Abstract

The long-term objectives of this project are to determine the role of craniofacial sensory feedback in normal function and to determine how these processes are altered in oro-facial dysfunctions including bruxism, masticatory muscle and temporomandibular disorders. Three hypotheses are proposed: 1) Trigeminal ganglion jaw muscle and joint primary afferent neurons comprise two general categories with brainstem axonal projections correlated to their functional modalities. Hypothesis 1 will be tested by characterizing the physiological and morphological properties of these neurons using in vivo intracellular recording and staining. 2) Sensory feedback from non-spindle muscle and joint afferents is relayed directly to trigeminothalamic, trigeminohypothalamic, trigemino-parabrachial, trigeminospinal and trigeminal premotor neurons. These pathways are expected to convey discriminative, autonomic and emotional aspects of orofacial nociception; as well as innocuous proprioceptive and autonomic sensory feedback. Hypothesis 2 will be tested by characterizing neuronal circuitry from trigeminal ganglion muscle and joint afferents to brainstem neurons by combining in vivo retrograde and intracellular neuronal labeling. 3) Transmission from trigeminal ganglion neurons relaying feedback from muscle and joint to brainstem neurons can be modulated via presynaptic mechanisms. It is also predicted that primary afferent depolarization (PAD) and centrifugal action potentials can be evoked in these afferent axons which may induce neurogenic inflammation. Hypothesis 3 will be tested by determining if the anatomical substrate for presynaptic modulation of non-spindle muscle and jaw joint afferent terminals is present using intracellular labeling, confocal and electron microscopy. This hypothesis will also be tested by directly monitoring the membrane potential in primary afferent axons using in vivo intra-axonal recording during electrical and chemical stimulation of orofacial tissues. Mechanisms of PAD will be explored using GABAA and GABAB agonists and antagonists. Data from experiments in this proposal will provide better understanding of the morphology and physiology of deep orofacial primary afferent neurons and their brainstem circuitry. This knowledge will not only lead to a better understanding of brain mechanisms but is needed to develop rational treatment strategies for managing musculoskeletal and orofacial disorders. These data will also be used to investigate potential gender differences in the morphological substrate and physiological mechanisms of primary afferent neurons involved in musculoskeletal and orofacial disorders including musculoskeletal pain, temporomandibular disorders (TMD), fibromyalgia and myofacial pain.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Project (R01)
Project #
5R01DE010132-15
Application #
6930445
Study Section
Integrative, Functional and Cognitive Neuroscience 8 (IFCN)
Program Officer
Kusiak, John W
Project Start
1991-07-01
Project End
2007-08-31
Budget Start
2005-09-01
Budget End
2006-08-31
Support Year
15
Fiscal Year
2005
Total Cost
$324,101
Indirect Cost

  Institution

Name
University of Maryland Baltimore
Department
Dentistry
Type
Schools of Dentistry
DUNS #
188435911
City
Baltimore
State
MD
Country
United States
Zip Code
21201

  Publications

Dessem, Dean (2011) Physiological, morphological and neurochemical characterization of neurons modulated by movement. J Vis Exp :
Dessem, Dean; Ambalavanar, Ranjinidevi; Evancho, Melena et al. (2010) Eccentric muscle contraction and stretching evoke mechanical hyperalgesia and modulate CGRP and P2X(3) expression in a functionally relevant manner. Pain 149:284-95
Ambalavanar, R; Dessem, D (2009) Emerging peripheral receptor targets for deep-tissue craniofacial pain therapies. J Dent Res 88:201-11
Ambalavanar, R; Yallampalli, C; Yallampalli, U et al. (2007) Injection of adjuvant but not acidic saline into craniofacial muscle evokes nociceptive behaviors and neuropeptide expression. Neuroscience 149:650-9
Dessem, Dean; Moritani, Masayuki; Ambalavanar, Ranjinidevi (2007) Nociceptive craniofacial muscle primary afferent neurons synapse in both the rostral and caudal brain stem. J Neurophysiol 98:214-23
Ambalavanar, Ranjinidevi; Moutanni, Aicha; Dessem, Dean (2006) Inflammation of craniofacial muscle induces widespread mechanical allodynia. Neurosci Lett 399:249-54
Masri, Radi; Ro, Jin Y; Dessem, Dean et al. (2006) Classification of muscle spindle afferents innervating the masseter muscle in rats. Arch Oral Biol 51:740-7
Ambalavanar, Ranjinidevi; Moritani, Masayuki; Moutanni, Aicha et al. (2006) Deep tissue inflammation upregulates neuropeptides and evokes nociceptive behaviors which are modulated by a neuropeptide antagonist. Pain 120:53-68
Ambalavanar, R; Dessem, D; Moutanni, A et al. (2006) Muscle inflammation induces a rapid increase in calcitonin gene-related peptide (CGRP) mRNA that temporally relates to CGRP immunoreactivity and nociceptive behavior. Neuroscience 143:875-84
Ambalavanar, Ranjinidevi; Moritani, Masayuki; Dessem, Dean (2005) Trigeminal P2X3 receptor expression differs from dorsal root ganglion and is modulated by deep tissue inflammation. Pain 117:280-91

Showing the most recent 10 out of 24 publications