Macrophages Stimulate Cholesteryl Ester Accumulation in Cocultured Smooth Muscle Cells Incubated With Lipoprotein-Proteoglycan Complex

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Arteriosclerosis, Thrombosis, and Vascular Biology. 1996;16:1112-1121

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(Arteriosclerosis, Thrombosis, and Vascular Biology. 1996;16:1112-1121.)
© 1996 American Heart Association, Inc.

Articles

Macrophages Stimulate Cholesteryl Ester Accumulation in Cocultured Smooth Muscle Cells Incubated With Lipoprotein-Proteoglycan Complex

Parakat Vijayagopal; D. Luke Glancy

the Section of Cardiology, Departments of Medicine (P.V., D.L.G.) and Anatomy (P.V.), Louisiana State University Medical Center, New Orleans.

Correspondence to Parakat Vijayagopal, PhD, Department of Medicine, Louisiana State University Medical Center, 1542 Tulane Ave, New Orleans, LA 70112.

Foam cells of atherosclerotic lesions originate from both macrophagesand smooth muscle cells (SMCs). We explored the mechanism bywhich SMCs may become lipid laden. Confluent bovine aortic SMCswere cocultured with P388D₁ macrophages, and the cocultureswere incubated for various times with low-density lipoprotein(LDL), acetyl-LDL, or lipoprotein-proteoglycan (PG) complexisolated from human atherosclerotic lesions. Macrophages werethen removed from the SMCs and the cholesteryl ester (CE) contentof the SMCs was quantitated. Lipoprotein-PG complex but notLDL or acetyl-LDL produced a 6-fold to 9-fold stimulation ofCE synthesis and a 4.4-fold increase in cellular CE mass incocultured SMCs relative to control SMCs. In similar studieswith human aortic SMC-macrophage cocultures, macrophages stimulatedlipoprotein-PG complex–mediated CE synthesis 7-fold to13-fold and CE mass 7.8-fold in cocultured SMCs compared withSMCs cultured alone. CE synthesis that was mediated by lipoprotein-PGcomplex was dose dependent and increased linearly with time.Incubation of lipoprotein-PG complex with SMC-macrophage coculturesbut not with SMCs or macrophages alone resulted in aggregationof the complex and stimulation of cholesterol esterificationin SMCs by the conditioned media containing the aggregated complex.Cytochalasin D, an inhibitor of phagocytosis, inhibited CE synthesismediated by lipoprotein-PG complex by 73%, whereas polyinosinicacid, an inhibitor of the scavenger receptor, had no effect.Upregulation or downregulation of apolipoprotein B,E receptorsdid not affect the lipoprotein-PG complex–mediated CE synthesisby cocultured SMCs. Lipoprotein-PG complex did not stimulateCE synthesis in SMCs cocultured with aortic endothelial cellsor macrophages cocultured with SMCs. These results indicatethat macrophages can stimulate CE synthesis and accumulationin cocultured SMCs when incubated with lipoprotein-PG complexesisolated from atherosclerotic lesions. This could be a potentialmechanism for myocyte foam cell formation.

Key Words: smooth muscle cells • macrophage coculture • lipoprotein-proteoglycan complex • cholesteryl ester synthesis

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