Bötzinger Expiratory-Augmenting Neurons and the Parafacial Respiratory Group

Fortuna, Michal G.; West, Gavin H.; Stornetta, Ruth L.; Guyenet, Patrice G.

doi:10.1523/jneurosci.5595-07.2008

Cited by 85 publications

(101 citation statements)

References 54 publications

(126 reference statements)

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“…However, microinjection of KYN into BötC did not abolish the AbN response to chemoreflex activation. To explain why the AbN response to chemoreflex activation was not abolished after bilateral microinjections of KYN into the RVLM/BötC, we must take into account the findings by Fortuna et al (2008) showing that some RTN neurons send projections to the retroambiguus region, the site of premotor bulbospinal expiratory neurons. We observed that the average increase in the magnitude of tSN in response to chemoreflex activation was not affected by bilateral microinjections of KYN into the RVLM/pre-BötC.…”

Section: Discussionmentioning

confidence: 99%

Sympathoexcitation during chemoreflex active expiration is mediated byl-glutamate in the RVLM/Bötzinger complex of rats

Moraes

Zoccal

Machado

2012

Journal of Neurophysiology

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Moraes DJ, Zoccal DB, Machado BH. Sympathoexcitation during chemoreflex active expiration is mediated by L-glutamate in the RVLM/Bötzinger complex of rats. J Neurophysiol 108: 610 -623, 2012. First published April 25, 2012 doi:10.1152/jn.00057.2012The involvement of glutamatergic neurotransmission in the rostral ventrolateral medulla/Bötzinger/pre-Bötzinger complexes (RVLM/ BötC/pre-BötC) on the respiratory modulation of sympathoexcitatory response to peripheral chemoreflex activation (chemoreflex) was evaluated in the working heart-brain stem preparation of juvenile rats. We identified different types of baro-and chemosensitive presympathetic and respiratory neurons intermingled within the RVLM/BötC/preBötC. Bilateral microinjections of kynurenic acid (KYN) into the rostral aspect of RVLM (RVLM/BötC) produced an additional increase in frequency of the phrenic nerve (PN: 0.38 Ϯ 0.02 vs. 1 Ϯ 0.08 Hz; P Ͻ 0.05; n ϭ 18) and hypoglossal (HN) inspiratory response (41 Ϯ 2 vs. 82 Ϯ 2%; P Ͻ 0.05; n ϭ 8), but decreased postinspiratory (35 Ϯ 3 vs. 12 Ϯ 2%; P Ͻ 0.05) and late-expiratory (24 Ϯ 4 vs. 2 Ϯ1%; P Ͻ 0.05; n ϭ 5) abdominal (AbN) responses to chemoreflex. Likewise, expiratory vagal (cVN; 67 Ϯ 6 vs. 40 Ϯ 2%; P Ͻ 0.05; n ϭ 5) and expiratory component of sympathoexcitatory (77 Ϯ 8 vs. 26 Ϯ 5%; P Ͻ 0.05; n ϭ 18) responses to chemoreflex were reduced after KYN microinjections into RVLM/BötC. KYN microinjected into the caudal aspect of the RVLM (RVLM/pre-BötC; n ϭ 16) abolished inspiratory responses [PN (n ϭ 16) and HN (n ϭ 6)], and no changes in magnitude of sympathoexcitatory (n ϭ 16) and expiratory (AbN and cVN; n ϭ 10) responses to chemoreflex, producing similar and phase-locked vagal, abdominal, and sympathetic responses. We conclude that in relation to chemoreflex activation 1) ionotropic glutamate receptors in RVLM/BötC and RVLM/preBötC are pivotal to expiratory and inspiratory responses, respectively; and 2) activation of ionotropic glutamate receptors in RVLM/BötC is essential to the coupling of active expiration and sympathoexcitatory response.

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Section: Discussionmentioning

confidence: 99%

Sympathoexcitation during chemoreflex active expiration is mediated byl-glutamate in the RVLM/Bötzinger complex of rats

Moraes

Zoccal

Machado

2012

Journal of Neurophysiology

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“…Consequently, they might be Phox2b-ir cells. A recent study (Fortuna et al, 2008) reported that a population of rostral ventral respiratory neurons (i.e., glycinergic expiratory augmenting neurons) develops a preinspiratory discharge during hypercapnic hypoxia in adult rat in vivo preparations. Despite differences between experimental conditions, these results also support existence of heterogeneous subpopulations of Pre-I neurons in the rostral medulla around the caudal end of the facial nucleus.…”

Section: Characteristics Of Parafacial Neurons In the Ventral Medullamentioning

confidence: 99%

CO₂-Sensitive Preinspiratory Neurons of the Parafacial Respiratory Group Express Phox2b in the Neonatal Rat

