Literature DB >> 2155608

Evaluation of synthetic sphingosine, lysosphingolipids and glycosphingolipids as inhibitors of functional responses of human neutrophils.

S Fiore1, K C Nicolaou, T Caulfield, H Kataoka, C N Serhan.   

Abstract

Human neutrophils, when exposed to soluble stimuli, aggregate, release oxygenated products of arachidonic acid and generate active oxygen species. Sphingolipid-derived products such as sphingosine and lysosphingolipids have been shown to exert selective actions on a variety of cell types, including neutrophils. Therefore, to determine the structural basis for selective inhibition of neutrophil responses by naturally occurring sphingolipids, seven compounds were prepared by total organic synthesis, and their impact on neutrophils in suspension has been studied. The compounds synthesized included sphingosine, psychosine, lactosyl lysosphingolipid, globotriaosyl (Gb3) lysosphingolipid, galactosyl cerebroside, lactosyl ceramide and Gb3 ceramide. The neutrophil responses studied were aggregation, leukotriene generation and superoxide anion production. When exposed to non-cytotoxic levels of the synthetic compounds, as monitored by exclusion of Trypan Blue, none of the synthetic sphingolipids inhibited A23187-induced aggregation of neutrophils. Only lactosyl lysosphingolipid, at a concentration of 1 microM, significantly inhibited aggregation induced by fMetLeuPhe; the other compounds in this series including sphingosine were without effect at equal molar concentrations (1 microM). Aggregation induced by phorbol 12-myristate 13-acetate (PMA) (0.1 microM) was significantly blocked by only two of the synthetic sphingolipids (1 microM). At concentrations below 1 microM, these inhibitory actions were not evident, nor was it possible to assign a structure-activity relationship for this series of compounds. None of the synthetic sphingolipids effectively inhibited the generation of superoxide anions induced by PMA. In addition, neither synthetic sphingosine nor psychosine affected either the formation or metabolism of leukotriene B4. Taken together, the results provide further evidence that sphingolipids, when added to intact cells, are not potent selective inhibitors of functional responses of human neutrophils.

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Year:  1990        PMID: 2155608      PMCID: PMC1131091          DOI: 10.1042/bj2660025

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  27 in total

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Review 5.  Release of inflammatory mediators from stimulated neutrophils.

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6.  Effects of leukotrienes and f-Met-Leu-Phe on oxidative metabolism of neutrophils and eosinophils.

Authors:  J Palmblad; H Gyllenhammar; J A Lindgren; C L Malmsten
Journal:  J Immunol       Date:  1984-06       Impact factor: 5.422

7.  PGBX, a prostagandin derivative, mimics the action of the calcium ionophore A23187 on human neutrophils.

Authors:  C N Serhan; H M Korchak; G Weissmann
Journal:  J Immunol       Date:  1980-11       Impact factor: 5.422

8.  The roles of degranulation and superoxide anion generation in neutrophil aggregation.

Authors:  H B Kaplan; H S Edelson; R Friedman; G Weissmann
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9.  Selective activation of the gamma-subspecies of protein kinase C from bovine cerebellum by arachidonic acid and its lipoxygenase metabolites.

Authors:  M S Shearman; Z Naor; K Sekiguchi; A Kishimoto; Y Nishizuka
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Authors:  C N Serhan; M J Broekman; H M Korchak; J E Smolen; A J Marcus; G Weissmann
Journal:  Biochim Biophys Acta       Date:  1983-06-02
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