4.4 Article

5-OMe-uridine-5′-O-(α-boranodiphosphate), a novel nucleotide derivative highly active at the human P2Y6 receptor protects against death-receptor mediated glial apoptosis

Journal

NEUROSCIENCE LETTERS
Volume 578, Issue -, Pages 80-84

Publisher

ELSEVIER IRELAND LTD
DOI: 10.1016/j.neulet.2014.06.030

Keywords

P2Y(6) receptor; TNF alpha; Apoptosis; Protection; Purinergic agonist

Categories

Funding

  1. German-Israeli Foundation [958/2007]

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P2Y receptors are activated by nucleotides and involved in numerous physiological/pathophysiological processes. However, investigations of specific P2Y receptor functions have been hampered by lack of suitable receptor agonists-antagonists. Recently, we identified the nucleotide 5-OMe-UDP as potent and selective agonist for human P2Y(6) receptors. We studied a series of derivatives of this analog with a P alpha-borano group substituting a non-bridging oxygen and found increased potency and receptor specificity. Rp-5-OMe-UDP alpha B (Rp-5-OMe-uridine 5'-O-alpha-boranodiphosphate) was most potent and selective in inducing intracellular calcium signaling in 1321N1 astrocytoma cells expressing the human P2Y(6) receptor. Here, we investigated whether Rp-5-OMe-UDP alpha B evokes cell protection through human P2Y(6) receptors. We tested a well-established model, tumor necrosis factor alpha (TNF alpha)-induced cell death in 1321N1 astrocytoma cells. Rp-5-OMe-UDP alpha B inhibited TNF alpha-induced cell death even stronger than UDP. These first data of a neuro-protective activity of the human P2Y(6) receptor emphasize the potential of the stable, selective, and potent Rp-5-OMe-UDP alpha B analog for exploiting P2Y(6) receptor-mediated cellular functions, like cytoprotection in human tissues, with suitability for future neuro-protective drug development. (C) 2014 Elsevier Ireland Ltd. All rights reserved.

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