The HIV protease inhibitor nelfinavir induces insulin resistance and increases basal lipolysis in 3T3-L1 adipocytes
A Rudich, S Vanounou, K Riesenberg, M Porat… - Diabetes, 2001 - Am Diabetes Assoc
A Rudich, S Vanounou, K Riesenberg, M Porat, A Tirosh, I Harman-Boehm, AS Greenberg…
Diabetes, 2001•Am Diabetes AssocHIV protease inhibitors (HPIs) are potent antiretroviral agents clinically used in the
management of HIV infection. Recently, HPI therapy has been linked to the development of
a metabolic syndrome in which adipocyte insulin resistance appears to play a major role. In
this study, we assessed the effect of nelfinavir on glucose uptake and lipolysis in
differentiated 3T3-L1 adipocytes. An 18-h exposure to nelfinavir resulted in an impaired
insulin-stimulated glucose uptake and activation of basal lipolysis. Impaired insulin …
management of HIV infection. Recently, HPI therapy has been linked to the development of
a metabolic syndrome in which adipocyte insulin resistance appears to play a major role. In
this study, we assessed the effect of nelfinavir on glucose uptake and lipolysis in
differentiated 3T3-L1 adipocytes. An 18-h exposure to nelfinavir resulted in an impaired
insulin-stimulated glucose uptake and activation of basal lipolysis. Impaired insulin …
HIV protease inhibitors (HPIs) are potent antiretroviral agents clinically used in the management of HIV infection. Recently, HPI therapy has been linked to the development of a metabolic syndrome in which adipocyte insulin resistance appears to play a major role. In this study, we assessed the effect of nelfinavir on glucose uptake and lipolysis in differentiated 3T3-L1 adipocytes. An 18-h exposure to nelfinavir resulted in an impaired insulin-stimulated glucose uptake and activation of basal lipolysis. Impaired insulin stimulation of glucose up take occurred at nelfinavir concentrations >10 μmol/l (EC50 = 20 μmol/l) and could be attributed to impaired GLUT4 translocation. Basal glycerol and free fatty acid (FFA) release were significantly enhanced with as low as 5 μmol/l nelfinavir, displaying fivefold stimulation of FFA release at 10 μmol/l. Yet, the antilipolytic action of insulin was preserved at this concentration. Potential underlying mechanisms for these metabolic effects included both impaired insulin stimulation of protein kinase B Ser 473 phosphorylation with preserved insulin receptor substrate tyrosine phosphorylation and decreased expression of the lipolysis regulator perilipin. Troglitazone pre- and cotreatment with nelfinavir partly protected the cells from the increase in basal lipoysis, but it had no effect on the impairment in insulin-stimulated glucose uptake induced by this HPI. This study demonstrates that nelfinavir induces insulin resistance and activates basal lipolysis in differentiated 3T3-L1 adipocytes, providing potential cellular mechanisms that may contribute to altered adipocyte metabolism in treated HIV patients.
Am Diabetes Assoc