Effect of inhibition of angiotensin converting enzyme and/or neutral endopeptidase on vascular and neural complications in high fat fed/low dose streptozotocin-diabetic rats

Davidson, Eric P.; Coppey, Lawrence J.; Holmes, Amey; Yorek, Mark A.

doi:10.1016/j.ejphar.2011.12.003

Cited by 47 publications

(62 citation statements)

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“…Ceramides are released as products of complex sphingolipid hydrolysis or synthetized from sphingoid base (Sph or dhSph) and LCFa-CoA at the level of sarcoplasmic reticulum (45). The rise in circulating FFA and elevated muscle ceramide levels was observed previously in soleus and red gastrocnemius skeletal muscle of streptozotocin-diabetic rats (8,16) and in muscle-specific insulin receptor knockout mice and streptozotocin-treated mice (23). De novo sphingolipid synthesis depends on the supply of LCFa-CoA for both the sphingosine backbone formation by SPT and subsequent sphingosine acylation to yield ceramide.…”

Section: Discussionmentioning

confidence: 99%

Impact of insulin deprivation and treatment on sphingolipid distribution in different muscle subcellular compartments of streptozotocin-diabetic C57Bl/6 mice

Zabielski

Błachnio-Zabielska

Lanza

et al. 2014

American Journal of Physiology-Endocrinology and Metabolism

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Insulin deprivation in type 1 diabetes (T1D) individuals increases lipolysis and plasma free fatty acids (FFA) concentration, which can stimulate synthesis of intramyocellular bioactive lipids such as ceramides (Cer) and longchain fatty acid-CoAs (LCFa-CoAs). Ceramide was shown to decrease muscle insulin sensitivity, and at mitochondrial levels it stimulates reactive oxygen species production. Here, we show that insulin deprivation in streptozotocin diabetic C57BL/6 mice increases quadriceps muscle Cer content, which was correlated with a concomitant decrease in the body fat and increased plasma FFA, glycosylated hemoglobin level (%Hb A 1c), and muscular LCFa-CoA content. The alternations were accompanied by an increase in protein expression in LCFa-CoA and Cer synthesis (FATP1/ACSVL5, CerS1, CerS5), a decrease in the expression of genes implicated in muscle insulin sensitivity (GLUT4, GYS1), and inhibition of insulin signaling cascade by Akt␣ and GYS3␤ phosphorylation under acute insulin stimulation. Both the content and composition of sarcoplasmic fraction sphingolipids were most affected by insulin deprivation, whereas mitochondrial fraction sphingolipids remained stable. The observed effects of insulin deprivation were reversed, except for content and composition of LCFa-CoA, CerS protein expression, GYS1 gene expression, and phosphorylation status of Akt and GYS3␤ when exogenous insulin was provided by subcutaneous insulin implants. Principal component analysis and Pearson's correlation analysis revealed close relationships between the features of the diabetic phenotype, the content of LCFa-CoAs and Cers containing C18-fatty acids in sarcoplasm, but not in mitochondria. Insulin replacement did not completely rescue the phenotype, especially regarding the content of LCFa-CoA, or proteins implicated in Cer synthesis and muscle insulin sensitivity. These persistent changes might contribute to muscle insulin resistance observed in T1D individuals. type 1 diabetes; skeletal muscle; mitochondria; ceramide; long-chain fatty acid-coenzyme A METICULOUS GLYCEMIC CONTROL in type 1 diabetic (T1D) individuals can be achieved by administration of prandial, shortacting, and long-acting insulin to mimic ␤-cell secretion in response to varying nutrient levels. Metabolic control in these individuals and stringent adherence to guidelines normalize the plasma glucose and glycosylated hemoglobin levels (%Hb A 1c ) and allow for relatively normal life in T1D. Yet T1D individuals are at greater risk of developing cardiovascular disorders and also known to develop insulin resistance (12, 17). The molecular mechanisms responsible for insulin resistance in T1D subjects are unclear, but variable glucose concentrations (28, 70), advanced glycation end products (62, 73), or desensitization of target tissues by insulin (61) have been proposed. Subcutaneous insulin delivery using an insulin pump partially mimics ␤-cell insulin secretion. However, unlike in nondiabetic individuals with twofold higher hepatic insulin concentration than in ...

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Section: Discussionmentioning

confidence: 99%

Impact of insulin deprivation and treatment on sphingolipid distribution in different muscle subcellular compartments of streptozotocin-diabetic C57Bl/6 mice

Zabielski

Błachnio-Zabielska

Lanza

et al. 2014

American Journal of Physiology-Endocrinology and Metabolism

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“…The renin-angiotensin system (RAS), which controls blood pressure, is upregulated in obesity, and may also contribute to development of type 2 diabetes (in part through promotion of IR and pro-inflammatory cytokine secretion from adipose tissue) 99 . Angiotensin-converting enzyme (ACE) inhibitors have been shown to improve diabetic neuropathy in animal studies 100, 101 , but the mechanism is unclear. Microvascular dysfunction in the nerve and decreased endoneurial perfusion are also thought to contribute to neuropathy 102 .…”

Section: Pathophysiology Of the Metabolic Syndrome On Neuropathymentioning

confidence: 99%

Diabetic neuropathy: clinical manifestations and current treatments

Callaghan¹,

Cheng²,

Stables³

et al. 2012

The Lancet Neurology

865

709

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Diabetic peripheral neuropathy is a prevalent, disabling condition. The most common manifestation is a distal symmetric polyneuropathy (DSP), but many patterns of nerve injury can occur. Currently, the only effective treatments are glucose control and pain management. While glucose control dramatically decreases the development of neuropathy in those with type 1 diabetes, the effect is likely much smaller in those with type 2 diabetes. High levels of evidence support the use of certain anticonvulsants and antidepressants for pain management in diabetic peripheral neuropathy. However, the lack of disease modifying therapies for diabetic DSP makes the identification of new modifiable risk factors essential. Intriguingly, growing evidence supports an association between metabolic syndrome components, including pre-diabetes, and neuropathy. Future studies are needed to further explore this relationship with implications for new treatments for this common disease.

