Activation of adult rat CNS endothelial cells by opioid-induced toll-like receptor 4 (TLR4) signaling induces proinflammatory, biochemical, morphological, and behavioral sequelae

P. M. Grace; K. M. Ramos; K. M. Rodgers; X. Wang; M. R. Hutchinson; M. T. Lewis; K. N. Morgan; J. L. Kroll; F. R. Taylor; K. A. Strand; Y. Zhang; D. Berkelhammer; M. G. Huey; L. I. Greene; T. A. Cochran; H. Yin; D. S. Barth; K. W. Johnson; K. C. Rice; S. F. Maier; L. R. Watkins

doi:10.1016/j.neuroscience.2014.09.020

Activation of adult rat CNS endothelial cells by opioid-induced toll-like receptor 4 (TLR4) signaling induces proinflammatory, biochemical, morphological, and behavioral sequelae

P. M. Grace, K. M. Ramos, K. M. Rodgers, X. Wang, M. R. Hutchinson, M. T. Lewis, K. N. Morgan, J. L. Kroll, F. R. Taylor, K. A. Strand, Y. Zhang, D. Berkelhammer, M. G. Huey, L. I. Greene, T. A. Cochran, H. Yin, D. S. Barth, K. W. Johnson, K. C. Rice, S. F. MaierL. R. Watkins

Research output: Contribution to journal › Article › peer-review

56 Scopus citations

Abstract

CNS immune signaling contributes to deleterious opioid effects including hyperalgesia, tolerance, reward, and dependence/withdrawal. Such effects are mediated by opioid signaling at toll-like receptor 4 (TLR4), presumptively of glial origin. Whether CNS endothelial cells express TLR4 is controversial. If so, they would be well positioned for activation by blood-borne opioids, contributing to opioid-induced pro-inflammatory responses. These studies examined adult primary rat CNS endothelial cell responses to (-)-morphine or its mu opioid receptor (MOR)-inactive metabolite morphine-3-glucuronide (M3G), both known TLR4 agonists. We demonstrate that adult rat CNS endothelial cells express functional TLR4. M3G activated nuclear factor kappaB (NF-κB), increased tumor necrosis factor-α (TNFα) and cyclooxygenase-2 (COX2) mRNAs, and released prostaglandin E₂ (PGE₂) from these cells. (-)-Morphine-induced upregulation of TNFα mRNA and PGE₂ release were unmasked by pre-treatment with nalmefene, a MOR antagonist without TLR4 activity (unlike CTAP, shown to have both MOR- and TLR4-activity), suggestive of an interplay between MOR and TLR4 co-activation by (-)-morphine. In support, MOR-dependent Protein Kinase A (PKA) opposed TLR4 signaling, as PKA inhibition (H-89) also unmasked (-)-morphine-induced TNFα and COX2 mRNA upregulation. Intrathecal injection of CNS endothelial cells, stimulated in vitro with M3G, produced TLR4-dependent tactile allodynia. Further, cortical suffusion with M3G in vivo induced TLR4-dependent vasodilation. Finally, endothelial cell TLR4 activation by lipopolysaccharide and/or M3G was blocked by the glial inhibitors AV1013 and propentofylline, demonstrating endothelial cells as a new target of such drugs. These data indicate that (-)-morphine and M3G can activate CNS endothelial cells via TLR4, inducing proinflammatory, biochemical, morphological, and behavioral sequelae. CNS endothelial cells may have previously unanticipated roles in opioid-induced effects, in phenomena blocked by presumptive glial inhibitors, as well as TLR4-mediated phenomena more broadly.

