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Vol. 284, Issue 2, 722-727, February 1998
Department of Molecular and Cellular Physiology, LSU Medical
Center, Shreveport, Louisiana
The objective of this study was to determine the effects that certain
nitric oxide synthase inhibitors have on the spontaneous intestinal and
colonic inflammation that develops in HLA-B27 transgenic rats and
compare these data to those obtained using sulfasalazine (SZ). In an
attempt to more closely mimic the clinical situation, drug treatment
was begun after the onset of colitis. HLA-B27 male rats that developed
clinical signs of colitis (diarrhea/loose stools) at 17 wk of age were
randomized into fours groups consisting of one untreated colitic group
and three treatment groups that received either aminoguanidine (AG; 52 µmol/kg/day), NG-nitro-L-arginine methyl
ester (L-NAME; 45 µmol/kg/day) or SZ (130 mg/kg/day) in their
drinking water for 14 days. Aged-matched Fisher 344 male rats were used
as healthy controls. After 3 wk of treatment, ileal and colonic mucosal
permeabilities, granulocyte infiltration and nitric oxide were
quantified using blood-to-lumen clearance of 51Cr-EDTA,
tissue myeloperoxidase activity, and plasma levels of nitrate and
nitrite, respectively. We found that both AG and L-NAME but not SZ
significantly attenuated the increases in plasma nitrate and nitrite
levels. Interestingly, all three drugs were effective at significantly
attenuating the increases in myeloperoxidase activity in the distal
colon. Treatment with AG and SZ but not L-NAME were effective at
significantly attenuating the increase in ileal and colonic
permeabilities. Quantitative histological analysis revealed that AG and
L-NAME but not SZ significantly attenuated the increase in the mucosal
thickness and crypt depth in the distal colon compared to untreated
colitis. Taken together, these data demonstrate that oral
administration of certain nitric oxide synthase inhibitors or SZ to
animals with active colitis attenuates the colonic inflammation by at
least two different mechanisms. One mechanism appears to be dependent
on inhibition of NO production whereas the other mechanism does not.
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  S. W. Kerr, W. W. Wolyniec, Z. Filipovic, S. G. Nodop, F. Braza, R. J. Winquist, and T. C. Noonan Repeated Measurement of Intestinal Permeability as an Assessment of Colitis Severity in HLA-B27 Transgenic Rats J. Pharmacol. Exp. Ther., November 1, 1999; 291(2): 903 - 910. [Abstract] [Full Text]
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 S. Kawachi, A. Cockrell, F. S. Laroux, L. Gray, D. N. Granger, H. C. van der Heyde, and M. B. Grisham Role of inducible nitric oxide synthase in the regulation of VCAM-1 expression in gut inflammation Am J Physiol Gastrointest Liver Physiol, September 1, 1999; 277(3): G572 - G576. [Abstract] [Full Text] [PDF]
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