REM sleep burst neurons, PGO waves, and eye movement information

Nelson, John P.; McCarley, R.W.; Hobson, J. Allan

doi:10.1152/jn.1983.50.4.784

Cited by 180 publications

(82 citation statements)

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“…Their inhibition by acetylcholine during REM sleep will de-inactivate their low-threshold calcium current and allow them to fire single spikes or a burst of action potentials when receiving excitatory input, which may originate from long-lead PGO related neurons in the dorsal mPRF (McCarley and Ito, 1983;Pare et al, 1990) and/or the caudoventral pontine tegmentum (Vanni-Mercier and Debilly, 1998). In the cat, PGO burst neurons with a short lead time (< 100 ms) prior to P-waves have been recorded in the parabrachial region which borders and overlaps with the subcoeruleus area recorded in this study in the rat (McCarley et al, 1978;Sakai and Jouvet, 1980;Nelson et al, 1983;Steriade et al, 1990;Datta and Hobson, 1994). Although neurons with these properties have also been recorded in other areas of the brainstem reticular formation, they seem to be particularly concentrated in the SubC area, which is consistent with this area being the best site to record P-waves Farber et al, 1980;Kaufman and Morrison, 1981) and the most sensitive site for carbachol to cause an enhancement of P-wave frequency (Datta et al, 1998).…”

Section: Responses To Carbacholsupporting

confidence: 59%

Electrophysiological characterization of neurons in the dorsolateral pontine rapid-eye-movement sleep induction zone of the rat: Intrinsic membrane properties and responses to carbachol and orexins

et al. 2006

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Pharmacological, lesion and single-unit recording techniques in several animal species have identified a region of the pontine reticular formation (Subcoeruleus, SubC) just ventral to the locus coeruleus as critically involved in the generation of rapid-eye-movement (REM) sleep. However, the intrinsic membrane properties and responses of SubC neurons to neurotransmitters important in REM sleep control, such as acetylcholine and orexins/hypocretins, have not previously been examined in any animal species and thus were targeted in this study.We obtained whole-cell patch-clamp recordings from visually identified SubC neurons in rat brain slices in vitro. Two groups of large neurons (mean diameter 30 and 27μm) were tentatively identified as cholinergic (rostral SubC) and noradrenergic (caudal SubC) neurons. SubC reticular neurons (noncholinergic, non-noradrenergic) showed a medium-sized depolarizing sag during hyperpolarizing current pulses and often had a rebound depolarization (low-threshold spike, LTS). During depolarizing current pulses they exhibited little adaptation and fired maximally at 30-90 Hz. Those SubC reticular neurons excited by carbachol (n=27) fired spontaneously at 6 Hz, often exhibited a moderately sized LTS, and varied widely in size (17-42 μm). Carbachol-inhibited SubC reticular neurons were medium-sized (15-25 μm) and constituted two groups. The larger group (n=22) was silent at rest and possessed a prominent LTS and associated 1-4 action potentials. The second, smaller group (n=8) had a delayed return to baseline at the offset of hyperpolarizing pulses. Orexins excited both carbachol excited and carbachol inhibited SubC reticular neurons.SubC reticular neurons had intrinsic membrane properties and responses to carbachol similar to those described for other reticular neurons but a larger number of carbachol inhibited neurons were found (> 50 %), the majority of which demonstrated a prominent LTS and may correspond to PGO-on neurons. Some or all carbachol-excited neurons are presumably REM-on neurons.Keywords rapid-eye-movement; whole-cell; in vitro; sublaterodorsal; hypocretin; narcolepsy NIH-PA Author ManuscriptNIH-PA Author Manuscript NIH-PA Author ManuscriptAbbreviations ACSF Artificial cerebrospinal fluid; AHP Afterhyperpolarization; AP Action potential; CARB Carbachol; CARB-E Carbachol excited; CARB-I Carbachol inhibited; CCD Charge coupled device; ChAT Choline acetyltransferase; DAB Diaminobenzidine; DC Direct current; GABA Gammaamino-butyric acid; GAD67 glutamic acid decarboxylase 67 kDa isoform; HCN Hyperpolarization activated and cyclic nucleotide gated cation channels; IACUC Institutional Animal Care and Use committee; IR-DIC Infra-red differential interference contrast; LC locus coeruleus; LDT laterodorsal tegmental nucleus; LTS low-threshold spike; mPRF medial pontine reticular formation; nNOS neuronal nitric oxide synthase; Ox A Orexin A; PGO pontine-geniculate-occipital waves; PnC pontine nucleus caudalis; PnO pontine nucleus oralis; P waves Pontine component of PGO wave...

