A Sensory-Labeled Line for Cold: TRPM8-Expressing Sensory Neurons Define the Cellular Basis for Cold, Cold Pain, and Cooling-Mediated Analgesia

Knowlton, Wendy; Palkar, Radhika; Lippoldt, Erika K.; McCoy, Daniel D.; Baluch, Farhan; Chen, Jessica; McKemy, David D.

doi:10.1523/jneurosci.1943-12.2013

Cited by 236 publications

(266 citation statements)

References 61 publications

(165 reference statements)

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“…WT mice show robust cold allodynia 2 d after unilateral injections of the inflammatory agent complete Freund's adjuvant (CFA) (Fig. 1A) (P < 0.01, pre-vs. post-CFA or ipsilateral vs. contralateral), which we and others have previously reported (22)(23)(24). In contrast, Gfrα3 −/− mice show no differences in their hind paw lift latencies between the ipsilateral (inflamed) and the contralateral (control) sides, and there were no differences in their sensitivity compared with the basal, preinflamed state (Fig.…”

Section: Significancesupporting

confidence: 50%

“…1B) (P < 0.01, preinjury vs. 7 d postinjury; P < 0.001, ipsilateral vs. contralateral), but cold sensitivity was remarkably unchanged in Gfrα3 −/− mice (ipsilateral vs. contralateral; preinjury vs. 7 d postinjury; P > 0.05). Lastly, one of the major side effects of platin-based chemotherapeutics is cold pain (26), a phenotype that can be modeled in mice given a single systemic injection of oxaliplatin (22,23). As with the previous pain models, the cold allodynia observed in WT mice (P < 0.001, basal vs. 7 d postinjection) was completely absent in mice null for GFRα3 ( Fig.…”

Section: Significancementioning

confidence: 65%

“…Artemin-and NGF-induced sensitization of cold responses is TRPM8-dependent, and multiple studies have shown that TRPM8 plays a role in the development of cold allodynia (8,(22)(23)(24)57). However, inflammatory cold allodynia is also diminished by both an TRPA1 antagonist and reduced TRPA1 transcript expression, and cold hypersensitivity can be induced by TRPA1 agonism in WT but not Trpa1 −/− mice (58, 59).…”

Section: Discussionmentioning

confidence: 99%

“…Adult WT or GFRα3 −/− mice (a gift from Brian Davis, University of Pittsburgh, Children's Hospital of Pittsburgh, Pittsburgh, PA) of both sexes were used in behavioral assays. Cold, heat, and mechanical sensitivity were assayed as described (19,22).…”

Section: Methodsmentioning

confidence: 99%

“…Next, to test the role of GFRα3 in pathological cold pain, we examined adult WT and Gfrα3 −/− littermates in classical models of inflammation, nerve injury, and chemotherapeutic-induced neuropathic pain (22,23). WT mice show robust cold allodynia 2 d after unilateral injections of the inflammatory agent complete Freund's adjuvant (CFA) (Fig.…”

Section: Significancementioning

confidence: 99%

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Inflammatory and neuropathic cold allodynia are selectively mediated by the neurotrophic factor receptor GFRα3

