Effects of L-arginine on the systemic, mesenteric, and hepatic circulation of patients with cirrhosis

Kakumitsu, Shigeru; Shijo, Hiroshi; Yokoyama, M; Kim, Tetsuhiro; Akiyoshi, Nobuo; K, Ota; Kubara, Katsuhiko; Okumura, Makoto; Inoue, Kazuhide

doi:10.1097/00042737-199804000-00016

Cited by 12 publications

(17 citation statements)

References 17 publications

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“…1,[23][24][25][26][27][28][29][30][31][32][33][34][35][36][37][38][39] In these studies, ICG was used and the hepatic extraction was measured and taken into account in the calculations. The median (of the reported mean HBF in the individual studies) was 1.18 L/min (range 0.93-1.90).…”

Section: Discussionmentioning

confidence: 99%

Hepatic blood flow and splanchnic oxygen consumption in patients with liver failure. Effect of high-volume plasmapheresis

Clemmesen

Gerbes²,

Gülberg³

et al. 1999

Hepatology

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Liver failure represents a major therapeutic challenge, and yet basic pathophysiological questions about hepatic perfusion and oxygenation in this condition have been poorly investigated. In this study, hepatic blood flow (HBF) and splanchnic oxygen delivery (DO 2,sp ) and oxygen consumption (VO 2,sp ) were assessed in patients with liver failure defined as hepatic encephalopathy grade II or more. Measurements were repeated after high-volume plasmapheresis (HVP) with exchange of 8 to 10 L of plasma. HBF was estimated by use of constant infusion of D-sorbitol and calculated according to Fick's principle from peripheral artery and hepatic vein concentrations. In 14 patients with acute liver failure (ALF), HBF (1.78 ؎ 0.78 L/min) and VO 2,sp (3.9 ؎ 0.9 mmol/min) were higher than in 11 patients without liver disease (1.07 ؎ 0.19 L/min, P F .01) and (2.3 ؎ 0.7 mmol/min, P F .001). In 9 patients with acute on chronic liver disease (AOCLD), HBF (1.96 ؎ 1.19 L/min) and VO 2,sp (3.9 ؎ 2.3 mmol/min) were higher than in 18 patients with stable cirrhosis (1.00 ؎ 0.36 L/min, P F .005; and 2.0 ؎ 0.6 mmol/min, P F .005). During HVP, HBF increased from 1.67 ؎ 0.72 to 2.07 ؎ 1.11 L/min (n‫)11؍‬ in ALF, and from 1.89 ؎ 1.32 to 2.34 ؎ 1.54 L/min (n‫)7؍‬ in AOCLD, P F .05 in both cases. In patients with ALF, cardiac output (thermodilution) was unchanged (6.7 ؎ 2.5 vs. 6.6 ؎ 2.2 L/min, NS) during HVP. Blood flow was redirected to the liver as the systemic vascular resistance index increased (1,587 ؎ 650 vs. 2,020 ؎ 806 Dyne · s · cm ؊5 · m 2 , P F .01) whereas splanchnic vascular resistance was unchanged. In AOCLD, neither systemic nor splanchnic vascular resistance was affected by HVP, but as cardiac output increased from 9.1 ؎ 2.8 to 10.1 ؎ 2.9 L/min (P F .01) more blood was directed to the splanchnic region. In all liver failure patients treated with HVP (n‫,)81؍‬ DO 2,sp increased by 15% (P F .05) whereas VO 2,sp was unchanged. Endothelin-1 (ET-1) and ET-3 were determined before and after HVP. Changes of ET-1 were positively correlated with changes in HBF (P F .005) and VO 2,sp (P F .05), indicating a role for ET-1 in splanchnic circulation and oxygenation. ET-3 was negatively correlated with systemic vascular resistance index before HVP (P F .05) but changes during HVP did not correlate. Our data suggest that liver failure is associated with increased HBF and VO 2,sp . HVP further increased HBF and DO 2,sp but VO 2,sp was unchanged, indicating that splanchnic hypoxia was not present.(HEPATOLOGY 1999;29: 347-355.)A basic requirement for organ function is adequate blood flow and oxygen delivery. Hepatic blood flow (HBF) and splanchnic oxygenation in patients with liver failure (in the present study, defined as having developed hepatic encephalopathy [HE] grade II or more) have not been assessed because a method to estimate HBF in such patients has not been available until recently. 1,2 Knowledge in this field, therefore, rests on indirect evidence and animal experiments. The observation that whole-body (systemic) oxygen consumpti...

