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D-galactosyl-beta1-1'-sphingosine and D-glucosyl-beta1-1'-sphingosine induce human natural killer cell apoptosis
Authors:Maghazachi Azzam A  Knudsen Eirunn  Jin Yixin  Jenstad Monica  Chaudhry Farrukh A
Affiliation:Department of Anatomy, Institute of Basic Medical Sciences, University of Oslo, P.O.B. 1105 Blindern, N-0317 Oslo, Norway. azzam.maghazachi@basalmed.uio.no
Abstract:Natural killer (NK) cells perform multiple biological functions including tumor cell lysis and eradicating virally infected cells. Here, we report for the first time that D-galactosyl-beta1-1' sphingosine and D-glucosyl-beta1- 1' sphingosine damage human NK cells. We show that these cells express T-cell-associated gene-8, the receptor for glycosphingolipids. D-galactosyl-beta1-1' sphingosine and D-glucosyl-beta1-1' sphingosine induce the in vitro chemotaxis of human NK cells. Both D-galactosyl-beta1-1' sphingosine and D-glucosyl-beta1-1' sphingosine inhibit the cytotoxicity and IFN-gamma secretion by these cells. Further analysis shows that the glycosphingolipids D-galactosyl-beta1-1' sphingosine and D-glucosyl-beta1-1' sphingosine but not any other lipid examined, which include D-lactosyl-beta1-1' sphingosine, sphingosine 1-phosphate, sphingosine, lysophosphatidic acid, and phosphatidic acid, induce the apoptosis, globoid-like formation, and multinucleation in human NK cells. These results may have important implications on diseases where glycosphingolipids accumulate.
Keywords:NK cells   Glycosphingolipids   Lysophospholipids   Apoptosis   Multinucleation   Vacuolation   Chemotaxis   Cytotoxicity   Interferon γ
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