Spino‐bulbo‐spinal pathway mediating vagal modulation of nociceptive‐neuroendocrine control of inflammation in the rat

Miao, Frederick Jia‐Pei; Jänig, Wilfrid; Jasmin, Luc; Levine, Jon D.

doi:10.1111/j.1469-7793.2001.0811e.x

Cited by 25 publications

(1 citation statement)

References 39 publications

(73 reference statements)

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“…This unexpected reduction of microglial activity may be explained by vagal inhibition of spinal sensory signaling. It has been previously demonstrated that vagal activity influences a pathway of descending inhibition from the hindbrain—presumably the NTS—to the spinal afferent terminals in the dorsal horns of the SC [30;31]. The subdiaphragmatic vagotomy performed in our study would disrupt the same descending pathway.…”

Section: Discussionsupporting

confidence: 52%

Changes in microglial activation within the hindbrain, nodose ganglia, and the spinal cord following subdiaphragmatic vagotomy

Gallaher

Ryu

Herzog

et al. 2012

Neuroscience Letters

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Damage to peripheral nerve branches triggers activation of microglia in CNS areas containing motor neuron soma and primary afferent terminals of the damaged fibers. Furthermore, microglial activation occurs in areas containing the soma and terminals of spared nerve branches of a damaged nerve. Because the abdominal viscera are innervated by spinal afferents as well as vagal afferents and efferents, we speculated that spinal nerves might respond like spared nerve branches following damage to vagal fibers. Therefore, we tested the hypothesis that damage to the abdominal vagus would result in microglial activation in vagal structures—the nucleus of the solitary tract (NTS), dorsal motor nucleus of the vagus nerve (DMV), and nodose ganglia (NG)—as well as spinal cord (SC) segments that innervate the abdominal viscera. To test this hypothesis, rats underwent subdiaphragmatic vagotomy or sham surgery and were treated with saline or the microglial inhibitor, minocycline. Microglial activation was determined by quantifying changes in the intensity of fluorescent staining with a primary antibody against ionizing calcium adapter binding molecule 1 (Iba1). We found that subdiaphragmatic vagotomy significantly activated microglia in the NTS, DMV, and NG two weeks post-vagotomy. Microglial activation remained significantly increased in the NG and DMV for at least 42 days. Surprisingly, vagotomy significantly decreased microglial activation in the SC. Minocycline treatment attenuated microglial activation in all studied areas. Our results indicate that microglial activation in vagal structures following abdominal vagal damage is accompanied by suppression of microglial activation in associated areas of the spinal cord.

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Section: Discussionsupporting

confidence: 52%