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Membrane organization determines barrier properties of endothelial cells and short-chain sphingolipid-facilitated doxorubicin influx
Authors:AJ van Hell  A KlymchenkoDM Gueth  WJ van BlitterswijkGA Koning  M Verheij
Abstract:The endothelial lining and its outer lipid membrane are the first major barriers drug molecules encounter upon intravenous administration. Our previous work identified lipid analogs that counteract plasma membrane barrier function for a series of amphiphilic drugs. For example, short-chain sphingolipids (SCS), like N-octanoyl-glucosylceramide, effectively elevated doxorubicin accumulation in tumor cells, both in vitro and in vivo, and in endothelial cells, whereas other (normal) cells remained unaffected. We hypothesize here that local membrane lipid composition and the degree of lipid ordering define SCS efficacy in individual cells. To this end, we study the differential effect of SCS on bovine aortic endothelial cells (BAEC) in its confluent versus proliferative state, as a model system. While their (plasma membrane) lipidome stays remarkably unaltered when BAECs reach confluency, their lipids segregate to form apical and basolateral domains. Using probe NR12S, we reveal that lipids in the apical membrane are more condensed/liquid-ordered. SCS preferentially attenuate the barrier posed by these condensed membranes and facilitate doxorubicin influx in these particular membrane regions. We confirm these findings in MDCK cells and artificial membranes. In conclusion, SCS-facilitated drug traversal acts on condensed membrane domains, elicited by confluency in resting endothelium.
Keywords:BAEC  bovine aortic endothelial cells  bFGF  basic fibroblast growth factor  CH  cholesterol  Dox  doxorubicin3  DPPC  di-palmitoyl-phosphatidylcholine  DSM  dehydrosphingomyelin  ePC  ether-linked phosphatidylethanolamine  GC  N-octanoyl-glucosylceramide  LUV  large unilamellar vesicle  MDCK  Madin&ndash  Darby canine kidney cells  PA  phosphatic acid  PBS  phosphate buffered saline  PC  phosphatidylcholine  PE-Cer  ceramide phosphoethanolamine  PG  phosphatidylglycerol  PI  phosphatidylinositol  POPC  palmitoyl-oleoyl-phosphatidylcholine  SCS  short-chain sphingolipid  SM  sphingomyelin
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