Pain sensitivity dysfunction in a mouse model of Attention-Deficit / Hyperactivity Disorder (ADHD)

L’ADHD (Attention-deficit/hyperactivity disorder) est une maladie du développement caractérisée par l’impulsivité, l’hyperactivité, et l’inattention. Les voies neuronales impliquées dans ces déficits indiquent des dysfonctionnements dans les réseaux catécholaminergiques frontal-sous-corticaux, impliquant l'innervation dopaminergique et noradrénergique. Des études récentes ont mis en évidence une hypersensibilité à la douleur chez les patients ADHD et soulignent une possible comorbidité entre l’ADHD et la douleur. Cependant, les mécanismes et les circuits neuraux impliqués dans ces interactions sont inconnus. Afin de décrypter cette relation, nous avons généré un modèle ADHD de souris à P5 par une lésion néonatale des voies dopaminergiques centrales avec la 6-Hydroxydopamine (6-OHDA) et nous avons démontré la validité du modèle pour mimer le syndrome ADHD. Ensuite, nous avons analysé les comportements douloureux dans le modèle de souris 6-OHDA. Ces derniers présentent un abaissement des seuils de la douleur, ce qui suggère que l’ADHD induit une sensibilisation à la douleur (comorbidité ADHD-Douleur). Nous avons confirmé à l’aide d’enregistrements extracellulaires unitaires, que les modifications de la sensibilité à la douleur des souris 6-OHDA sont dues à une augmentation de l’excitabilité des neurones nociceptifs de la moelle épinière. Cette sensibilisation passe donc par une altération de l’intégration sensorielle dans la moelle épinière via la mise en jeu de contrôles descendants. La connectivité "cortex cingulaire antérieur (ACC) – insula postérieur (PI)" est la clé dans cette comorbidité ADHD-douleur, impliquée dans les fonctions exécutives, les émotions et elle envoie aussi des projections vers la corne dorsale de la moelle épinière. En effet, en combinant les analyses électrophysiologiques, optogénétiques et comportementales, nous avons démontré que les effets de l’ADHD sur la sensibilisation douloureuse passent par la mise en jeu de l’ACC et de la voie ACC – PI. En conclusion, nous montrons que les conditions ADHD induisent une hyperactivation des neurones nociceptifs de la moelle épinière et une hypersensibilité à la douleur. Nous suggérons également que le circuit ACC – PI pourrait déclencher un dysfonctionnement des neurones de la moelle épinière sur la douleur dans les conditions ADHD.Attention deficit hyperactivity disorder (ADHD) is characterized by the core symptoms of inattention, hyperactivity and impulsivity. Neural pathways underlying these deficits point to deficits within frontal-subcortical catecholaminergic networks, involving dopaminergic and noradrenergic innervation. Hence, impairment of the dopaminergic neurotransmission is a frequent target of ADHD medication. Low-dose psychostimulants, including methylphenidate (MpH) and amphetamines (AMP) are the most widely used treatments of ADHD. Recent evidence pointed to pain hypersensitivity in subjects with ADHD history, and suggests possible comorbidity of ADHD with pain. However, the mechanisms and neural circuits involved in these interactions are unknown. In order to understand this comorbidity, the first objective was to create a good animal model of ADHD. We generated a mouse model at P5 by neonatal disruption of central dopaminergic pathways with 6-Hydroxydopamine (6-OHDA) and we demonstrated the validity of the model to mimic ADHD syndrome. Next, we analyzed nociceptive responses in the 6-OHDA mouse model of ADHD. We found that 6-OHDA mice exhibited a marked decrease of withdrawal thresholds, suggesting that ADHD increase nociceptive sensitivity. Interestingly, by using in vivo electrophysiological recordings, we demonstrated that allodynia and hyperalgesia may be caused by neuronal hyperexcitability in the dorsal spinal cord. Moreover, we found that both lowered wihdrawal threshold and increased activity of nociceptive neurons in ADHD-like mice was not normalized by MpH. We tested the hypothesis that descending controls are responsible for pain alterations through the modulation of spinal circuits. The ‘anterior cingulate cortex (ACC) – posterior insular (PI)’ connectivity is at the cross-road of ADHD and pain, being involved in executive functions and emotions, as well as sending projections to the dorsal horn of the spinal cord. By combining electrophysiological, optogenetic and behavioral analyzes, we have shown that the effects of ADHD on painful sensitization involve the implication of ACC and the ACC - PI pathway. In conclusion, we showed that ADHD conditions induce spinal cord nociceptive neurons hyperactivation and pain hypersensitivity. We also suggest that the ACC - PI circuit may trigger dysfunction of spinal cord neurons in ADHD conditions

