Autoimmunity contributes to nociceptive sensitization in a mouse model of complex regional pain syndrome

Li, Wenwu; Guo, Tian-Zhi; Shi, Xiaoshuang; Czirr, Eva; Stan, Trisha; Sahbaie, Peyman; Wyss‐Coray, Tony; Kingery, Wade S.; Clark, J. David

doi:10.1016/j.pain.2014.09.007

Cited by 78 publications

(99 citation statements)

References 66 publications

(79 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Sera from patients with CRPS has been reported to harbor autoantibodies targeting autonomic neurons [64,65], and IgG extracted from these sera reproduce some CRPS features in mice [66]. These early passive transfer experiments suggest roles for B cells and IgM [67], and IgG autoantibodies [66]. Additionally, there is strong pathological and physiological evidence that focal injury to nerves sustained during surgery (which breaches the blood-nerve barrier) sometimes triggers autoimmune neuropathy [68].…”

Section: Complex Regional Pain Syndromementioning

confidence: 99%

Immunotherapy Prospects for Painful Small-fiber Sensory Neuropathies and Ganglionopathies

Oaklander

2016

Neurotherapeutics

View full text Add to dashboard Cite

The best-known peripheral neuropathies are those affecting the large, myelinated motor and sensory fibers. These have well-established immunological causes and therapies. Far less is known about the somatic and autonomic "small fibers"; the unmyelinated C-fibers, thinly myelinated A-deltas, and postganglionic sympathetics. The small fibers sense pain and itch, innervate internal organs and tissues, and modulate the inflammatory and immune responses. Symptoms of small-fiber neuropathy include chronic pain and itch, sensory impairment, edema, and skin color, temperature, and sweating changes. Small-fiber polyneuropathy (SFPN) also causes cardiovascular, gastrointestinal, and urological symptoms, the neurologic origin of which often remains unrecognized. Routine electrodiagnostic study does not detect SFPN, so skin biopsies immunolabeled to reveal axons are recommended for diagnostic confirmation. Preliminary evidence suggests that dysimmunity causes some cases of small-fiber neuropathy. Several autoimmune diseases, including Sjögren and celiac, are associated with painful small-fiber ganglionopathy and distal axonopathy, and some patients with "idiopathic" SFPN have evidence of organ-specific dysimmunity, including serological markers. Dysimmune SFPN first came into focus in children and teenagers as they lack other risk factors, for example diabetes or toxic exposures. In them, the rudimentary evidence suggests humoral rather than cellular mechanisms and complement consumption. Preliminary evidence supports efficacy of corticosteroids and immunoglobulins in carefully selected children and adult patients. This paper reviews the evidence of immune causality and the limited data regarding immunotherapy for small-fiberpredominant ganglionitis, regional neuropathy (complex regional pain syndrome), and distal SFPN. These demonstrate the need to develop case definitions and outcome metrics to improve diagnosis, enable prospective trials, and dissect the mechanisms of small-fiber neuropathy.

show abstract

Section: Complex Regional Pain Syndromementioning

confidence: 99%

Immunotherapy Prospects for Painful Small-fiber Sensory Neuropathies and Ganglionopathies

Oaklander

2016

Neurotherapeutics

View full text Add to dashboard Cite

show abstract

“…105 Interestingly, autoimmunity has been suggested as one of the pathophysiological mechanisms that might underlie CRPS, because of the compelling evidence that CRPS is associated with an autoantibody-mediated autoimmune process in some patients 106 and in the CRPS animal model. 107 Moreover, anti-CD20 (B cell) treatment reduces IL-1 production and nociceptive responses in a laboratory model of CRPS. 107 Examination and characterization of the interactive pathways between the inflammasome and adaptive immunity leading to CRPS may provide insight into the pathophysiology and optimal treatment of CRPS.…”

Section: Complex Regional Pain Syndromementioning

confidence: 99%

“…107 Moreover, anti-CD20 (B cell) treatment reduces IL-1 production and nociceptive responses in a laboratory model of CRPS. 107 Examination and characterization of the interactive pathways between the inflammasome and adaptive immunity leading to CRPS may provide insight into the pathophysiology and optimal treatment of CRPS.…”

