RÉSUMÉ
OBJECTIVE: To explore and characterize somatosensory dysfunction in patients with post-polio syndrome and chronic pain, by conducting examinations with Quantitative Sensory Testing. DESIGN: A cross-sectional, descriptive, pilot study conducted during 1 month. SUBJECTS/PATIENTS: Six patients with previously established post-polio syndrome and related chronic pain. METHODS: All subjects underwent a neurological examination including neuromuscular function, bedside sensory testing, a thorough pain anamnesis, and pain drawing. Screening for neuropathic pain was done with 2 questionnaires. A comprehensive Quantitative Sensory Testing battery was conducted with z-score transformation of obtained data, enabling comparison with published reference values and the creation of sensory profiles, as well as comparison between the study site (more polio affected extremity) and internal control site (less affected extremity) for each patient. RESULTS: Derived sensory profiles showed signs of increased prevalence of sensory aberrations compared with reference values, especially Mechanical Pain Thresholds, with significant deviation from reference data in 5 out of 6 patients. No obvious differences in sensory functions were seen between study sites and internal control sites. CONCLUSION: Post-polio syndrome may be correlated with a mechanical hyperalgesia/allodynia and might be correlated to a somatosensory dysfunction. With lack of evident side-to-side differences, the possibility of a generalized dysfunction in the somatosensory system might be considered.
Sujet(s)
Syndrome post-poliomyélitique , Humains , Syndrome post-poliomyélitique/physiopathologie , Syndrome post-poliomyélitique/complications , Projets pilotes , Études transversales , Femelle , Mâle , Adulte d'âge moyen , Sujet âgé , Mesure de la douleur , Seuil nociceptif/physiologie , Douleur chronique/physiopathologie , Douleur chronique/étiologie , Douleur chronique/diagnostic , Troubles somatosensoriels/étiologie , Troubles somatosensoriels/physiopathologie , Troubles somatosensoriels/diagnostic , Adulte , Examen neurologique/méthodes , Hyperalgésie/physiopathologie , Hyperalgésie/diagnostic , Névralgie/étiologie , Névralgie/diagnostic , Névralgie/physiopathologieRÉSUMÉ
The potential brain mechanism underlying resilience to socially transferred allodynia remains unknown. Here, we utilize a well-established socially transferred allodynia paradigm to segregate male mice into pain-susceptible and pain-resilient subgroups. Brain screening results show that ventral tegmental area glutamatergic neurons are selectively activated in pain-resilient mice as compared to control and pain-susceptible mice. Chemogenetic manipulations demonstrate that activation and inhibition of ventral tegmental area glutamatergic neurons bi-directionally regulate resilience to socially transferred allodynia. Moreover, ventral tegmental area glutamatergic neurons that project specifically to the nucleus accumbens shell and lateral habenula regulate the development and maintenance of the pain-resilient phenotype, respectively. Together, we establish an approach to explore individual variations in pain response and identify ventral tegmental area glutamatergic neurons and related downstream circuits as critical targets for resilience to socially transferred allodynia and the development of conceptually innovative analgesics.
Sujet(s)
Acide glutamique , Hyperalgésie , Neurones , Noyau accumbens , Aire tegmentale ventrale , Animaux , Mâle , Hyperalgésie/physiopathologie , Aire tegmentale ventrale/physiopathologie , Souris , Acide glutamique/métabolisme , Noyau accumbens/physiopathologie , Neurones/métabolisme , Mésencéphale , Souris de lignée C57BL , Résilience psychologique , Habénula , Modèles animaux de maladie humaineRÉSUMÉ
Neuropathic pain, defined as the most terrible of all tortures, which a nerve wound may inflict, is a common chronic painful condition caused by gradual damage or dysfunction of the somatosensory nervous system. As with many chronic diseases, neuropathic pain has a profound economic and emotional impact worldwide and represents a major public health issue from a treatment standpoint. This condition involves multiple sensory symptoms including impaired transmission and perception of noxious stimuli, burning, shooting, spontaneous pain, mechanical or thermal allodynia and hyperalgesia. Current pharmacological options for the treatment of neuropathic pain are limited, ineffective and have unacceptable side effects. In this framework, a deeper understanding of the pathophysiology and molecular mechanisms associated with neuropathic pain is key to the development of promising new therapeutical approaches. For this purpose, a plethora of experimental models that mimic common clinical features of human neuropathic pain have been characterized in rodents, with the spinal nerve ligation (SNL) model being one of the most widely used. In this chapter, we provide a detailed surgical procedure of the SNL model used to induce neuropathic pain in rats and mice. We further describe the behavioral approaches used for stimulus-evoked and spontaneous pain assessment in rodents. Finally, we demonstrate that our SNL model induces multiple pain behaviors in rats and mice.
