Abstract
Insulin at physiological concentrations can suppress catecholamine activation of the membrane transport of long chain fatty acids in the adipocyte. We have previously shown that the stimulatory effect of catecholamines was mediated by a beta-receptor interaction and cAMP (Abumrad, N.A., Park, C.R., and Whitesell, R. R. (1986) J. Biol. Chem. 261, 13082-13086). In this study we have investigated the mechanism of insulin action to antagonize transport activation. Fatty acid transport was stimulated using different cAMP derivatives with varying susceptibilities to hydrolysis by the cAMP-degrading enzyme phosphodiesterase. Insulin was effective in antagonizing the effect of cAMP analogs which were good substrates for the phosphodiesterase and failed to suppress the effect of those which were poorly hydrolyzed by the enzyme. Addition of increasing concentrations (1-100 microM) of the phosphodiesterase inhibitor methylisobutylxanthine (MIX) to norepinephrine (0.1 microgram/ml) gradually abolished insulin's antagonism. Insulin was completely ineffective in inhibiting stimulation by norepinephrine and 20 microM methylisobutylxanthine. Also consistent with involvement of cAMP lowering in insulin action was the finding that adenosine removal greatly diminished insulin's responsiveness. Treatment of cells with adenosine deaminase (1 unit/ml) enhanced the effect of norepinephrine by about 30%. A 10-fold higher range of insulin concentrations was then required to produce inhibition of fatty acid transport. The effect of adenosine removal was reversed by addition of phenylisopropyladenosine (500 nM), which is resistant to hydrolysis by the deaminase. Finally, exposure of insulin-treated cells (1 nM for 5 min) to dinitrophenol (1 mM for 5 min) reversed insulin action, consistent with reports of reversal of insulin's activation of the phosphodiesterase. In conclusion, our studies support the involvement of cAMP lowering in insulin's antagonism of fatty acid transport stimulation in the adipocyte.
Highlights
STUDIES ON ITS MECHANISM OF ACTION*Insulin at physiological concentrations can suppress of catecholamines on fatty acid transport was shown to be catecholamine activation of the membrane transport mediated by cAMP and its protein kinase [2]
From the Department of Molecular Phy.siolog” y and BwDhysics, Vanderbilt University School of Medicine, Nashuille, Tennessee 37232
Insulin at physiological concentrations can suppress of catecholamines on fatty acid transport was shown to be catecholamine activation of the membrane transport mediated by cAMP and its protein kinase [2]
Summary
Insulin at physiological concentrations can suppress of catecholamines on fatty acid transport was shown to be catecholamine activation of the membrane transport mediated by cAMP and its protein kinase [2]. The antagoof long chain fatty acids in the adipocyte. We have nistic influence of insulin on the transport system was very previously shown that the stimulatory effect of cate- sensitive and was observed at very low insulin concentrations cholamines was mediated by a &receptor interaction (10-50 PM) which were similar to those shown to be antiliand cAMP We have examdiesterase and failed to suppress the effect of those ined the ability of adenosine and methylisobutylxanthine to which werepoorly hydrolyzed btyhe enzyme. Of increasing concentrations (1-100 PM) of the phosphodiesterase inhibitor methylisobutylxanthine (MIX)
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