Pain sensitivity dysfunction in a mouse model of Attention-Deficit / Hyperactivity Disorder (ADHD)

L’ADHD (Attention-deficit/hyperactivity disorder) est une maladie du développement caractérisée par l’impulsivité, l’hyperactivité, et l’inattention. Les voies neuronales impliquées dans ces déficits indiquent des dysfonctionnements dans les réseaux catécholaminergiques frontal-sous-corticaux, impliquant l'innervation dopaminergique et noradrénergique. Des études récentes ont mis en évidence une hypersensibilité à la douleur chez les patients ADHD et soulignent une possible comorbidité entre l’ADHD et la douleur. Cependant, les mécanismes et les circuits neuraux impliqués dans ces interactions sont inconnus. Afin de décrypter cette relation, nous avons généré un modèle ADHD de souris à P5 par une lésion néonatale des voies dopaminergiques centrales avec la 6-Hydroxydopamine (6-OHDA) et nous avons démontré la validité du modèle pour mimer le syndrome ADHD. Ensuite, nous avons analysé les comportements douloureux dans le modèle de souris 6-OHDA. Ces derniers présentent un abaissement des seuils de la douleur, ce qui suggère que l’ADHD induit une sensibilisation à la douleur (comorbidité ADHD-Douleur). Nous avons confirmé à l’aide d’enregistrements extracellulaires unitaires, que les modifications de la sensibilité à la douleur des souris 6-OHDA sont dues à une augmentation de l’excitabilité des neurones nociceptifs de la moelle épinière. Cette sensibilisation passe donc par une altération de l’intégration sensorielle dans la moelle épinière via la mise en jeu de contrôles descendants. La connectivité "cortex cingulaire antérieur (ACC) – insula postérieur (PI)" est la clé dans cette comorbidité ADHD-douleur, impliquée dans les fonctions exécutives, les émotions et elle envoie aussi des projections vers la corne dorsale de la moelle épinière. En effet, en combinant les analyses électrophysiologiques, optogénétiques et comportementales, nous avons démontré que les effets de l’ADHD sur la sensibilisation douloureuse passent par la mise en jeu de l’ACC et de la voie ACC – PI. En conclusion, nous montrons que les conditions ADHD induisent une hyperactivation des neurones nociceptifs de la moelle épinière et une hypersensibilité à la douleur. Nous suggérons également que le circuit ACC – PI pourrait déclencher un dysfonctionnement des neurones de la moelle épinière sur la douleur dans les conditions ADHD.Attention deficit hyperactivity disorder (ADHD) is characterized by the core symptoms of inattention, hyperactivity and impulsivity. Neural pathways underlying these deficits point to deficits within frontal-subcortical catecholaminergic networks, involving dopaminergic and noradrenergic innervation. Hence, impairment of the dopaminergic neurotransmission is a frequent target of ADHD medication. Low-dose psychostimulants, including methylphenidate (MpH) and amphetamines (AMP) are the most widely used treatments of ADHD. Recent evidence pointed to pain hypersensitivity in subjects with ADHD history, and suggests possible comorbidity of ADHD with pain. However, the mechanisms and neural circuits involved in these interactions are unknown. In order to understand this comorbidity, the first objective was to create a good animal model of ADHD. We generated a mouse model at P5 by neonatal disruption of central dopaminergic pathways with 6-Hydroxydopamine (6-OHDA) and we demonstrated the validity of the model to mimic ADHD syndrome. Next, we analyzed nociceptive responses in the 6-OHDA mouse model of ADHD. We found that 6-OHDA mice exhibited a marked decrease of withdrawal thresholds, suggesting that ADHD increase nociceptive sensitivity. Interestingly, by using in vivo electrophysiological recordings, we demonstrated that allodynia and hyperalgesia may be caused by neuronal hyperexcitability in the dorsal spinal cord. Moreover, we found that both lowered wihdrawal threshold and increased activity of nociceptive neurons in ADHD-like mice was not normalized by MpH. We tested the hypothesis that descending controls are responsible for pain alterations through the modulation of spinal circuits. The ‘anterior cingulate cortex (ACC) – posterior insular (PI)’ connectivity is at the cross-road of ADHD and pain, being involved in executive functions and emotions, as well as sending projections to the dorsal horn of the spinal cord. By combining electrophysiological, optogenetic and behavioral analyzes, we have shown that the effects of ADHD on painful sensitization involve the implication of ACC and the ACC - PI pathway. In conclusion, we showed that ADHD conditions induce spinal cord nociceptive neurons hyperactivation and pain hypersensitivity. We also suggest that the ACC - PI circuit may trigger dysfunction of spinal cord neurons in ADHD conditions