Original language	English (US)
Pages (from-to)	299-317
Number of pages	19
Journal	Neuroscience
Volume	280
DOIs	https://doi.org/10.1016/j.neuroscience.2014.09.020
State	Published - Nov 7 2014
Externally published	Yes

Keywords

CTAP
Endothelial cell
M3G
Morphine
Nalmefene
TLR4

ASJC Scopus subject areas

General Neuroscience

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10.1016/j.neuroscience.2014.09.020

Cite this

Grace, P. M., Ramos, K. M., Rodgers, K. M., Wang, X., Hutchinson, M. R., Lewis, M. T., Morgan, K. N., Kroll, J. L., Taylor, F. R., Strand, K. A., Zhang, Y., Berkelhammer, D., Huey, M. G., Greene, L. I., Cochran, T. A., Yin, H., Barth, D. S., Johnson, K. W., Rice, K. C., ... Watkins, L. R. (2014). Activation of adult rat CNS endothelial cells by opioid-induced toll-like receptor 4 (TLR4) signaling induces proinflammatory, biochemical, morphological, and behavioral sequelae. Neuroscience, 280, 299-317. https://doi.org/10.1016/j.neuroscience.2014.09.020

Grace, PM, Ramos, KM, Rodgers, KM, Wang, X, Hutchinson, MR, Lewis, MT, Morgan, KN, Kroll, JL, Taylor, FR, Strand, KA, Zhang, Y, Berkelhammer, D, Huey, MG, Greene, LI, Cochran, TA, Yin, H, Barth, DS, Johnson, KW, Rice, KC, Maier, SF & Watkins, LR 2014, 'Activation of adult rat CNS endothelial cells by opioid-induced toll-like receptor 4 (TLR4) signaling induces proinflammatory, biochemical, morphological, and behavioral sequelae', Neuroscience, vol. 280, pp. 299-317. https://doi.org/10.1016/j.neuroscience.2014.09.020

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title = "Activation of adult rat CNS endothelial cells by opioid-induced toll-like receptor 4 (TLR4) signaling induces proinflammatory, biochemical, morphological, and behavioral sequelae",

abstract = "CNS immune signaling contributes to deleterious opioid effects including hyperalgesia, tolerance, reward, and dependence/withdrawal. Such effects are mediated by opioid signaling at toll-like receptor 4 (TLR4), presumptively of glial origin. Whether CNS endothelial cells express TLR4 is controversial. If so, they would be well positioned for activation by blood-borne opioids, contributing to opioid-induced pro-inflammatory responses. These studies examined adult primary rat CNS endothelial cell responses to (-)-morphine or its mu opioid receptor (MOR)-inactive metabolite morphine-3-glucuronide (M3G), both known TLR4 agonists. We demonstrate that adult rat CNS endothelial cells express functional TLR4. M3G activated nuclear factor kappaB (NF-κB), increased tumor necrosis factor-α (TNFα) and cyclooxygenase-2 (COX2) mRNAs, and released prostaglandin E2 (PGE2) from these cells. (-)-Morphine-induced upregulation of TNFα mRNA and PGE2 release were unmasked by pre-treatment with nalmefene, a MOR antagonist without TLR4 activity (unlike CTAP, shown to have both MOR- and TLR4-activity), suggestive of an interplay between MOR and TLR4 co-activation by (-)-morphine. In support, MOR-dependent Protein Kinase A (PKA) opposed TLR4 signaling, as PKA inhibition (H-89) also unmasked (-)-morphine-induced TNFα and COX2 mRNA upregulation. Intrathecal injection of CNS endothelial cells, stimulated in vitro with M3G, produced TLR4-dependent tactile allodynia. Further, cortical suffusion with M3G in vivo induced TLR4-dependent vasodilation. Finally, endothelial cell TLR4 activation by lipopolysaccharide and/or M3G was blocked by the glial inhibitors AV1013 and propentofylline, demonstrating endothelial cells as a new target of such drugs. These data indicate that (-)-morphine and M3G can activate CNS endothelial cells via TLR4, inducing proinflammatory, biochemical, morphological, and behavioral sequelae. CNS endothelial cells may have previously unanticipated roles in opioid-induced effects, in phenomena blocked by presumptive glial inhibitors, as well as TLR4-mediated phenomena more broadly.",