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Section: Responses To Carbacholsupporting

confidence: 59%

Electrophysiological characterization of neurons in the dorsolateral pontine rapid-eye-movement sleep induction zone of the rat: Intrinsic membrane properties and responses to carbachol and orexins

et al. 2006

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“…PGO pontine pathways project through the tegmentum and communicate with the L/MVN, providing evidence, as do our results, of involvement of the vestibular system in the generation of PGO waves [58]. Additionally, there is agreement from physiological, pharmacological, and lesion studies that PGO-on neurons in the pontine tegmentum are considered to be the final transferring output components of the PGO generator network [15,60,85]. This is a relevant point, since even dramatic conditions such as labyrinthectomy, that significantly changes the spontaneous firing rate of L/MVN neurons, do not modify c-fos expression in the L/MVN [12], whereas we find that LTPE does.…”

Section: Molecular and Network Implications Of Regional C-fos Expressionsupporting

confidence: 82%

From synapse to gene product: prolonged expression of c-fos induced by a single microinjection of carbachol in the pontomesencephalic tegmentum

Quattrochi

Bazalakova

Hobson

2005

Molecular Brain Research

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It is not known how the brain modifies its regulatory systems in response to the application of a drug, especially over the long term of weeks and months. We have developed a model system approach to this question by manipulating cholinergic cell groups of the laterodorsal and pedunculopontine tegmental (LDT/PPT) nuclei in the pontomesencephalic tegmentum (PMT), which are known to be actively involved in the timing and quantity of rapid eye movement (REM) sleep. In a freely moving feline model, a single microinjection of the cholinergic agonist carbachol conjugated to a latex nanosphere delivery system into the caudolateral PMT elicits a long-term enhancement of one distinguishing phasic event of REM sleep, ponto-geniculo-occipital (PGO) waves, lasting 5 days but without any significant change in REM sleep or other behavioral state. Here, we test the hypothesis that cholinergic activation within the caudolateral PMT alters the postsynaptic excitability of the PGO network, stimulating the prolonged expression of c-fos that underlies this long-term PGO enhancement (LTPE) effect. Using quantitative Fos immunohistochemistry, we found that the number of Fos-immunoreactive (Fos-IR) neurons surrounding the caudolateral PMT injection site decreased sharply by postcarbachol day 03, while the number of Fos-IR neurons in the more rostral LDT/PPT increased >30-fold and remained at a high level following the course of LTPE. These results demonstrate a sustained c-fos expression in response to pharmacological stimulation of the brain and suggest that carbachol's acute effects induce LTPE via cholinergic receptors, with subsequent transsynaptic activation of the LDT/PPT maintaining the LTPE effect.

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“…Furthermore, the temporal relation of PGO waves to REMs across species is also not clear yet. That is, whereas REMs are highly correlated with PGO-waves in the cat (Nelson et al 1983;Datta and Hobson 1994), PGO-waves in humans are incompletely associated with REMs (Lim et al 2007). The present study emphasizes that further research will be needed to more fully understand the functional neuroanatomy of PGO waves and REMs across species.…”

Section: Activation Accompanying Remmentioning

confidence: 99%

Human brain activity time-locked to rapid eye movements during REM sleep

et al. 2008

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To identify the neural substrate of rapid eye movements (REMs) during REM sleep in humans, we conducted simultaneous functional magnetic resonance imaging (fMRI) and polysomnographic recording during REM sleep. Event-related fMRI analysis time-locked to the occurrence of REMs revealed that the pontine tegmentum, ventroposterior thalamus, primary visual cortex, putamen and limbic areas (the anterior cingulate, parahippocampal gyrus and amygdala) were activated in association with REMs. A control experiment during which subjects made self-paced saccades in total darkness showed no activation in the visual cortex. The REM-related activation of the primary visual cortex without visual input from the retina provides neural evidence for the existence of human pontogeniculo-occipital waves (PGO waves) and a link between REMs and dreaming. Furthermore, the time-course analysis of blood oxygenation level-dependent responses indicated that the activation of the pontine tegmentum, ventroposterior thalamus and primary visual cortex started before the occurrence of REMs. On the other hand, the activation of the putamen and limbic areas accompanied REMs. The activation of the parahippocampal gyrus and amygdala simultaneously with REMs suggests that REMs and/or their generating mechanism are not merely an epiphenomenon of PGO waves, but may be linked to the triggering activation of these areas.

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REM sleep burst neurons, PGO waves, and eye movement information

Cited by 180 publications

References 0 publications

Electrophysiological characterization of neurons in the dorsolateral pontine rapid-eye-movement sleep induction zone of the rat: Intrinsic membrane properties and responses to carbachol and orexins

Electrophysiological characterization of neurons in the dorsolateral pontine rapid-eye-movement sleep induction zone of the rat: Intrinsic membrane properties and responses to carbachol and orexins

From synapse to gene product: prolonged expression of c-fos induced by a single microinjection of carbachol in the pontomesencephalic tegmentum

Human brain activity time-locked to rapid eye movements during REM sleep

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