Renal Microvascular Responses to Sepsis Are Dependent on Nitric Oxide

Nitric oxide (NO) is an important mediator of the hemodynamic response to sepsis; however, its visceral microcirculatory effects are largely unknown. To determine the role of NO in renal microvascular responses to bacteremia, rat hydronephrotic kidneys with intact neurovascular supplies were exterio...

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Veröffentlicht in:The Journal of surgical research 1994-06, Vol.56 (6), p.524-529
Hauptverfasser: Spain, David A., Wilson, Mark A., Bloom, Ian T.M., Garrison, R.Neal
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Sprache:eng
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Zusammenfassung:Nitric oxide (NO) is an important mediator of the hemodynamic response to sepsis; however, its visceral microcirculatory effects are largely unknown. To determine the role of NO in renal microvascular responses to bacteremia, rat hydronephrotic kidneys with intact neurovascular supplies were exteriorized into a tissue bath. Videomicroscopy was used to measure vessel diameters (interlobular artery, ILA; afferent arteriole, AFF; efferent arteriole, EFF) and optical Doppler velocimetry was used to quantitate ILA flow. In controls, topical l-arginine (l-Arg; 104M), the NO synthase (NO-S) substrate, resulted in mild pre- and postglomerular dilation and increased flow. Inhibition of NO-S by Nω-nitro-l-arginine methyl ester (lNAME; 10-4M) caused preglomerular constriction (ILA = -22%; AFF = -20% from baseline) and reduced ILA flow by 39%, while postglomerular diameters (EFF) were unchanged. Bacteremic rats had similar alterations (ILA = -22%; AFF = -20%; flow = -56%). Topical l -NAME in bacteremic rats resulted in further constriction (ILA = -38%; AFF -37%), decreased ILA flow (-75%) and constricted EFF (-30%). l-Arg ameliorated constriction (ILA = -11%; AFF = -7%) and flow (-34%) during bacteremia. We conclude that: (1) NO is important in basal preglomerular tone; (2) Escherichia coli causes selective preglomerular constriction and hypoperfusion; (3) maintenance of EFF tone during bacteremia is NO dependent; and (4) different pre- and postglomerular NO mechanisms exist during basal and bacteremic states. These data indicate that NO is an important mediator of renal microvascular responses to sepsis.
ISSN:0022-4804
1095-8673
DOI:10.1006/jsre.1994.1084