Glucose and Insulin Stimulate Heparin-releasable Lipoprotein Lipase Activity in Mouse Islets and INS-1 Cells

Cruz, Wilhelm S.; Kwon, Guim; Marshall, Connie A.; McDaniel, Michael L.; Semenkovich, Clay F.

doi:10.1074/jbc.m010707200

Cited by 48 publications

(45 citation statements)

References 51 publications

(34 reference statements)

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“…Hypertriglyceridemia prioritizing the utilization of TAG as fuels inhibits the intake and oxidization of glucose; 27 intracellular fatty acid metabolites interfere with propagation of insulin signaling cascade; 28 and delivering more FFA to pancreatic b-cells impairs b-cell function and promote apoptosis. 29 The above findings may be partly responsible for the association between LPL and T2D.…”

Section: Lpl and T2dmentioning

confidence: 93%

“…A recent study found that the reduced LPL delivery in skeletal muscle in skeletal muscle-specific LPL knockout mouse (SMLPLÀ/À) induced increased insulin sensitivity in skeletal muscle but insulin resistance in other metabolic tissues, and ultimately led to obesity and systematic insulin resistance. 29 These results suggested that systematic overexpression of LPL might improve insulin resistance, although the underlying mechanism is not clear. These controversies suggest that the association between the LPL gene and T2D may be tissue specific.…”

Section: Lpl and T2dmentioning

confidence: 97%

“…These controversies suggest that the association between the LPL gene and T2D may be tissue specific. Some results relevant to the underlying mechanisms have been reported as follows: Cruz et al 29 study indicated that more FFA could be delivered to pancreatic b-cells by increasing LPL activity, consequently impairing b-cell function and promoting apoptosis in the patients with hyperglyceridemia, hyperinsulinemia and T2D. Hypertriglyceridemia prioritizing the utilization of TAG as fuels inhibits the intake and oxidization of glucose; 27 intracellular fatty acid metabolites interfere with propagation of insulin signaling cascade; 28 and delivering more FFA to pancreatic b-cells impairs b-cell function and promote apoptosis.…”

Section: Lpl and T2dmentioning

confidence: 99%

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The common biological basis for common complex diseases: evidence from lipoprotein lipase gene

et al. 2009

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The lipoprotein lipase (LPL) gene encodes a rate-limiting enzyme protein that has a key role in the hydrolysis of triglycerides. Hypertriglyceridemia, one widely prevalent syndrome of LPL deficiency and dysfunction, may be a risk factor in the development of dyslipidemia, type II diabetes (T2D), essential hypertension (EH), coronary heart disease (CHD) and Alzheimer's disease (AD). Findings from earlier studies indicate that LPL may have a role in the pathology of these diseases and therefore is a common or shared biological basis for these common complex diseases. To examine this hypothesis, we reviewed articles on the molecular structure, expression and function of the LPL gene, and its potential role in the etiology of diseases. Evidence from these studies indicate that LPL dysfunction is involved in dyslipidemia, T2D, EH, CHD and AD; and support the hypothesis that there is a common or shared biological basis for these common complex diseases.

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Section: Lpl and T2dmentioning

confidence: 93%

Section: Lpl and T2dmentioning

confidence: 97%

Section: Lpl and T2dmentioning

confidence: 99%

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The common biological basis for common complex diseases: evidence from lipoprotein lipase gene

et al. 2009

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“…For these reasons, extracellular NEFA can be expected to rapidly distribute in the available lipid bilayers and to move rapidly from cell to cell, potentially acting as paracrine mediators. In addition, islets express low-density lipoprotein receptors [71] and lipoprotein lipase [72] and could also obtain fatty acids from circulating lipoproteins.…”

