Corticotropin-Releasing Factor in the Brain and Blocking Spinal Descending Signals Induce Hyperalgesia in the Latent Sensitization Model of Chronic Pain

Chen, Wenling; Taché, Yvette; Marvizón, Juan Carlos G.

doi:10.1016/j.neuroscience.2018.03.024

Cited by 23 publications

(23 citation statements)

References 67 publications

(95 reference statements)

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“…Contralateral latent sensitization is poorly understood, and possible mechanisms for future study include not only descending facilitation (Chai et al, 2012;Porreca et al, 2002;Taylor and Corder, 2014) and suppression of descending inhibition from brainstem nuclei (Chen et al, 2018), but also neuroimmune interactions (Cairns et al, 2015) and communication of reactive astrocytes through gap junction connexins (Gao and Ji, 2010), although neither naltrexone (Corder et al, 2013) nor LY2456302 ( Figure 7) induced pERK activation in astrocytes.…”

Section: Accepted Manuscriptmentioning

confidence: 99%

Sex differences in kappa opioid receptor inhibition of latent postoperative pain sensitization in dorsal horn

Custodio-Patsey

Donahue

et al. 2020

Neuropharmacology

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Tissue injury produces a delicate balance between latent pain sensitization (LS) and compensatory endogenous opioid receptor analgesia that continues for months, even after re-establishment of normal pain thresholds. To evaluate the contribution of mu (MOR), delta (DOR), and/or kappa (KOR) opioid receptors to the silencing of chronic postoperative pain, we performed plantar incision at the hindpaw, waited 21 days for the resolution of hyperalgesia, and then intrathecally injected subtype-selective ligands. We found that the MOR-selective inhibitor CTOP (1-1000ng) dose-dependently reinstated mechanical hyperalgesia. Two DOR-selective inhibitors naltrindole (1-10 µg) and TIPP[Ψ] (1-20µg) reinstated mechanical hyperalgesia, but only at the highest dose that also produced itching, licking, and tail biting. Both the prototypical KOR-selective inhibitors nor-BNI (0.1-10µg) and the newer KOR inhibitor with more canonical pharmocodynamic effects, LY2456302 (0.1-10µg), reinstated mechanical hyperalgesia. Furthermore, LY2456302 (10µg) increased the expression of phosphorylated signalregulated kinase (pERK), a marker of central sensitization, in dorsal horn neurons but not glia. Sex studies revealed that LY2456302 (0.3 µg) reinstated hyperalgesia and pERK expression to a greater degree in female as compared to male mice. Our results suggest that spinal MOR and KOR, but not DOR, maintain LS within a state of remission to reduce the intensity and duration of postoperative pain, and that endogenous KOR but not MOR analgesia is greater in female mice.

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Section: Accepted Manuscriptmentioning

confidence: 99%

Sex differences in kappa opioid receptor inhibition of latent postoperative pain sensitization in dorsal horn

Custodio-Patsey

Donahue

et al. 2020

Neuropharmacology

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“…The transition to chronic pain can also occur through another recently described mechanism known as “latent sensitization” (LS). LS is pathological pain following injury or inflammation that is “masked” during apparent recovery by endogenous opioid receptor function and “unmasked” by treatment with an opioid inverse agonist, such as naltrexone, or by stress [3–10]. In this study, we compare the effects of morphine and a novel opioid on both the paradoxical exacerbation of pain and on LS, with the goal of assessing the new analog for preventing the transition from acute to chronic pain.…”

Section: Introductionmentioning

confidence: 99%

“…Comprehensively described by Taylor [8], Corder [4], and Marvizon [3, 6], LS and endogenous dependence are best thought of as two sides of the same coin; the phenomena are inextricably linked and cause a susceptibility to unmasking pain through either stress or chemical inactivation of Mu-opioid receptor (MOR) constitutive activity. The initial pain insult activates pain pathways (“accelerator”) and descending pathways induce constitutive activity at the MOR (MOR CA ) to counteract pain (“brake”).…”

Section: Introductionmentioning

confidence: 99%

Morphine immunomodulation prolongs inflammatory and postoperative pain while the novel analgesic ZH853 accelerates recovery and protects against latent sensitization

