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. 2002 Nov;59(11):1999–2003. doi: 10.1007/PL00012522

Ectoprotein kinase-mediated phosphorylation of FAT/CD36 regulates palmitate uptake by human platelets

F Guthmann 1, P Maehl 1, J Preiss 1, I Kolleck 1, B Rüstow 1
PMCID: PMC11337428  PMID: 12530530

Abstract.

Glycoprotein IV (FAT/CD36) has been shown to be phosphorylated by a cAMP-dependent, platelet membrane-bound ectokinase. In this study, we demonstrate that ectophosphorylation of FAT/CD36 regulates initial palmitate uptake. This is the first time that short-term regulation of the activity of a long-chain fatty acid carrier could be shown. Phosphorylation of FAT/CD36 was paralleled by a significant decrease in initial palmitate uptake by morphologically and functionally intact platelets. Maximum inhibition of palmitate uptake was achieved at 0.5 nM extracellular ATP, being significantly decreased to 72% compared to the control. Inhibition of palmitate uptake was abolished by co-incubation with the specific protein kinase A inhibitor peptide PKI or with β,γ-methylene-ATP, and was reversible upon addition of alkaline phosphatase. An extracellular ATP concentration above 5 μM completely prevented the ectophosphorylation-mediated inhibition of palmitate uptake. We conclude that FAT/CD36-mediated palmitate uptake by human platelets is short-term regulated via cAMP-dependent ectophosphorylation of FAT/CD36.

Keywords: Key words. Ectoprotein kinase; purinergic receptor; adenylyl-(β,γ-methylene)triphosphate; long-chain fatty acid; transmembrane transport.

Footnotes

Received 18 July 2002; received after revision 29 August 2002; accepted 19 September 2002

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