TY - JOUR
T1 - Functional interactions between sphingolipids and sterols in biological membranes regulating cell physiology
AU - Guan, Xue Li
AU - Souza, Cleiton M.
AU - Pichler, Harald
AU - Dewhurst, Gisele
AU - Schaad, Olivier
AU - Kajiwara, Kentaro
AU - Wakabayashi, Hirotomo
AU - Ivanova, Tanya
AU - Castillon, Guillaume A.
AU - Piccolis, Manuele
AU - Abe, Fumiyoshi
AU - Loewith, Robbie
AU - Funato, Kouichi
AU - Wenk, Markus R.
AU - Riezman, Howard
PY - 2009/4/1
Y1 - 2009/4/1
N2 - Sterols and sphingolipids are limited to eukaryotic cells, and their interaction has been proposed to favor formation of lipid microdomains. Although there is abundant biophysical evidence demonstrating their interaction in simple systems, convincing evidence is lacking to show that they function together in cells. Using lipid analysis by mass spectrometry and a genetic approach on mutants in sterol metabolism, we show that cells adjust their membrane composition in response to mutant sterol structures preferentially by changing their sphingolipid composition. Systematic combination of mutations in sterol biosynthesis with mutants in sphingolipid hydroxylation and head group turnover give a large number of synthetic and suppression phenotypes. Our unbiased approach provides compelling evidence that sterols and sphingolipids function together in cells. We were not able to correlate any cellular phenotype we measured with plasma membrane fluidity as measured using fluorescence anisotropy. This questions whether the increase in liquid order phases that can be induced by sterol-sphingolipid interactions plays an important role in cells. Our data revealing that cells have a mechanism to sense the quality of their membrane sterol composition has led us to suggest that proteins might recognize sterol-sphingolipid complexes and to hypothesize the coevolution of sterols and sphingolipids.
AB - Sterols and sphingolipids are limited to eukaryotic cells, and their interaction has been proposed to favor formation of lipid microdomains. Although there is abundant biophysical evidence demonstrating their interaction in simple systems, convincing evidence is lacking to show that they function together in cells. Using lipid analysis by mass spectrometry and a genetic approach on mutants in sterol metabolism, we show that cells adjust their membrane composition in response to mutant sterol structures preferentially by changing their sphingolipid composition. Systematic combination of mutations in sterol biosynthesis with mutants in sphingolipid hydroxylation and head group turnover give a large number of synthetic and suppression phenotypes. Our unbiased approach provides compelling evidence that sterols and sphingolipids function together in cells. We were not able to correlate any cellular phenotype we measured with plasma membrane fluidity as measured using fluorescence anisotropy. This questions whether the increase in liquid order phases that can be induced by sterol-sphingolipid interactions plays an important role in cells. Our data revealing that cells have a mechanism to sense the quality of their membrane sterol composition has led us to suggest that proteins might recognize sterol-sphingolipid complexes and to hypothesize the coevolution of sterols and sphingolipids.
UR - https://www.scopus.com/pages/publications/65249154315
U2 - 10.1091/mbc.E08-11-1126
DO - 10.1091/mbc.E08-11-1126
M3 - Article
C2 - 19225153
AN - SCOPUS:65249154315
SN - 1059-1524
VL - 20
SP - 2083
EP - 2095
JO - Molecular Biology of the Cell
JF - Molecular Biology of the Cell
IS - 7
ER -