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“…When the NEP 24.11 inhibitor candoxatril was administered in pigs undergoing GLP-1 infusion, glucose tolerance improved, likely through the improvement of GLP-1 pharmacokinetics (33). NEP 24.11 inhibition also led to improved vascular and neural complications in HFD-induced and streptozotocin-induced diabetic rats (9,10,30). These observations collectively suggest that the prevention of NEP 24.11-mediated GLP-1 degradation confers benefits to glucose homeostasis, which is conceptually in contradiction to the notion that GLP-1(28 -36)a exerts beneficial effects in glucose metabolism.…”

Section: Discussionmentioning

confidence: 58%

GLP-1-derived nonapeptide GLP-1(28–36)amide represses hepatic gluconeogenic gene expression and improves pyruvate tolerance in high-fat diet-fed mice

Shao

Chiang

et al. 2013

American Journal of Physiology-Endocrinology and Metabolism

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T. GLP-1-derived nonapeptide GLP-1(28 -36)amide represses hepatic gluconeogenic gene expression and improves pyruvate tolerance in high-fat diet-fed mice. Certain "degradation" products of GLP-1 were found to possess beneficial effects on metabolic homeostasis. Here, we investigated the function of the COOH-terminal fragment of GLP-1, the nonapeptide GLP-1(28 -36)amide, in hepatic glucose metabolism. C57BL/6 mice fed a highfat diet (HFD) for 13 wk were injected intraperitoneally with GLP-1(28 -36)amide for 6 wk. A significant reduction in body weight gain in response to HFD feeding was observed in GLP-1(28 -36)amidetreated mice. GLP-1(28 -36)amide administration moderately improved glucose disposal during glucose tolerance test but more drastically attenuated glucose production during pyruvate tolerance test, which was associated with reduced hepatic expression of the gluconeogenic genes Pck1, G6pc, and Ppargc1a. Mice treated with GLP-1(28 -36)amide exhibited increased phosphorylation of PKA targets, including cAMP response element-binding protein (CREB), ATF-1, and ␤-catenin. In primary hepatocytes, GLP-1(28 -36)amide reduced glucose production and expression of Pck1, G6pc, and Ppargc1a, which was associated with increased cAMP content and PKA target phosphorylation. These effects were attenuated by PKA inhibition. We suggest that GLP-1(28 -36)amide represses hepatic gluconeogenesis involving the activation of components of the cAMP/PKA signaling pathway. This study further confirmed that GLP-1(28 -36)amide possesses therapeutic potential for diabetes and other metabolic disorders.glucagon-like peptide-1; hepatic glucose production; adenosine 3=,5=-cyclic monophosphate; protein kinase A; type 2 diabetes THE INCRETIN HORMONE GLUCAGON-LIKE PEPTIDE-1 (GLP-1) is secreted by intestinal endocrine L cells upon food intake and hormone regulation (2, 4, 25). GLP-1 stimulates insulin secretion in a glucose concentration-dependent manner and positively regulates pro-insulin gene expression (38) and ␤-cell survival, as well as proliferation of pancreatic ␤-cells (4, 25, 48). Extrapancreatic effects of GLP-1 have also been recognized, including the induction of satiety (47), central regulation of metabolism (18), improvement in cardiac and vascular function (6, 8), reduction in gastric emptying (24), and repression of hepatic glucose production (34), as reviewed in detail elsewhere (4, 48). Owing to its important function in controlling blood glucose homeostasis, two new categories of antidiabetic drugs have been developed in the past decade, namely GLP-1 receptor (GLP-1R) agonists and dipeptidyl peptidase-4 (DPP-4) inhibitors, both of which act to increase the activity of GLP-1 signaling to lower plasma glucose levels (4, 48).The active form of GLP-1 is typically considered to be the GLP-1(7-36)amide and GLP-1(7-37) peptides, which are produced from the prohormone proglucagon via the cleavage by the prohormone convertase PC1/3 (11, 31). In the circulation, GLP-1(7-36)amide and GLP-1(7-37) have a very short halflife of aroun...

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Effect of inhibition of angiotensin converting enzyme and/or neutral endopeptidase on vascular and neural complications in high fat fed/low dose streptozotocin-diabetic rats

Cited by 47 publications

References 44 publications

Impact of insulin deprivation and treatment on sphingolipid distribution in different muscle subcellular compartments of streptozotocin-diabetic C57Bl/6 mice

Impact of insulin deprivation and treatment on sphingolipid distribution in different muscle subcellular compartments of streptozotocin-diabetic C57Bl/6 mice

Diabetic neuropathy: clinical manifestations and current treatments

GLP-1-derived nonapeptide GLP-1(28–36)amide represses hepatic gluconeogenic gene expression and improves pyruvate tolerance in high-fat diet-fed mice

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