Feehan

Zadina

2019

J Neuroinflammation

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Background: Numerous studies have identified the proinflammatory, pronociceptive effects of morphine which ultimately exacerbate pain. Our novel endomorphin analog ZH853 does not produce proinflammatory effects on its own and gives potent, long-lasting analgesia. This study investigates whether ZH853's lack of interaction with the neuroimmune system reduces the risk of prolonged pain. Methods: Adult male Sprague-Dawley rats were subjected to one of two treatment paradigms. Either (1) chronic pain followed by chronic treatment with morphine, ZH853 or vehicle, or (2) chronic drug administered prior to pain induction. Complete Freund's adjuvant (CFA) was injected or paw incision surgery was performed on the left hind plantar foot pad. Drugs were administered through Alzet osmotic minipumps at a rate of 1 μl/h for 5 days at appropriate doses based on prior experiments. Animals were tested for mechanical allodynia and thermal hyperalgesia using von Frey filaments and the Hargreaves apparatus, respectively. Additionally, several gait parameters were measured using the CatWalk XT. When all animals had recovered from pain, 1 mg/kg of naltrexone was administered to test for development of latent sensitization (LS). A second set of animals was used to investigate dorsal horn inflammation following CFA and drug treatment. ANOVAs were used to assess differences between drug treatment groups. Results: As expected, morphine increased and prolonged pain in all experiments compared to vehicle treatment. However, ZH853 treatment reduced the overall time spent in pain and the severity of pain scores compared to morphine. ZH853 not only reduced inflammation versus morphine treatment but also, in some instances, acted as an anti-inflammatory drug compared to vehicle treatment. Finally, ZH853 prevented the development of LS while vehicle-and morphine-treated animals showed robust relapse to pain. Conclusions: ZH853 has a favorable side effect profile versus morphine and provides superior analgesia in a number of pain states. We now know that chronic use of this compound reduces time spent in a chronic pain state, the opposite of common opioids like morphine, and reduces the risk of LS, making ZH853 an excellent candidate for clinical development in humans for inflammatory and postoperative pain.

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“…Hill (2000) suggested that the analgesic effects of NK1R antagonists could be due to their supraspinal effects on stress (Rupniak and Kramer, 2017). Indeed, stress induces hyperalgesia in rats with latent sensitization (Chen et al, 2018b;Rivat et al, 2007). However, in this study both RP67580 and NTX were given intrathecally, so it is unlikely that they had supraspinal effects.…”

Section: Failure Of Nk1r Antagonists In Clinical Trialsmentioning

confidence: 73%

“…Mechanical allodynia was measured with von Frey filaments (Touch-Test) using the twoout-of-three method (Chen et al, 2018b;Jarahi et al, 2014;Kingery et al, 2000;Michot et al, 2012;Walwyn et al, 2016). Measures were done by putting the rats in acrylic enclosures on an elevated metal grid (IITC Life Science Inc., CA), to which the rats were habituated for 30 min, daily for 3 days.…”

Section: Measures Of Mechanical Hyperalgesiamentioning

confidence: 99%

Neurokinin 1 receptor activation in the rat spinal cord maintains latent sensitization, a model of inflammatory and neuropathic chronic pain

Chen

Marvizón

2020

Preprint

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Latent sensitization is a model of chronic pain in which a persistent state of pain hypersensitivity is suppressed by opioid receptors, as evidenced by the ability of opioid antagonists to induce a period of mechanical allodynia. Our objective was to determine if substance P and its neurokinin 1 receptor (NK1R) mediate the maintenance of latent sensitization. Latent sensitization was induced by injecting rats in the hindpaw with complete Freund's adjuvant (CFA), or by spared nerve injury (SNI). When responses to von Frey filaments returned to baseline (day 28), the rats were injected intrathecally with saline or the NK1R antagonist RP67580, followed 15 min later by intrathecal naltrexone. In both pain models, the saline-injected rats developed allodynia for 2 h after naltrexone, but not the RP67580injected rats. Saline or RP67580 were injected daily for two more days. Five days later (day 35), naltrexone was injected intrathecally. Again, the saline-injected rats, but not the RP67580injected rats, developed allodynia in response to naltrexone. To determine if there is sustained activation of NK1Rs during latent sensitization, NK1R internalization was measured in lamina I neurons in rats injected in the paw with saline or CFA, and then injected intrathecally with saline or naltrexone on day 28. The rats injected with CFA had a small amount of NK1R internalization that was significantly higher than in the saline-injected rats. Naltrexone increased NK1R internalization in the CFA-injected rats but nor in the saline-injected rats. Therefore, sustained activation of NK1Rs maintains pain hypersensitivity during latent sensitization.

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Corticotropin-Releasing Factor in the Brain and Blocking Spinal Descending Signals Induce Hyperalgesia in the Latent Sensitization Model of Chronic Pain

Cited by 23 publications

References 67 publications

Sex differences in kappa opioid receptor inhibition of latent postoperative pain sensitization in dorsal horn

Sex differences in kappa opioid receptor inhibition of latent postoperative pain sensitization in dorsal horn

Morphine immunomodulation prolongs inflammatory and postoperative pain while the novel analgesic ZH853 accelerates recovery and protects against latent sensitization

Neurokinin 1 receptor activation in the rat spinal cord maintains latent sensitization, a model of inflammatory and neuropathic chronic pain

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