Sensibilisation à la douleur chez un modèle murin de troubles du déficit de l'attention et de l'hyperactivité

Attention deficit hyperactivity disorder (ADHD) is characterized by the core symptoms of inattention, hyperactivity and impulsivity. Neural pathways underlying these deficits point to deficits within frontal-subcortical catecholaminergic networks, involving dopaminergic and noradrenergic innervation. Hence, impairment of the dopaminergic neurotransmission is a frequent target of ADHD medication. Low-dose psychostimulants, including methylphenidate (MpH) and amphetamines (AMP) are the most widely used treatments of ADHD. Recent evidence pointed to pain hypersensitivity in subjects with ADHD history, and suggests possible comorbidity of ADHD with pain. However, the mechanisms and neural circuits involved in these interactions are unknown. In order to understand this comorbidity, the first objective was to create a good animal model of ADHD. We generated a mouse model at P5 by neonatal disruption of central dopaminergic pathways with 6-Hydroxydopamine (6-OHDA) and we demonstrated the validity of the model to mimic ADHD syndrome. Next, we analyzed nociceptive responses in the 6-OHDA mouse model of ADHD. We found that 6-OHDA mice exhibited a marked decrease of withdrawal thresholds, suggesting that ADHD increase nociceptive sensitivity. Interestingly, by using in vivo electrophysiological recordings, we demonstrated that allodynia and hyperalgesia may be caused by neuronal hyperexcitability in the dorsal spinal cord. Moreover, we found that both lowered wihdrawal threshold and increased activity of nociceptive neurons in ADHD-like mice was not normalized by MpH. We tested the hypothesis that descending controls are responsible for pain alterations through the modulation of spinal circuits. The ‘anterior cingulate cortex (ACC) – posterior insular (PI)’ connectivity is at the cross-road of ADHD and pain, being involved in executive functions and emotions, as well as sending projections to the dorsal horn of the spinal cord. By combining electrophysiological, optogenetic and behavioral analyzes, we have shown that the effects of ADHD on painful sensitization involve the implication of ACC and the ACC - PI pathway. In conclusion, we showed that ADHD conditions induce spinal cord nociceptive neurons hyperactivation and pain hypersensitivity. We also suggest that the ACC - PI circuit may trigger dysfunction of spinal cord neurons in ADHD conditions.L’ADHD (Attention-deficit/hyperactivity disorder) est une maladie du développement caractérisée par l’impulsivité, l’hyperactivité, et l’inattention. Les voies neuronales impliquées dans ces déficits indiquent des dysfonctionnements dans les réseaux catécholaminergiques frontal-sous-corticaux, impliquant l'innervation dopaminergique et noradrénergique. Des études récentes ont mis en évidence une hypersensibilité à la douleur chez les patients ADHD et soulignent une possible comorbidité entre l’ADHD et la douleur. Cependant, les mécanismes et les circuits neuraux impliqués dans ces interactions sont inconnus. Afin de décrypter cette relation, nous avons généré un modèle ADHD de souris à P5 par une lésion néonatale des voies dopaminergiques centrales avec la 6-Hydroxydopamine (6-OHDA) et nous avons démontré la validité du modèle pour mimer le syndrome ADHD. Ensuite, nous avons analysé les comportements douloureux dans le modèle de souris 6-OHDA. Ces derniers présentent un abaissement des seuils de la douleur, ce qui suggère que l’ADHD induit une sensibilisation à la douleur (comorbidité ADHD-Douleur). Nous avons confirmé à l’aide d’enregistrements extracellulaires unitaires, que les modifications de la sensibilité à la douleur des souris 6-OHDA sont dues à une augmentation de l’excitabilité des neurones nociceptifs de la moelle épinière. Cette sensibilisation passe donc par une altération de l’intégration sensorielle dans la moelle épinière via la mise en jeu de contrôles descendants. La connectivité "cortex cingulaire antérieur (ACC) – insula postérieur (PI)" est la clé dans cette comorbidité ADHD-douleur, impliquée dans les fonctions exécutives, les émotions et elle envoie aussi des projections vers la corne dorsale de la moelle épinière. En effet, en combinant les analyses électrophysiologiques, optogénétiques et comportementales, nous avons démontré que les effets de l’ADHD sur la sensibilisation douloureuse passent par la mise en jeu de l’ACC et de la voie ACC – PI. En conclusion, nous montrons que les conditions ADHD induisent une hyperactivation des neurones nociceptifs de la moelle épinière et une hypersensibilité à la douleur. Nous suggérons également que le circuit ACC – PI pourrait déclencher un dysfonctionnement des neurones de la moelle épinière sur la douleur dans les conditions ADHD