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Section: Discussionmentioning

confidence: 99%

Hepatic blood flow and splanchnic oxygen consumption in patients with liver failure. Effect of high-volume plasmapheresis

Clemmesen

Gerbes²,

Gülberg³

et al. 1999

Hepatology

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“…35,75 Moreover, invitro perfusion of cirrhotic livers with L-arginine reduces microcirculatory hyperreactivity to norepinephrine. 76 Whereas systemic application of L-arginine to patients with cirrhosis induces marked hepatic vasodilation, 77 the mechanism of these effects is not clear; perhaps reduced bioavailability of tetrahydrobiopterin (BH 4 ) leads to a "paradoxical" deficiency of L-arginine. It is assumed that there is cooperation between BH 4 and L-arginine binding sites on NOS, thereby reducing the Kd for each other.…”

Section: Increased Lipidperoxidationmentioning

confidence: 99%

The paradox of nitric oxide in cirrhosis and portal hypertension: Too much, not enough

2002

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C hronic liver diseases are often characterized by portal hypertension, an important component of which is increased intrahepatic vascular resistance (IHVR). We have long understood that structural changes, viewed by light microscopy, are largely irreversible with our current therapeutic tools. In supplementing liver histology with liver and vascular physiology, we have encountered the existence of dynamic, nonstructural components that are in fact, reversible.Bhatal et al. first showed in in-vitro perfused cirrhotic rat livers, that nitroprusside and papaverine reduced portal resistance up to 15%. This change represents up to 28% of the magnitude by which the IHVR of the cirrhotic liver exceeds that of normal livers. 1 Interestingly the magnitude of effect in the diseased liver seems to be similar for different vasodilators, whereas it is almost negligible in the normal liver. 2 This difference shows the presence of an enhanced intrinsic vascular tone in the intrahepatic microvascular bed of the cirrhotic liver that is not present in nondiseased livers.For years, nitrovasodilators were in clinical use as vasorelaxants before a mechanism of action was uncovered. Investigators identified nitric oxide (NO), an endothelium-derived relaxing factor, in 1987. 3 It is now established that NO is a key factor in the hemodynamic abnormalities associated with liver cirrhosis and chronic portal hypertension. Owing to the lack of a basement membrane and to the presence of fenestrae, sinusoidal endothelial cells are anatomically and biologically distinct from endothelial cells in other vasculature. They are, however, similar to other endothelial cells in that they produce and release NO. 4 By means of sinusoidal and other endothelial cells, the liver modulates local intrahepatic vascular tone and resistance and determines the physiological adaptation or pathophysiological dysfunction of the intrahepatic microcirculation.Under physiologic and tightly regulated conditions, nitric oxide synthases (NOS) generate NO. Alterations in the synthesis of NO, which is seen in cirrhosis, may therefore form a basis for future developments in its therapy. Furthermore, the development of optimal potential therapy is dependent on a detailed knowledge of the chemistry and metabolism of NO, and especially the diverse effects it induces. Therefore, the purpose of this review is to (1) summarize the chemical reactions in which NO participates and the effects mediated by those reactions, (2) give a short overview of the regulation of NOS, and (3) to outline the available data and current concepts regarding the involvement of NO in the hemodynamic abnormalities associated with liver cirrhosis. By no means, in this review, are we denying the participation of other mediators not only in the increased intrahepatic vascular resistance (e.g., endothelins) but also in the vasodilatation and hyperdynamic state observed in the splanchnic (e.g., anandamide) and systemic circulation (e.g., sodium and water retention). However, the focus of this review is NO.

