Ulrike B. Depner scite author profile

Prostaglandin E2 (PGE2) is a crucial mediator of inflammatory pain sensitization. Here, we demonstrate that inhibition of a specific glycine receptor subtype (GlyR alpha3) by PGE2-induced receptor phosphorylation underlies central inflammatory pain sensitization. We show that GlyR alpha3 is distinctly expressed in superficial layers of the spinal cord dorsal horn. Mice deficient in GlyR alpha3 not only lack the inhibition of glycinergic neurotransmission by PGE2 seen in wild-type mice but also show a reduction in pain sensitization induced by spinal PGE2 injection or peripheral inflammation. Thus, GlyR alpha3 may provide a previously unrecognized molecular target in pain therapy.

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Spinal inflammatory hyperalgesia is mediated by prostaglandin E receptors of the EP2 subtype

Reinold

et al. 2005

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Blockade of prostaglandin (PG) production by COX inhibitors is the treatment of choice for inflammatory pain but is also prone to severe side effects. Identification of signaling elements downstream of COX inhibition, particularly of PG receptor subtypes responsible for pain sensitization (hyperalgesia), provides a strategy for better-tolerated analgesics. Here, we have identified PGE2 receptors of the EP2 receptor subtype as key signaling elements in spinal inflammatory hyperalgesia. Mice deficient in EP2 receptors (EP2-/- mice) completely lack spinal PGE2-evoked hyperalgesia. After a peripheral inflammatory stimulus, EP2-/- mice exhibit only short-lasting peripheral hyperalgesia but lack a second sustained hyperalgesic phase of spinal origin. Electrophysiological recordings identify diminished synaptic inhibition of excitatory dorsal horn neurons as the dominant source of EP2 receptor-dependent hyperalgesia. Our results thus demonstrate that inflammatory hyperalgesia can be treated by targeting of a single PG receptor subtype and provide a rational basis for new analgesic strategies going beyond COX inhibition.

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Ulrike B. Depner

GlyR α3: An Essential Target for Spinal PGE ₂ -Mediated Inflammatory Pain Sensitization

Spinal inflammatory hyperalgesia is mediated by prostaglandin E receptors of the EP2 subtype

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Ulrike B. Depner

GlyR α3: An Essential Target for Spinal PGE 2 -Mediated Inflammatory Pain Sensitization

Spinal inflammatory hyperalgesia is mediated by prostaglandin E receptors of the EP2 subtype

Contact Info

Product

Resources

About

GlyR α3: An Essential Target for Spinal PGE ₂ -Mediated Inflammatory Pain Sensitization