Sujet(s)
Modèles animaux de maladie humaine , Névralgie , Nerfs spinaux , Animaux , Névralgie/anatomopathologie , Névralgie/physiopathologie , Névralgie/étiologie , Ligature/méthodes , Ligature/effets indésirables , Rats , Souris , Hyperalgésie/physiopathologie , Mesure de la douleur/méthodes , MâleRÉSUMÉ
BACKGROUND: Central poststroke pain (CPSP) is one of the primary sequelae following stroke, yet its underlying mechanisms are poorly understood. METHODS: By lesioning the lateral thalamic nuclei, we first established a CPSP model that exhibits mechanical and thermal hypersensitivity. Innocuous mechanical stimuli following the thalamic lesion evoked robust neural activation in somatosensory corticospinal neurons (CSNs), as well as in the deep dorsal horn, where low threshold mechanosensory afferents terminate. In this study, we used viral-based mapping and intersectional functional manipulations to decipher the role of somatosensory CSNs and their spinal targets in the CPSP pathophysiology. RESULTS: We first mapped the post-synaptic spinal targets of lumbar innervating CSNs using an anterograde trans-synaptic AAV1-based strategy and showed these spinal interneurons were activated by innocuous tactile stimuli post-thalamic lesion. Functionally, tetanus toxin-based chronic inactivation of spinal neurons targeted by CSNs prevented the development of CPSP. Consistently, transient chemogenetic silencing of these neurons alleviated established mechanical pain hypersensitivity and innocuous tactile stimuli evoked aversion linked to the CPSP. In contrast, chemogenetic activation of these neurons was insufficient to induce robust mechanical allodynia typically observed in the CPSP. CONCLUSION: The CSNs and their spinal targets are required but insufficient for the establishment of CPSP hypersensitivity. Our study provided novel insights into the neural mechanisms underlying CPSP and potential therapeutic interventions to treat refractory central neuropathic pain conditions.
Sujet(s)
Névralgie , Tractus pyramidaux , Accident vasculaire cérébral , Animaux , Névralgie/étiologie , Névralgie/physiopathologie , Mâle , Accident vasculaire cérébral/complications , Neurones , Hyperalgésie/physiopathologie , Hyperalgésie/étiologie , Rat Sprague-Dawley , Rats , Modèles animaux de maladie humaine , Moelle spinaleRÉSUMÉ
An intriguing perspective about human emotion, the theory of constructed emotion considers emotions as generative models according to the Bayesian brain hypothesis. This theory brings fresh insight to existing findings, but its complexity renders it challenging to test experimentally. We argue that laboratory studies of pain could support the theory because although some may not consider pain to be a genuine emotion, the theory must at minimum be able to explain pain perception and its dysfunction in pathology. We review emerging evidence that bear on this question. We cover behavioral and neural laboratory findings, computational models, placebo hyperalgesia, and chronic pain. We conclude that there is substantial evidence for a predictive processing account of painful experience, paving the way for a better understanding of neuronal and computational mechanisms of other emotions.
Sujet(s)
Théorème de Bayes , Émotions , Perception de la douleur , Humains , Émotions/physiologie , Perception de la douleur/physiologie , Encéphale/physiologie , Douleur/psychologie , Douleur/physiopathologie , Hyperalgésie/physiopathologie , Hyperalgésie/psychologie , Douleur chronique/psychologie , Douleur chronique/physiopathologieRÉSUMÉ
Spinal cord dorsal horn inhibition is critical to the processing of sensory inputs, and its impairment leads to mechanical allodynia. How this decreased inhibition occurs and whether its restoration alleviates allodynic pain are poorly understood. Here, we show that a critical step in the loss of inhibitory tone is the change in the firing pattern of inhibitory parvalbumin (PV)-expressing neurons (PVNs). Our results show that PV, a calcium-binding protein, controls the firing activity of PVNs by enabling them to sustain high-frequency tonic firing patterns. Upon nerve injury, PVNs transition to adaptive firing and decrease their PV expression. Interestingly, decreased PV is necessary and sufficient for the development of mechanical allodynia and the transition of PVNs to adaptive firing. This transition of the firing pattern is due to the recruitment of calcium-activated potassium (SK) channels, and blocking them during chronic pain restores normal tonic firing and alleviates chronic pain. Our findings indicate that PV is essential for controlling the firing pattern of PVNs and for preventing allodynia. Developing approaches to manipulate these mechanisms may lead to different strategies for chronic pain relief.
