Prototypical Imidazoline-1 Receptor Ligand Moxonidine Activates Alpha2-Adrenoceptors in Bulbospinal Neurons of the RVL

Hayar, Abdallah; Guyenet, Patrice G.

doi:10.1152/jn.2000.83.2.766

Cited by 19 publications

(7 citation statements)

References 39 publications

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“…The significant SKF 86466 pretreatment × time interaction effect with the preserved but smaller initial increase in blood pressure in our study suggests that the α 2 ‐antagonist may counteract the clonidine‐evoked hypotension. While this observation is consistent with the study in humans by Hayar & Guyenet (2000), the trend for a hypotensive effect of SKF 86466 ( P = 0.07) in our study does not permit unequivocal acceptance of this interpretation.…”

Section: Discussionsupporting

confidence: 71%

Clonidine‐evoked respiratory effects in anaesthetized rats

Kaczyńska

Szereda-Przestaszewska

2005

Experimental Physiology

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The respiratory effects of stimulation of α 2 -adrenergic receptors were studied in spontaneously breathing anaesthetized rats that were neurally intact, or bilaterally vagotomized, or subjected to bilateral combined midcervical vagotomy and section of the carotid sinus nerves. An intravenous clonidine bolus (15 µg kg -1 ) evoked a prolonged slowing of the respiratory rate in all the neural states explored. Vagotomy reduced the early clonidine-evoked decline, but not the augmentation of tidal volume that followed the decline. After section of the carotid sinus nerves, clonidine challenge continued to decrease the respiratory rate, but not the tidal volume. Blockade of α 2 -adrenergic receptors with intravenous doses of SKF 86466 (200 µg kg -1 ) abolished all respiratory effects of the clonidine challenge. In all the neural states studied, clonidine evoked a significant short-lived rise in mean arterial blood pressure followed by a decrease below the respective prechallenge value. The SKF 86466 pretreatment lowered mean arterial blood pressure control values and reduced the magnitude of postclonidine changes. These results indicate that: (i) clonidine-evoked activation of α 2 -adrenergic receptors affects the two components of the breathing pattern differently, and this occurs beyond the lung vagi; and (ii) changes in tidal volume result from excitation of the carotid bodies and are coupled with centrally mediated slowing of the respiratory rhythm.

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Section: Discussionsupporting

confidence: 71%

Clonidine‐evoked respiratory effects in anaesthetized rats

Kaczyńska

Szereda-Przestaszewska

2005

Experimental Physiology

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“…These results are in agreement with previous studies performed in brain stem slices of neonatal rats [30]. Nevertheless, in that study the authors used either an extracellular recording technique or a whole cell recording technique to study putative premotor sympathetic neurons which were identified mainly as retrogradely labeled RVLM bulbospinal neurons [30]. In our present study putative premotor sympathetic neurons were identified by their electrophysiological characteristics, as described in previous publications [13,25].…”

Section: Granatasupporting

confidence: 93%

“…However, this hypothesis is not supported by the experiments reported by Hayar and Guyenet [30] showing that: (1) moxonidine, at concentrations similar to those used in the present study, produced a consistent inhibitory effect on different types of RVLM neurons recorded in an in vitro slice preparation, and this effect is due in part to postsynaptic hyperpolarization; (2) the inhibitory effects of moxonidine were substantially blocked by the selective antagonist of · 2 -adrenergic receptors SKF 86466, while on the other hand, the imidazoline type-1 antagonist AGN 192403 was ineffective in changing neuronal activity, and (3) the inhibitory effects of moxonidine characterized at pre-and postsynaptic levels are similar to those generated by norepinephrine and other · 2 -adrenergic agonists on putative presympathetic RVLM neurons. Similar results were reported by Szabo et al [31] in experiments performed on the rat locus coeruleus neurons in vitro.…”

Section: Granatamentioning

confidence: 66%

Effect of Moxonidine on Putative Sympathetic Neurons in the Rostral Ventrolateral Medulla of the Rat

Granata

2004

Neurosignals

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We used an intracellular recording technique in vitro to investigate the effects of moxonidine on neurons in the rostral ventrolateral medulla (RVLM) with electrophysiological properties similar to premotor sympathetic neurons in vivo. These neurons were classified as firing regularly and irregularly, according to previous reports. Moxonidine is a sympathoinhibitory and antihypertensive agent that is thought to be a ligand of α₂-adrenergic receptors and imidazoline type-1 receptors in the RVLM. Moxonidine (2–10 µM) was applied to the perfusate on 4 irregularly firing neurons, and 2 regularly firing neurons. Moxonidine (2 µM) produced only minor depolarization in 2 of these neurons. However, on 4 tested neurons, moxonidine (10 µM) elicited a profound inhibitory effect with hyperpolarization (near –20 mV); these neurons practically ceased firing. These changes were partially reversible. The results would indicate that neurons in the RVLM, recorded in vitro and with similar electrophysiological characteristics to a group of neurons previously identified in vivo in the same bulbar region as barosensitive premotor sympathetic neurons, can be modulated by imidazoline-derivative adrenergic agonists. These results could help to understand the hypotensive effects of moxonidine.

