<scp>GLT</scp>1 overexpression reverses established neuropathic pain‐related behavior and attenuates chronic dorsal horn neuron activation following cervical spinal cord injury

Falnikar, Aditi; Hala, Tamara J.; Poulsen, David J.; Lepore, Angelo C.

doi:10.1002/glia.22936

Cited by 62 publications

(39 citation statements)

References 44 publications

(73 reference statements)

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“…Overactivation of DH projection neurons is a mechanism that underlies the manifestation of pain (41). Glutamate is the principal neurotransmitter that mediates the hyperexcitability of DH neurons, and dysregulation of extracellular glutamate homeostasis has been implicated in increased pain (34,(74)(75)(76)(77). Rapid and efficient clearance of glutamate in the CNS is mediated by astrocytes, which are the principal cell type that expresses GLAST and GLT1 (78).…”

Section: Female-specific Alterations In Glutamate Transporter Expressmentioning

confidence: 99%

Impaired sensitivity to pain stimuli in plasma membrane calcium ATPase 2 (PMCA2) heterozygous mice: a possible modality‐ and sex‐specific role for PMCA2 in nociception

Khariv

Ratnayake

et al. 2016

FASEB j.

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Plasma membrane calcium ATPase 2 (PMCA2) is a calcium pump that plays important roles in neuronal function. Although it is expressed in pain-associated regions of the CNS, including in the dorsal horn (DH), its contribution to pain remains undefined. The present study assessed the role of PMCA2 in pain responsiveness and the link between PMCA2 and glutamate receptors, GABA receptors (GABARs), and glutamate transporters that have been implicated in pain processing in the DH of adult female and male PMCA2 and PMCA2 mice. Behavioral assays evaluated mechanical and thermal pain responsiveness. Mechanical sensitivity was significantly increased by 52% and heat sensitivity was reduced by 29% in female, but not male, PMCA2 mice compared with PMCA2 controls. There were female-specific changes in metabotropic glutamate receptor 1, NMDA receptor 2A, α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor subunit GluR1, GABAR1, and GABAR2 levels, whereas metabotropic glutamate receptor 5, NMDA receptor 2B, GluR2, and GABARα2 levels were not altered. Glutamate aspartate transporter levels were higher and glial glutamate transporter 1 levels were lower in the DH of female, but not male, PMCA2 mice. These findings indicate a novel role for PMCA2 in modality- and sex-dependent pain responsiveness. Female-specific molecular changes potentially account for the altered pain responses.-Khariv, V., Ni, L., Ratnayake, A., Sampath, S., Lutz, B. M., Tao, X.-X., Heary, R. F., Elkabes, S. Impaired sensitivity to pain stimuli in plasma membrane calcium ATPase 2 (PMCA2) heterozygous mice: a possible modality- and sex-specific role for PMCA2 in nociception.

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Section: Female-specific Alterations In Glutamate Transporter Expressmentioning

confidence: 99%

Impaired sensitivity to pain stimuli in plasma membrane calcium ATPase 2 (PMCA2) heterozygous mice: a possible modality‐ and sex‐specific role for PMCA2 in nociception

Khariv

Ratnayake

et al. 2016

FASEB j.

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“…Neuronal hyperexcitability in the dorsal horn has also been implicated in SCI‐induced neuropathic pain (Zhang et al, ; Gwak et al, ; Gwak and Hulsebosch, ). This might occur through dysregulation of glutamate release, uptake, and receptor expression (Leem et al, ; Gwak et al, ; Putatunda et al, ; Falnikar et al, ); dendritic spine remodeling (Tan et al, ; Zhao et al, ); loss of local inhibitory (GABAergic) tone (Drew et al, ; Lu et al, ; Meisner et al, ; Berrocal et al, ; Lee‐Kubli et al, ); descending (particularly serotonergic) inhibitory input to spinal nociceptive circuitry (Hains et al, ; Kalous et al, ; Lin et al, ); or increased expression of the calcium channel subunit Ca v α2δ‐1 (Boroujerdi et al, ). The latter finding may partially explain the (small) benefit of gabapentinoids (which bind α2δ‐1) in neuropathic pain (Baastrup and Finnerup, ).…”

