Oleic Acid–Induced Mitogenic Signaling in Vascular Smooth Muscle Cells

Abstract

As an initial step in testing the hypothesis that high oleic acid concentrations contribute to vascular remodeling in obese hypertensive patients by activating protein kinase C (PKC), the effects of oleic acid on primary cultures of rat aortic smooth muscle cells (RASMCs) were studied. Oleic acid, an 18-carbon cis -monounsaturated fatty acid (18:1 [ cis ]), from 25 to 200 μmol/L significantly increased [ 3 H]thymidine uptake in RASMCs with an EC 50 of 41.0 μmol/L and a maximal response of 196±15% of control ( P <.01). Oleic acid from 25 to 200 μmol/L caused a concentration-dependent increase in the number of RASMCs in culture at 6 days, reaching a maximum of 210±13% of control at 100 μmol/L ( P <.001). PKC inhibition with 4 μmol/L bisindolylmaleimide I and PKC depletion (α, μ, ι, and ζ) with 24-hour exposure to 200 nmol/L phorbol 12-myristate 13-acetate in RASMCs eliminated the mitogenic effects of oleic acid but did not reduce responses to 10% FBS. Stimulation of intact cells with oleic acid induced a peak increase of cytosolic PKC activity, reaching 328±8% of control ( P <.001), but did not enhance PKC activity in the membrane fraction (105±4%, P =NS). The oleic acid–induced increase of PKC activity in cell lysates was similar in the presence and absence of Ca 2+ , phosphatidylserine, and diolein (maximum response, 360±4% versus 342±9% of control, P =NS). Unlike phorbol 12-myristate 13-acetate, oleic acid over 24 hours did not downregulate any of the four PKC isoforms detected in RASMCs. Oleic acid treatment activated mitogen-activated protein (MAP) kinase. PKC depletion in RASMCs eliminated the rise in thymidine uptake, activation of PKC, and activation of MAP kinase in response to oleic acid. In contrast to oleic acid, 50 to 200 μmol/L stearic (18:0) and elaidic (18:1 [ trans ]) acids, which are less effective activators of PKC than oleic acid, did not enhance thymidine uptake. These data suggest that oleic acid induces proliferation of RASMCs by activating PKC, particularly one or more of the Ca 2+ -independent isoforms, and raise the possibility that the higher oleic acid concentrations observed in obese hypertensive patients may contribute to vascular remodeling.