS-treated group. These results suggest
that LPS causes the production of other mediator(s), in addition to NO,
which also stimulates soluble GC (i.e., increases the formation of
cGMP) and then activates the large-conductance KCa channels in the vascular
smooth muscle causing vascular hyporeactivity.
lipopolysaccharide; dexamethasone; aminoguanidine; calcium-activated potassium channels; rat thoracic aortas
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