Anti-inflammatory, Antinociceptive, and Antioxidant Activities of Methanol and Aqueous Extracts of Anacyclus pyrethrum Roots

Anacyclus pyrethrum (L.) is a plant widely used in Moroccan traditional medicine to treat inflammatory and painful diseases. The objective of the present study was to evaluate the antinociceptive, anti-inflammatory and antioxidant activities of aqueous and methanol extracts of Anacyclus pyrethrum roots (AEAPR and MEAPR). The anti-inflammatory effect of AEAPR and MEAPR was determined in xylene–induced ear edema and Complete Freund’s Adjuvant (CFA)-induced paw edema. The antinociceptive activity of AEAPR and MEAPR (125, 250, and 500 mg/kg) administered by gavage was examined in mice by using acetic acid-induced writhing, hot plate, and formalin tests, and the mechanical allodynia were assessed in CFA-induced paw edema. In addition, the in vitro antioxidant activities of the extracts were determined by using 2,2-diphenyl-1-picrylhydrazyl (DPPH) radical scavenging method, ferric reducing power and β-carotene-linoleic acid assay systems. AEAPR and MEAPR produced significant reductions in CFA-induced paw edema and xylene-induced ear edema. A single oral administration of these extracts at 250 and 500 mg/kg significantly reduced mechanical hypersensitivity induced by CFA, which had begun 1 h 30 after the treatment, and was maintained till 7 h. Chronic treatment with both extracts significantly reduced mechanical hypersensitivity in persistent pain conditions induced by CFA. Acute pretreatment with AEAPR or MEAPR at high dose caused a significant decrease in the number of abdominal writhes induced by acetic acid injection (52.2 and 56.7%, respectively), a marked increase of the paw withdrawal latency in the hot plate test, and also a significant inhibition of both phases of the formalin test. This antinociceptive effect was partially reversed by naloxone pretreatment in the hot plate and formalin tests. Additionally, a significant scavenging activity in DPPH, reducing power and protection capacity of β-carotene was observed in testing antioxidant assays. The present study suggests that AEAPR and MEAPR possess potent anti-inflammatory, antinociceptive and antioxidant effects which could be related to the presence of alkaloids and phenols in the plant. In addition, the antinociceptive effect of APR extracts seems to partly involve the opioid system. Taken together, these results suggest that Anacylcus pyrethrum may indeed be useful in the treatment of pain and inflammatory disorders in humans

