Abstract

Approximately 6% of the American population suffers from intractable pain following nerve injury; yet available treatment options are only marginally effective. Persistent pain was previously attributed exclusively to sensory neuron functions; however, recent discoveries indicate that glial cells also contribute to chronic pain. Activation of satellite glial cells (SGCs), the type of glial cell surrounding primary sensory neurons, correlates with increased sensory neuron excitability. A better understanding of this glia-induced hyper-excitability is likely to open the door to new therapies for nerve-injured patients. Until recently, means of studying the role of glial cells in nerve injury were limited. By using stereotactically targeted RNA interference (RNAi) to inhibit gene expression, we can now silence specific genes in single sensory ganglia of adult rats. Here, we have chosen to study a series of SGC-specific genes involved in neuronal excitability including genes that code for a neurotransmitter receptor (P2Y4), an enzyme (guanylyl cyclase), a calcium-activated potassium channel (SK3), and a component of the gap junction (connexin 43). These genes are likely to play key roles in neuropathic pain since they regulate neuron-SGC communication and control neuronal excitability following injury. Our preliminary experiments utilizing RNAi-mediated gene silencing at the trigeminal ganglion, where SGCs surround the cell bodies of primary sensory neurons innervating the face, show that this approach selectively and reversibly silences SGC genes in freely behaving rats. We can quantify the effects of gene silencing in these animals through several behavioral tests, as well as by anatomical and physiological analyses. This proposal aims to elucidate the contribution of SGC-specific genes to the control of neuronal excitability and sensory behavior following trigeminal nerve injury. With these results we hope to define genetic targets for the development of therapies that could improve the lives of individuals suffering from the long-term effects of nerve injury. The Principal Investigator of this proposed study directs, and serves as the neurosurgeon for, the Interdepartmental Pain Group at Cedars-Sinai Medical Center and is a member of the Cedars-Sinai Gene Therapeutics Research Institute, where this work will be completed. Fifty percent of the Principle Investigator's time is protected to pursue research.

Public Health Relevance

Approximately 6% of the American population suffers from intractable pain following nerve injury; yet available treatment options are only marginally effective. Persistent pain was previously attributed exclusively to sensory neuron functions; however, recent discoveries indicate that glial cells also contribute to chronic pain. Activation of satellite glial cells (SGCs), the type of glial cell surrounding primary sensory neurons, correlates with increased sensory neuron excitability. A better understanding of this glia-induced hyper-excitability is likely to open the door to new therapies for nerve-injured patients. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS061241-01A1
Application #
7528994
Study Section
Cellular and Molecular Biology of Glia Study Section (CMBG)
Program Officer
Porter, Linda L
Project Start
2008-06-01
Project End
2009-02-28
Budget Start
2008-06-01
Budget End
2009-02-28
Support Year
1
Fiscal Year
2008
Total Cost
$55,367
Indirect Cost

  Institution

Name
Cedars-Sinai Medical Center
Department
Type
DUNS #
075307785
City
Los Angeles
State
CA
Country
United States
Zip Code
90048

  Publications

Gong, Kerui; Bhargava, Aditi; Jasmin, Luc (2016) GluN2B N-methyl-D-aspartate receptor and excitatory amino acid transporter 3 are upregulated in primary sensory neurons after 7 days of morphine administration in rats: implication for opiate-induced hyperalgesia. Pain 157:147-58
Gong, Kerui; Kung, Ling-Hsuan; Magni, Giulia et al. (2014) Increased response to glutamate in small diameter dorsal root ganglion neurons after sciatic nerve injury. PLoS One 9:e95491
Donegan, Macayla; Kernisant, Melanie; Cua, Criselda et al. (2013) Satellite glial cell proliferation in the trigeminal ganglia after chronic constriction injury of the infraorbital nerve. Glia 61:2000-8
Kung, Ling-Hsuan; Gong, Kerui; Adedoyin, Mary et al. (2013) Evidence for glutamate as a neuroglial transmitter within sensory ganglia. PLoS One 8:e68312
Kaan, Timothy K Y; Ohara, Peter T; Jasmin, Luc (2012) Orofacial pain models and behavior assessment. Methods Mol Biol 851:159-70
Jasmin, Luc; Vit, Jean-Philippe; Bhargava, Aditi et al. (2010) Can satellite glial cells be therapeutic targets for pain control? Neuron Glia Biol 6:63-71
Jasmin, Luc; Ohara, Peter T (2010) Close encounters of the third kind: evidence for contact with TNF-alpha. Pain 151:241-2
Ohara, Peter T; Vit, Jean-Philippe; Bhargava, Aditi et al. (2009) Gliopathic pain: when satellite glial cells go bad. Neuroscientist 15:450-63
Kernisant, Melanie; Gear, Robert W; Jasmin, Luc et al. (2008) Chronic constriction injury of the infraorbital nerve in the rat using modified syringe needle. J Neurosci Methods 172:43-7