Morphine paradoxically prolongs neuropathic pain in rats by amplifying spinal NLRP3 inflammasome activation

Peter M. Grace; Keith A. Strand; Erika L. Galer; Daniel J. Urban; Xiaohui Wang; Michael V. Baratta; Timothy J. Fabisiak; Nathan D. Anderson; Kejun Cheng; Lisa I. Greene; Debra Berkelhammer; Yingning Zhang; Amanda L. Ellis; Hang Hubert Yin; Serge Campeau; Kenner C. Ricei; Bryan L. Roth; Steven F. Maier; Linda R. Watkins

doi:10.1073/pnas.1602070113

Morphine paradoxically prolongs neuropathic pain in rats by amplifying spinal NLRP3 inflammasome activation

Peter M. Grace, Keith A. Strand, Erika L. Galer, Daniel J. Urban, Xiaohui Wang, Michael V. Baratta, Timothy J. Fabisiak, Nathan D. Anderson, Kejun Cheng, Lisa I. Greene, Debra Berkelhammer, Yingning Zhang, Amanda L. Ellis, Hang Hubert Yin, Serge Campeau, Kenner C. Ricei, Bryan L. Roth, Steven F. Maier, Linda R. Watkins

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278 Scopus citations

Abstract

Opioid use for pain management has dramatically increased,with little assessment of potential pathophysiological consequences for the primary pain condition. Here, a short course of morphine, starting 10 d after injury in male rats, paradoxically and remarkably doubled the duration of chronic constriction injury (CCI)-allodynia, months after morphine ceased. No such effect of opioids on neuropathic pain has previously been reported. Using pharmacologic and genetic approaches, we discovered that the initiation and maintenance of this multimonth prolongation of neuropathic pain was mediated by a previously unidentified mechanism for spinal cord and pain-namely, morphine-induced spinal NOD-like receptor protein 3 (NLRP3) inflammasomes and associated release of interleukin-1β (IL-1β). As spinal dorsal horn microglia expressed this signaling platform, these cells were selectively inhibited in vivo after transfection with a novel Designer Receptor Exclusively Activated by Designer Drugs (DREADD). Multiday treatment with the DREADD-specific ligand clozapine-Noxide prevented and enduringly reversed morphine-induced persistent sensitization for weeks to months after cessation of clozapine- N-oxide. These data demonstrate both the critical importance of microglia and that maintenance of chronic pain created by early exposure to opioids can be disrupted, resetting pain to normal. These data also provide strong support for the recent "two-hit hypothesis" of microglial priming, leading to exaggerated reactivity after the second challenge, documented here in the context of nerve injury followed by morphine. This study predicts that prolonged pain is an unrealized and clinically concerning consequence of the abundant use of opioids in chronic pain.

Original language	English (US)
Pages (from-to)	E3441-E3450
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	113
Issue number	24
DOIs	https://doi.org/10.1073/pnas.1602070113
State	Published - Jun 14 2016
Externally published	Yes

Keywords

DAMP
Danger signals
Opioid-induced hyperalgesia
P2X7R
TLR4

ASJC Scopus subject areas

General

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10.1073/pnas.1602070113

Cite this

Grace, P. M., Strand, K. A., Galer, E. L., Urban, D. J., Wang, X., Baratta, M. V., Fabisiak, T. J., Anderson, N. D., Cheng, K., Greene, L. I., Berkelhammer, D., Zhang, Y., Ellis, A. L., Yin, H. H., Campeau, S., Ricei, K. C., Roth, B. L., Maier, S. F., & Watkins, L. R. (2016). Morphine paradoxically prolongs neuropathic pain in rats by amplifying spinal NLRP3 inflammasome activation. Proceedings of the National Academy of Sciences of the United States of America, 113(24), E3441-E3450. https://doi.org/10.1073/pnas.1602070113

Grace, PM, Strand, KA, Galer, EL, Urban, DJ, Wang, X, Baratta, MV, Fabisiak, TJ, Anderson, ND, Cheng, K, Greene, LI, Berkelhammer, D, Zhang, Y, Ellis, AL, Yin, HH, Campeau, S, Ricei, KC, Roth, BL, Maier, SF & Watkins, LR 2016, 'Morphine paradoxically prolongs neuropathic pain in rats by amplifying spinal NLRP3 inflammasome activation', Proceedings of the National Academy of Sciences of the United States of America, vol. 113, no. 24, pp. E3441-E3450. https://doi.org/10.1073/pnas.1602070113

