TRPM2 contributes to antigen-stimulated Ca^sup 2+^ influx in mucosal mast cells

Food allergy (FA) is a common allergic disease without any currently available effective drug therapies. Mucosal mast cells (MMCs) play a particularly important role in FA, and the increase in their cytosolic Ca^sup 2+^ concentration ([Ca^sup 2+^]^sub cyt^) is considered to be a principal component...

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Bibliographic Details
Published in:Pflügers Archiv 2013-07, Vol.465 (7), p.1023
Main Authors: Oda, Satoshi, Uchida, Kunitoshi, Wang, Xiaoyu, Lee, Jaemin, Shimada, Yutaka, Tominaga, Makoto, Kadowaki, Makoto
Format: Article
Language:English
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Summary:Food allergy (FA) is a common allergic disease without any currently available effective drug therapies. Mucosal mast cells (MMCs) play a particularly important role in FA, and the increase in their cytosolic Ca^sup 2+^ concentration ([Ca^sup 2+^]^sub cyt^) is considered to be a principal component of the degranulation process. However, the mechanisms governing Ca^sup 2+^ influx remain poorly understood in MMCs. Recent reports have highlighted the functions of the transient receptor potential melastatin 2 (TRPM2) channel in immunocytes, including its role in monocyte chemokine production and macrophage phagocytic activity. Although TRPM2 gene expression has been demonstrated in mast cells, the significance of such expression remains virtually unknown. In this study, we found that antigen-stimulated degranulation was significantly reduced in mucosal-type bone marrow-derived mast cells (mBMMCs) prepared from TRPM2-knockout (TRPM2-KO) mice (TRPM2-KO mBMMCs) and was suppressed following the administration of three TRPM2 inhibitors with different chemical structures, including econazole, flufenamic acid (FFA), and 2-aminoethoxydiphenyl borate. Furthermore, the antigen-stimulated increase in [Ca^sup 2+^]^sub cyt^ was significantly decreased in TRPM2-KO mBMMCs and was also suppressed by the TRPM2 inhibitors econazole and FFA. In addition, thapsigargin-induced increase in [Ca^sup 2+^]^sub cyt^ was significantly decreased in TRPM2-KO mBMMCs. These results suggest that TRPM2 may participate in antigen-induced extracellular Ca^sup 2+^ influx and subsequent degranulation. In addition, TRPM2 inhibitors were shown to improve food allergic reactions in a mouse model. Together, these results suggest that TRPM2 inhibitors suppress MMC degranulation via regulation of the increase in [Ca^sup 2+^]^sub cyt^. Thus, TRPM2 may play a key role in degranulation by modulating intracellular Ca^sup 2+^ in MMCs.[PUBLICATION ABSTRACT]
ISSN:0031-6768
1432-2013
DOI:10.1007/s00424-013-1219-y