Synaptically Released and Exogenous ACh Activates Different Nicotinic Receptors to Enhance Evoked Glutamatergic Transmission in the Lateral Geniculate Nucleus

Guo, Jian-Zhong; Liu, Yingbing; Sorenson, Eva M.; Chiappinelli, Vincent A.

doi:10.1152/jn.00339.2005

Cited by 22 publications

(23 citation statements)

References 49 publications

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“…Synaptically released glutamate, serotonin, acetylcholine and other neurotransmitters have been studied in detail (Webster, 2001). However, very little in vivo information has been available about the origin and function of the pool of glutamate (Baker et al, 2002;Timmerman and Westerink, 1997), serotonin (Adell et al, 2002), acetylcholine (David and Pitman, 1982;Descarries et al, 1997;Guo et al, 2005) and other neurotransmitters which appear to be present in micromolar concentrations in the extracellular space outside the synaptic cleft (Nyitrai et al, 2006). Our results support one hypothesis in that extracellular neurotransmitters may be involved in shaping synaptic activity in vivo (Baker et al, 2002;Timmerman and Westerink, 1997;Coggan et al, 2005).…”

Section: G H)supporting

confidence: 79%

Temporal neurotransmitter conditioning restores the functional activity of adult spinal cord neurons in long-term culture

Das

Bhargava

Bhalkikar

et al. 2008

Experimental Neurology

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The ability to culture functional adult mammalian spinal-cord neurons represents an important step in the understanding and treatment of a spectrum of neurological disorders including spinal cord injury. Previously, the limited functional recovery of these cells, as characterized by a diminished ability to initiate action potentials and to exhibit repetitive firing patterns, has arisen as a major impediment to their physiological relevance. In this report we demonstrate that single temporal doses of the neurotransmitters serotonin, glutamate (N-acetyl-DL-glutamic acid) and acetylcholinechloride leads to the full electrophysiological functional recovery of adult mammalian spinal-cord neurons, when they are cultured under defined serum-free conditions. Approximately 60% of the neurons treated regained their electrophysiological signature, often firing single, double and, most importantly, multiple action potentials.

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Section: G H)supporting

confidence: 79%

Temporal neurotransmitter conditioning restores the functional activity of adult spinal cord neurons in long-term culture

Das

Bhargava

Bhalkikar

et al. 2008

Experimental Neurology

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“…Throughout this study, all bath solutions contained 10 μM bicuculline to block GABA A receptor-mediated responses and 50 μM AP5 to block NMDA receptors. Previous work demonstrated that >95% of the optic tract-evoked glutamatergic response under these conditions was mediated by non-NMDA receptors (Guo et al, 2005). Bath application of ACh (100 μM for 2 min) had a biphasic effect on optic tract-evoked PSCs.…”

Section: Resultsmentioning

confidence: 95%

“…Because the optic tract is well-delineated in fresh brain slices, it is possible to selectively stimulate the retinal ganglion cell axons. Optic tract stimulation elicits monosynaptic glutamatergic PSCs in LGNv principal neurons that are mediated almost entirely by non-NMDA receptors, and these evoked responses are increased by exogenous nicotinic agonists (Guo et al, 2005). There is also more direct evidence that the cholinergic fibers within the LGNv modulate retinogeniculate transmission.…”

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confidence: 99%

“…There is also more direct evidence that the cholinergic fibers within the LGNv modulate retinogeniculate transmission. Electrical stimulation of the lateral portion of the LGNv prior to optic-tract stimulation results in a marked enhancement of optic tract-evoked glutamatergic PSCs recorded in principal LGNv neurons (Guo et al, 2005). This enhanced response is completely blocked by nicotinic antagonists, demonstrating that it is due to the stimulated release of endogenous ACh from cholinergic fibers in the LGNv activating nicotinic receptors.…”

mentioning

confidence: 99%

“…This enhanced response is completely blocked by nicotinic antagonists, demonstrating that it is due to the stimulated release of endogenous ACh from cholinergic fibers in the LGNv activating nicotinic receptors. Since neither ACh nor nicotine have any effect on postsynaptic responses to exogenously applied glutamate, the nicotinic receptors mediating enhanced neurotransmission in the LGNv appear to be located on the presynaptic nerve terminals of the retinal ganglion cells (Guo et al, 2005). In these previous functional studies, 1 μM atropine was present throughout the experiments to prevent activation of muscarinic receptors.…”