Lippoldt

Ongun

Kusaka

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Tissue injury prompts the release of a number of proalgesic molecules that induce acute and chronic pain by sensitizing pain-sensing neurons (nociceptors) to heat and mechanical stimuli. In contrast, many proalgesics have no effect on cold sensitivity or can inhibit cold-sensitive neurons and diminish cooling-mediated pain relief (analgesia). Nonetheless, cold pain (allodynia) is prevalent in many inflammatory and neuropathic pain settings, with little known of the mechanisms promoting pain vs. those dampening analgesia. Here, we show that cold allodynia induced by inflammation, nerve injury, and chemotherapeutics is abolished in mice lacking the neurotrophic factor receptor glial cell line-derived neurotrophic factor family of receptors-α3 (GFRα3). Furthermore, established cold allodynia is blocked in animals treated with neutralizing antibodies against the GFRα3 ligand, artemin. In contrast, heat and mechanical pain are unchanged, and results show that, in striking contrast to the redundant mechanisms sensitizing other modalities after an insult, cold allodynia is mediated exclusively by a single molecular pathway, suggesting that artemin-GFRα3 signaling can be targeted to selectively treat cold pain.W hen pain continues past its usefulness as a warning of potential tissue damage, it becomes a debilitating condition for which few viable treatments are currently available. The result can be an exacerbation of pain in response to both innocuous (allodynia) and noxious (hyperalgesia) stimuli (1). For example, pain felt with normally pleasant mild cooling (cold allodynia) occurs in many pathological conditions, such as fibromyalgia, multiple sclerosis, stroke, and chemotherapeutic-induced polyneuropathy, but what underlies this specific form of pain at the cellular or molecular level is largely unknown (2-5). Pain-sensing afferent neurons (nociceptors) are sensitized during injury or disease, in part, by a vast array of proalgesic compounds termed the "inflammatory soup" (e.g., neurotrophic factors, protons, bradykinin, prostaglandins, and ATP) (1). These substances are released locally at the site of injury by infiltrating immune cells, such as macrophages, neutrophils, and T cells, as well as resident cells, including keratinocytes and mast cells (6), and either directly activate sensory receptors or sensitize them to subsequent stimuli (7). Moreover, prolonged inflammation can lead to central sensitization (in the spinal cord and brain) and bring about long-lasting chronic pain that persists after acute inflammation has resolved. Thus, a better understanding of the molecules involved in neuroinflammation may lead to therapeutic options for acute and chronic pain.Of the range of proalgesics known to promote pain, only nerve growth factor (NGF) and the glial cell line-derived neurotrophic factor family ligand (GFL) artemin have been shown to lead to cold hypersensitivity (8-11). Both are major components of the inflammatory soup and produce nociceptor sensitization and pain through their cognate cell surface rece...

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Section: Significancesupporting

confidence: 50%

Section: Significancementioning

confidence: 65%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Significancementioning

confidence: 99%

See 3 more Smart Citations

Inflammatory and neuropathic cold allodynia are selectively mediated by the neurotrophic factor receptor GFRα3

Lippoldt

Ongun

Kusaka

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Overview of chemesthesis with a look to the future

Carstens

2016

Chemesthesis

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Piezo2 expression in corneal afferent neurons

Bron

Wood

Brock

et al. 2014

J of Comparative Neurology

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Recently, a novel class of mechanically sensitive channels has been identified and have been called Piezo channels. In this study, we explored Piezo channel expression in sensory neurons supplying the guinea pig corneal epithelium, which have well-defined modalities in this species. We hypothesized that a proportion of corneal afferent neurons express Piezo2, and that these neurons are neurochemically distinct from corneal polymodal nociceptors or cold-sensing neurons. We used a combination of retrograde tracing to identify corneal afferent neurons and double label in situ hybridization and/or immunohistochemistry to determine their molecular and/or neurochemical profile. We found that Piezo2 expression occurs in ∼26% of trigeminal ganglion neurons and 30% of corneal afferent neurons. Piezo2 corneal afferent neurons are almost exclusively non-calcitonin gene-related peptide (CGRP)-immunoreactive (-IR), medium- to large-sized neurons that are NF200-IR, suggesting they are not corneal polymodal nociceptors. There was no coexpression of Piezo2 and transient receptor potential cation channel subfamily M member 8 (TRPM8) transcripts in any corneal afferent neurons, further suggesting that Piezo2 is not expressed in corneal cold-sensing neurons. We also noted that TRPM8-IR or CGRP-IR corneal afferent neurons are almost entirely small and lack NF200-IR. Piezo2 expression occurs in a neurochemically distinct subpopulation of corneal afferent neurons that are not polymodal nociceptors or cold-sensing neurons, and is likely confined to a subpopulation of pure mechano-nociceptors in the cornea. This provides the first evidence in an in vivo system that Piezo2 is a strong candidate for a channel that transduces noxious mechanical stimuli.

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A Sensory-Labeled Line for Cold: TRPM8-Expressing Sensory Neurons Define the Cellular Basis for Cold, Cold Pain, and Cooling-Mediated Analgesia

Cited by 236 publications

References 61 publications

Inflammatory and neuropathic cold allodynia are selectively mediated by the neurotrophic factor receptor GFRα3

Inflammatory and neuropathic cold allodynia are selectively mediated by the neurotrophic factor receptor GFRα3

Overview of chemesthesis with a look to the future

Piezo2 expression in corneal afferent neurons

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