Section: Nefa Metabolism In the Beta Cellmentioning

confidence: 99%

Fatty acid metabolism and insulin secretion in pancreatic beta cells

2003

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Increases in glucose or fatty acids affect metabolism via changes in long-chain acyl-CoA formation and chronically elevated fatty acids increase total cellular CoA. Understanding the response of pancreatic beta cells to increased amounts of fuel and the role that altered insulin secretion plays in the development and maintenance of obesity and Type 2 diabetes is important. Data indicate that the activated form of fatty acids acts as an effector molecule in stimulus-secretion coupling. Glucose increases cytosolic long-chain acylCoA because it increases the "switch" compound malonyl-CoA that blocks mitochondrial β-oxidation, thus implementing a shift from fatty acid to glucose oxidation. We present arguments in support of the following: (i) A source of fatty acid either exogenous or endogenous (derived by lipolysis of triglyceride) is necessary to support normal insulin secretion; (ii) a rapid increase of fatty acids potentiates glucose-stimulated secretion by increasing fatty acyl-CoA or complex lipid concentrations that act distally by modulating key enzymes such as protein kinase C or the exocytotic machinery; (iii) a chronic increase of fatty acids enhances basal secretion by the same mechanism, but promotes obesity and a diminished response to stimulatory glucose; (iv) agents which raise cAMP act as incretins, at least in part, by stimulating lipolysis via beta-cell hormone-sensitive lipase activation. Furthermore, increased triglyceride stores can give higher rates of lipolysis and thus influence both basal and stimulated insulin secretion. These points highlight the important roles of NEFA, LC-CoA, and their esterified derivatives in affecting insulin secretion in both normal and pathological states. [Diabetologia (2003[Diabetologia ( ) 46:1297[Diabetologia ( -1312

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“…Second, during in vitro experiments, ␤-cells are exposed to stable, constantly elevated levels of fatty acids, a situation clearly different from the cyclical variations of fatty acid levels that occur in vivo during the prandial cycle. Third, the local concentration of biologically active fatty acids (unbound to albumin) in the vicinity of the ␤-cell is essentially unknown and determined by many factors, including the total fatty acid concentration, the molar ratio of fatty acids to albumin, and the activity of lipoprotein lipase (14).…”

mentioning

confidence: 99%

Cyclical and Alternating Infusions of Glucose and Intralipid in Rats Inhibit Insulin Gene Expression and Pdx-1 Binding in Islets

et al. 2008

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OBJECTIVE—Prolonged exposure of isolated islets of Langerhans to elevated levels of fatty acids, in the presence of high glucose, impairs insulin gene expression via a transcriptional mechanism involving nuclear exclusion of pancreas-duodenum homeobox-1 (Pdx-1) and loss of MafA expression. Whether such a phenomenon also occurs in vivo is unknown. Our objective was therefore to ascertain whether chronic nutrient oversupply inhibits insulin gene expression in vivo. RESEARCH DESIGN AND METHODS—Wistar rats received alternating 4-h infusions of glucose and Intralipid for a total of 72 h. Control groups received alternating infusions of glucose and saline, saline and Intralipid, or saline only. Insulin and C-peptide secretion were measured under hyperglycemic clamps. Insulin secretion and gene expression were assessed in isolated islets, and β-cell mass was quantified by morphometric analysis. RESULTS—Neither C-peptide secretion nor insulin sensitivity was different among infusion regimens. Insulin content and insulin mRNA levels were lower in islets isolated from rats infused with glucose plus Intralipid. This was associated with reduced Pdx-1 binding to the endogenous insulin promoter, and an increased proportion of Pdx-1 localized in the cytoplasm versus the nucleus. In contrast, MafA mRNA and protein levels and β-cell mass and proliferation were unchanged. CONCLUSIONS—Cyclical and alternating infusions of glucose and Intralipid in normal rats inhibit insulin gene expression without affecting insulin secretion or β-cell mass. We conclude that fatty acid inhibition of insulin gene expression, in the presence of high glucose, is an early functional defect that may contribute to β-cell failure in type 2 diabetes.

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Glucose and Insulin Stimulate Heparin-releasable Lipoprotein Lipase Activity in Mouse Islets and INS-1 Cells

Cited by 48 publications

References 51 publications

The common biological basis for common complex diseases: evidence from lipoprotein lipase gene

The common biological basis for common complex diseases: evidence from lipoprotein lipase gene

Fatty acid metabolism and insulin secretion in pancreatic beta cells

Cyclical and Alternating Infusions of Glucose and Intralipid in Rats Inhibit Insulin Gene Expression and Pdx-1 Binding in Islets

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