Human Foot Outperforms the Hand in Mechanical Pain Discrimination

Tactile discrimination has been extensively studied, but mechanical pain discrimination remains poorly characterized. Here, we measured the capacity for mechanical pain discrimination using a two-alternative forced choice paradigm, with force-calibrated indentation stimuli (Semmes–Weinstein monofilaments) applied to the hand and foot dorsa of healthy human volunteers. In order to characterize the relationship between peripheral nociceptor activity and pain perception, we recorded single-unit activity from myelinated (A) and unmyelinated (C) mechanosensitive nociceptors in the skin using microneurography. At the perceptual level, we found that the foot was better at discriminating noxious forces than the hand, which stands in contrast to that for innocuous force discrimination, where the hand performed better than the foot. This observation of superior mechanical pain discrimination on the foot compared to the hand could not be explained by the responsiveness of individual nociceptors. We found no significant difference in the discrimination performance of either the myelinated or unmyelinated class of nociceptors between skin regions. This suggests the possibility that other factors such as skin biophysics, receptor density or central mechanisms may underlie these regional differences.</jats:p

Switch of serotonergic descending inhibition into facilitation by a spinal chloride imbalance in neuropathic pain

International audienceDescending control from the brain to the spinal cord shapes our pain experience, ranging from powerful analgesia to extreme sensitivity. Increasing evidence from both preclinical and clinical studies points to an imbalance toward descending facilitation as a substrate of pathological pain, but the underlying mechanisms remain unknown. We used an optogenetic approach to manipulate serotonin (5-HT) neurons of the nucleus raphe magnus that project to the dorsal horn of the spinal cord. We found that 5-HT neurons exert an analgesic action in naïve mice that becomes proalgesic in an experimental model of neuropathic pain. We show that spinal KCC2 hypofunction turns this descending inhibitory control into paradoxical facilitation; KCC2 enhancers restored 5-HT–mediated descending inhibition and analgesia. Last, combining selective serotonin reuptake inhibitors (SSRIs) with a KCC2 enhancer yields effective analgesia against nerve injury–induced pain hypersensitivity. This uncovers a previously unidentified therapeutic path for SSRIs against neuropathic pain

PIEZO2-dependent rapid pain system in humans and mice.

The PIEZO2 ion channel is critical for transducing light touch into neural signals but is not considered necessary for transducing acute pain in humans. Here, we discovered an exception - a form of mechanical pain evoked by hair pulling. Based on observations in a rare group of individuals with PIEZO2 deficiency syndrome, we demonstrated that hair-pull pain is dependent on PIEZO2 transduction. Studies in control participants showed that hair-pull pain triggered a distinct nocifensive response, including a nociceptive reflex. Observations in rare Aβ deafferented individuals and nerve conduction block studies in control participants revealed that hair-pull pain perception is dependent on Aβ input. Single-unit axonal recordings revealed that a class of cooling-responsive myelinated nociceptors in human skin is selectively tuned to painful hair-pull stimuli. Further, we pharmacologically mapped these nociceptors to a specific transcriptomic class. Finally, using functional imaging in mice, we demonstrated that in a homologous nociceptor, Piezo2 is necessary for high-sensitivity, robust activation by hair-pull stimuli. Together, we have demonstrated that hair-pulling evokes a distinct type of pain with conserved behavioral, neural, and molecular features across humans and mice