Sujet(s)
Douleur chronique , Parvalbumines , Parvalbumines/métabolisme , Animaux , Douleur chronique/métabolisme , Douleur chronique/physiopathologie , Souris , Neurones/métabolisme , Neurones/physiologie , Hyperalgésie/métabolisme , Hyperalgésie/physiopathologie , Mâle , Potentiels d'action/physiologie , Canaux potassiques calcium-dépendants de petite conductance/métabolismeRÉSUMÉ
Empathetic relationships and the social transference of behaviours have been shown to occur in humans, and more recently through the development of rodent models, where both fear and pain phenotypes develop in observer animals. Clinically, observing traumatic events can induce 'trauma and stressor-related disorders' as defined in the DSM 5. These disorders are often comorbid with pain and gastrointestinal disturbances; however, our understanding of how gastrointestinal - or visceral - pain can be vicariously transmitted is lacking. Visceral pain originates from the internal organs, and despite its widespread prevalence, remains poorly understood. We established an observation paradigm to assess the impact of witnessing visceral pain. We utilised colorectal distension (CRD) to induce visceral pain behaviours in a stimulus rodent while the observer rodent observed. Twenty four hours post-observation, the observer rodent's visceral sensitivity was assessed using CRD. The observer rodents were found to have significant hyperalgesia as determined by lower visceral pain threshold and higher number of total pain behaviours compared with controls. The behaviours of the observer animals during the observation were found to be correlated with the behaviours of the stimulus animal employed. We found that observer animals had hypoactivity of the hypothalamic-pituitary-adrenal (HPA) axis, highlighted by reduced corticosterone at 90 minutes post-CRD. Using c-Fos immunohistochemistry we showed that observer animals also had increased activation of the anterior cingulate cortex, and decreased activation of the paraventricular nucleus, compared with controls. These results suggest that witnessing another animal in pain produces a behavioural phenotype and impacts the brain-gut axis.
Sujet(s)
Modèles animaux de maladie humaine , Stress psychologique , Douleur viscérale , Animaux , Mâle , Douleur viscérale/physiopathologie , Douleur viscérale/psychologie , Rats , Stress psychologique/physiopathologie , Rat Sprague-Dawley , Axe hypothalamohypophysaire/physiopathologie , Axe hypothalamohypophysaire/métabolisme , Hyperalgésie/physiopathologie , Axe hypophyso-surrénalien/physiopathologie , Axe hypophyso-surrénalien/métabolisme , Protéines proto-oncogènes c-fos/métabolisme , Seuil nociceptif/physiologieSujet(s)
Tolérance aux médicaments , Hyperalgésie , Morphine , Morphine/pharmacologie , Morphine/effets indésirables , Hyperalgésie/induit chimiquement , Hyperalgésie/physiopathologie , Animaux , Tolérance aux médicaments/physiologie , Facteurs d'échange de nucléotides guanyliques/métabolisme , Facteurs d'échange de nucléotides guanyliques/génétique , Souris , Analgésiques morphiniques/pharmacologie , HumainsRÉSUMÉ
Negative expectations can increase pain sensitivity, leading to nocebo hyperalgesia. However, the physiological and psychological factors that predispose individuals to this phenomenon are still not well understood. The present study examined whether stress induced by a social stressor affects nocebo hyperalgesia, and whether this effect is mediated by self-reported and physiological stress responses. We recruited 52 healthy participants (15 men) who were randomly assigned to either the Trier Social Stress Test (TSST) or a control condition (a friendly version of the TSST). Nocebo hyperalgesia was induced using negative suggestions combined with a validated pain conditioning paradigm. We assessed self-reported (anxiety and stress) and physiological (cortisol, alpha-amylase, heart rate, and skin conductance) responses to stress. Both groups exhibited significant nocebo hyperalgesia. The stress group showed higher levels of anxiety, self-reported stress, and cortisol levels compared to the control group while no significant differences were found in other physiological markers. The stress and control groups did not differ in the magnitude of nocebo hyperalgesia, but anxiety levels partially mediated the effects of the stress test on nocebo hyperalgesia. Our findings suggest that an external social stressor does not directly affect nocebo hyperalgesia, but that increased anxiety due to the stressor enhances its magnitude. Thus, it may be worthwhile to investigate whether reducing stress-related anxiety in clinical settings would help alleviate nocebo effects.
