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J Physiol Volume 525, Number 1, 143-158, May 15, 2000
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The Journal of Physiology (2000), 525.1, pp. 143-158
© Copyright 2000 The Physiological Society

Co-release of ATP and ACh mediates hypoxic signalling at rat carotid body chemoreceptors

Min Zhang, Huijun Zhong, Cathy Vollmer and Colin A. Nurse

Department of Biology, McMaster University, Hamilton, Ontario, Canada L8S 4K1

  1. Using functional co-cultures of rat carotid body (CB) O2 chemoreceptors and 'juxtaposed' petrosal neurones (JPNs), we tested whether ATP and ACh acted as co-transmitters.

  2. Perforated-patch recordings from JPNs often revealed spontaneous and hypoxia-evoked (PO2~5 mmHg) excitatory postsynaptic responses. The P2X purinoceptor blocker, suramin (50 µM) or a nicotinic ACh receptor (nAChR) blocker (hexamethonium, 100 µM; mecamylamine, 1 µM) only partially inhibited these responses, but together, blocked almost all activity.

  3. Under voltage clamp (-60 mV), fast perfusion of 100 µM ATP over hypoxia-responsive JPNs induced suramin-sensitive (IC50 = 73 µM), slowly-desensitizing, inward currents (IATP) with time constant of activation tauon = 30·6 ± 4·8 ms (n = 7). IATP reversed at 0·33 ± 3·7 mV (n = 4), and the dose-response curve was fitted by the Hill equation (EC50 = 2·7 µM; Hill coefficient ~0·9). These purinoceptors contained immunoreactive P2X2 subunits, but their activation by alpha,beta-methylene ATP (alpha,beta-meATP; EC50 = 2·1 µM) suggests they are P2X2/P2X3 heteromultimers.

  4. Suramin and nAChR blockers inhibited the extracellular chemosensory discharge in the intact rat carotid body-sinus nerve preparation in vitro. Further, P2X2 immunoreactivity was widespread in rat petrosal ganglia in situ, and co-localized in neurones expressing the CB chemo-afferent marker, tyrosine hydroxylase (TH). P2X2 labelling in the CB co-localized with nerve-terminal markers, and was intimately associated with TH-positive type 1 cells.

  5. Thus ATP and ACh are co-transmitters during chemotransduction in the rat carotid body.



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