4.6 Article

Characterization of eicosanoid synthesis in a genetic ablation model of ceramide kinase

期刊

JOURNAL OF LIPID RESEARCH
卷 54, 期 7, 页码 1834-1847

出版社

ELSEVIER
DOI: 10.1194/jlr.M035683

关键词

eicosanoids; ceramide-1-phosphate; cytosolic phospholipase A(2); inflammation

资金

  1. Veteran's Administration (VA Merit Review I)
  2. Veteran's Administration (Research Career Scientist Award)
  3. National Institutes of Health [HL-072925, CA-154314, NH1C06-RR-17393]
  4. National Research Service Award-T32 Post-Doctoral Fellowship in Wound Healing [GM008695]
  5. Career Development Award from the Department of Veterans Affairs [CDA1]
  6. National Research Service Award-T31 Pre-Doctoral Fellowship in Functional Lipidomics in Cardiovascular and Respiratory Diseases [HL094290]
  7. Aubery Sage MacFarlane Endowment for Acute Lung Injury Research

向作者/读者索取更多资源

Multiple reports have demonstrated a role for ceramide kinase (CERK) in the production of eicosanoids. To examine the effects of the genetic ablation of CERK on eicosanoid synthesis, primary mouse embryonic fibroblasts (MEFs) and macrophages were isolated from CERK-/- and CERK+/+ mice, and the ceramide-1-phosphate (C1P) and eicosanoid profiles were investigated. Significant decreases were observed in multiple C1P subspecies in CERK-/- cells as compared to CERK+/+ cells with overall 24% and 48% decreases in total C1P. In baseline experiments, the levels of multiple eicosanoids were significantly lower in the CERK-/- cells compared with wild-type cells. Importantly, induction of eicosanoid synthesis by calcium ionophore was significantly reduced in the CERK-/- MEFs. Our studies also demonstrate that the CERK-/- mouse has adapted to loss of CERK in regards to airway hyper-responsiveness as compared with CERK siRNA treatment. Overall, we demonstrate that there are significant differences in eicosanoid levels in ex vivo CERK-/- cells compared with wild-type counterparts, but the effect of the genetic ablation of CERK on eicosanoid synthesis and the serum levels of C1P was not apparent in vivo.

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