Sujet(s)
Réflexe psychogalvanique , Rythme cardiaque , Hydrocortisone , Hyperalgésie , Effet nocebo , Autorapport , Stress psychologique , Humains , Mâle , Femelle , Hyperalgésie/physiopathologie , Hyperalgésie/psychologie , Hydrocortisone/métabolisme , Hydrocortisone/analyse , Jeune adulte , Stress psychologique/physiopathologie , Stress psychologique/psychologie , Réflexe psychogalvanique/physiologie , Adulte , Rythme cardiaque/physiologie , Anxiété/physiopathologie , Anxiété/psychologie , Stress physiologique/physiologie , Mesure de la douleur , Salive/métabolisme , Salive/composition chimique , alpha-Amylases/métabolisme , alpha-Amylases/analyse , Seuil nociceptif/physiologie , Seuil nociceptif/psychologieRÉSUMÉ
ABSTRACT: Evidence from previous studies supports the concept that spinal cord injury (SCI)-induced neuropathic pain (NP) has its neural roots in the peripheral nervous system. There is uncertainty about how and to which degree mechanoreceptors contribute. Sensorimotor activation-based interventions (eg, treadmill training) have been shown to reduce NP after experimental SCI, suggesting transmission of pain-alleviating signals through mechanoreceptors. The aim of the present study was to understand the contribution of mechanoreceptors with respect to mechanical allodynia in a moderate mouse contusion SCI model. After genetic ablation of tropomyosin receptor kinase B expressing mechanoreceptors before SCI, mechanical allodynia was reduced. The identical genetic ablation after SCI did not yield any change in pain behavior. Peptidergic nociceptor sprouting into lamina III/IV below injury level as a consequence of SCI was not altered by either mechanoreceptor ablation. However, skin-nerve preparations of contusion SCI mice 7 days after injury yielded hyperexcitability in nociceptors, not in mechanoreceptors, which makes a substantial direct contribution of mechanoreceptors to NP maintenance unlikely. Complementing animal data, quantitative sensory testing in human SCI subjects indicated reduced mechanical pain thresholds, whereas the mechanical detection threshold was not altered. Taken together, early mechanoreceptor ablation modulates pain behavior, most likely through indirect mechanisms. Hyperexcitable nociceptors seem to be the main drivers of SCI-induced NP. Future studies need to focus on injury-derived factors triggering early-onset nociceptor hyperexcitability, which could serve as targets for more effective therapeutic interventions.
Sujet(s)
Modèles animaux de maladie humaine , Hyperalgésie , Mécanorécepteurs , Souris de lignée C57BL , Traumatismes de la moelle épinière , Animaux , Traumatismes de la moelle épinière/complications , Traumatismes de la moelle épinière/métabolisme , Traumatismes de la moelle épinière/physiopathologie , Souris , Hyperalgésie/physiopathologie , Hyperalgésie/étiologie , Hyperalgésie/métabolisme , Mécanorécepteurs/métabolisme , Mécanorécepteurs/physiologie , Mâle , Humains , Seuil nociceptif/physiologie , Femelle , Mesure de la douleur , Souris transgéniques , Névralgie/étiologie , Névralgie/métabolisme , Névralgie/physiopathologieRÉSUMÉ
Fibromyalgia (FM) is characterized by chronic widespread musculoskeletal pain accompanied by fatigue and muscle atrophy. Although its etiology is not known, studies have shown that FM patients exhibit altered function of the sympathetic nervous system (SNS), which regulates nociception and muscle plasticity. Nevertheless, the precise SNS-mediated mechanisms governing hyperalgesia and skeletal muscle atrophy in FM remain unclear. Thus, we employed two distinct FM-like pain models, involving intramuscular injections of acidic saline (pH 4.0) or carrageenan in prepubertal female rats, and evaluated the catecholamine content, adrenergic signaling and overall muscle proteolysis. Subsequently, we assessed the contribution of the SNS to the development of hyperalgesia and muscle atrophy in acidic saline-injected rats treated with clenbuterol (a selective ß2-adrenergic receptor agonist) and in animals maintained under baseline conditions and subjected to epinephrine depletion through adrenodemedullation (ADM). Seven days after inducing an FM-like model with acidic saline or carrageenan, we observed widespread mechanical hyperalgesia along with loss of strength and/or muscle mass. These changes were associated with reduced catecholamine content, suggesting a common underlying mechanism. Notably, treatment with a ß2-agonist alleviated hyperalgesia and prevented muscle atrophy in acidic saline-induced FM-like pain, while epinephrine depletion induced mechanical hyperalgesia and increased muscle proteolysis in animals under baseline conditions. Together, the results suggest that reduced sympathetic activity is involved in the development of pain and muscle atrophy in the murine model of FM analyzed.
