Repeated hapten exposure induces persistent tactile sensitivity in mice modeling localized provoked vulvodynia

Landry, Jasmine; Martinov, Tijana; Mengistu, Hanna; Dhanwada, Jyothi; Benck, Charles J.; Kline, Jessica; Boo, Beebie; Swanson, Linnea; Tonc, Elena; Daughters, Randy S.; Fife, Brian T.; Chatterjea, Devavani

doi:10.1371/journal.pone.0169672

Cited by 14 publications

(37 citation statements)

References 52 publications

(77 reference statements)

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“…Our finding regarding proliferation of CGRP-containing nerve fibres is consistent with that shown in the oxazolone hypersensitivity model of vulvodynia (Landry et al, 2017), and proliferation of CGRP-containing nerve fibres identified in a subset of mice (40%) that demonstrated hyperalgesia in the repeated fungal infection model of vulvodynia, following three rounds of candida albicans infection (Farmer et al, 2011). Further work is required to precisely identify the origin of nerve fibres, however it has been shown that CGRP-and SP-containing nerve fibres in the mouse vagina are associated with lumbar and sacral DRG, and these peptides are not found in autonomic ganglion neurons associated with the vagina (Jobling and Lim, 2008, Vilimas et al, 2011, Barry et al, 2017).…”

Section: Infiltration Of Immune-competent Cells Is a Hallmark Of Inflsupporting

confidence: 91%

“…Resident mast cells are part of the innate immune system and release mediators that contribute to nociceptor sensitisation (Drummond, 2004, Ren andDubner, 2010). Mast cell accumulation in vulvar tissue has been described in a mouse model of oxazolone induced hypersensitivity, concurrent with hyperinnervation involving CGRP-immunoreactive nerve fibres (Landry et al, 2017). The results of clinical studies are variable.…”

Section: Infiltration Of Immune-competent Cells Is a Hallmark Of Inflmentioning

confidence: 99%

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Innervation Changes Induced by Inflammation in the Murine Vagina

Sharma

Yap

et al. 2018

Neuroscience

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Vulvodynia is a prevalent chronic pain disorder associated with high medical costs and often ineffective treatments. The major pathological feature is proliferation of vaginal nerve fibers. This study aimed to develop a highly reproducible animal model to study neuroproliferation in the vagina and aid the identification of appropriately targeted treatments for conditions such as vulvodynia. Mild chronic inflammation was induced using microinjection of complete Freund's adjuvant in the distal vagina of C57Bl/6 mice. Control mice received saline. Inflammation and innervation density were assessed at 7 and 28 days after a single administration or 14 days following repeated administration of complete Freund's adjuvant or saline. Histochemistry and blinded-analysis of images were used to assess vaginal morphology (H & E) and abundance of macrophages (CD68-labeling), mast cells (toluidine blue staining, mast cell tryptase-immunoreactivity), blood vessels (αSMA-immunoreactivity) and nerve fibers immunoreactive for the pan-neuronal marker PGP9.5. Subpopulations of nerve fibers were identified using immunoreactivity for calcitonin gene-related peptide (CGRP), substance P (SP), vasoactive intestinal peptide (VIP) and neuropeptide Y (NPY). Single administration of complete Freund's adjuvant resulted in vaginal swelling, macrophage infiltration, vascular proliferation and increased abundance of nerve fibers immunoreactive for CGRP, SP, VIP and/or PGP9.5 but not NPY, evident at seven days. Inflammation further increased following repeated administration of complete Freund's adjuvant but nerve fiber proliferation did not. Nerve fiber proliferation continued to be evident at 28 days. The inter-individual differences within each treatment group were small, indicating that this model may be useful to study mechanisms underlying vaginal nerve fiber proliferation associated with inflammation.

