Abstract

The overall objective of the research of program is the clarification of trigeminal nociceptive mechanisms, especially in the brainstem, related to acute and chronic pain conditions that afflict the face and mouth. Our recent NIH-supported studies, which have produced 10 papers and 7 abstracts in 1981 and 1982, have helped provide some of the insights into the brainstem mechanisms involved in dental and facial pain in particular. Major gaps or uncertainties in our knowledge however still exist in the neural mechanisms underlying dental, joint and muscle pain especially and in the processes associated with pain conditions that may be related to muscle dysfunction (e.g. TMJ or myofascial pain dysfunction syndrome) or to sensory loss (e.g. painful sensory neuropathies, neuralgias, causalgias). We will use our expertise and experience gained over the last 18 years with the trigeminal system of the cat and monkey and continue to examine functionally identified single noticeptive and nonnociceptive neurons recorded electrophysiologically in the trigeminal spinal tract nucleus of the cat. In particular, we now propose to determine which types of neurons relay joint and musle nociceptive information and to study the response properties and convergent patterns seen in these neurons with stimulation of muscle, joint and other orofacial afferents (Aim i); to determine if these responses can be modulated by other sensory inputs and by descending influences from brainstem, cortex and thalamic sites implicated in pain and analgesia and gain insights into the underlying neurochemical mechanisms by studying the effects on the modulatory influences of antagonists to the possible neurochemicals involved (Aim ii); and continue to investigate the effects of sensory loss on the functional organization of these neurons by delineating further the changes in their functional properties that we have shown to occur with tooth pulp extirpation and comparing them with likely changes that may be induced by deafferentation of other orofacial structures or interruption of the modulatory interaction that has been demonstrated between different components of the nucleus (Aim iii). We anticipate that our findings will lead to future studies in kittens and chronic recording investigations in adult animals to examine maturational and behavioral changes that may be associated with orofacial sensory alterations.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Project (R01)
Project #
5R01DE004786-12
Application #
3219146
Study Section
Communication Sciences and Disorders (CMS)
Project Start
1978-01-01
Project End
1990-09-14
Budget Start
1989-01-01
Budget End
1990-09-14
Support Year
12
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
University of Toronto
Department
Type
DUNS #
259999779
City
Toronto
State
ON
Country
Canada
Zip Code
M5 1S8

  Publications

Yao, Dongyuan; Yoshida, Mitsuhiro; Sessle, Barry J (2015) Dura-evoked neck muscle activity involves purinergic and N-methyl-D-aspartate receptor mechanisms. Neuroreport 26:1155-60
Wang, Hua; Cao, Ye; Chiang, Chen-Yu et al. (2014) The gap junction blocker carbenoxolone attenuates nociceptive behavior and medullary dorsal horn central sensitization induced by partial infraorbital nerve transection in rats. Pain 155:429-35
Cao, Ye; Wang, Hua; Chiang, Chen-Yu et al. (2013) Pregabalin suppresses nociceptive behavior and central sensitization in a rat trigeminal neuropathic pain model. J Pain 14:193-204
Matsuura, Shingo; Shimizu, Kohei; Shinoda, Masamichi et al. (2013) Mechanisms underlying ectopic persistent tooth-pulp pain following pulpal inflammation. PLoS One 8:e52840
Wang, H; Xie, Y F; Chiang, C Y et al. (2013) Central ?-adrenoceptors contribute to mustard oil-induced central sensitization in the rat medullary dorsal horn. Neuroscience 236:244-52
Cao, Ye; Li, Kai; Fu, Kai-Yuan et al. (2013) Central sensitization and MAPKs are involved in occlusal interference-induced facial pain in rats. J Pain 14:793-807
Kumar, Naresh; Cherkas, Pavel S; Varathan, Vidya et al. (2013) Systemic pregabalin attenuates facial hypersensitivity and noxious stimulus-evoked release of glutamate in medullary dorsal horn in a rodent model of trigeminal neuropathic pain. Neurochem Int 62:831-5
Kiyomoto, Masaaki; Shinoda, Masamichi; Okada-Ogawa, Akiko et al. (2013) Fractalkine signaling in microglia contributes to ectopic orofacial pain following trapezius muscle inflammation. J Neurosci 33:7667-80
Narita, N; Kumar, N; Cherkas, P S et al. (2012) Systemic pregabalin attenuates sensorimotor responses and medullary glutamate release in inflammatory tooth pain model. Neuroscience 218:359-66
Kumar, Naresh; Cherkas, Pavel S; Chiang, C Y et al. (2012) Involvement of ATP in noxious stimulus-evoked release of glutamate in rat medullary dorsal horn: a microdialysis study. Neurochem Int 61:1276-9

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