Sujet(s)
Clenbutérol , Modèles animaux de maladie humaine , Fibromyalgie , Hyperalgésie , Amyotrophie , Système nerveux sympathique , Animaux , Femelle , Fibromyalgie/anatomopathologie , Fibromyalgie/physiopathologie , Amyotrophie/anatomopathologie , Amyotrophie/physiopathologie , Hyperalgésie/physiopathologie , Hyperalgésie/anatomopathologie , Système nerveux sympathique/physiopathologie , Système nerveux sympathique/effets des médicaments et des substances chimiques , Système nerveux sympathique/anatomopathologie , Clenbutérol/pharmacologie , Rats , Carragénane/toxicité , Rat Sprague-Dawley , Douleur/anatomopathologie , Douleur/physiopathologie , Épinéphrine , Muscles squelettiques/anatomopathologie , Muscles squelettiques/effets des médicaments et des substances chimiques , Muscles squelettiques/physiopathologie , Catécholamines/métabolisme , Agonistes bêta-adrénergiques/pharmacologieRÉSUMÉ
Vestibulodynia is a complex pain disorder characterized by chronic discomfort in the vulvar region, often accompanied by tactile allodynia and spontaneous pain. In patients a depressive behaviour is also observed. In this study, we have used a model of vestibulodynia induced by complete Freund's adjuvant (CFA) focusing our investigation on the spinal cord neurons and microglia. We investigated tactile allodynia, spontaneous pain, and depressive-like behavior as key behavioral markers of vestibulodynia. In addition, we conducted in vivo electrophysiological recordings to provide, for the first time to our knowledge, the characterization of the spinal sacral neuronal activity in the L6-S1 dorsal horn of the spinal cord. Furthermore, we examined microglia activation in the L6-S1 dorsal horn using immunofluorescence, unveiling hypertrophic phenotypes indicative of neuroinflammation in the spinal cord. This represents a novel insight into the role of microglia in vestibulodynia pathology. To address the therapeutic aspect, we employed pharmacological interventions using GABApentin, amitriptyline, and PeaPol. Remarkably, all three drugs, also used in clinic, showed efficacy in alleviating tactile allodynia and depressive-like behavior. Concurrently, we also observed a normalization of the altered neuronal firing and a reduction of microglia hypertrophic phenotypes. In conclusion, our study provides a comprehensive understanding of the CFA-induced model of vestibulodynia, encompassing behavioral, neurophysiological and neuroinflammatory aspects. These data pave the way to investigate spinal cord first pain plasticity in vestibulodynia.
Sujet(s)
Modèles animaux de maladie humaine , Adjuvant Freund , Hyperalgésie , Microglie , Neurones , Moelle spinale , Vulvodynie , Animaux , Moelle spinale/métabolisme , Moelle spinale/physiopathologie , Souris , Hyperalgésie/physiopathologie , Hyperalgésie/métabolisme , Vulvodynie/physiopathologie , Vulvodynie/métabolisme , Femelle , Microglie/métabolisme , Neurones/métabolisme , Maladies neuro-inflammatoires/physiopathologie , Gabapentine/pharmacologie , Amitriptyline/pharmacologie , Dépression/physiopathologie , Dépression/métabolisme , Souris de lignée C57BLRÉSUMÉ
Delayed-onset muscle soreness (DOMS) is a common phenomenon that occurs following a sudden increase in exercise intensity or unfamiliar exercise, significantly affecting athletic performance and efficacy in athletes and fitness individuals. DOMS is characterized by allodynia and hyperalgesia, and their mechanisms remain unclear. Recent studies have reported that neurotrophic factors, such as nerve growth factor (NGF) and glial cell derived neurotrophic factor (GDNF), are involved in the development and maintenance of DOMS. This article provides a review of the research progress on the signaling pathways related to the involvement of NGF and GDNF in DOMS, hoping to provide novel insights into the mechanisms underlying allodynia and hyperalgesia in DOMS, as well as potential targeted treatment.
