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Publication : Extracellular ATP Augments Antigen-Induced Murine Mast Cell Degranulation and Allergic Responses via P2X4 Receptor Activation.

First Author  Yoshida K Year  2020
Journal  J Immunol Volume  204
Issue  12 Pages  3077-3085
PubMed ID  32358018 Mgi Jnum  J:294654
Mgi Id  MGI:6445326 Doi  10.4049/jimmunol.1900954
Citation  Yoshida K, et al. (2020) Extracellular ATP Augments Antigen-Induced Murine Mast Cell Degranulation and Allergic Responses via P2X4 Receptor Activation. J Immunol 204(12):3077-3085
abstractText  Extracellular ATP released from stimulated and/or damaged cells modulates physiological responses via stimulation of various purinoceptors. We previously showed that ATP potentiated the Ag-induced mast cell (MC) degranulation via purinoceptors pharmacologically similar to the ionotropic P2X4 receptor. In this study, we investigated the role of P2X4 receptor in MC degranulation induced by stimulation of IgE-FcepsilonRI complex with Ag, using bone marrow-derived MCs (BMMCs) prepared from wild type and P2X4 receptor-deficient (P2rx4(-/-) ) mice. ATP significantly increased Ag-induced degranulation in BMMCs prepared from wild type mice. This effect of ATP was reduced in BMMCs prepared from P2rx4(-/-) mice. The potentiating effect of ATP was restored by expressing P2X4 receptor in P2rx4(-/-) BMMCs. The P2X4 receptor-mediated effects were maintained even after differentiating into the connective tissue-type MCs. P2X4 receptor stimulation did not affect the Ag-induced Ca(2+) response but enhanced Ag-induced early signals, such as tyrosine phosphorylation of Syk and phospholipase C-gamma. Interestingly, these effects of ATP on Syk phosphorylation were not impaired by pretreatment with Cu(2+), an inhibitor of the P2X4 receptor channel, or removal of external Ca(2+), suggesting that a mechanisms other than Ca(2+) influx through ion channel activity may be involved. In vivo experiments revealed that systemic and intradermal passive anaphylaxis responses were significantly alleviated in P2rx4(-/-) mice. Taken together, the present data suggest that the P2X4 receptor plays an essential role in ATP-induced upregulation of MC degranulation in response to Ag, and also contributes to the Ag-induced allergic response in vivo.
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