AI Article Synopsis

  • The study explored how low concentrations of okadaic acid (0.25-0.5 microM) enhance phospholipase D (PLD) activation by formyl peptides in immune cells, while higher concentrations (2-3 microM) inhibit this effect despite increasing protein phosphorylation.
  • It was found that when PLD activation was primed with cytochalasin B, both the enhancing and inhibiting effects of okadaic acid on PLD activity became stronger.
  • Additionally, stimulation with mastoparan showed that okadaic acid could have varying impacts on the production of phosphatidylethanol, suggesting that protein phosphatases play a significant role in regulating cellular signaling events involving G proteins.

Article Abstract

The activation of phospholipase D (PLD) induced by formyl peptides (fMLP), as evaluated by production of tritiated phosphatidylethanol (PEt) and phosphatidic acid (PA) in polymorphonuclear leukocytes (PMN), was markedly enhanced (50-125%) by low okadaic acid concentrations (0.25-0.5 microM) but inhibited by higher concentrations (2-3 microM), although the drug caused protein hyperphosphorylation. Both effects of okadaic acid were amplified when PLD activation was primed with cytochalasin B. Stimulation of PMN with mastoparan, a wasp venom toxin that activates Pertussis toxin(PTX)-sensitive G proteins, resulted in a weak calcium-dependent production of PEt which was respectively enhanced and inhibited by okadaic acid (1-2 microM) in unprimed and cytochalasin-primed PMN. The results show that low okadaic acid concentrations primed fMLP-mediated activation of PLD, in keeping with a down-regulatory role of protein phosphatases. The contrasting effects of okadaic acid in mastoparan-stimulated PMN further suggest that protein phosphatases may regulate the generation of second messengers through alteration of major signaling events at/or downstream of PTX-sensitive G proteins (Gi).

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Source
http://dx.doi.org/10.1006/bbrc.1994.2832DOI Listing

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