Section: Complex Regional Pain Syndromementioning

confidence: 99%

The inflammasome as a target for pain therapy

Zhang¹,

Li²,

Li³

et al. 2016

British Journal of Anaesthesia

View full text Add to dashboard Cite

The interleukin-1 family of cytokines are potent inducers of inflammation and pain. Proteolytic activation of this family of cytokines is under the control of several innate immune receptors that coordinate to form large multiprotein signalling platforms, termed inflammasomes. Recent evidence suggests that a wide range of inflammatory diseases, cancers, and metabolic and autoimmune disorders, in which pain is a common complaint, may be coordinated by inflammasomes. Activation of inflammasomes results in cleavage of caspase-1, which subsequently induces downstream initiation of several potent pro-inflammatory cascades. Therefore, it has been proposed that targeting inflammasome activity may be a novel and effective therapeutic strategy for these pain-related diseases. The purpose of this narrative review article is to provide the reader with an overview of the activation and regulation of inflammasomes and to investigate the potential therapeutic role of inflammasome inhibition in the treatment of diseases characterized by pain, including the following: complex regional pain syndrome, gout, rheumatoid arthritis, inflammatory pain, neuropathic pain, chronic prostatitis, chronic pelvic pain syndrome, and fibromyalgia. We conclude that the role of the inflammasome in pain-associated diseases is likely to be inflammasome subtype and disease specific. The currently available evidence suggests that disease-specific targeting of the assembly and activity of the inflammasome complex may be a novel therapeutic opportunity for the treatment of refractory pain in many settings.

show abstract

“…[16][17][18]58 Recently we observed that B cells contributed to the development and maintenance of CRPS -like changes in the mouse fracture model and postulated that IgM autoantibodies directed at antigens in the fracture limb skin and nerves contribute to nociceptive sensitization in CRPS. 23 Clinical support for this hypothesis include a recent study demonstrating that a third of CRPS patients exhibit strongly positive antinuclear antibody tests, a standard diagnostic test for autoimmune disease, 59 and small randomized trial of low dose IVIG demonstrated that some chronic CRPS patients had prolonged and dramatic symptom improvement after a single IVIG treatment 60 . Consistent with our prior results in fracture mice, at 4 weeks post-fracture in rats there was a dramatic increase in IgM and IgG deposition in the skin and sciatic nerve of the injured limb, and 4 weeks of zoledronate treatment failed to inhibit this increase (Fig.…”

Section: Discussionmentioning

confidence: 99%

“…After tibia fracture elevated levels of IgM complexes were observed in the skin and sciatic nerve of the injured limb, and fracture mice lacking B cells and immunoglobulin had attenuated post-fracture nociceptive sensitization. 23 Bisphosphonates can inhibit monocyte/ macrophage/dendritic cell migration, proliferation, and differentiation in vitro and reduce monocyte expression of TNF, IL-1, and IL-6 cytokines. [24][25][26][27][28][29] Bisphosphonate treatment also reduces serum levels of TNF, IL-1, and IL-6 in osteoporosis patients.…”

Section: Introductionmentioning

confidence: 99%

Bisphosphonates Inhibit Pain, Bone Loss, and Inflammation in a Rat Tibia Fracture Model of Complex Regional Pain Syndrome: Erratum

2017

Anesthesia &Amp; Analgesia

View full text Add to dashboard Cite

BACKGROUND-Bisphosphonates are used to prevent the bone loss and fractures associated with osteoporosis, bone metastases, multiple myeloma, and osteogenis deformans. Distal limb fractures cause regional bone loss with cutaneous inflammation and pain in the injured limb that can develop into complex regional pain syndrome (CRPS). Clinical trials have reported that antiresorptive bisphosphonates can prevent fracture-induced bone loss, inhibit serum inflammatory cytokine levels, and alleviate CRPS pain. Previously we observed that the inhibition of inflammatory cytokines or adaptive immune responses attenuated the development of pain behavior in a rat fracture model of CRPS and we hypothesized that bisphosphonates could prevent pain behavior, trabecular bone loss, post-fracture cutaneous cytokine up-regulation, and adaptive immune responses in this CRPS model.

show abstract

Autoimmunity contributes to nociceptive sensitization in a mouse model of complex regional pain syndrome

Cited by 78 publications

References 66 publications

Immunotherapy Prospects for Painful Small-fiber Sensory Neuropathies and Ganglionopathies

Immunotherapy Prospects for Painful Small-fiber Sensory Neuropathies and Ganglionopathies

The inflammasome as a target for pain therapy

Bisphosphonates Inhibit Pain, Bone Loss, and Inflammation in a Rat Tibia Fracture Model of Complex Regional Pain Syndrome: Erratum

Contact Info

Product

Resources

About