Hepatic arterial perfusion decreases intrahepatic shunting and maintains glucose uptake in the rat liver

Berndt, Alexander; Rogers, Camilla; Naftalin, Richard J

doi:10.1007/s00424-002-0815-z

Cited by 9 publications

(8 citation statements)

References 43 publications

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“…This indicates that the main site of confluence of the hepatic artery with the portal vein is intrasinusoidal, in zone II, thus substantiating earlier work. 13 If this were presinusoidal, microspheres should reduce hepatic arterial sorbitol uptake to the same extent as portal venous sorbitol uptake and this did not happen. Haemodynamic observations showed a limited reduction in hepatic arterial blood flow after microsphere injection, possibly secondary to the decreased mean arterial pressure.…”

Section: Discussionmentioning

confidence: 99%

“…This indicates that the main site of confluence of the hepatic artery with the portal vein is intrasinusoidal, in zone II, thus substantiating earlier work. 13 If this Figure 7 Illustration of the relationship between intrahepatic shunts, hepatic sorbitol uptake, and microsphere induced presinusoidal occlusion in the normal rat liver. (A) Under normal conditions, portal blood flows through the sinusoids with extremely low resistance.…”

Section: Discussionmentioning

confidence: 99%

“…7 We have demonstrated the existence of intrahepatic shunts, with diameters of up to 80-90 µm, in the normal rat liver using conventional physiological indices 8 9 and have confirmed their existence in the dual perfused normal rat liver using glucose uptake measurements where intrahepatic portal blockade by microspheres significantly increased intrahepatic shunting, as indicated by the reduced portal venous uptake of glucose but retained bromosulphthalein (BSP) uptake. [10][11][12][13] Further in vivo studies of intrahepatic shunting have been hindered by the lack of a reliable technique to measure functional hepatic blood flow and intrahepatic shunt flow. Radioactive microsphere techniques measure the shunt fraction by recording pulmonary recovery of microspheres usually injected intraportally.…”

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Location and function of intrahepatic shunts in anaesthetised rats

Benjamin²,

Naftalin³

et al. 2003

Gut

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Background: In the present study we determined the proportion of shunt flow due to patent intrahepatic portal systemic shunts in the normal rat liver and its relationship with microsphere induced portal hypertension. Methods: Systemic and hepatic haemodynamics were measured continuously before, during, and after intraportal injection of 15 µm diameter microspheres in anaesthetised male Wistar rats. Functional hepatic blood flow and intrahepatic shunt flow were determined by the use of constant intraportal infusion of sorbitol and simultaneous measurements in the portal vein, hepatic vein, and carotid artery. The percentage of large shunts of diameter >15 µm were estimated by intraportal injection of 51 Cr labelled 15 µm diameter microspheres. Results: Hepatic sorbitol uptake was 97.9 (0.5)% in normal control rats, with functional hepatic blood flow equalling total hepatic blood flow (2.52 (0.23) ml/min/100 g body weight). Microsphere injection decreased sorbitol uptake to 12.8 (4.3)% and further to 4.1 (0.7)% when followed by hepatic arterial ligation. In the latter two groups, intrahepatic shunt flow (1.46 (0.15) and 1.16 (0.19) ml/min/100 g body weight, respectively) was not significantly different from portal venous flow (1.36 (0.20) and 1.20 (0.20) ml/min/100 g body weight, respectively). Portal venous flow remained at 70% of basal values and portal venous pressure only increased by 50% from baseline. 51 Cr labelled microsphere shunt fraction through large shunts (>15 µm) was less than 1.0%. Conclusion: The site of confluence between the hepatic artery and portal vein is in zone II. Intrahepatic shunts originate in presinusoidal regions in zone I in the normal liver and, when activated by intraportal injection of microspheres, divert 70% of the total portal blood flow away from zone III and thereby reduce acute increases in portal venous pressure.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Location and function of intrahepatic shunts in anaesthetised rats

Benjamin²,

Naftalin³

et al. 2003

Gut

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“…No studies have been done with gradients as large as Ϫ163 mg/dl, however, so a bell-shaped response remains possible. A second likely explanation for the blunting of the response to the portal signal in the HAL po dogs may lie in the importance of the hepatic artery in regulation of hepatic circulation (4,5). It has been proposed that the architecture of the liver allows shunting of portal vein blood away from the areas of hepatic glucose uptake (zone III), and the presence of hepatic artery flow decreases intrahepatic shunting and thus stimulates glucose uptake (5).…”