Sujet(s)
Facteur neurotrophique dérivé des cellules gliales , Myalgie , Facteur de croissance nerveuse , Humains , Myalgie/physiopathologie , Facteur de croissance nerveuse/métabolisme , Facteur de croissance nerveuse/physiologie , Facteur neurotrophique dérivé des cellules gliales/métabolisme , Facteur neurotrophique dérivé des cellules gliales/physiologie , Transduction du signal , Animaux , Hyperalgésie/physiopathologie , Muscles squelettiques/physiopathologie , Muscles squelettiques/physiologie , Exercice physique/physiologieRÉSUMÉ
The objective of this study is to determine whether the change in pain intensity over time differs between somatosensory functioning evolution profiles in knee osteoarthritis (KOA) patients undergoing total knee arthroplasty (TKA). This longitudinal prospective cohort study, conducted between March 2018 and July 2023, included KOA patients undergoing TKA in four hospitals in Belgium and the Netherlands. The evolution of the Knee Injury and Osteoarthritis Outcome Score (KOOS) subscale pain over time (baseline, 3 months, and 1 year post-TKA scores) was the outcome variable. The evolution scores of quantitative sensory testing (QST) and Central Sensitization Inventory (CSI) over time (baseline and 1 year post-TKA scores) were used to make subgroups. Participants were divided into separate normal, recovered, and persistent disturbed somatosensory subgroups based on the CSI, local and widespread pressure pain threshold [PPT] and heat allodynia, temporal summation [TS], and conditioned pain modulation [CPM]. Linear mixed model analyses were performed. Two hundred twenty-three participants were included. The persistent disturbed somatosensory functioning group had less pronounced pain improvement (based on CSI and local heat allodynia) and worse pain scores 1 year post-TKA (based on CSI, local PPT and heat allodynia, and TS) compared to the normal somatosensory functioning group. This persistent group also had worse pain scores 1 year post-TKA compared to the recovered group (based on CSI). The study suggests the presence of a "centrally driven central sensitization" subgroup in KOA patients awaiting TKA in four of seven grouping variables, comprising their less pain improvement or worse pain score after TKA. Future research should validate these findings further. The protocol is registered at clinicaltrials.gov (NCT05380648).
Sujet(s)
Arthroplastie prothétique de genou , Gonarthrose , Mesure de la douleur , Humains , Gonarthrose/chirurgie , Gonarthrose/physiopathologie , Femelle , Mâle , Études prospectives , Sujet âgé , Adulte d'âge moyen , Études longitudinales , Seuil nociceptif , Douleur postopératoire/étiologie , Belgique , Pays-Bas , Hyperalgésie/physiopathologieRÉSUMÉ
ABSTRACT: Few analgesics identified using preclinical models have successfully translated to clinical use. These translational limitations may be due to the unidimensional nature of behavioral response measures used to assess rodent nociception. Advances in high-speed videography for pain behavior allow for objective quantification of nuanced aspects of evoked paw withdrawal responses. However, whether videography-based assessments of mechanical hypersensitivity outperform traditional measurement reproducibility is unknown. First, we determined whether high-speed videography of paw withdrawal was reproducible across experimenters. Second, we examined whether this method distinguishes behavioral responses exhibited by naive mice and mice with complete Freund's adjuvant (CFA)-induced inflammation. Twelve experimenters stimulated naive C57BL/6 mice with varying mechanical stimuli. Paw withdrawal responses were recorded with high-speed videography and scored offline by one individual. Our group was unable to replicate the original findings produced by high-speed videography analysis. Surprisingly, â¼80% of variation was not accounted for by variables previously reported to distinguish between responses to innocuous and noxious stimuli (paw height, paw velocity, and pain score), or by additional variables (experimenter, time-of-day, and animal), but rather by unidentified factors. Similar high-speed videography assessments were performed in CFA- and vehicle-treated animals, and the cumulative data failed to reveal an effect of CFA injection on withdrawal as measured by high-speed videography. This study does not support using paw height, velocity, or pain score measurements from high-speed recordings to delineate behavioral responses to innocuous and noxious stimuli. Our group encourages the continued use of traditional mechanical withdrawal assessments until additional high-speed withdrawal measures are validated in established pain models.
