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Sphingomyelin synthase SMS2 displays dual activity as ceramide phosphoethanolamine synthase

机译:鞘磷脂合酶SMS2具有神经酰胺磷酸乙醇胺合酶的双重活性

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摘要

Sphingolipids are vital components of eukaryotic membranes involved in the regulation of cell growth, death, intracellular trafficking, and the barrier function of the plasma membrane (PM). While sphingomyelin (SM) is the major sphingolipid in mammals, previous studies indicate that mammalian cells also produce the SM analog ceramide phosphoethanolamine (CPE). Little is known about the biological role of CPE or the enzyme(s) responsible for CPE biosynthesis. SM production is mediated by the SM synthases SMS1 in the Golgi and SMS2 at the PM, while a closely related enzyme, SMSr, has an unknown biochemical function. We now demonstrate that SMS family members display striking differences in substrate specificity, with SMS1 and SMSr being monofunctional enzymes with SM and CPE synthase activity, respectively, and SMS2 acting as a bifunctional enzyme with both SM and CPE synthase activity. In agreement with the PM residency of SMS2, we show that both SM and CPE synthase activities are enhanced at the surface of SMS2-overexpressing HeLa cells. Our findings reveal an unexpected diversity in substrate specificity among SMS family members that should enable the design of specific inhibitors to target the biological role of each enzyme individually.
机译:鞘脂是真核膜的重要组成部分,参与调节细胞的生长,死亡,细胞内运输以及质膜(PM)的屏障功能。虽然鞘磷脂(SM)是哺乳动物中的主要鞘脂,但先前的研究表明,哺乳动物细胞还产生SM类似物神经酰胺磷酸乙醇胺(CPE)。关于CPE或负责CPE生物合成的酶的生物学作用知之甚少。 SM的产生是由高尔基体中的SM合成酶SMS1和PM处的SMS2介导的,而密切相关的酶SMSr具有未知的生化功能。现在,我们证明SMS家庭成员在底物特异性上显示出显着差异,其中SMS1和SMSr分别是具有SM和CPE合酶活性的单功能酶,而SMS2作为具有SM和CPE合酶活性的双功能酶。与SMS2的PM驻留一致,我们表明SM和CPE合酶活性在SMS2过表达的HeLa细胞表面均得到增强。我们的发现揭示了SMS家族成员之间底物特异性的出乎意料的多样性,这应该能够设计特异性抑制剂来靶向每种酶的生物学作用。

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