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Literature DB >> 25605874

All members in the sphingomyelin synthase gene family have ceramide phosphoethanolamine synthase activity.

Tingbo Ding¹, Inamul Kabir², Yue Li¹, Caixia Lou³, Amirfarbod Yazdanyar², Jiachen Xu⁴, Jibin Dong⁴, Hongwen Zhou⁵, Taesik Park⁶, Mohamed Boutjdir⁷, Zhiqiang Li², Xian-Cheng Jiang⁸.

Abstract

Sphingomyelin synthase-related protein (SMSr) synthesizes the sphingomyelin analog ceramide phosphoethanolamine (CPE) in cells. Previous cell studies indicated that SMSr is involved in ceramide homeostasis and is crucial for cell function. To further examine SMSr function in vivo, we generated Smsr KO mice that were fertile and had no obvious phenotypic alterations. Quantitative MS analyses of plasma, liver, and macrophages from the KO mice revealed only marginal changes in CPE and ceramide as well as other sphingolipid levels. Because SMS2 also has CPE synthase activity, we prepared Smsr/Sms2 double KO mice. We found that CPE levels were not significantly changed in macrophages, suggesting that CPE levels are not exclusively dependent on SMSr and SMS2 activities. We then measured CPE levels in Sms1 KO mice and found that Sms1 deficiency also reduced plasma CPE levels. Importantly, we found that expression of Sms1 or Sms2 in SF9 insect cells significantly increased not only SM but also CPE formation, indicating that SMS1 also has CPE synthase activity. Moreover, we measured CPE synthase Km and Vmax for SMS1, SMS2, and SMSr using different NBD ceramides. Our study reveals that all mouse SMS family members (SMSr, SMS1, and SMS2) have CPE synthase activity. However, neither CPE nor SMSr appears to be a critical regulator of ceramide levels in vivo.

Entities: Chemical Disease Gene Species

Keywords: mouse gene knockout; sphingomyelin synthase 1; sphingomyelin synthase 2; sphingomyelin synthase-related protein

Mesh：

Substances：

Year: 2015 PMID： 25605874 PMCID： PMC4340302 DOI： 10.1194/jlr.M054627

Source DB: PubMed Journal: J Lipid Res ISSN： 0022-2275 Impact factor: 5.922

32 in total

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6. Sphingomyelin synthase SMS2 displays dual activity as ceramide phosphoethanolamine synthase.

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10. Sphingomyelin synthase-related protein SMSr controls ceramide homeostasis in the ER.

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2. Switching head group selectivity in mammalian sphingolipid biosynthesis by active-site-engineering of sphingomyelin synthases.

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7. ER residency of the ceramide phosphoethanolamine synthase SMSr relies on homotypic oligomerization mediated by its SAM domain.

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Review 9. Potential therapeutic targets for atherosclerosis in sphingolipid metabolism.

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