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“…liver cirrhosis; nitric oxide; excretion SODIUM AND VOLUME RETENTION is a common problem in patients with liver cirrhosis (33, 34). Neurohumoral vasoconstrictors but also the production of a vasodilator like nitric oxide are considerably activated (16,21,22,27,29,31,42).Inhibition of the sympathetic nervous system (1, 35) or angiotensin II in patients (30, 38) or animal models (10,14,20) could improve sodium and water excretion transiently, although possible decreases in blood pressure or renal perfusion could eventually worsen volume homeostasis instead of improving it (1, 8, 9). …”

mentioning

confidence: 99%

mentioning

confidence: 99%

Effects of sympathetic nerves and angiotensin II on renal sodium and water handling in rats with common bile duct ligature

Veelken¹,

Hilgers²,

Porst³

et al. 2005

American Journal of Physiology-Renal Physiology

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. Effects of sympathetic nerves and angiotensin II on renal sodium and water handling in rats with common bile duct ligature. Am J Physiol Renal Physiol 288: F1267-F1275, 2005. First published February 8, 2005 doi:10.1152/ajprenal.00069.2003.-We tested the hypothesis that angiotensin II is likely to be mandatory for the neurogenic sodium and volume retention in cirrhotic rats with common bile duct ligature (BDL) following an acute volume load. To assess the neural control of volume homeostasis, 21 days after common BDL rats underwent volume expansion (0.9% NaCL; 10% body wt over 30 min) to decrease renal sympathetic nerve activity. Untreated animals, rats with renal denervation or pretreated with a nonhypotensive dose of an angiotensin II type 1 receptor antagonist were studied. The renal renin-angiotensin system was assessed by immunohistochemistry and RT-PCR. Rats with BDL excreted only 71 Ϯ 4% of the administered volume load. In cirrhotic rats pretreated with an angiotensin II AT1 inhibitor or after renal denervation, these values ranged significantly higher from 98 to 103% (P Ͻ 0.05 for all comparisons). Renal sympathetic nerve activity decreases by volume expansion were impaired in BDL rats (P Ͻ 0.05) but unaffected by angiotensin II receptor inhibition. In kidneys of BDL animals, renin mRNA was increased, and immunohistochemistry revealed increased staining for peritubular angiotensin II. Renal denervation in BDL animals reduced renin expression within 5 days to control levels. In conclusion, the impaired excretion of an acute volume load in rats with liver cirrhosis is due to effects of an increased renal sympathetic nerve activity that are likely to be dependent on intrarenal angiotensin II and renin. We speculate that similar changes may contribute to long-term volume retention in liver cirrhosis. liver cirrhosis; nitric oxide; excretion SODIUM AND VOLUME RETENTION is a common problem in patients with liver cirrhosis (33, 34). Neurohumoral vasoconstrictors but also the production of a vasodilator like nitric oxide are considerably activated (16,21,22,27,29,31,42).Inhibition of the sympathetic nervous system (1, 35) or angiotensin II in patients (30, 38) or animal models (10,14,20) could improve sodium and water excretion transiently, although possible decreases in blood pressure or renal perfusion could eventually worsen volume homeostasis instead of improving it (1, 8, 9).We could demonstrate in rats that the effects of increased renal sympathetic nerve activity (RSNA) on renal sodium and water excretion could be inhibited by very low doses of an angiotensin II AT 1 receptor inhibitor not interfering with systemic angiotensin II effects or renal hemodynamics (39). These results suggested a tonic, indispensable influence of angiotensin II on the intrarenal effects of increased sympathetic drive. With respect to liver cirrhosis, these findings suggest the possibility that renal sodium and water handling could be improved by inducing a functional renal sympathetic inhibition with angiotensin II AT 1 rec...

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Effects of L-arginine on the systemic, mesenteric, and hepatic circulation of patients with cirrhosis

Cited by 12 publications

References 17 publications

Hepatic blood flow and splanchnic oxygen consumption in patients with liver failure. Effect of high-volume plasmapheresis

Hepatic blood flow and splanchnic oxygen consumption in patients with liver failure. Effect of high-volume plasmapheresis

The paradox of nitric oxide in cirrhosis and portal hypertension: Too much, not enough

Effects of sympathetic nerves and angiotensin II on renal sodium and water handling in rats with common bile duct ligature

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