Onimaru¹,

Ikeda²,

Kawakami³

2008

J. Neurosci.

145

161

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Phox2b protein is a specific marker for neurons in the parafacial region of the ventral medulla, which are proposed to play a role in central chemoreception and postnatal survival. Mutations of PHOX2B cause congenital central hypoventilation syndrome. However, there have been no reports concerning electrophysiological characteristics of these Phox2b-expressing neurons in the parafacial region of the neonate immediately after birth. This region overlaps with the parafacial respiratory group (pFRG) composed predominantly of preinspiratory (Pre-I) neurons that are involved in respiratory rhythm generation. We studied (1) whether pFRG neurons are Phox2b immunoreactive or not and (2) whether they show intrinsic CO 2 chemosensitivity. We found that most pFRG/Pre-I neurons were Phox2b immunoreactive and depolarized upon increase in CO 2 concentration under condition of action potential-dependent synaptic transmission blockade by tetrodotoxin. We also confirmed that these pFRG neurons expressed neurokinin-1 receptor. They were tyrosine hydroxylase negative and presumed to be glutamatergic. Our findings suggest that Phox2b-expressing parafacial neurons play a role in respiratory rhythm generation as well as central chemoreception and thus are essential for postnatal survival.

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“…Motor activity during late (active) expiration emerges during forced breathing and involves active contraction of abdominal and thoracic expiratory muscle groups. The active or late phase of expiration is always present centrally, but in terms of the motor act of exhalation, it may be only activated during high metabolic demands (Fortuna et al 2008) or after experimental challenges involving intermittent hypoxia (Zoccal et al 2008). However, active expiration under physiological conditions is always preceded by post-I and thus, the alternating phases of inspiration and expiration are largely governed by central oscillations between inspiratory and post-I neurons.…”

Section: The Motor Pattern Of Breathingmentioning

confidence: 99%

Pontine respiratory activity involved in inspiratory/expiratory phase transition

Mörschel

Dutschmann

2009

Phil. Trans. R. Soc. B

100

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Control of the timing of the inspiratory/expiratory (IE) phase transition is a hallmark of respiratory pattern formation. In principle, sensory feedback from pulmonary stretch receptors (BreuerHering reflex, BHR) is seen as the major controller for the IE phase transition, while pontine-based control of IE phase transition by both the pontine Kölliker-Fuse nucleus (KF) and parabrachial complex is seen as a secondary or backup mechanism. However, previous studies have shown that the BHR can habituate in vivo. Thus, habituation reduces sensory feedback, so the role of the pons, and specifically the KF, for IE phase transition may increase dramatically.Pontine-mediated control of the IE phase transition is not completely understood. In the present review, we discuss existing models for ponto-medullary interaction that may be involved in the control of inspiratory duration and IE transition. We also present intracellular recordings of pontine respiratory units derived from an in situ intra-arterially perfused brainstem preparation of rats. With the absence of lung inflation, this preparation generates a normal respiratory pattern and many of the recorded pontine units demonstrated phasic respiratory-related activity. The analysis of changes in membrane potentials of pontine respiratory neurons has allowed us to propose a number of pontine-medullary interactions not considered before. The involvement of these putative interactions in pontine-mediated control of IE phase transitions is discussed.

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Bötzinger Expiratory-Augmenting Neurons and the Parafacial Respiratory Group

Cited by 85 publications

References 54 publications

Sympathoexcitation during chemoreflex active expiration is mediated byl-glutamate in the RVLM/Bötzinger complex of rats

Sympathoexcitation during chemoreflex active expiration is mediated byl-glutamate in the RVLM/Bötzinger complex of rats

CO₂-Sensitive Preinspiratory Neurons of the Parafacial Respiratory Group Express Phox2b in the Neonatal Rat

Pontine respiratory activity involved in inspiratory/expiratory phase transition

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Bötzinger Expiratory-Augmenting Neurons and the Parafacial Respiratory Group

Cited by 85 publications

References 54 publications

Sympathoexcitation during chemoreflex active expiration is mediated byl-glutamate in the RVLM/Bötzinger complex of rats

Sympathoexcitation during chemoreflex active expiration is mediated byl-glutamate in the RVLM/Bötzinger complex of rats

CO2-Sensitive Preinspiratory Neurons of the Parafacial Respiratory Group Express Phox2b in the Neonatal Rat

Pontine respiratory activity involved in inspiratory/expiratory phase transition

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CO₂-Sensitive Preinspiratory Neurons of the Parafacial Respiratory Group Express Phox2b in the Neonatal Rat