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Traceless synthesis of ceramides in living cells reveals saturation-dependent apoptotic effects.


ABSTRACT: Mammalian cells synthesize thousands of distinct lipids, yet the function of many of these lipid species is unknown. Ceramides, a class of sphingolipid, are implicated in several cell-signaling pathways but poor cell permeability and lack of selectivity in endogenous synthesis pathways have hampered direct study of their effects. Here we report a strategy that overcomes the inherent biological limitations of ceramide delivery by chemoselectively ligating lipid precursors in vivo to yield natural ceramides in a traceless manner. Using this method, we uncovered the apoptotic effects of several ceramide species and observed differences in their apoptotic activity based on acyl-chain saturation. Additionally, we demonstrate spatiotemporally controlled ceramide synthesis in live cells through photoinitiated lipid ligation. Our in situ lipid ligation approach addresses the long-standing problem of lipid-specific delivery and enables the direct study of unique ceramide species in live cells.

SUBMITTER: Rudd AK 

PROVIDER: S-EPMC6055205 | biostudies-literature | 2018 Jul

REPOSITORIES: biostudies-literature

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Traceless synthesis of ceramides in living cells reveals saturation-dependent apoptotic effects.

Rudd Andrew K AK   Devaraj Neal K NK  

Proceedings of the National Academy of Sciences of the United States of America 20180702 29


Mammalian cells synthesize thousands of distinct lipids, yet the function of many of these lipid species is unknown. Ceramides, a class of sphingolipid, are implicated in several cell-signaling pathways but poor cell permeability and lack of selectivity in endogenous synthesis pathways have hampered direct study of their effects. Here we report a strategy that overcomes the inherent biological limitations of ceramide delivery by chemoselectively ligating lipid precursors in vivo to yield natural  ...[more]

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