keywords = "CTAP, Endothelial cell, M3G, Morphine, Nalmefene, TLR4",

author = "Grace, {P. M.} and Ramos, {K. M.} and Rodgers, {K. M.} and X. Wang and Hutchinson, {M. R.} and Lewis, {M. T.} and Morgan, {K. N.} and Kroll, {J. L.} and Taylor, {F. R.} and Strand, {K. A.} and Y. Zhang and D. Berkelhammer and Huey, {M. G.} and Greene, {L. I.} and Cochran, {T. A.} and H. Yin and Barth, {D. S.} and Johnson, {K. W.} and Rice, {K. C.} and Maier, {S. F.} and Watkins, {L. R.}",

note = "Funding Information: This work was supported by the American Pain Society Future Leaders in Pain Research Small Grants Program ( KMR 2009–2011 ); F32NS066665 from NINDS ( KMR 2010–2013 ); NIH grants DA024044 , DE017782 , and DA023132 (LRW); American Australian Association Merck Company Foundation (MRH) and Sir Keith Murdoch (PMG) Fellowships; a National Health and Medical Research Council CJ Martin Fellowship (ID 465423, MRH 2007-2010; ID 1054091, PMG 2013-); an Australian Research Council Research Fellowship (DP110100297, MRH 2011-); and GM103843 and GM101279 (HY). The work of the Drug Design and Synthesis Section, CBRB, NIDA, and NIAAA was supported by the NIH Intramural Research Programs of the National Institute on Drug Abuse (NIDA) and the National Institute of Alcohol Abuse and Alcoholism (NIAAA). Publisher Copyright: {\textcopyright} 2014 IBRO.",

year = "2014",

month = nov,

day = "7",

doi = "10.1016/j.neuroscience.2014.09.020",

language = "English (US)",

volume = "280",

pages = "299--317",

journal = "Neuroscience",

issn = "0306-4522",

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TY - JOUR

T1 - Activation of adult rat CNS endothelial cells by opioid-induced toll-like receptor 4 (TLR4) signaling induces proinflammatory, biochemical, morphological, and behavioral sequelae

AU - Grace, P. M.

AU - Ramos, K. M.

AU - Rodgers, K. M.

AU - Wang, X.

AU - Hutchinson, M. R.

AU - Lewis, M. T.

AU - Morgan, K. N.

AU - Kroll, J. L.

AU - Taylor, F. R.

AU - Strand, K. A.

AU - Zhang, Y.

AU - Berkelhammer, D.

AU - Huey, M. G.

AU - Greene, L. I.

AU - Cochran, T. A.

AU - Yin, H.

AU - Barth, D. S.

AU - Johnson, K. W.

AU - Rice, K. C.

AU - Maier, S. F.

AU - Watkins, L. R.

N1 - Funding Information: This work was supported by the American Pain Society Future Leaders in Pain Research Small Grants Program ( KMR 2009–2011 ); F32NS066665 from NINDS ( KMR 2010–2013 ); NIH grants DA024044 , DE017782 , and DA023132 (LRW); American Australian Association Merck Company Foundation (MRH) and Sir Keith Murdoch (PMG) Fellowships; a National Health and Medical Research Council CJ Martin Fellowship (ID 465423, MRH 2007-2010; ID 1054091, PMG 2013-); an Australian Research Council Research Fellowship (DP110100297, MRH 2011-); and GM103843 and GM101279 (HY). The work of the Drug Design and Synthesis Section, CBRB, NIDA, and NIAAA was supported by the NIH Intramural Research Programs of the National Institute on Drug Abuse (NIDA) and the National Institute of Alcohol Abuse and Alcoholism (NIAAA). Publisher Copyright: © 2014 IBRO.

