Persisting dysfunctional neuroplasticity in peripheral nerves as well as in the brain exert powerful influences on the pain experience. For example, facial trauma suffered by military personnel may heal, yet months later progress to a chronic neuropathic pain state. A facial laceration trigeminal nerve trauma model (CCI-ION) is utilized in our pursuit of mechanistic support for repurposing a noradrenergic (NA) therapeutic currently in use for treatment of post-traumatic stress disorder (PTSD) in active duty and Veteran military personnel to reduce chronic pain. The proposed studies address novel hypotheses to explore mechanistic changes that cause overactivation of NA neurons in the nucleus locus coeruleus (LC) neurons that modulate pain and their dysfunctional NA receptor signaling in two targeted brain regions. Our Preliminary Data support our overall hypothesis that neuroplastic changes in the pain network and related limbic structures modulate a shift to chronic pain. This also causes anxiety and depression related behavioral measures in our preclinical model. Our studies are unique in that we test through an extended time course compared to studies using acute injuries, to provide more clinically relevant information. We have discovered that switch from pain inhibition to facilitatio occurs through paradoxical ongoing dysregulation of NA LC neurons (Aim 1) that can be reversed pharmacologically (Aim 2). Long-term block of NA?1 receptor facilitation is proposed as therapy for chronic pain behaviors, overactivation, and maladaptive neuropathology (Aim 3).
Aim 1 tests the hypothesis that chronic trigeminal neuropathic pain facilitates central sensitization by overactivation and dysregulation of LC NA neurons producing a functional shift from pain inhibition to facilitation. Maladaptive signaling mechanisms have been identified during chronic pain. Biomarker changes indicate overactivation of the LC, an important NA modulator of pain processing. Removal of LC NA influence with intracerebroventricular or trigeminal dorsal horn (spVc) microinjections of neurotoxic saporin conjugated dopamine-beta-hydroxylase antibodies specifically ablates NA neurons, reducing mechanical hypersensitivity.
Aim 2 tests the hypothesis that trigeminal nerve injury shifts NA?2 receptor mediated inhibition to NA?1 receptor mediated facilitation of chronic pain assisted by GABA dysregulation. Pharmacological findings indicate that during chronic pain GABA disinhibition occurs. Thus, in chronic pain ligand-gated GABAA receptor chloride signaling becomes excitatory instead of inhibitory. Injury-induced long-term neuronal excitation causes intracellular chloride accumulation and equilibrium potential shift. Concomitant dysfunctional shift from NA?2 receptor inhibition to NA?1 receptor facilitation results in the medial prefrontal limbic cortex (mPFC) and spVc targeted by the NA LC neurons.
Aim 3 tests the hypothesis that long-term treatment with prazosin will reduce the effects of dysregulated NA LC signaling. Efficacy of long-term treatment with orally dosed prazosin, a clinically used NA receptor antagonist, will be tested in the chronic facial laceration and nerve injury model. Attenuation is anticipated of hypersensitivity, anxiety, depression, and cognition related measures based on its efficacy for the treatment of Veterans with PTSD. Chronic pain induced histopathological changes, i.e. biomarker expression of cellular overactivation, cortical neuronal death and glial scar formation, are expected to be improved by long-term treatment with prazosin. The long term goal of the proposed studies is greater understanding of pain generators and neuroplastic changes precipitating dysfunctional neuronal signaling that produce chronic pain. Completion of the studies will provide scientific justification for repurposing FDA approved noradrenergic therapies that (1) have potential to decrease chronic neuropathic pain and (2) will move quickly through regulatory approvals. This would improve quality of life, return to work rates for Veterans, and decrease costs for the VA system.

Public Health Relevance

Head laceration and chronic nerve injury pain are chief complaints of approximately 772,000 of the 2.5 million military personnel deployed since 2001 that have sought out the VA health care system. We have identified two dysregulated signaling mechanisms that occur only after chronic pain is established. The dysregulated mechanisms involve a major neuronal group in the brain with connections to pain processing regions. This neuronal group which normally reduces pain begins to facilitate pain and damages brain neurons. The proposed studies will provide better rationale for the beneficial effects of noradrenergic drugs for pain in addition to their current use for PTSD and sleep disturbance suffered by many Veterans after face and head injuries associated with blast explosions and other combat incidences.

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
5I01BX002695-04
Application #
9636468
Study Section
Neurobiology B (NURB)
Project Start
2016-01-01
Project End
2020-12-31
Budget Start
2019-01-01
Budget End
2019-12-31
Support Year
4
Fiscal Year
2019
Total Cost
Indirect Cost
Name
Albuquerque VA Medical Center
Department
Type
DUNS #
073242369
City
Albuquerque
State
NM
Country
United States
Zip Code
87108
Danaher, Robert J; Zhang, Liping; Donley, Connor J et al. (2018) Histone deacetylase inhibitors prevent persistent hypersensitivity in an orofacial neuropathic pain model. Mol Pain 14:1744806918796763
Lyons, Danielle N; Zhang, Liping; Pandya, Jignesh D et al. (2018) Combination Drug Therapy of Pioglitazone and D-cycloserine Attenuates Chronic Orofacial Neuropathic Pain and Anxiety by Improving Mitochondrial Function Following Trigeminal Nerve Injury. Clin J Pain 34:168-177
Taylor, Bradley K; Westlund, Karin N (2017) The noradrenergic locus coeruleus as a chronic pain generator. J Neurosci Res 95:1336-1346
Lyons, Danielle N; Zhang, Liping; Danaher, Robert J et al. (2017) PPAR? Agonists Attenuate Trigeminal Neuropathic Pain. Clin J Pain 33:1071-1080
McIlwrath, S L; Nesemeier, R; Ma, F et al. (2017) Inflammatory 'double hit' model of temporomandibular joint disorder with elevated CCL2, CXCL9, CXCL10, RANTES and behavioural hypersensitivity in TNFR1/R2-/- mice. Eur J Pain 21:1209-1223
Hansen, Barbara C; Gografe, Sylvia; Pritt, Stacy et al. (2017) Ensuring due process in the IACUC and animal welfare setting: considerations in developing noncompliance policies and procedures for institutional animal care and use committees and institutional officials. FASEB J 31:4216-4225
Ma, Fei; Wang, Chunmei; Yoder, William E et al. (2016) Efficacy of Herpes Simplex Virus Vector Encoding the Human Preproenkephalin Gene for Treatment of Facial Pain in Mice. J Oral Facial Pain Headache 30:42-50
Kaushal, R; Taylor, B K; Jamal, A B et al. (2016) GABA-A receptor activity in the noradrenergic locus coeruleus drives trigeminal neuropathic pain in the rat; contribution of NA?1 receptors in the medial prefrontal cortex. Neuroscience 334:148-159
Ma, F; Zhang, L; Oz, H S et al. (2015) Dysregulated TNF? promotes cytokine proteome profile increases and bilateral orofacial hypersensitivity. Neuroscience 300:493-507
Lyons, D N; Kniffin, T C; Zhang, L P et al. (2015) Trigeminal Inflammatory Compression (TIC) injury induces chronic facial pain and susceptibility to anxiety-related behaviors. Neuroscience 295:126-38

Showing the most recent 10 out of 11 publications