甘氨酸受体α3：脊髓中前列腺素E2介导的炎性疼痛敏化的关键靶点。

GlyR alpha3: an essential target for spinal PGE2-mediated inflammatory pain sensitization.

作者信息

Harvey Robert J, Depner Ulrike B, Wässle Heinz, Ahmadi Seifollah, Heindl Cornelia, Reinold Heiko, Smart Trevor G, Harvey Kirsten, Schütz Burkhard, Abo-Salem Osama M, Zimmer Andreas, Poisbeau Pierrick, Welzl Hans, Wolfer David P, Betz Heinrich, Zeilhofer Hanns Ulrich, Müller Ulrike

机构信息

Department of Pharmacology, The School of Pharmacy, London WC1N 1AX, UK.

出版信息

Science. 2004 May 7;304(5672):884-7. doi: 10.1126/science.1094925.

DOI:10.1126/science.1094925

PMID:15131310

Abstract

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.

摘要

前列腺素E2（PGE2）是炎症性疼痛敏化的关键介质。在此，我们证明，PGE2诱导的受体磷酸化对特定甘氨酸受体亚型（GlyRα3）的抑制作用是中枢性炎症性疼痛敏化的基础。我们发现，GlyRα3在脊髓背角浅层有明显表达。缺乏GlyRα3的小鼠不仅没有野生型小鼠中所见的PGE2对甘氨酸能神经传递的抑制作用，而且脊髓注射PGE2或外周炎症诱导的疼痛敏化也有所减轻。因此，GlyRα3可能为疼痛治疗提供一个此前未被认识的分子靶点。

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甘氨酸受体α3：脊髓中前列腺素E2介导的炎性疼痛敏化的关键靶点。

GlyR alpha3: an essential target for spinal PGE2-mediated inflammatory pain sensitization.

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