Effects of Insulin, Glucagon, and Insulin/Glucagon Infusions on Liver Morphology and Cell Division After Complete Portacaval Shunt in Dogs

Starzl, Thomas E.; Porter, Kenneth Wiggins; Watanabe, Kazuo; Putnam, CW

doi:10.1016/s0140-6736(76)90477-3

Cited by 210 publications

(143 citation statements)

References 23 publications

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“…Such findings are in contrast to the results of insulin infusion experiments using a computer controlled insulin infusion pump that have shown no significant difference between peripheral and intraportal routes of insulin administration in maintaining blood glucose levels following a glucose load [21], or portocaval shunt experiments which show glucose tolerance to be unaltered by such a procedure [22,23]. However a portocaval shunt in dogs does lead to rapid atrophy and other structural abnormalities of the liver, which can be partly prevented by infusion of insulin into the portal vein [24].…”

Section: Discussionmentioning

confidence: 99%

“…This portal systemic ratio is probably an important aspect of normal glucose metabolism. The systemic delivery of insulin in diabetes via the subcutaneous route or directly into the systemic circulation after a segmental pancreatic graft does not restore normal physiological control of glucose metabolism [24]. Experimental diabetes can be corrected in the rat by transplantation of isolated islets into the liver via the portal vein or into the splenic parenchyma, and in the dog by implantation of dispersed pancreas into the spleen.…”

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confidence: 99%

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Glucose and insulin changes following a renoportal shunt in streptozotocin diabetic rats with pancreatic islet isografts under the kidney capsule

McShane

Morris

1982

Diabetologia

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Summary. The effect on glucose metabolism of altering the site of the venous drainage of an isograft of isolated adult islets implanted beneath the renal capsule, from the systemic circulation to the portal circulation was determined in streptozotocininduced diabetic rats. Reversal of diabetes was accomplished by the transplantation of 1000-1200 isolated islets beneath the left kidney capsule. The rate of fall of the glucose concentration (as expressed by the K value) was found to be significantly decreased in transplanted animals (1.7 _+ 0.5%/rain; mean + SD) compared with normal animals (2.4 + 0.5%/rain). Draining the left renal vein into the portal circulation restored the K value to that of normal animals (2.5 + 0.4%). However the fasting glucose concentration was significantly higher and the basal insulin levels lower in both normal and transplanted rats with a renoportal shunt.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Glucose and insulin changes following a renoportal shunt in streptozotocin diabetic rats with pancreatic islet isografts under the kidney capsule

McShane

Morris

1982

Diabetologia

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“…In this study, this method was used to investigate the consequences of PCS and PCS in conjunction with cyclosporin treatment on hepatic function and basal energy status. The response of the liver to a fructose challenge was monitored by examining the changes in ATP, Pi, and F-1-P levels within the liver as a function of time (28).The dog with a portacaval shunt was chosen as a well-established model for studying hepatic atrophy and contemporaneous hyperplasia (17)(18)(19)(20). The typical injury pattern after PCS consists of a severe reduction in hepatocyte cell size (atrophy) plus organelle disruption and a moderate but persistent stimulation of cell renewal (hyperplasia).…”

mentioning

confidence: 99%

“…The typical injury pattern after PCS consists of a severe reduction in hepatocyte cell size (atrophy) plus organelle disruption and a moderate but persistent stimulation of cell renewal (hyperplasia). Insulin and cytosolic extract of the regenerating liver are able to restore the hepatocyte to normal size and to further stimulate hyperplasia (19,20). A disadvantage of earlier studies was that the animals had to be killed, and in vitro assays of the metabolites of interest could be obtained only at selected times.…”

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confidence: 99%

Effect of cyclosporine on hepatic energy status and on fructose metabolism after portacaval shunt in dog as monitored by phosphorus-31 nuclear magnetic resonance spectroscopy in vivo,

