| Literature DB >> 29653252 |
Andreas Bickert1, Paul Kern2, Martina van Uelft1, Stefanie Herresthal3, Thomas Ulas3, Katharina Gutbrod4, Bernadette Breiden5, Joachim Degen1, Konrad Sandhoff5, Joachim L Schultze3, Peter Dörmann4, Dieter Hartmann6, Reinhard Bauer2, Klaus Willecke7.
Abstract
The replacement of two consecutive histidine residues by alanine residues in the catalytic center of ceramide synthase 2 in a new transgenic mouse mutant (CerS2 H/A) leads to inactivation of catalytic activity and reduces protein level to 60% of the WT level. We show here by qRT-PCR and transcriptome analyses that several transcripts of genes involved in lipid metabolism and cell division are differentially regulated in livers of CerS2 H/A mice. Thus, very long chain ceramides produced by CerS2 are required for transcriptional regulation of target genes. The hepatocellular carcinomata previously described in old CerS2 KO mice were already present in 8-week-old CerS2 H/A animals and thus are caused by the loss of CerS2 catalytic activity already during early life.Entities:
Keywords: Cell division; Ceramide synthase 2; Hepatocellular carcinoma; Lipid metabolism; Sphingolipids; Transcriptional control
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Year: 2018 PMID: 29653252 DOI: 10.1016/j.bbalip.2018.04.006
Source DB: PubMed Journal: Biochim Biophys Acta Mol Cell Biol Lipids ISSN: 1388-1981 Impact factor: 4.698