The NMDA-receptor antagonist CPP abolishes neurogenic ‘wind-up pain’ after intrathecal administration in humans

Kristensen, Jens D.; Svensson, Bo; Gordh, Torsten

doi:10.1016/0304-3959(92)90266-e

Cited by 286 publications

(98 citation statements)

References 18 publications

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“…Among clinically assessed NMDA antagonists, however, the narrow separation between effectiveness and liabilities such as sedation, memory impairments, motor incoordination, and psychotomimetic effects has severely hampered their utility for the treatment of neuropathic pain. For example, intrathecal administration of CPP, a competitive NMDA antagonist, prevented radiation of the pain outside the territory of the injured nerve in a patient suffering from surgery-induced nerve injury, 74 but psychotomimetic adverse effects of the drug resulted in the termination of the study.…”

Section: Preclinical and Clinical Studies Of Nmda Receptor Antagonistsmentioning

confidence: 99%

Targeting the NMDA Receptor Subunit NR2B for the Treatment of Neuropathic Pain

2009

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Summary:Neuropathic pain is generally defined as a chronic pain state resulting from peripheral or central nerve injury, or both. An effective treatment for neuropathic pain is still lacking. The NMDA receptor, one type of the ionotropic glutamate receptors, is known to be important for triggering long-lasting changes in synapses. NMDA receptor-dependent synaptic plasticity plays roles not only in physiological functions such as learning and memory, but also in unwanted pathological conditions such as chronic pain. This review addresses recent progress on NMDA receptors in neuropathic pain, with particular emphasis on the NR2B-subunitcontaining receptors. The expression and function of NMDA receptors in synaptic plasticity in the pain transmission pathway from dorsal root ganglia to the anterior cingulate cortex is reviewed, and preclinical and clinical investigations of selective NMDA receptor in neuropathic pain are discussed. The NMDA receptors, in particular NR2B-containing NMDA receptors, serve as promising targets for treatment of neuropathic pain.

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Section: Preclinical and Clinical Studies Of Nmda Receptor Antagonistsmentioning

confidence: 99%

Targeting the NMDA Receptor Subunit NR2B for the Treatment of Neuropathic Pain

2009

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“…However, NMDA antagonists have significant side effects. In adult humans they trigger psychosis, [1][2][3][4][5][6][7][8][9][10] and in adult rats they produce neurotoxicity. [11][12][13][14][15][16][17][18][19][20][21] Developing methods for controlling or preventing these adverse reactions is an important goal, as it may permit the therapeutic potential of these agents to be realized.…”

Section: Introductionmentioning

confidence: 99%

Receptor mechanisms and circuitry underlying NMDA antagonist neurotoxicity

et al. 2002

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NMDA glutamate receptor antagonists are used in clinical anesthesia, and are being developed as therapeutic agents for preventing neurodegeneration in stroke, epilepsy, and brain trauma. However, the ability of these agents to produce neurotoxicity in adult rats and psychosis in adult humans compromises their clinical usefulness. In addition, an NMDA receptor hypofunction (NRHypo) state might play a role in neurodegenerative and psychotic disorders, like Alzheimer's disease and schizophrenia. Thus, understanding the mechanism underlying NRHypo-induced neurotoxicity and psychosis could have significant clinically relevant benefits. NRHypo neurotoxicity can be prevented by several classes of agents (eg antimuscarinics, non-NMDA glutamate antagonists, and ␣ 2 adrenergic agonists) suggesting that the mechanism of neurotoxicity is complex. In the present study a series of experiments was undertaken to more definitively define the receptors and complex neural circuitry underlying NRHypo neurotoxicity. Injection of either the muscarinic antagonist scopolamine or the non-NMDA antagonist NBQX directly into the cortex prevented NRHypo neurotoxicity. Clonidine, an ␣ 2 adrenergic agonist, protected against the neurotoxicity when injected into the basal forebrain. The combined injection of muscarinic and non-NMDA Glu agonists reproduced the neurotoxic reaction. Based on these and other results, we conclude that the mechanism is indirect, and involves a complex network disturbance, whereby blockade of NMDA receptors on inhibitory neurons in multiple subcortical brain regions, disinhibits glutamatergic and cholinergic projections to the cerebral cortex. Simultaneous excitotoxic stimulation of muscarinic (m 3 ) and glutamate (AMPA/kainate) receptors on cerebrocortical neurons appears to be the proximal mechanism by which the neurotoxic and psychotomimetic effects of NRHypo are mediated.

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“…In man, both ketamine (Stannard & Porter, 1993;Backonja et al, 1994;Park et al, 1994;Arendt-Neilson et al, 1995;Cherry et al, 1995;Persson et al, 1995) and the competitive glutamate recognition site antagonist, CPP (Kristensen et al, 1992) have been shown to have analgesic properties in a variety of experimental and clinical pain states. However, even in studies in which the drug is given intrathecally, psychotomimetic effects are seen with these agents (White et al, 1982;Kristensen et al, 1992;Backonja et al, 1994;Park et al, 1994). In order to exploit the therapeutic potential of this class of compounds it is therefore important to develop NMDA antagonists with reduced side-effect liability.…”

Section: Introductionmentioning

confidence: 99%