Effects of intraportal exenatide on hepatic glucose metabolism in the conscious dog

Edgerton, Dale S.; An, Zhibo; Johnson, Ken; Farmer, Tiffany D.; Farmer, Ben; Neal, Doss W.; Cherrington, Alan D.

doi:10.1152/ajpendo.00160.2013

Cited by 1 publication

(2 citation statements)

References 70 publications

(99 reference statements)

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“…The improvements in patient glycaemic responses elicited by GLP-1 agonists, or dipeptidyl peptidase inhibitors that retard GLP-1 degradation, within the circulation, or AMPK activators, e.g. metformin or other biguanides 40 , 64 , 98 and reversal of the pathological effects of NAFLD and NASH by GLP-1 agonists 85 , 99 tend to corroborate the view that GLP-1 deficiency is a cause of metabolic disease. GLP-1 agonists, such as exenatide, used in treatment of 2TDM, have been shown to be effective in reducing hyperglycaemia and hyperinsulinaemia namely 100 .…”

Section: Part 2 Simulations Of Nafld Nash and T2dmmentioning

confidence: 67%

“…Two important effects of hepatic and portal endothelial dysfunction are increased hepatic vascular resistance resulting in reduced hepatic sinus blood flow and raised portal blood pressure 81 – 83 . Additionally, reduction in hepatic glucokinase activity, associated with NASH and T2DM, reduces hepatic insulin-and GLP-1-dependent glucose uptake and metabolism 84 , 85 .…”

Section: Part 2 Simulations Of Nafld Nash and T2dmmentioning

confidence: 99%

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A computer model simulating human glucose absorption and metabolism in health and metabolic disease states

Naftalin

2016

F1000Res

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A computer model designed to simulate integrated glucose-dependent changes in splanchnic blood flow with small intestinal glucose absorption, hormonal and incretin circulation and hepatic and systemic metabolism in health and metabolic diseases e.g. non-alcoholic fatty liver disease, (NAFLD), non-alcoholic steatohepatitis, (NASH) and type 2 diabetes mellitus, (T2DM) demonstrates how when glucagon-like peptide-1, (GLP-1) is synchronously released into the splanchnic blood during intestinal glucose absorption, it stimulates superior mesenteric arterial (SMA) blood flow and by increasing passive intestinal glucose absorption, harmonizes absorption with its distribution and metabolism. GLP-1 also synergises insulin-dependent net hepatic glucose uptake (NHGU). When GLP-1 secretion is deficient post-prandial SMA blood flow is not increased and as NHGU is also reduced, hyperglycaemia follows. Portal venous glucose concentration is also raised, thereby retarding the passive component of intestinal glucose absorption. Increased pre-hepatic sinusoidal resistance combined with portal hypertension leading to opening of intrahepatic portosystemic collateral vessels are NASH-related mechanical defects that alter the balance between splanchnic and systemic distributions of glucose, hormones and incretins.The model reveals the latent contribution of portosystemic shunting in development of metabolic disease. This diverts splanchnic blood content away from the hepatic sinuses to the systemic circulation, particularly during the glucose absorptive phase of digestion, resulting in inappropriate increases in insulin-dependent systemic glucose metabolism. This hastens onset of hypoglycaemia and thence hyperglucagonaemia. The model reveals that low rates of GLP-1 secretion, frequently associated with T2DM and NASH, may be also be caused by splanchnic hypoglycaemia, rather than to intrinsic loss of incretin secretory capacity. These findings may have therapeutic implications on GLP-1 agonist or glucagon antagonist usage.

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