Sujet(s)
Adjuvant Freund , Inflammation , Souris de lignée C57BL , Mesure de la douleur , Animaux , Souris , Mâle , Mesure de la douleur/méthodes , Adjuvant Freund/toxicité , Modèles animaux de maladie humaine , Hyperalgésie/physiopathologie , Enregistrement sur magnétoscope/méthodes , Reproductibilité des résultats , Stimulation physique/effets indésirables , Comportement animal/physiologie , Comportement animal/effets des médicaments et des substances chimiquesRÉSUMÉ
The measurement of withdrawal to experimenter-delivered mechanical stimuli (von Frey test) and to heat stimuli (radiant heat paw-withdrawal or Hargreaves' test) applied to the hind paws is ubiquitous in preclinical pain research, but no normative values for the most-common applications of these tests have ever been published. We analyzed a retrospective data set of withdrawal thresholds or latencies in 8,150 mice in which these measures were taken using replicate determinations, before and after injection of inflammatory substances or experimental nerve damage producing pain hypersensitivity, totaling 97,332 measurements. All mice were tested in the same physical laboratory over a 20-year period using similar equipment and procedures. We nonetheless find evidence of large interindividual variability, affected by tester, genotype, mouse sex, tester sex, replicate order, and injury. These factors are discussed, and we believe that these normative data will serve as a useful reference for expected values in preclinical pain testing. PERSPECTIVE: This article presents a retrospective analysis of a large data set of mouse von Frey and radiant heat paw-withdrawal (Hargreaves' test) measurements collected in a single laboratory over 20 years. In addition to serving as a normative guide, sources of variability are identified including genotype, tester, and sex.
Sujet(s)
Mesure de la douleur , Seuil nociceptif , Animaux , Souris , Femelle , Mâle , Mesure de la douleur/méthodes , Études rétrospectives , Seuil nociceptif/physiologie , Température élevée/effets indésirables , Douleur/diagnostic , Douleur/physiopathologie , Modèles animaux de maladie humaine , Stimulation physique , Hyperalgésie/diagnostic , Hyperalgésie/physiopathologieRÉSUMÉ
Abstract With the recovery of motor function, some spinal cord injury (SCI) patients still suffer from severe pain-like behaviors symptoms. Whether motor function correlates with neuropathic pain-like behaviors remain unclear. In this study, a longitudinal cohort study of mice with moderate thoracic 10 contusion was performed to explore the characteristics of neuropathic pain-like behaviors and its correlation with motor function in different sexes. Pain-like behaviors data up to 42 days post-injury (dpi) were collected and compared. Mice of both sexes were divided into three groups based on their Basso Mouse Scale at 42 dpi. There was no significant difference in motor function recovery between the sexes. Female mice showed more significant mechanical allodynia than males at 14 dpi, which was sustained until 42 dpi without significant dynamic changes. However, males showed a gradually worsening state and more severe mechanical allodynia than females at 28 dpi, and then the differences disappeared. Interestingly, male mice obtained more severe cold hyperalgesia symptoms than females. Additionally, we found that there was a correlation between the occurrence of mechanical allodynia and cold and thermal hyperalgesia. Importantly, motor function recovery was positively associated with the outcomes of neuropathic pain-like behaviors after SCI, which was more obvious in female mice. Our data not only revealed the characteristics of neuropathic pain-like behaviors but also clarified the correlations between motor function recovery and neuropathic pain-like behaviors after SCI. These findings may provide new opinions and suggestions for promoting the clinical diagnosis and treatment of neuropathic pain-like behaviors after SCI.
Sujet(s)
Hyperalgésie , Névralgie , Traumatismes de la moelle épinière , Animaux , Traumatismes de la moelle épinière/physiopathologie , Traumatismes de la moelle épinière/complications , Névralgie/physiopathologie , Névralgie/étiologie , Souris , Femelle , Mâle , Études longitudinales , Hyperalgésie/physiopathologie , Hyperalgésie/étiologie , Activité motrice/physiologie , Récupération fonctionnelle/physiologie , Comportement animal/physiologie , Souris de lignée C57BLRÉSUMÉ
ABSTRACT: Neuropathic corneal pain (NCP) is a new and ill-defined disease characterized by pain, discomfort, aching, burning sensation, irritation, dryness, and grittiness. However, the mechanism underlying NCP remain unclear. Here, we reported a novel rat model of primary NCP induced by long ciliary nerve (LCN) ligation. After sustained LCN ligation, the rats developed increased corneal mechanical and chemical sensitivity, spontaneous blinking, and photophobia, which were ameliorated by intraperitoneal injection of morphine or gabapentin. However, neither tear reduction nor corneal injury was observed in LCN-ligated rats. Furthermore, after LCN ligation, the rats displayed a significant reduction in corneal nerve density, as well as increased tortuosity and beading nerve ending. Long ciliary nerve ligation also notably elevated corneal responsiveness under resting or menthol-stimulated conditions. At a cellular level, we observed that LCN ligation increased calcitonin gene-related peptide (neuropeptide)-positive cells in the trigeminal ganglion (TG). At a molecular level, upregulated mRNA levels of ion channels Piezo2, TRPM8, and TRPV1, as well as inflammatory factors TNF-α, IL-1ß, and IL-6, were also detected in the TG after LCN ligation. Meanwhile, consecutive oral gabapentin attenuated LCN ligation-induced corneal hyperalgesia and increased levels of ion channels and inflammation factors in TG. This study provides a reliable primary NCP model induced by LCN ligation in rats using a simple, minimally invasive surgery technique, which may help shed light on the underlying cellular and molecular bases of NCP and aid in developing a new treatment for the disease.
