2018
DOI: 10.7554/elife.30839
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Activity-induced Ca2+ signaling in perisynaptic Schwann cells of the early postnatal mouse is mediated by P2Y1 receptors and regulates muscle fatigue

Abstract: Perisynaptic glial cells respond to neural activity by increasing cytosolic calcium, but the significance of this pathway is unclear. Terminal/perisynaptic Schwann cells (TPSCs) are a perisynaptic glial cell at the neuromuscular junction that respond to nerve-derived substances such as acetylcholine and purines. Here, we provide genetic evidence that activity-induced calcium accumulation in neonatal TPSCs is mediated exclusively by one subtype of metabotropic purinergic receptor. In P2ry1 mutant mice lacking t… Show more

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Cited by 25 publications
(38 citation statements)
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“…This blockade was reversible because Ca 2+ elevations were induced after a 20-min washout of the drug (300.20% ± 12.00% DF/F0, n = 20 PSCs; paired t test, p < 0.0001). This is consistent with recent work showing that purine-induced PSC Ca 2+ responses are mediated exclusively by P2Y1Rs (Heredia et al, 2018) and further confirms that ATP-dependent activation of PSCs is mediated by P2Y1Rs.…”
Section: Synaptic Potentiation Is Mediated By Psc P2y1rs and Presynapsupporting
confidence: 93%
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“…This blockade was reversible because Ca 2+ elevations were induced after a 20-min washout of the drug (300.20% ± 12.00% DF/F0, n = 20 PSCs; paired t test, p < 0.0001). This is consistent with recent work showing that purine-induced PSC Ca 2+ responses are mediated exclusively by P2Y1Rs (Heredia et al, 2018) and further confirms that ATP-dependent activation of PSCs is mediated by P2Y1Rs.…”
Section: Synaptic Potentiation Is Mediated By Psc P2y1rs and Presynapsupporting
confidence: 93%
“…These results using single-cell electroporation are similar to those using bulk loading of the Ca 2+ indicator in PSCs (Darabid et al, 2013). Moreover, PSCs also responded to the local application of ATP (5 mM; Figure 1C; 131.50% ± 48.19% DF/F0; N = 4), which is the main neurotransmitter activating PSCs at developing NMJs (Darabid et al, 2013;Heredia et al, 2018) and is commonly used to assess PSC excitability and health (Arbour et al, 2015;Darabid et al, 2013;Rochon et al, 2001). Altogether, these results confirm that PSCs at a dually innervated NMJ decode synaptic competition and that PSCs can be targeted specifically by single-cell electroporation without undesired effects.…”
Section: Pscs Decode Synaptic Competitionsupporting
confidence: 71%
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