Abstract

N-type calcium channels regulate release of glutamate and substance P from primary sensory afferents in the superficial dorsal horn of the spinal cord. Presynaptic N-type calcium channels in the spinal dorsal horn are major targets of drugs to treat neuropathic and chronic pain syndromes. However, we don't yet understand why N-type calcium channel blockade is so effective against neuropathic pain and we don't understand how important they are in mediating the spinal analgesic actions of opiates. In this second phase of our project we will test our hypothesis that a distinct isoform of N-type calcium channels is essential for spinal level analgesic actions of a sub-set of drugs including opiates in vivo. During the 1st funding period of this grant we discovered that this novel splice isoform the N-type calcium channel, CaV2.2-e37a, is significantly more sensitive to drugs that act through G protein coupled receptors, including morphine. This is important because i) we previously showed that CaV2.2-e37a channels are enriched in nociceptors whereas CaV2.2-e37b channels are found throughout the nervous system, and ii) spinal level analgesic actions of morphine and other drugs are, at least in part, mediated by inhibition of presynaptic N-type channels in the dorsal horn. We are now ready to test the functional significance of CaV2.2-e37a in vivo in normal and disease states. We have developed four novel mouse lines using single exon gene targeting. These mice are genetically modified to express exclusively N-type channels containing either CaV2.2-e37a or CaV2.2-e37b but not both. We have developed all the necessary technical expertise to assess these mice at electrophysiology, biochemical, immunohistochemical, and behavioral levels. We will ask if CaV2.2-e37a channels mediate basal nociception and basal analgesic effects of morphine. We will also ask if CaV2.2-e37a channels are required for hyperalgesia to develop with neuropathic pain, and if they are necessary to mediate the analgesic effects of morphine during neuropathic pain. Our studies are highly relevant to the challenge of finding effective treatment for neuropathic and more generally chronic pain. Peripheral neuropathies can develop following acute nerve injury, and are strongly associated with diabetes, autoimmune disorders, malnutrition, and infections. There are no effective treatments for the millions of neuropathic and chronic pain sufferers.

Public Health Relevance

Our studies are highly relevant to finding effective treatment for neuropathic and more generally chronic pain. By studying a novel form of the N-type calcium channel in the pain pathway, our studies of novel knock-in mice should lead to new strategies for inhibiting the activity of this N-type calcium channel and alleviating pain sufferers. )

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
3R01NS055251-08S1
Application #
8851323
Study Section
Neurotransporters, Receptors, and Calcium Signaling Study Section (NTRC)
Program Officer
Silberberg, Shai D
Project Start
2006-08-02
Project End
2015-01-31
Budget Start
2013-02-01
Budget End
2015-01-31
Support Year
8
Fiscal Year
2014
Total Cost
$81,250
Indirect Cost
$31,250

  Institution

Name
Brown University
Department
Neurosciences
Type
Schools of Medicine
DUNS #
001785542
City
Providence
State
RI
Country
United States
Zip Code
02912

  Publications

Pradier, Bruno; Shin, Hye Bin; Kim, Duk Soo et al. (2018) Long-Term Depression Induced by Optogenetically Driven Nociceptive Inputs to Trigeminal Nucleus Caudalis or Headache Triggers. J Neurosci 38:7529-7540
Lipscombe, Diane; Lopez-Soto, Eduardo Javier (2018) Protected by a Fox. Neuron 98:3-5
Mustafá, Emilio R; López Soto, Eduardo J; Martínez Damonte, Valentina et al. (2017) Constitutive activity of the Ghrelin receptor reduces surface expression of voltage-gated Ca2+ channels in a CaV?-dependent manner. J Cell Sci 130:3907-3917
Tong, Xia-Jing; López-Soto, Eduardo Javier; Li, Lei et al. (2017) Retrograde Synaptic Inhibition Is Mediated by ?-Neurexin Binding to the ?2? Subunits of N-Type Calcium Channels. Neuron 95:326-340.e5
Andrade, A; Hope, J; Allen, A et al. (2016) A rare schizophrenia risk variant of CACNA1I disrupts CaV3.3 channel activity. Sci Rep 6:34233
Groen, Justus L; Andrade, Arturo; Ritz, Katja et al. (2015) CACNA1B mutation is linked to unique myoclonus-dystonia syndrome. Hum Mol Genet 24:987-93
Lipscombe, Diane; Andrade, Arturo (2015) Calcium Channel CaV?? Splice Isoforms - Tissue Specificity and Drug Action. Curr Mol Pharmacol 8:22-31
Lipscombe, Diane; Pan, Jen Q; Schorge, Stephanie (2015) Tracks through the genome to physiological events. Exp Physiol 100:1429-40
Lipscombe, Diane; Allen, Summer E; Toro, Cecilia P (2013) Control of neuronal voltage-gated calcium ion channels from RNA to protein. Trends Neurosci 36:598-609
Lipscombe, Diane; Andrade, Arturo; Allen, Summer E (2013) Alternative splicing: functional diversity among voltage-gated calcium channels and behavioral consequences. Biochim Biophys Acta 1828:1522-9

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