Rossaro¹

1991

Hepatology

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The effect of cyclosporin A on the hepatic energy status and intracellular pH of the liver and its response to a fructose challenge has been investigated using in vivo phosphorus-31 nuclear magnetic resonance spectroscopy in dogs. Three experimental groups were studied: (a) control dogs (n = 5), (b) dogs 4 days after the creation of an end-to-side portacaval shunt (n = 5), and (c) dogs 4 days after portacaval shunt and continuous infusion of cyclosporin A (4 mg/kg/day) by way of the left portal vein (portacaval shunt plus cyclosporin A, n = 5). The phosphorus-31 nuclear magnetic resonance spectra were obtained at 81 MHz using a Bruker BIOSPEC II 4.7-tesla nuclear magnetic resonance system equipped with a 40-cm horizontal bore superconducting solenoid. The phosphomonoesters (p < 0.01), inorganic phosphate and ATP levels (p < 0.05) were decreased significantly in portacaval shunt-treated and in portacaval shunt-plus-cyclosporin A-treated dogs compared with unshunted control dogs. After a fructose challenge (750 mg/kg body wt, intravenously), fructose-1-phosphate metabolism was reduced in portacaval shunt-treated dogs compared with either the normal or portacaval shunt-plus-cyclosporin A-treated dogs (p < 0.05). Both portacaval shunt-and portacaval shunt-plus-cyclosporin A-treated dogs demonstrated a reduced decline in ATP levels after fructose infusion when compared with the controls (p < 0.05). Immediately after the fructose challenge, the intracellular pH decreased from 7.30 ± 0.03 to 7.00 ± 0.05 in all animals (p < 0.01) and then gradually returned to normal over 60 min. These data, obtained in vivo using phosphorus-31 nuclear magnetic resonance spectroscopy of the liver after a portacaval shunt, suggest that: (a) the energy status of the liver is reduced in dogs with a portacaval shunt compared with that of normal controls and (b) cyclosporin A treatment ameliorates the reduction in hepatic metabolism normally observed after a fructose challenge to the liver with a portacaval shunt. In this study, the dog with portacaval shunt (PCS) (Eck's fistula) was used. PCS usually is associated with hepatic atrophy and low-grade hepatocyte hyperplasia (16)(17)(18)(19)(20)(21). We have previously shown in this model that CsA prevents the atrophy and augments the hyperplasia (21). In this report, the effect of CsA treatment on the metabolic events caused by PCS is examined in vivo using phosphorus-31 nuclear magnetic resonance ( 31 P-NMR) spectroscopy.Various in vivo studies using 31 P-NMR spectroscopy (22-24) have reported on the intracellular pH (pH i ), the hepatic content of ATP, sugar phosphates and inorganic phosphate (Pi) under basal conditions and after a physiological challenge with fructose. The only other NMR study relevant to hepatic regeneration or hepatocyte growth control was performed in vitro and used perchloric-acid extracts of tissue samples to calculate phosphate metabolites (25). Materials and Methods Experimental DesignFifteen female purebred Beagle dogs weighing between 8.5 kg and 15 kg were ...

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“…2 Because information about the evolution of these changes within the first 4 days was required to interpret the results of our experiments, control animals had a large side-to-side portacaval shunt with individual ligation of the right and left portal branches, and were killed from ½ to 4 days later (table I). In most of the experiments (tables II and III), a catheter was placed in the ligated left portal branch and led through a subcutaneous tunnel to an infusion pump.…”

Section: Methodsmentioning

confidence: 99%

Growth-Stimulating Factor in Regenerating Canine Liver

et al. 1979

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SummaryExtracts from dog livers which had been regenerating for 24, 48, and 72 h after hepatectomy were infused for 6 h into the left portal vein of animals which had fresh portacaval shunts (Eck fistula) and which were killed 2 and 3 days later. The brief exposure to the 48-h and especially the 72-h regenerating liver extracts induced a delayed proliferative response predominantly in the left liver lobes, with a slight spillover effect to the right liver lobes but none to the kidney. The response reached its peak 3 days later. In the left but not the right liver lobes, both the 48-h and the 72-h regenerating liver extract reversed the atrophy ordinarily caused by Eck fistula in 3 days and partly prevented the ultrastructural hepatocyte deterioration characteristic of Eck fistula. The active liver extracts apparently contained a growth-control factor or factors which is (are) not insulin or glucagon.

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Effects of Insulin, Glucagon, and Insulin/Glucagon Infusions on Liver Morphology and Cell Division After Complete Portacaval Shunt in Dogs

Cited by 210 publications

References 23 publications

Glucose and insulin changes following a renoportal shunt in streptozotocin diabetic rats with pancreatic islet isografts under the kidney capsule

Glucose and insulin changes following a renoportal shunt in streptozotocin diabetic rats with pancreatic islet isografts under the kidney capsule

Effect of cyclosporine on hepatic energy status and on fructose metabolism after portacaval shunt in dog as monitored by phosphorus-31 nuclear magnetic resonance spectroscopy in vivo,

Growth-Stimulating Factor in Regenerating Canine Liver

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