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title = "Morphine paradoxically prolongs neuropathic pain in rats by amplifying spinal NLRP3 inflammasome activation",

abstract = "Opioid use for pain management has dramatically increased,with little assessment of potential pathophysiological consequences for the primary pain condition. Here, a short course of morphine, starting 10 d after injury in male rats, paradoxically and remarkably doubled the duration of chronic constriction injury (CCI)-allodynia, months after morphine ceased. No such effect of opioids on neuropathic pain has previously been reported. Using pharmacologic and genetic approaches, we discovered that the initiation and maintenance of this multimonth prolongation of neuropathic pain was mediated by a previously unidentified mechanism for spinal cord and pain-namely, morphine-induced spinal NOD-like receptor protein 3 (NLRP3) inflammasomes and associated release of interleukin-1β (IL-1β). As spinal dorsal horn microglia expressed this signaling platform, these cells were selectively inhibited in vivo after transfection with a novel Designer Receptor Exclusively Activated by Designer Drugs (DREADD). Multiday treatment with the DREADD-specific ligand clozapine-Noxide prevented and enduringly reversed morphine-induced persistent sensitization for weeks to months after cessation of clozapine- N-oxide. These data demonstrate both the critical importance of microglia and that maintenance of chronic pain created by early exposure to opioids can be disrupted, resetting pain to normal. These data also provide strong support for the recent {"}two-hit hypothesis{"} of microglial priming, leading to exaggerated reactivity after the second challenge, documented here in the context of nerve injury followed by morphine. This study predicts that prolonged pain is an unrealized and clinically concerning consequence of the abundant use of opioids in chronic pain.",

keywords = "DAMP, Danger signals, Opioid-induced hyperalgesia, P2X7R, TLR4",

author = "Grace, {Peter M.} and Strand, {Keith A.} and Galer, {Erika L.} and Urban, {Daniel J.} and Xiaohui Wang and Baratta, {Michael V.} and Fabisiak, {Timothy J.} and Anderson, {Nathan D.} and Kejun Cheng and Greene, {Lisa I.} and Debra Berkelhammer and Yingning Zhang and Ellis, {Amanda L.} and Yin, {Hang Hubert} and Serge Campeau and Ricei, {Kenner C.} and Roth, {Bryan L.} and Maier, {Steven F.} and Watkins, {Linda R.}",

note = "Funding Information: This work was supported by the American Pain Society Future Leaders in Pain Research Grants Program (P.M.G.); National Health and Medical Research Council CJ Martin Fellowship ID 1054091 (to P.M.G.); American Australian Association Sir KeithMurdoch Fellowship (P.M.G.); National Natural Science Foundation of China Grant 21543013 (to X.W.); Natural Science Foundation of Jilin Province Grant 20160101211JC (to X.W.); and NIH Grants DE021966, DA023132 (to L.R.W.), DA017204 (to D.J.U. and B.L.R.), U01MH105892 (to B.L.R.), and GM101279 (to H.H.Y.). The work of the Chemical Biology Research Branch was supported by the NIH Intramural Research Programs of the National Institute on Drug Abuse and the National Institute of Alcohol Abuse and Alcoholism.",

year = "2016",

month = jun,

day = "14",

doi = "10.1073/pnas.1602070113",

language = "English (US)",

volume = "113",

pages = "E3441--E3450",

journal = "Proceedings of the National Academy of Sciences of the United States of America",

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publisher = "National Academy of Sciences",

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T1 - Morphine paradoxically prolongs neuropathic pain in rats by amplifying spinal NLRP3 inflammasome activation

AU - Grace, Peter M.

AU - Strand, Keith A.

AU - Galer, Erika L.

AU - Urban, Daniel J.

AU - Wang, Xiaohui

AU - Baratta, Michael V.

AU - Fabisiak, Timothy J.

AU - Anderson, Nathan D.

AU - Cheng, Kejun

AU - Greene, Lisa I.

AU - Berkelhammer, Debra

AU - Zhang, Yingning

AU - Ellis, Amanda L.

AU - Yin, Hang Hubert

AU - Campeau, Serge

AU - Ricei, Kenner C.

