Passive transfer of fibromyalgia symptoms from patients to mice
Andreas Goebel, … , Camilla I. Svensson, David A. Andersson
Andreas Goebel, … , Camilla I. Svensson, David A. Andersson
Published July 1, 2021
Citation Information: J Clin Invest. 2021;131(13):e144201. https://doi.org/10.1172/JCI144201.
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Research Article Neuroscience

Passive transfer of fibromyalgia symptoms from patients to mice

Abstract

Fibromyalgia syndrome (FMS) is characterized by widespread pain and tenderness, and patients typically experience fatigue and emotional distress. The etiology and pathophysiology of fibromyalgia are not fully explained and there are no effective drug treatments. Here we show that IgG from FMS patients produced sensory hypersensitivity by sensitizing nociceptive neurons. Mice treated with IgG from FMS patients displayed increased sensitivity to noxious mechanical and cold stimulation, and nociceptive fibers in skin-nerve preparations from mice treated with FMS IgG displayed an increased responsiveness to cold and mechanical stimulation. These mice also displayed reduced locomotor activity, reduced paw grip strength, and a loss of intraepidermal innervation. In contrast, transfer of IgG-depleted serum from FMS patients or IgG from healthy control subjects had no effect. Patient IgG did not activate naive sensory neurons directly. IgG from FMS patients labeled satellite glial cells and neurons in vivo and in vitro, as well as myelinated fiber tracts and a small number of macrophages and endothelial cells in mouse dorsal root ganglia (DRG), but no cells in the spinal cord. Furthermore, FMS IgG bound to human DRG. Our results demonstrate that IgG from FMS patients produces painful sensory hypersensitivities by sensitizing peripheral nociceptive afferents and suggest that therapies reducing patient IgG titers may be effective for fibromyalgia.

Authors

Andreas Goebel, Emerson Krock, Clive Gentry, Mathilde R. Israel, Alexandra Jurczak, Carlos Morado Urbina, Katalin Sandor, Nisha Vastani, Margot Maurer, Ulku Cuhadar, Serena Sensi, Yuki Nomura, Joana Menezes, Azar Baharpoor, Louisa Brieskorn, Angelica Sandström, Jeanette Tour, Diana Kadetoff, Lisbet Haglund, Eva Kosek, Stuart Bevan, Camilla I. Svensson, David A. Andersson

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Figure 3

Passive transfer of hypersensitivity by IgG pooled from multiple patients.

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Passive transfer of hypersensitivity by IgG pooled from multiple patient...
Visual analog pain scores (VAS, A) and pressure-pain thresholds (PPT, B) in 2 pools of FMS patients and healthy control (HC) subjects. Pool 1, n = 8 FMS and n = 12 HC; Pool 2, n = 14 FMS and n = 10 HC. **P < 0.01, ***P < 0.001 by Mann-Whitney U test. Administration of IgG pooled from FMS patients produced mechanical (C) and cold (D) hypersensitivity in mice compared with pooled HC IgG, 4 days after the first injection. Pool 1, n = 6 mice per group; Pool 2, n = 12; line and whiskers indicate mean ± SEM. **P < 0.01, ***P < 0.001 by unpaired, 2-tailed t test. Time course of mechanical (E) and cold (F) hypersensitivity following administration of pooled IgG (Pool 1). *P < 0.05, FM vs. HC IgG; 2-way repeated measure ANOVA with Sidak’s correction. P < 0.05, ††P < 0.01, compared with day zero; 2-way repeated measure ANOVA followed by Dunnett’s test. Data in E and F are mean ± SEM of 6 mice per group.