Immune cell–derived opioids protect against neuropathic pain in mice

Łabuz, Dominika; Schmidt, Yvonne; Schreiter, Anja; Rittner, Heike L.; Mousa, Shaaban A.; Machelska, Halina

doi:10.1172/jci36246

Cited by 67 publications

(106 citation statements)

References 50 publications

(118 reference statements)

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“…CRF applied at the CCI site in the most effective doses (20 ng at 2 days or 100 ng at 14 days) found earlier2930, significantly elevated von Frey thresholds, completely reversing mechanical hypersensitivity (to the thresholds before CCI) measured 30 min after injection, on days 2 and 14 following CCI in wild-type mice. In contrast, these CRF analgesic effects were virtually absent in END-KO, PENK-KO and PDYN-KO mice (Fig.…”

Section: Resultsmentioning

confidence: 91%

Distinct roles of exogenous opioid agonists and endogenous opioid peptides in the peripheral control of neuropathy-triggered heat pain

Łabuz

Celik

Zimmer

et al. 2016

Sci Rep

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Neuropathic pain often results from peripheral nerve damage, which can involve immune response. Local leukocyte-derived opioid peptides or exogenous opioid agonists inhibit neuropathy-induced mechanical hypersensitivity in animal models. Since neuropathic pain can also be augmented by heat, in this study we investigated the role of opioids in the modulation of neuropathy-evoked heat hypersensitivity. We used a chronic constriction injury of the sciatic nerve in wild-type and opioid peptide-knockout mice, and tested opioid effects in heat and mechanical hypersensitivity using Hargreaves and von Frey tests, respectively. We found that although perineural exogenous opioid agonists, including peptidergic ligands, were effective, the endogenous opioid peptides β-endorphin, Met-enkephalin and dynorphin A did not alleviate heat hypersensitivity. Specifically, corticotropin-releasing factor, an agent triggering opioid peptide secretion from leukocytes, applied perineurally did not attenuate heat hypersensitivity in wild-type mice. Exogenous opioids, also shown to release opioid peptides via activation of leukocyte opioid receptors, were equally analgesic in wild-type and opioid peptide-knockout mice, indicating that endogenous opioids do not contribute to exogenous opioid analgesia in heat hypersensitivity. Furthermore, exogenously applied opioid peptides were ineffective as well. Conversely, opioid peptides relieved mechanical hypersensitivity. Thus, both opioid type and sensory modality may determine the outcome of neuropathic pain treatment.

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Section: Resultsmentioning

confidence: 91%

Distinct roles of exogenous opioid agonists and endogenous opioid peptides in the peripheral control of neuropathy-triggered heat pain

Łabuz

Celik

Zimmer

et al. 2016

Sci Rep

Self Cite

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“…Also, the expression of opioid receptors on peripheral neurons is enhanced under inflammatory conditions 38,39 . Endogenous opioid peptides in sites of inflammation can be released spontaneously, though release is augmented by the presence of corticotropin-releasing factor or stress 40–42 . Importantly, in models of inflammation and metastatic bone cancer pain, the local injection of opioid receptor antagonists or antibodies enhance nociceptive sensitization by blocking local opioid signaling 15,42,43 .…”

Section: Discussionmentioning

confidence: 99%

“…Neutrophil depletion attenuated nerve injury induced hyperalgesia by potentially decreasing mediators responsible for induction of pain. However, local application of corticotropin-releasing factor to the site of nerve injury produced analgesia mediated by opioid containing leukocytes 40 . Therefore, it seems that the neutrophils and opioid peptides produced by them are participating in an intensely localized inflammatory response.…”

Section: Discussionmentioning

confidence: 99%

Roles of Gr-1+Leukocytes in Postincisional Nociceptive Sensitization and Inflammation

Sahbaie¹,

Li²,

Shi³

et al. 2012

Anesthesiology

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Background Neutrophils are one of the predominant immune cells migrating to surgical wound edges initially. They produce mediators both associated with supporting (interleukin [IL]-1β, C5a) and reducing (opioid peptides) pain. Studies demonstrate neutrophil depletion/blockade reduces nociceptive sensitization after nerve injury and carrageenan administration, but enhance sensitization in Complete Freund's Adjuvant inflammation. This research identifies the contribution of infiltrating neutrophils to incisional pain and inflammation. Methods Antibody-mediated Gr1+ neutrophil depletion preceded hind paw incisions. Sensitization to mechanical and thermal stimuli, effects on edema and local levels of IL-1β and C5a were measured. Local effects of C5a or IL-1 receptor antagonists, PMX53 and Anakinra on sensitization after neutrophil depletion were examined. Groups of 4–8 mice were used. Results Anti-Gr1 antibody depleted >90% of circulating and infiltrating skin neutrophils after incision. Neutrophil depletion did not change magnitude or duration of mechanical hypersensitivity in incised mice. However, paw edema was significantly reduced and heat hypersensitivity was slightly increased in depleted animals. In depleted animals IL-1β levels were half of controls 24 h after incision, while C5a levels were elevated in both. Prominent IL-1β immunohistochemical staining of epidermis was seen in both groups. PMX53 and Anakinra reduced incisional mechanical and heat nociceptive sensitization to the same extent regardless of neutrophil depletion. Conclusions Neutrophil-derived IL-1β and C5a do not appear to contribute critically to peri-incisional nociceptive signaling. Other sources of mediators like epidermal cells may need to be considered. Controlling inflammatory activation of resident cells in epidermis/deeper structures may show therapeutic efficacy in reducing pain from surgical incisions.

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“…In patients undergoing arthroscopic knee surgery, opioid-containing immune cells are detectable in the inflamed synovium and the blockade of intra-articular opioid receptors by naloxone results in significantly increased postoperative pain for up to 4 h (Stein et al, 1993). More recently, peripheral opioid analgesia has also been reported in experimental neuropathic pain (Labuz et al, 2009, 2010). …”

Section: Clinical Implications and Perspectivesmentioning

confidence: 99%

Targeting peripheral opioid receptors to promote analgesic and anti-inflammatory actions

2013

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Mechanisms of endogenous pain control are significant. Increasing studies have clearly produced evidence for the clinical usefulness of opioids in peripheral analgesia. The immune system uses mechanisms of cell migration not only to fight pathogens but also to control pain and inflammation within injured tissue. It has been demonstrated that peripheral inflammatory pain can be effectively controlled by an interaction of immune cell-derived opioid peptides with opioid receptors on peripheral sensory nerve terminals. Experimental and clinical studies have clearly shown that activation of peripheral opioid receptors with exogenous opioid agonists and endogenous opioid peptides are able to produce significant analgesic and anti-inflammatory effects, without central opioid mediated side effects (e.g., respiratory depression, sedation, tolerance, dependence). This article will focus on the role of opioids in peripheral inflammatory conditions and the clinical implications of targeting peripheral opioid receptors.

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Immune cell–derived opioids protect against neuropathic pain in mice

Cited by 67 publications

References 50 publications

Distinct roles of exogenous opioid agonists and endogenous opioid peptides in the peripheral control of neuropathy-triggered heat pain

Distinct roles of exogenous opioid agonists and endogenous opioid peptides in the peripheral control of neuropathy-triggered heat pain

Roles of Gr-1+Leukocytes in Postincisional Nociceptive Sensitization and Inflammation

Targeting peripheral opioid receptors to promote analgesic and anti-inflammatory actions

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