Affiliation:
1. Department of Medicine, Division of Biochemistry, University of Fribourg, Fribourg
2. Swiss Institute of Bioinformatics, Epalinges, Switzerland
Abstract
ABSTRACT
Sterol homeostasis in eukaryotic cells relies on the reciprocal interconversion of free sterols and steryl esters. The formation of steryl esters is well characterized, but the mechanisms that control steryl ester mobilization upon cellular demand are less well understood. We have identified a family of three lipases of
Saccharomyces cerevisiae
that are required for efficient steryl ester mobilization. These lipases, encoded by
YLL012/YEH1
,
YLR020/YEH2
, and
TGL1
, are paralogues of the mammalian acid lipase family, which is composed of the lysosomal acid lipase, the gastric lipase, and four novel as yet uncharacterized human open reading frames. Lipase triple-mutant yeast cells are completely blocked in steryl ester hydrolysis but do not affect the mobilization of triacylglycerols, indicating that the three lipases are required for steryl ester mobilization in vivo. Lipase single mutants mobilize steryl esters to various degrees, indicating partial functional redundancy of the three gene products. Lipase double-mutant cells in which the third lipase is expressed from the inducible
GAL1
promoter have greatly reduced steady-state levels of steryl esters, indicating that overexpression of any of the three lipases is sufficient for steryl ester mobilization in vivo. The three yeast enzymes constitute a novel class of membrane-anchored lipases that differ in topology and subcellular localization.
Publisher
American Society for Microbiology
Subject
Cell Biology,Molecular Biology
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