[No authors listed]
Ceramide is synthesized in yeast by two redundant acyl-CoA dependent synthases, Lag1 and Lac1. In lag1â lac1â cells, free fatty acids and sphingoid bases are elevated, and ceramides are produced through the redundant alkaline ceramidases Ypc1 and Ydc1, working backwards. Even with all four of these genes deleted, cells are surviving and continue to contain small amounts of complex sphingolipids. Here we show that these residual sphingolipids are not synthesized by YPR114w or YJR116w, proteins of unknown function showing a high degree of homology to Lag1 and Lac1. Indeed, the hextuple lag1â lac1â ypc1â ydc1â ypr114wâ yjr116wâ mutant still contains ceramides and complex sphingolipids. Yjr116wâ exhibit an oxygen-dependent hypersensitivity to Cu2+ due to an increased mitochondrial production of reactive oxygen species and a mitochondrially orchestrated programmed cell death in presence of copper, but also a general copper hypersensitivity that cannot be counteracted by the antioxidant N-acetyl-cysteine (NAC). Myriocin efficiently represses the synthesis of sphingoid bases of ypr114wâ, but not its growth. Both yjr116wâ and ypr114wâ have fragmented vacuoles and produce less than wild type, before and after diauxic shift. Ypr114wâ/ypr114wâ have an increased chronological life span. Thus, Yjr116w and Ypr114w are related, but not functionally redundant.
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