Autocrine activation of P2Y1 receptors couples Ca2+ influx to Ca2+ release in human pancreatic beta cells

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Abstract

Aims/hypothesis There is evidence that ATP acts as an auto-crine signal in beta cells but the receptors and pathways involved are incompletely understood. Here we investigate the receptor subtype(s) and mechanism(s) mediating the effects of ATP on human beta cells. Methods We examined the effects of purinergic agonists and antagonists on membrane potential, membrane currents, intra-cellular Ca2+ ([Ca2+]i) and insulin secretion in human beta cells. Results Extracellular application of ATP evoked small inward currents (3.4±0.7 pA) accompanied by depolarisation of the membrane potential (by 14.4±2.4 mV) and stimulation of electrical activity at 6 mmol/l glucose. ATP increased [Ca2+]iby stimulating Ca2+ influx and evoking Ca2+ release via InsP3-receptors in the endoplasmic reticulum (ER). ATP-evoked Ca2+ release was sufficient to trigger exocytosis in cells voltage-clamped at -70 mV. All effects of ATP were mimicked by the P2Y(1/12/13) agonist ADP and the P2Y1 agonist MRS-2365, whereas the P2X(1/3) agonist α,β-methyleneadenosine-5-triphosphate only had a small effect. The P2Y1 antagonists MRS-2279 and MRS-2500 hyperpolarised glucose-stimulated beta cells and lowered [Ca2+]i in the absence of exogenously added ATP and inhibited glucose-induced insulin secretion by 35%. In voltage-clamped cells subjected to action potential-like stimulation, MRS-2279 decreased [Ca2+]i and exocytosis without affecting Ca2+ influx. Conclusions/interpretation These data demonstrate that ATP acts as a positive autocrine signal in human beta cells by activating P2Y1 receptors, stimulating electrical activity and coupling Ca2+ influx to Ca2+ release from ER stores.

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Khan, S., Yan-Do, R., Duong, E., Wu, X., Bautista, A., Cheley, S., … Braun, M. (2014). Autocrine activation of P2Y1 receptors couples Ca2+ influx to Ca2+ release in human pancreatic beta cells. Diabetologia, 57(12), 2535–2545. https://doi.org/10.1007/s00125-014-3368-8

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