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Section: Infiltration Of Immune-competent Cells Is a Hallmark Of Inflsupporting

confidence: 91%

Section: Infiltration Of Immune-competent Cells Is a Hallmark Of Inflmentioning

confidence: 99%

Innervation Changes Induced by Inflammation in the Murine Vagina

Sharma

Yap

et al. 2018

Neuroscience

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“…Tissue levels of Cxcl2, IL-1β and IL-6 were evaluated as previously described [ 20 , 21 ], from whole cell lysates using cytokine specific duo-set ELISA kits (R&D Systems, Minneapolis, MN, USA). Total serum Immunoglobulin E (IgE) content was measured by ELISA (Bethyl Laboratories, Montogomery, TX, USA) in serum isolated from blood collected either from the sub-manibular vein or by post-mortem heart puncture.…”

Section: Methodsmentioning

confidence: 99%

“…Before taking sensitivity measurements, the mice were placed in individual Plexiglass von Frey chambers over a wire mesh grating for fifteen minutes to acclimate [ 19 ]. We have previously shown that hapten sensitization alone does not change tactile sensitivity neither does estrus stage [ 19 , 20 ]. Two baseline measurements are taken at 1 and 2 days prior to sensitization for about twice the number of mice needed for the experiment.…”

Section: Methodsmentioning

confidence: 99%

Repeated dermal application of the common preservative methylisothiazolinone triggers local inflammation, T cell influx, and prolonged mast cell-dependent tactile sensitivity in mice

et al. 2020

Self Cite

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Occupational exposure to toxic chemicals increases the risk of developing localized provoked vulvodynia—a prevalent, yet poorly understood, chronic condition characterized by sensitivity to touch and pressure, and accumulation of mast cells in painful tissues. Here, we topically sensitized female ND4 Swiss mice to the common household and industrial preservative methylisothiazolinone (MI) and subsequently challenged them daily with MI or acetone and olive oil vehicle on the labiar skin. MI-challenged mice developed significant, persistent tactile sensitivity and long-lasting local accumulation of mast cells alongside early, transient increases in CD4 + and CD8 + T cells, eosinophils, neutrophils, and increases in pro-inflammatory cytokines. Therapeutic administration of imatinib, a c-Kit inhibitor known to inhibit mast cell survival, led to reduced mast cell accumulation and alleviated tactile genital pain. We provide the first pre-clinical evidence of dermal MI-induced mast-cell dependent pain and lay the groundwork for detailed understanding of these intersections between MI-driven immunomodulation and chronic pain.

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“… 7 , 31 There is evidence that both peripheral and central nervous system mechanisms contribute to the onset and persistence of vulvodynia. Biological factors thought to precipitate vulvodynia include atopic disease leading to vestibular mast-cell proliferation, 32 , 33 vestibular mucosa alterations linked to combined hormonal contraception use 34 , 35 (see also Reed et al), 36 pelvic floor-muscle dysfunction, 37 , 38 gene polymorphisms that interfere with pain regulation, 39 and nociceptor proliferation and sensitization. 40 , 41 Genetic predispositions to infection, inflammation, and/or hormonal changes have also been identified as risk factors for the development of vulvodynia.…”

Section: Introductionmentioning

confidence: 99%

Vulvodynia: a consideration of clinical and methodological research challenges and recommended solutions

Corsini‐Munt¹,

Rancourt²,

Dubé³

et al. 2017

JPR

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Vulvodynia, an idiopathic chronic vulvar pain, is a prevalent genital pain condition that results in significant impairment to sexual, relational, and psychological functioning of affected women and their romantic partners. Despite its high prevalence, there remain gaps in knowledge and health care access for women coping with vulvodynia, given its varied clinical presentation and no widely accepted treatment protocol. The past several decades have seen important advancements in understanding vulvodynia and developing effective treatments; however, progress has been impeded due to clinical and methodological challenges in conducting research with this vulnerable population. This review presents a brief overview of vulvodynia correlates, consequences, etiology, and treatment, and then turns its attention to considering the clinical and methodological challenges that hinder vulvodynia research. Identifying these barriers alongside potential mitigating solutions is essential to developing empirically supported treatments for all women affected by vulvodynia, across all age and minority groups. Potential solutions will require researchers to broaden eligibility criteria, examine subgroups of women, and expand definitions of treatment outcomes, and may be best facilitated by more active collaboration among research groups and across relevant disciplines. Engagement in these solutions may contribute to more representative findings and the development and dissemination of empirically based treatment options for this complex pain condition.

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Repeated hapten exposure induces persistent tactile sensitivity in mice modeling localized provoked vulvodynia

Cited by 14 publications

References 52 publications

Innervation Changes Induced by Inflammation in the Murine Vagina

Innervation Changes Induced by Inflammation in the Murine Vagina

Repeated dermal application of the common preservative methylisothiazolinone triggers local inflammation, T cell influx, and prolonged mast cell-dependent tactile sensitivity in mice

Vulvodynia: a consideration of clinical and methodological research challenges and recommended solutions

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