PY - 2014/11/7

Y1 - 2014/11/7

N2 - CNS immune signaling contributes to deleterious opioid effects including hyperalgesia, tolerance, reward, and dependence/withdrawal. Such effects are mediated by opioid signaling at toll-like receptor 4 (TLR4), presumptively of glial origin. Whether CNS endothelial cells express TLR4 is controversial. If so, they would be well positioned for activation by blood-borne opioids, contributing to opioid-induced pro-inflammatory responses. These studies examined adult primary rat CNS endothelial cell responses to (-)-morphine or its mu opioid receptor (MOR)-inactive metabolite morphine-3-glucuronide (M3G), both known TLR4 agonists. We demonstrate that adult rat CNS endothelial cells express functional TLR4. M3G activated nuclear factor kappaB (NF-κB), increased tumor necrosis factor-α (TNFα) and cyclooxygenase-2 (COX2) mRNAs, and released prostaglandin E2 (PGE2) from these cells. (-)-Morphine-induced upregulation of TNFα mRNA and PGE2 release were unmasked by pre-treatment with nalmefene, a MOR antagonist without TLR4 activity (unlike CTAP, shown to have both MOR- and TLR4-activity), suggestive of an interplay between MOR and TLR4 co-activation by (-)-morphine. In support, MOR-dependent Protein Kinase A (PKA) opposed TLR4 signaling, as PKA inhibition (H-89) also unmasked (-)-morphine-induced TNFα and COX2 mRNA upregulation. Intrathecal injection of CNS endothelial cells, stimulated in vitro with M3G, produced TLR4-dependent tactile allodynia. Further, cortical suffusion with M3G in vivo induced TLR4-dependent vasodilation. Finally, endothelial cell TLR4 activation by lipopolysaccharide and/or M3G was blocked by the glial inhibitors AV1013 and propentofylline, demonstrating endothelial cells as a new target of such drugs. These data indicate that (-)-morphine and M3G can activate CNS endothelial cells via TLR4, inducing proinflammatory, biochemical, morphological, and behavioral sequelae. CNS endothelial cells may have previously unanticipated roles in opioid-induced effects, in phenomena blocked by presumptive glial inhibitors, as well as TLR4-mediated phenomena more broadly.

AB - CNS immune signaling contributes to deleterious opioid effects including hyperalgesia, tolerance, reward, and dependence/withdrawal. Such effects are mediated by opioid signaling at toll-like receptor 4 (TLR4), presumptively of glial origin. Whether CNS endothelial cells express TLR4 is controversial. If so, they would be well positioned for activation by blood-borne opioids, contributing to opioid-induced pro-inflammatory responses. These studies examined adult primary rat CNS endothelial cell responses to (-)-morphine or its mu opioid receptor (MOR)-inactive metabolite morphine-3-glucuronide (M3G), both known TLR4 agonists. We demonstrate that adult rat CNS endothelial cells express functional TLR4. M3G activated nuclear factor kappaB (NF-κB), increased tumor necrosis factor-α (TNFα) and cyclooxygenase-2 (COX2) mRNAs, and released prostaglandin E2 (PGE2) from these cells. (-)-Morphine-induced upregulation of TNFα mRNA and PGE2 release were unmasked by pre-treatment with nalmefene, a MOR antagonist without TLR4 activity (unlike CTAP, shown to have both MOR- and TLR4-activity), suggestive of an interplay between MOR and TLR4 co-activation by (-)-morphine. In support, MOR-dependent Protein Kinase A (PKA) opposed TLR4 signaling, as PKA inhibition (H-89) also unmasked (-)-morphine-induced TNFα and COX2 mRNA upregulation. Intrathecal injection of CNS endothelial cells, stimulated in vitro with M3G, produced TLR4-dependent tactile allodynia. Further, cortical suffusion with M3G in vivo induced TLR4-dependent vasodilation. Finally, endothelial cell TLR4 activation by lipopolysaccharide and/or M3G was blocked by the glial inhibitors AV1013 and propentofylline, demonstrating endothelial cells as a new target of such drugs. These data indicate that (-)-morphine and M3G can activate CNS endothelial cells via TLR4, inducing proinflammatory, biochemical, morphological, and behavioral sequelae. CNS endothelial cells may have previously unanticipated roles in opioid-induced effects, in phenomena blocked by presumptive glial inhibitors, as well as TLR4-mediated phenomena more broadly.

KW - CTAP

KW - Endothelial cell

KW - M3G

KW - Morphine

KW - Nalmefene

KW - TLR4

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Activation of adult rat CNS endothelial cells by opioid-induced toll-like receptor 4 (TLR4) signaling induces proinflammatory, biochemical, morphological, and behavioral sequelae

Abstract

Keywords

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