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confidence: 99%

“…A second likely explanation for the blunting of the response to the portal signal in the HAL po dogs may lie in the importance of the hepatic artery in regulation of hepatic circulation (4,5). It has been proposed that the architecture of the liver allows shunting of portal vein blood away from the areas of hepatic glucose uptake (zone III), and the presence of hepatic artery flow decreases intrahepatic shunting and thus stimulates glucose uptake (5). Nevertheless, the fact that the HAL dogs responded qualitatively, even if not completely quantitatively, to both peripheral and portal glucose infusion implies that redundant sensing sites are normally operational or that chronic adaptation to the loss of the hepatic artery allowed other sensing sites to become evident, even though the redundant site or sites may not be as effective as the intrahepatic site.…”

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Chronic hepatic artery ligation does not prevent liver from differentiating portal vs. peripheral glucose delivery

Moore

Burish

Farmer

et al. 2003

American Journal of Physiology-Endocrinology and Metabolism

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Chronic hepatic artery ligation does not prevent liver from differentiating portal vs. peripheral glucose delivery. Am J Physiol Endocrinol Metab 285: E845-E853, 2003. First published May 28, 2003 10.1152/ajpendo.00130.2003.-Infusion of glucose into the hepatic artery blocks the stimulatory effect of the "portal signal" on net hepatic glucose uptake (NHGU) during portal glucose delivery. We hypothesized that hepatic artery ligation (HAL) would result in enhanced NHGU during peripheral glucose infusion because the arterial glucose concentration would be perceived as lower than that in the portal vein. Fourteen dogs underwent HAL ϳ16 days before study. Conscious 42-h-fasted dogs received somatostatin, intraportal insulin, and glucagon infusions at fourfold basal and at basal rates, respectively, and peripheral glucose infusion to create hyperglycemia. After 90 min (period 1), seven dogs (HAL po) received intraportal glucose (3.8 mg ⅐ kg Ϫ1 ⅐ min Ϫ1 ) and seven (HALpe) continued to receive only peripheral glucose for 90 min (period 2). These two groups were compared with nine non-HAL control dogs (control) treated as were HALpe. During period 2, the arterial plasma insulin concentrations (24 Ϯ 3, 20 Ϯ 1, and 24 Ϯ 2 U/ml) and hepatic glucose loads (39.1 Ϯ 2.5, 43.8 Ϯ 2.9, and 37.7 Ϯ 3.7 mg ⅐ kg Ϫ1 ⅐ min Ϫ1 ) were not different in HALpe, HAL po, and control, respectively. HALpo exhibited greater (P Ͻ 0.05) NHGU than HAL pe and control (3.1 Ϯ 0.3, 2.0 Ϯ 0.4, and 2.0 Ϯ 0.1 mg ⅐ kg Ϫ1 ⅐ min Ϫ1 , respectively). Net hepatic carbon retention was approximately twofold greater (P Ͻ 0.05) in HAL po than in HALpe and control. NHGU and net hepatic glycogen synthesis during peripheral glucose infusion were not enhanced by HAL. Even though there exists an intrahepatic arterial reference site for the portal vein glucose concentration, the failure of HAL to result in enhanced NHGU during peripheral glucose infusion suggests the existence of one or more comparison sites outside the liver. liver glucose uptake; portal vein NET HEPATIC GLUCOSE UPTAKE (NHGU) is enhanced approximately twofold when glucose is delivered via the hepatic portal vein vs. a peripheral vein (29,34). This "portal signal" appears to be neurally mediated (1). When glucose is delivered via the portal vein, the portal venous glucose concentration is greater than the glucose concentration in the arterial circulation, i.e., a negative arterial-portal (A-P) gradient exists. The rate of NHGU is related not to the portal vein glucose level per se (29) but instead to the magnitude of the negative A-P glucose gradient, up to approximately Ϫ18 mg/dl (35). This implies that the portal vein glucose concentration is compared with the arterial concentration at some site, triggering a neural response that includes enhancement of NHGU. The most likely reference sites for comparison with the portal vein glucose concentration would appear to be arteries perfusing the brain (specifically the hypothalamus; see Refs. 33 and 38), the carotid bodies (6,7,36), and the liver itself (14,4...

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