Different metabolic recycling of the lipid components of exogenous sulphatide in human fibroblasts

Author:

Trinchera M1,Wiesmann U2,Pitto M1,Acquotti D1,Ghidoni R12

Affiliation:

1. Department of Medical Chemistry and Biochemistry, Via Saldini 50, The Medical School, University of Milan, Milan, Italy

2. Department of Pediatrics, University of Bern, Bern, Switzerland

Abstract

Cultured human fibroblasts were fed with two differently labelled sulphatide molecules [one labelled on C-3 of the sphingosine (Sph) moiety [(Sph-3H]sulphatide), the second on C-1 of stearic acid [(stearoyl-14C]sulphatide)], and the intracellular metabolic fate of radioactivity was monitored. Incorporated radioactivity was almost all recovered in the total lipid extract, regardless of the labelling position of the added sulphatide; however, large differences in the level of incorporation occurred among labelled glycosphingolipids. For example, sphingomyelin was present as the major radiolabelled lipid after [Sph-3H]-sulphatide incubation, but was detectable only in trace amounts after [stearoyl-14C]sulphatide administration; in the latter case the radioactivity was located predominantly in glycerophospholipids. From this finding it can be inferred that the free long-chain base (sphingosine) that originates from lysosomal catabolism of sulphatide is mainly, and quite specifically, utilized for sphingomyelin biosynthesis, whereas the ceramide moiety is not; conversely the fatty acid released from ceramide is non-specifically re-utilized for phospholipid biosynthesis.

Publisher

Portland Press Ltd.

Subject

Cell Biology,Molecular Biology,Biochemistry

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