Abstract

Dysfunction of the sacral autonomic systems controlling micturition, defecation and copulation is an area of particular concern in the management of patients with spinal injuries or urinary incontinence. The anatomical basis involved in normal pelvic visceral function and the changes in circuitry during postnatal development and following spinal injury have not been adequately explored. The final path of the pelvic autonomic circuitry and the focus of this proposal is the sacral parasympathetic preganglionic (SPP) neuron. The first hypothesis of this proposal is that primary afferent, descending and propriospinal input, each with specific molecular markers, directly synapse on sacral parasympathetic preganglionic neurons. The second hypothesis is that alterations in this circuitry occur during postnatal development and following spinal transection, so that these can be quantified by light and electron microscopic immunohistochemistry. Specifically, the distribution, location, and density of immunostained primary afferent, descending, and propriospinal terminals that synapse on intracellularly labeled sacral parasympathetic preganglionic neurons will be determined. These data will be compared with normal neonatal and adult rats as well as acute and chronic spinal transected adult rats. An understanding of the normal and post-injury changes in the organization of peptidergic or aminergic terminals may lead to new pharmacological approaches to promote the recovery of visceral function in patients with spinal cord injuries or with urinary incontinence.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Program Projects (P01)
Project #
5P01NS011255-21
Application #
3738160
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
21
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Texas Medical Br Galveston
Department
Type
DUNS #
041367053
City
Galveston
State
TX
Country
United States
Zip Code
77555

  Publications

Carter, Michael W; Johnson, Kathia M; Lee, Jun Yeon et al. (2016) Comparison of Mechanical Allodynia and Recovery of Locomotion and Bladder Function by Different Parameters of Low Thoracic Spinal Contusion Injury in Rats. Korean J Pain 29:86-95
Hammell, D C; Zhang, L P; Ma, F et al. (2016) Transdermal cannabidiol reduces inflammation and pain-related behaviours in a rat model of arthritis. Eur J Pain 20:936-48
Young, E E; Bryant, C D; Lee, S E et al. (2016) Systems genetic and pharmacological analysis identifies candidate genes underlying mechanosensation in the von Frey test. Genes Brain Behav 15:604-15
Yuan, Su-Bo; Ji, Guangchen; Li, Bei et al. (2015) A Wnt5a signaling pathway in the pathogenesis of HIV-1 gp120-induced pain. Pain 156:1311-9
Ji, Guangchen; Li, Zhen; Neugebauer, Volker (2015) Reactive oxygen species mediate visceral pain-related amygdala plasticity and behaviors. Pain 156:825-36
Neugebauer, Volker (2015) Amygdala pain mechanisms. Handb Exp Pharmacol 227:261-84
Hassler, Shayne N; Johnson, Kathia M; Hulsebosch, Claire E (2014) Reactive oxygen species and lipid peroxidation inhibitors reduce mechanical sensitivity in a chronic neuropathic pain model of spinal cord injury in rats. J Neurochem 131:413-7
Ji, Guangchen; Neugebauer, Volker (2014) CB1 augments mGluR5 function in medial prefrontal cortical neurons to inhibit amygdala hyperactivity in an arthritis pain model. Eur J Neurosci 39:455-66
Medina, Georgina; Ji, Guangchen; Grégoire, Stéphanie et al. (2014) Nasal application of neuropeptide S inhibits arthritis pain-related behaviors through an action in the amygdala. Mol Pain 10:32
Kiritoshi, Takaki; Sun, Hao; Ren, Wenjie et al. (2013) Modulation of pyramidal cell output in the medial prefrontal cortex by mGluR5 interacting with CB1. Neuropharmacology 66:170-8

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