Transient fusion ensures granule replenishment to enable repeated release after IgE-mediated mast cell degranulation

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Abstract

To ensure normal immune function, mast cells employ different pathways to release mediators. Here, we report a thus far unknown capacity of mast cells to recycle and reuse secretory granules after an antigen-evoked degranulation process under physiological conditions; this phenomenon involves the existence of a recycling secretory granule pool that is available for release in a short time scale. Rapid endocytic modes contributed to the recycling of ~60% of the total secretory granule population, which involved kiss-and-run and cavicapture mechanisms, causing retention of the intragranular matrix. We found the presence of normal-size granules and giant actomyosin- and dynamin-dependent granules, which were characterized by large quantal content. These large structures allowed the recovered mast cells to release a large amount of 5-HT, compensating for the decrease in the number of exocytosed secretory granules. This work uncovers a new physiological role of the exo-endocytosis cycle in the immunological plasticity of mast cells and reveals a new property of their biological secretion.

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APA

Balseiro-Gomez, S., Flores, J. A., Acosta, J., Ramirez-Ponce, M. P., & Ales, E. (2016). Transient fusion ensures granule replenishment to enable repeated release after IgE-mediated mast cell degranulation. Journal of Cell Science, 129(21), 3989–4000. https://doi.org/10.1242/jcs.194340

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