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“…Nevertheless, its weak affinity for ␣2-adrenergic receptors (Ferry et al, 1988;Ernsberger et al, 1993) may have accounted for the observed inhibition of IPSCs. Hayar and Guyenet (2000) revealed that inhibition of both EPSCs and IPSCs by moxonidine in bulbospinal neurons of the rostral ventrolateral medulla is mediated via ␣2-adrenergic receptors. Indeed, in the present study, application of noradrenaline under blockade of both ␣1-and ␤-adrenergic receptors with prazosin and propranolol, respectively, resulted in ␣2-adrenergic receptor-mediated inhibition of IPSCs, as was demonstrated by the apparent lack of inhibition by noradrenaline when combined with either yohimbine or SKF86466, which are non-imidazoline antagonists selective for ␣2-adrenergic receptors.…”

Section: -Imidazoline Receptors Mediate Moxonidine-induced Inhibimentioning

confidence: 99%

Presynaptic I₁-Imidazoline Receptors Reduce GABAergic Synaptic Transmission in Striatal Medium Spiny Neurons

et al. 2006

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Imidazoline receptors are expressed widely in the CNS. In the present study, whole-cell patch-clamp recordings were made from medium spiny neurons in dorsal striatum slices from the rat brain, and the roles of I 1 -imidazoline receptors in the modulation of synaptic transmission were studied. Moxonidine, an I 1 -imidazoline receptor agonist, decreased the GABA A receptor-mediated IPSCs in a concentration-dependent manner. However, glutamate-mediated EPSCs were hardly affected. The depression of IPSCs by moxonidine was antagonized by either idazoxan or efaroxan, which are both imidazoline receptor antagonists containing an imidazoline moiety. In contrast, yohimbine and SKF86466 (6-chloro-2,3,4,5-tetrahydro-3-methyl-1H-3-benzazepine), which are ␣2-adrenergic receptor antagonists with no affinity for imidazoline receptors, did not affect the moxonidine-induced inhibition of IPSCs. Moxonidine increased the paired-pulse ratio and reduced the frequency of miniature IPSCs without affecting their amplitude, indicating that this agent inhibits IPSCs via presynaptic mechanisms. Moreover, the sulfhydryl alkylating agent N-ethylmaleimide (NEM) significantly reduced the moxonidine-induced inhibition of IPSCs. Thus, the activation of presynaptic I 1 -imidazoline receptors decreases GABA-mediated inhibition of medium spiny neurons in the striatum, in which NEM-sensitive proteins such as G i/o -type G-proteins play an essential role. The adenylate cyclase activator forskolin partly opposed IPSC inhibition elicited by subsequently applied moxonidine. Furthermore, the protein kinase C (PKC) activator phorbol 12,13-dibutyrate attenuated and the PKC inhibitor chelerythrine potentiated the moxonidineinduced inhibition of IPSCs. These results suggest that IPSC inhibition via presynaptic I 1 -imidazoline receptors involves intracellular adenylate cyclase activity and is influenced by static PKC activity in the striatum.

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Prototypical Imidazoline-1 Receptor Ligand Moxonidine Activates Alpha2-Adrenoceptors in Bulbospinal Neurons of the RVL

Cited by 19 publications

References 39 publications

Clonidine‐evoked respiratory effects in anaesthetized rats

Clonidine‐evoked respiratory effects in anaesthetized rats

Effect of Moxonidine on Putative Sympathetic Neurons in the Rostral Ventrolateral Medulla of the Rat

Presynaptic I₁-Imidazoline Receptors Reduce GABAergic Synaptic Transmission in Striatal Medium Spiny Neurons

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Prototypical Imidazoline-1 Receptor Ligand Moxonidine Activates Alpha2-Adrenoceptors in Bulbospinal Neurons of the RVL

Cited by 19 publications

References 39 publications

Clonidine‐evoked respiratory effects in anaesthetized rats

Clonidine‐evoked respiratory effects in anaesthetized rats

Effect of Moxonidine on Putative Sympathetic Neurons in the Rostral Ventrolateral Medulla of the Rat

Presynaptic I1-Imidazoline Receptors Reduce GABAergic Synaptic Transmission in Striatal Medium Spiny Neurons

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Presynaptic I₁-Imidazoline Receptors Reduce GABAergic Synaptic Transmission in Striatal Medium Spiny Neurons