Section: Etiology Of Neuropathic Pain Following Traumatic Sci: Evidenmentioning

confidence: 99%

“…Widespread astrogliosis is also a feature of SCI (Carlton et al, ; Gwak and Hulsebosch, ; Gwak et al, ; Putatunda et al, ; Watson et al, ), and astroglial connexin hemichannels have been implicated in SCI pain (Chen et al, ). The astroglial glutamate reuptake transporter GLT1 is downregulated following SCI, and its overexpression reduces pain‐related behaviors and immunohistochemical markers of neuronal activity (Putatunda et al, ; Falnikar et al, ).…”

Section: Etiology Of Neuropathic Pain Following Traumatic Sci: Evidenmentioning

confidence: 99%

Neuropathic pain following traumatic spinal cord injury: Models, measurement, and mechanisms

Kramer

Minhas

Jutzeler

et al. 2016

J of Neuroscience Research

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Neuropathic pain following spinal cord injury (SCI) is notoriously difficult to treat and is a high priority for many in the SCI population. Resolving this issue requires animal models fidelic to the clinical situation in terms of injury mechanism and pain phenotype. This Review discusses the means by which neuropathic pain has been induced and measured in experimental SCI and compares these with human outcomes, showing that there is a substantial disconnection between experimental investigations and clinical findings in a number of features. Clinical injury level is predominantly cervical, whereas injury in the laboratory is modeled mainly at the thoracic cord. Neuropathic pain is primarily spontaneous or tonic in people with SCI (with a relatively smaller incidence of allodynia), but measures of evoked responses (to thermal and mechanical stimuli) are almost exclusively used in animals. There is even the question of whether pain per se has been under investigation in most experimental SCI studies rather than simply enhanced reflex activity with no affective component. This Review also summarizes some of the problems related to clinical assessment of neuropathic pain and how advanced imaging techniques may circumvent a lack of patient/clinician objectivity and discusses possible etiologies of neuropathic pain following SCI based on evidence from both clinical studies and animal models, with examples of cellular and molecular changes drawn from the entire neuraxis from primary afferent terminals to cortical sensory and affective centers. © 2016 Wiley Periodicals, Inc.

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“…In all cases, it is essential to generate the appropriate population of cells and to optimize survival and integration of the transplants. One consideration is the inclusion of therapeutic factors (using scaffolds, genetic modification of donor cells, or cotransplantation with other cell populations) to promote survival and integration, thus increasing the efficacy of the transplant [42], but it is also likely that NPC transplantation will be combined with other treatments such as neuroprotective drugs, exercise or electrical stimulation.…”

Section: Using Defined Populations Of Progenitorsmentioning

confidence: 99%

Improving the therapeutic efficacy of neural progenitor cell transplantation following spinal cord injury

Lane

Lepore

Fischer

2016

Expert Review of Neurotherapeutics

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Introduction There have been a wide range of preclinical studies testing cellular therapies to repair the injured spinal cord, yet they remain a challenge to translate because of inconsistencies in efficacy, limited number of patients with acute/subacute SCI and the high costs of clinical trials. Area covered This paper focusses on the therapeutic potential of neural precursor cells (NPCs) because they can provide the cellular components capable of promoting repair and enhancing functional improvement following spinal cord injury (SCI). The authors discuss the challenges of NPC transplantation with respect to different populations of NPCs of glial and neuronal lineages, the timing of treatment relative to acute and chronic injury, and the progress in ongoing clinical trials. Expert commentary Preclinical research will continue to elucidate mechanisms of recovery associated with NPC transplants, including increasing the partnership with related fields such as spinal atrophies and multiple sclerosis. The clinical trials landscape will grow and include both acute and chronic SCI with increased partnership and strengthened communication between biotechnology, government and academia. There will also be growing effort to develop better biomarkers, imaging and outcome measures for detailed assessment of neurological function and measures of quality of life.

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GLT1 overexpression reverses established neuropathic pain‐related behavior and attenuates chronic dorsal horn neuron activation following cervical spinal cord injury

Cited by 62 publications

References 44 publications

Impaired sensitivity to pain stimuli in plasma membrane calcium ATPase 2 (PMCA2) heterozygous mice: a possible modality‐ and sex‐specific role for PMCA2 in nociception

Impaired sensitivity to pain stimuli in plasma membrane calcium ATPase 2 (PMCA2) heterozygous mice: a possible modality‐ and sex‐specific role for PMCA2 in nociception

Neuropathic pain following traumatic spinal cord injury: Models, measurement, and mechanisms

Improving the therapeutic efficacy of neural progenitor cell transplantation following spinal cord injury

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