AU - Roth, Bryan L.

AU - Maier, Steven F.

AU - Watkins, Linda R.

N1 - Funding Information: This work was supported by the American Pain Society Future Leaders in Pain Research Grants Program (P.M.G.); National Health and Medical Research Council CJ Martin Fellowship ID 1054091 (to P.M.G.); American Australian Association Sir KeithMurdoch Fellowship (P.M.G.); National Natural Science Foundation of China Grant 21543013 (to X.W.); Natural Science Foundation of Jilin Province Grant 20160101211JC (to X.W.); and NIH Grants DE021966, DA023132 (to L.R.W.), DA017204 (to D.J.U. and B.L.R.), U01MH105892 (to B.L.R.), and GM101279 (to H.H.Y.). The work of the Chemical Biology Research Branch was supported by the NIH Intramural Research Programs of the National Institute on Drug Abuse and the National Institute of Alcohol Abuse and Alcoholism.

PY - 2016/6/14

Y1 - 2016/6/14

N2 - Opioid use for pain management has dramatically increased,with little assessment of potential pathophysiological consequences for the primary pain condition. Here, a short course of morphine, starting 10 d after injury in male rats, paradoxically and remarkably doubled the duration of chronic constriction injury (CCI)-allodynia, months after morphine ceased. No such effect of opioids on neuropathic pain has previously been reported. Using pharmacologic and genetic approaches, we discovered that the initiation and maintenance of this multimonth prolongation of neuropathic pain was mediated by a previously unidentified mechanism for spinal cord and pain-namely, morphine-induced spinal NOD-like receptor protein 3 (NLRP3) inflammasomes and associated release of interleukin-1β (IL-1β). As spinal dorsal horn microglia expressed this signaling platform, these cells were selectively inhibited in vivo after transfection with a novel Designer Receptor Exclusively Activated by Designer Drugs (DREADD). Multiday treatment with the DREADD-specific ligand clozapine-Noxide prevented and enduringly reversed morphine-induced persistent sensitization for weeks to months after cessation of clozapine- N-oxide. These data demonstrate both the critical importance of microglia and that maintenance of chronic pain created by early exposure to opioids can be disrupted, resetting pain to normal. These data also provide strong support for the recent "two-hit hypothesis" of microglial priming, leading to exaggerated reactivity after the second challenge, documented here in the context of nerve injury followed by morphine. This study predicts that prolonged pain is an unrealized and clinically concerning consequence of the abundant use of opioids in chronic pain.

AB - Opioid use for pain management has dramatically increased,with little assessment of potential pathophysiological consequences for the primary pain condition. Here, a short course of morphine, starting 10 d after injury in male rats, paradoxically and remarkably doubled the duration of chronic constriction injury (CCI)-allodynia, months after morphine ceased. No such effect of opioids on neuropathic pain has previously been reported. Using pharmacologic and genetic approaches, we discovered that the initiation and maintenance of this multimonth prolongation of neuropathic pain was mediated by a previously unidentified mechanism for spinal cord and pain-namely, morphine-induced spinal NOD-like receptor protein 3 (NLRP3) inflammasomes and associated release of interleukin-1β (IL-1β). As spinal dorsal horn microglia expressed this signaling platform, these cells were selectively inhibited in vivo after transfection with a novel Designer Receptor Exclusively Activated by Designer Drugs (DREADD). Multiday treatment with the DREADD-specific ligand clozapine-Noxide prevented and enduringly reversed morphine-induced persistent sensitization for weeks to months after cessation of clozapine- N-oxide. These data demonstrate both the critical importance of microglia and that maintenance of chronic pain created by early exposure to opioids can be disrupted, resetting pain to normal. These data also provide strong support for the recent "two-hit hypothesis" of microglial priming, leading to exaggerated reactivity after the second challenge, documented here in the context of nerve injury followed by morphine. This study predicts that prolonged pain is an unrealized and clinically concerning consequence of the abundant use of opioids in chronic pain.

KW - DAMP

KW - Danger signals

KW - Opioid-induced hyperalgesia

KW - P2X7R

KW - TLR4

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Morphine paradoxically prolongs neuropathic pain in rats by amplifying spinal NLRP3 inflammasome activation

Abstract

Keywords

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