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confidence: 99%

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Cholinergic modulation of non-N-methyl-d-aspartic acid glutamatergic transmission in the chick ventral lateral geniculate nucleus

2010

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Neurotransmission between glutamatergic terminals of retinal ganglion cells and principal neurons of the ventral lateral geniculate nucleus (LGNv) was examined with patch clamp recordings in chick brain slices during electrical stimulation of the optic tract. Since muscarinic and nicotinic receptors are present in high densities in LGNv, the present study examined possible roles of both receptors in modulating retinogeniculate transmission. During whole-cell recordings from LGNv neurons, acetylcholine (ACh, 100 μM) caused an initial increase in amplitudes of optic tract-evoked non-NMDA glutamatergic postsynaptic currents (PSCs). This increase was unchanged when 1 μM atropine was present, indicating that this initial enhancement of PSCs was due entirely to activation of nicotinic receptors. However, during washout of ACh the amplitudes of evoked PSCs became significantly decreased by 40.4±5.0% for several minutes before recovering to their original amplitudes, an effect blocked by 1 μM atropine. Exogenously applied muscarine (10 μM) markedly depressed optic tract-evoked PSCs, and this decrease in amplitude was blocked by atropine. In a second set of experiments, we examined effects of releasing endogenous ACh prior to optic tract stimulation. This was accomplished by stimulation of the lateral portion of LGNv via a separate conditioning electrode. Following a brief train of low intensity conditioning stimuli, non-NMDA glutamatergic PSCs evoked by optic tract stimulation were potentiated. However, at higher conditioning stimulus intensities the PSCs were markedly decreased compared with control, and this decrease was partially blocked by atropine (1 μM). Neither ACh nor muscarine altered amplitudes of PSCs elicited by exogenously applied glutamate. Muscarine significantly reduced the frequency but not the amplitudes of miniature PSCs, consistent with a presynaptic location for muscarinic receptors mediating these effects. Thus while activation of nicotinic receptors potentiates retinogeniculate transmission, activation of muscarinic receptors mediates depression of transmission, demonstrating a complex cholinergic modulation of sensory information in LGNv.

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Morphology, projection pattern, and neurochemical identity of Cajal's “centrifugal neurons”: The cells of origin of the tectoventrogeniculate pathway in pigeon (Columba livia) and chicken (Gallus gallus)

Vega‐Zuniga

Mpodozis

Karten

et al. 2014

J of Comparative Neurology

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The nucleus geniculatus lateralis pars ventralis (GLv) is a prominent retinal target in all amniotes. In birds, it is in receipt of a dense and topographically organized retinal projection. The GLv is also the target of substantial and topographically organized projections from the optic tectum and the visual wulst (Hyperpallium). Tectal and retinal afferents terminate homotopically within the external GLv-neuropil. Efferents from the GLv follow a descending course through the tegmentum, and can be traced into the medial pontine nucleus. At present, the cells of origin of the Tecto-GLv projection are only partially described. Here we have characterized the laminar location, morphology, projection pattern and neurochemical identity of these cells, by means of neural tracer injections and intracellular fillings in slice preparations and extracellular tracer injections in-vivo. The Tecto-GLv projection arises from a distinct subset of layer 10 bipolar neurons, whose apical dendrites show a complex transverse arborization at the level of layer 7. Axons of these bipolar cells arise from the apical dendrites and follow a course through the optic tract to finally form very fine and restricted terminal endings inside the GLv-neuropil. Double label experiments showed that these bipolar cells were ChAT immunoreactive. Our results strongly suggest that Tecto-GLv neurons form a pathway by which integrated tectal activity rapidly feeds back to the GLv and exerts a focal cholinergic modulation of incoming retinal inputs.

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Synaptically Released and Exogenous ACh Activates Different Nicotinic Receptors to Enhance Evoked Glutamatergic Transmission in the Lateral Geniculate Nucleus

Cited by 22 publications

References 49 publications

Temporal neurotransmitter conditioning restores the functional activity of adult spinal cord neurons in long-term culture

Temporal neurotransmitter conditioning restores the functional activity of adult spinal cord neurons in long-term culture

Cholinergic modulation of non-N-methyl-d-aspartic acid glutamatergic transmission in the chick ventral lateral geniculate nucleus

Morphology, projection pattern, and neurochemical identity of Cajal's “centrifugal neurons”: The cells of origin of the tectoventrogeniculate pathway in pigeon (Columba livia) and chicken (Gallus gallus)

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