Abstract

In neurons, synaptic and intrinsic plasticity is dependent on the regulated control of mRNA translation. Over the past decade our work has focused on how translation regulation signaling is involved in neuronal plasticity that drives chronic pain. Our findings demonstrate that inflammatory and neuropathic injuries stimulate translation regulation signaling pathways in dorsal root ganglion (DRG) nociceptors, neurons that detect injurious or potentially injurious stimuli. The result of activation of these pathways is increased excitability of nociceptors, behavioral signs of ongoing pain and sensitization to mechanical and thermal stimulation. This body of work, supports the idea that therapeutics targeting translation regulation signaling pathways can be used for the efficacious treatment of chronic pain. Our overarching hypothesis for this continuing project is that MNK1 activation in nociceptors is the key regulatory factor for the translation of a subset of mRNAs that encode proteins that augment the excitability of nociceptors causing enhanced pain phenotypes. We will test this hypothesis using new transgenic mouse lines, cell type-specific translating ribosome affinity purification (TRAP), highly specific inhibitors of MNK1/2 and new generation inhibitors that are specific for MNK1. Our preliminary data indicates that the key MNK isoform for nociceptive behavioral plasticity is MNK1. Based on our electrophysiology experiments we hypothesize that the site of action for this kinase is in DRG neurons. Our first specific aim will test the hypothesis that MNK1 expression in nociceptors is a key driver of behavioral expression of chronic pain. We have created a TRAP line that expresses L10a-tagged ribosomes in neurons that express the Scn10a gene (Scn10aTRAP). In our second specific aim we will examine how translation of specific mRNAs is regulated in preclinical neuropathic pain models with and without genetic or pharmacological manipulations of MNK-eIF4E signaling. This will yield unprecedented molecular insight into plasticity-driven changes in gene expression in nociceptors in neuropathic pain. The third specific aim will focus on pharmacologically or genetically targeting mechanisms discovered using approaches in aims 1 and 2. For instance, our TRAP approach captures translational upregulation of the Mrgrpd receptor in a neuropathic model. We will use knockout mice to investigate the role of this receptor in sensory neuron excitability in neuropathic pain. The proposed specific aims will highlight a key regulatory pathway for neuropathic pain and give new insight into novel therapeutic targets for neuropathic pain.

Public Health Relevance

Our work is aimed at gaining a better understanding of molecular events that drive neuropathic pain and then using this knowledge to identify new molecular targets for neuropathic pain treatment. Our work has found a key signaling pathway that regulates nociceptor excitability changes that occur in neuropathic pain. An exciting aspect of this discovery is that this signaling pathway can be targeted by drugs that are in phase II clinical trials. The combined use of pharmacology, genetics and next generation sequencing technologies in our project will give new insight into mechanisms of neuropathic pain and will identify novel therapeutic opportunities to treat this highly prevalent and exceedingly difficult to manage neurological disorder

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS065926-09
Application #
9722739
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Oshinsky, Michael L
Project Start
2010-03-15
Project End
2024-01-31
Budget Start
2019-03-01
Budget End
2020-01-31
Support Year
9
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
University of Texas-Dallas
Department
Type
Sch Allied Health Professions
DUNS #
800188161
City
Richardson
State
TX
Country
United States
Zip Code
75080

  Publications

Megat, Salim; Shiers, Stephanie; Moy, Jamie K et al. (2018) A Critical Role for Dopamine D5 Receptors in Pain Chronicity in Male Mice. J Neurosci 38:379-397
Black, Bryan J; Atmaramani, Rahul; Kumaraju, Rajeshwari et al. (2018) Adult mouse sensory neurons on microelectrode arrays exhibit increased spontaneous and stimulus-evoked activity in the presence of interleukin-6. J Neurophysiol 120:1374-1385
Shepherd, Andrew J; Copits, Bryan A; Mickle, Aaron D et al. (2018) Angiotensin II Triggers Peripheral Macrophage-to-Sensory Neuron Redox Crosstalk to Elicit Pain. J Neurosci 38:7032-7057
Paige, Candler; Maruthy, Gayathri Batchalli; Mejia, Galo et al. (2018) Spinal Inhibition of P2XR or p38 Signaling Disrupts Hyperalgesic Priming in Male, but not Female, Mice. Neuroscience 385:133-142
Hassler, Shayne N; Ahmad, Fatima B; Burgos-Vega, Carolina C et al. (2018) Protease activated receptor 2 (PAR2) activation causes migraine-like pain behaviors in mice. Cephalalgia :333102418779548
Uttam, Sonali; Wong, Calvin; Price, Theodore J et al. (2018) eIF4E-Dependent Translational Control: A Central Mechanism for Regulation of Pain Plasticity. Front Genet 9:470
Khoutorsky, Arkady; Price, Theodore J (2018) Translational Control Mechanisms in Persistent Pain. Trends Neurosci 41:100-114
Barragán-Iglesias, Paulino; Lou, Tzu-Fang; Bhat, Vandita D et al. (2018) Inhibition of Poly(A)-binding protein with a synthetic RNA mimic reduces pain sensitization in mice. Nat Commun 9:10
Megat, Salim; Price, Theodore J (2018) Therapeutic opportunities for pain medicines via targeting of specific translation signaling mechanisms. Neurobiol Pain 4:8-19
Moy, Jamie K; Kuhn, Jasper L; Szabo-Pardi, Thomas A et al. (2018) eIF4E phosphorylation regulates ongoing pain, independently of inflammation, and hyperalgesic priming in the mouse CFA model. Neurobiol Pain 4:45-50

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