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ARTICLE, Behavioral/Systems

Chronic Hypersensitivity For Inflammatory Nociceptor Sensitization Mediated by the ε Isozyme of Protein Kinase C

K. O. Aley, Robert O. Messing, Daria Mochly-Rosen and Jon D. Levine
Journal of Neuroscience 15 June 2000, 20 (12) 4680-4685; https://doi.org/10.1523/JNEUROSCI.20-12-04680.2000
K. O. Aley
1National Institutes of Health Pain Center, University of California, San Francisco, San Francisco, California 94143-0440,
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Robert O. Messing
2Ernest Gallo Clinic and Research Center, University of California, Emeryville, California 94608, and
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Daria Mochly-Rosen
3Molecular Pharmacology, Stanford University, Stanford, California 94305
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Jon D. Levine
1National Institutes of Health Pain Center, University of California, San Francisco, San Francisco, California 94143-0440,
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    Fig. 1.

    A, Dose (0.1–2%)–response curve of carrageenan (Carr; n = 12) induced mechanical hyperalgesia measured at 4 hr in the hindpaw of the normal rat. The Randall-Selitto paw-withdrawal test is an established method to assess heightened nociception in animals in which this subjective experience of pain cannot be directly determined. Measures using this technique have been shown to correlate with pain-like behaviors in animals. B, Time course of hyperalgesia induced by carrageenan 1% (5 μl, n = 24) in normal rats.

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    Fig. 2.

    A, PGE2 (100 ng,n = 24), 5-HT (1 μg, n = 6), and CGS-21680 (100 ng, n = 6)-induced mechanical hyperalgesia at 30 min, 4 hr, and 24 hr after injection in rats treated 5 d previously with carrageenan. B, Mechanical hyperalgesia induced by PGE2 (n = 12), 5-HT (n = 6), and CGS-21680 (n= 6) at 30 min, 4 hr, and 24 hr after injection in rats treated 21 d previously with carrageenan. C, Time course of PGE2-, 5-HT-, and CGS-21680-induced mechanical hyperalgesia in rats 5 d after vehicle used for carrageenan (n = 12 each).

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    Fig. 3.

    A, Effect of PKA inhibitor WIPTIDE (WIP/E2; 1 μg/100 ng, n = 24), nitric oxide synthase inhibitorNG-methyl-l-arginine (L-NMA/E2; 1 μg/100 ng, n = 12), PKC inhibitor bisindolylmalemide 1 hydrochloride (Bis/E2; 1 μg/100 ng, n = 12), PKCε inhibitor (PKCεV1–2/E2; 1 μg/100 ng,n = 12), administered 5 min before PGE2, on PGE2(E2)-induced mechanical hyperalgesia measured at 30 min after PGE2 injection in control rats and in rats treated 5 d previously with carrageenan. B, Effect of PKA inhibitor WIP/E2 (n = 24), nitric oxide synthase inhibitor L-NMA/E2 (n= 12), PKC inhibitor Bis/E2 (n = 12), PKCε inhibitor PKCεV1–2/E2) (n = 12), administered 5 min before PGE2, on PGE2(E2)-induced mechanical hyperalgesia measured at 4 hr after PGE2 injection in control rats and in rats treated 5 d previously with carrageenan.

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    Fig. 4.

    A, Effect of PKA inhibitor WIPTIDE (WIP/Carr; n = 24) and PKG inhibitor (PKGI/Carr; n = 8) on carrageenan-induced mechanical hyperalgesia in the rat hindpaw. Agents were administered 5 min before carrageenan. All readings were taken 4 hr after carrageenan. B, C, Effect of PGE2 injected at different times (30 min to 96 hr) in different groups of rats after injection of carrageenan plus WIPTIDE (B) or PKGI (C). All readings were taken 4 hr after prostaglandin E2 injection.n = 6 each group.

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    Fig. 5.

    A, Dose–response curve of ψεR (0.1–10,000 ng, n = 8)-induced mechanical hyperalgesia measured at 30 min in the hindpaw of the rat.B, PGE2-induced hyperalgesia at 30 min, 4 hr, and 24 hr in rats treated 5 d previously with ψεR (1 μg,n = 6). C, Time course of ψεR (1 μg/paw, n = 12)-induced hyperalgesia (1 μg).D, Role of second messengers important in ψεR-induced hyperalgesia. PKA inhibitor WIPTIDE (WIP/ΨεR; both 1 μg, n = 24), the nitric oxide synthase inhibitor NG-methyl-l-arginine (L-NMA/ΨεR; both 1 μg,n = 12), the PKC inhibitor bisindolylmalemide 1 hydrochloride (Bis/ΨεR; both 1 μg, n = 12), the PKCε inhibitor (PKCεV1–2/ΨεR; both 1 μg,n = 12), the PKG inhibitor (PKGI/ΨεR; both 1 μg,n = 8), the guanylyl cyclase inhibitor ODQ (ODQ/ΨεR; both 1 μg,n = 6), the calcium transport antagonist 3,4,5-trimethoxybezoic acid 8-(diethylamino) octyl ester (TMB/ΨεR; both 1 μg,n = 6), the calcium chelator (2-[(2-bis-[carboxymethyl] amino-5-methylphenoxy) methyl]-6-methoxy-8-bis[carboxymethy] aminoquinoline (Quin/ΨεR; both 1 μg, n = 6), or the NMDA receptor antagonist MK-801 (MK801/ΨεR; both 1 μg,n = 8) 5 min before injection of ψεR (1 μg). All readings were taken 30 min after injection of ψεR.E, Role of second messengers in PGE2-induced hyperalgesia in rats pretreated with ψεR. Rats were administered the PKA inhibitor WIPTIDE (E2/WIP; 100 ng/1 μg,n = 6), the nitric oxide synthase inhibitorl-NMA (E2/ L-NMA; 100 ng/1 μg,n = 6), the PKC inhibitor Bis (E2/Bis; 100 ng/1 μg, n = 10), the PKCε inhibitor (E2/PKCεV1–2; 100 ng/1 μg, n = 6), the calcium antagonists Quin-2 and TMB-8 (E2/Quin and E2/TMB; both 100 ng/1 μg, both n = 6), or the NMDA receptor antagonist MK-801 (E2/MK801; 100 ng/1 μg,n = 10) 5 min before injection of PGE2(E2) (100 ng) on the fifth day after receiving ψεR (1 μg). All readings were taken 4 hr after injection of PGE2.

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The Journal of Neuroscience: 20 (12)
Journal of Neuroscience
Vol. 20, Issue 12
15 Jun 2000
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Chronic Hypersensitivity For Inflammatory Nociceptor Sensitization Mediated by the ε Isozyme of Protein Kinase C
K. O. Aley, Robert O. Messing, Daria Mochly-Rosen, Jon D. Levine
Journal of Neuroscience 15 June 2000, 20 (12) 4680-4685; DOI: 10.1523/JNEUROSCI.20-12-04680.2000

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Chronic Hypersensitivity For Inflammatory Nociceptor Sensitization Mediated by the ε Isozyme of Protein Kinase C
K. O. Aley, Robert O. Messing, Daria Mochly-Rosen, Jon D. Levine
Journal of Neuroscience 15 June 2000, 20 (12) 4680-4685; DOI: 10.1523/JNEUROSCI.20-12-04680.2000
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Keywords

  • carrageenan
  • chronic pain
  • inflammation
  • prostaglandin E2
  • protein kinase Cε
  • second messenger

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