Sujet(s)
Cornée , Modèles animaux de maladie humaine , Gabapentine , Névralgie , Rat Sprague-Dawley , Animaux , Névralgie/étiologie , Mâle , Rats , Gabapentine/pharmacologie , Gabapentine/usage thérapeutique , Ligature , Cornée/innervation , Ganglion trigéminal/métabolisme , Analgésiques/pharmacologie , Analgésiques/usage thérapeutique , Acide gamma-amino-butyrique/métabolisme , Acides cyclohexanecarboxyliques/pharmacologie , Acides cyclohexanecarboxyliques/usage thérapeutique , Peptide relié au gène de la calcitonine/métabolisme , Amines/pharmacologie , Amines/usage thérapeutique , Morphine/pharmacologie , Morphine/usage thérapeutique , Douleur oculaire/étiologie , Hyperalgésie/étiologie , Hyperalgésie/physiopathologieRÉSUMÉ
ABSTRACT: Women more often experience chronic pain conditions than men. Central sensitization (CS) is one key mechanism in chronic pain that can differ between the sexes. It is unknown whether CS processes are already more pronounced in healthy women than in men. In 66 subjects (33 women), a thermal CS induction protocol was applied to the dorsum of one foot and a sham protocol to the other. Spatial extent [cm 2 ] of secondary mechanical hyperalgesia (SMH) and dynamic mechanical allodynia were assessed as subjective CS proxy measures, relying on verbal feedback. Changes in nociceptive withdrawal reflex magnitude (NWR-M) and response rate (NWR-RR) recorded through surface electromyography at the biceps and rectus femoris muscles were used as objective CS proxies. The effect of the CS induction protocol on SMH was higher in women than in men (effect size 2.11 vs 1.68). Nociceptive withdrawal reflex magnitude results were statistically meaningful for women (effect size 0.31-0.36) but not for men (effect size 0.12-0.29). Differences between men and women were not meaningful. Nociceptive withdrawal reflex response rate at the rectus femoris increased in women after CS induction and was statistically different from NWR-RR in men (median differences of 13.7 and 8.4% for 120 and 140% reflex threshold current). The objective CS proxy differences indicate that dorsal horn CS processes are more pronounced in healthy women. The even larger sex differences in subjective CS proxies potentially reflect greater supraspinal influence in women. This study shows that sex differences are present in experimentally induced CS in healthy subjects, which might contribute to women's vulnerability for chronic pain.
Sujet(s)
Sensibilisation du système nerveux central , Électromyographie , Hyperalgésie , Caractères sexuels , Humains , Femelle , Mâle , Sensibilisation du système nerveux central/physiologie , Adulte , Hyperalgésie/physiopathologie , Jeune adulte , Seuil nociceptif/physiologie , Réflexe/physiologie , Mesure de la douleur/méthodes , Adulte d'âge moyenRÉSUMÉ
ABSTRACT: Abnormal encoding of somatosensory modalities (ie, mechanical, cold, and heat) are a critical part of pathological pain states. Detailed phenotyping of patients' responses to these modalities have raised hopes that analgesic treatments could one day be tailored to a patient's phenotype. Such precise treatment would require a profound understanding of the underlying mechanisms of specific pain phenotypes at molecular, cellular, and circuitry levels. Although preclinical pain models have helped in that regard, the lack of a unified assay quantifying detailed mechanical, cold, and heat pain responses on the same scale precludes comparing how analgesic compounds act on different sensory phenotypes. The conflict avoidance assay is promising in that regard, but testing conditions require validation for its use with multiple modalities. In this study, we improve upon the conflict avoidance assay to provide a validated and detailed assessment of all 3 modalities within the same animal, in mice. We first optimized testing conditions to minimize the necessary amount of training and to reduce sex differences in performances. We then tested what range of stimuli produce dynamic stimulus-response relationships for different outcome measures in naive mice. We finally used this assay to show that nerve injury produces modality-specific sex differences in pain behavior. Our improved assay opens new avenues to study the basis of modality-specific abnormalities in pain behavior.
