Literature DB >> 9089789

Receptors controlling transmitter release from sympathetic neurons in vitro.

S Boehm1, S Huck.   

Abstract

Primary cultures of postganglionic sympathetic neurons were established more than 30 years ago. More recently, these cultures have been used to characterize various neurotransmitter receptors that govern sympathetic transmitter release. These receptors may be categorized into at least three groups: (1) receptors which evoke transmitter release: (2) receptors which facilitate; (3) receptors which inhibit, depolarization-evoked release. Group (1) comprises nicotinic and muscarinic acetylcholine receptors, P2X purinoceptors and pyrimidinoceptors. Group (2) currently harbours beta-adrenoceptors, P2 purinoceptors, receptors for PACAP and VIP, as well as prostanoid EP1 receptors. In group (3), muscarinic cholinoceptors, alpha 2- and beta-adrenoceptors, P2 purinoceptors, and receptors for the neuropeptides NPY, somatostatin (SRIF1) and LHRH, as well as opioid (delta and kappa) receptors can be found. Receptors which regulate transmitter release from neurons in cell culture may be located either at the somatodendritic region or at the sites of exocytosis, i.e. the presynaptic specializations of axons. Most of the receptors that evoke release are located at the soma. There ionotropic receptors cause depolarizations to generate action potentials which then trigger Ca(2+)-dependent exocytosis at axon terminals. The signalling mechanisms of metabotropic receptors which evoke release still remain to be identified. Receptors which facilitate depolarization-evoked release appear to be located preferentially at presynaptic sites and presumably act via an increase in cyclic AMP. Receptors which inhibit stimulation evoked release are also presynaptic origin and most commonly rely on a G protein-mediated blockade of voltage-gated Ca2+ channels. Results obtained with primary cell cultures of postganglionic sympathetic neurons have now supplemented previous data about neurotransmitter receptors involved in the regulation of ganglionic as well as sympatho-effector transmission. In the future, this technique may prove useful to identify yet unrecognized receptors which control the output of the sympathetic nervous system and to elucidate underlying signalling mechanisms.

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Year:  1997        PMID: 9089789     DOI: 10.1016/s0301-0082(96)00056-1

Source DB:  PubMed          Journal:  Prog Neurobiol        ISSN: 0301-0082            Impact factor:   11.685


  10 in total

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Review 2.  Regulation of feeding-associated peptides and receptors by nicotine.

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Authors:  S Boehm; R J Harvey; A von Holst; H Rohrer; H Betz
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6.  Activation of M1 muscarinic receptors triggers transmitter release from rat sympathetic neurons through an inhibition of M-type K+ channels.

Authors:  Stefan G Lechner; Martina Mayer; Stefan Boehm
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7.  ATP stimulates sympathetic transmitter release via presynaptic P2X purinoceptors.

Authors:  S Boehm
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8.  Endocannabinoids mediate muscarine-induced synaptic depression at the vertebrate neuromuscular junction.

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9.  P2 receptors in cardiovascular regulation and disease.

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10.  Electrophysiological Investigation of the Subcellular Fine Tuning of Sympathetic Neurons by Hydrogen Sulfide.

Authors:  Manuel Dominguez-Rodriguez; Helmut Drobny; Stefan Boehm; Isabella Salzer
Journal:  Front Pharmacol       Date:  2017-08-04       Impact factor: 5.810

  10 in total

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