Your search keyword '"Dickenson AH"' showing total 367 results

1. Unusual Pain Disorders – What Can Be Learned from Them?

Author

Sachau J, Kersebaum D, Baron R, and Dickenson AH

Subjects

pain mechanisms, sodium channelopathies, hereditary pain diseases, sensory modulation disorder, central sensitization, gene silencing, Medicine (General), R5-920

Abstract

Juliane Sachau,1 Dilara Kersebaum,1 Ralf Baron,1 Anthony H Dickenson2 1Division of Neurological Pain Research and Therapy, Department of Neurology, University Hospital Schleswig-Holstein, Campus Kiel, Kiel, 24105, Germany; 2Department of Neuroscience, Physiology and Pharmacology, University College London, London, WC1E 6BT, UKCorrespondence: Juliane SachauDivision of Neurological Pain Research and Therapy, Department of Neurology, Universitätsklinikum Schleswig-Holstein, Campus Kiel, Arnold-Heller-Strasse 3, Haus D, Kiel, 24105, GermanyTel +49 431 500 23911Fax +49 431 500 23914Email juliane.sachau@uksh.deAbstract: Pain is common in many different disorders and leads to a significant reduction in quality of life in the affected patients. Current treatment options are limited and often result in insufficient pain relief, partly due to the incomplete understanding of the underlying pathophysiological mechanisms. The identification of these pathomechanisms is therefore a central object of current research. There are also a number of rare pain diseases, that are generally little known and often undiagnosed, but whose correct diagnosis and examination can help to improve the management of pain disorders in general. In some of these unusual pain disorders like sodium-channelopathies or sensory modulation disorder the underlying pathophysiological mechanisms have only recently been unravelled. These mechanisms might serve as pharmacological targets that may also play a role in subgroups of other, more common pain diseases. In other unusual pain disorders, the identification of pathomechanisms has already led to the development of new drugs. A completely new therapeutic approach, the gene silencing, can even stop progression in hereditary transthyretin amyloidosis and porphyria, ie in pain diseases that would otherwise be rapidly fatal if left untreated. Thus, pain therapists and researchers should be aware of these rare and unusual pain disorders as they offer the unique opportunity to study mechanisms, identify new druggable targets and finally because early diagnosis might save many patient lives.Keywords: pain mechanisms, sodium channelopathies, hereditary pain diseases, sensory modulation disorder, central sensitization, gene silencing

Published

2021

2. Pharmacological rationale for tapentadol therapy: a review of new evidence

Author

Romualdi P, Grilli M, Canonico PL, Collino M, and Dickenson AH

Subjects

tapendatol, neuropathic pain, pain chronicization, Medicine (General), R5-920

Abstract

Patrizia Romualdi,1 Mariagrazia Grilli,2 Pier Luigi Canonico,3 Massimo Collino,4 Anthony H Dickenson5 1Department of Pharmacy and Biotechnologies Alma Mater Studiorum, University of Bologna, Bologna 40126, Italy; 2Laboratory of Neuroplasticity, Department Pharmaceutical Sciences, University of Piemonte Orientale, Novara 28100, Italy; 3Departiment of Pharmacological Sciences, University of Piemonte Orientale, Novara 28100, Italy; 4Department of Drug Science and Technology, University of Turin, Turin 10121, Italy; 5Neuroscience, Physiology and Pharmacology, University College London, London WC1E 6BT, UK Abstract: Chronic pain could be considered as a neurological disorder. Therefore, appropriate selection of the therapy, which should consider the pathophysiological mechanisms of pain, can result in a successful analgesic outcome. Tapentadol is an analgesic drug which acts both as a μ-opioid receptor (MOR) agonist and as a noradrenaline reuptake inhibitor (NRI), thereby generating a synergistic action in terms of analgesic efficacy, but not for the burden of adverse effects. Therefore, tapentadol can be defined as the first “MOR-NRI” drug. This molecule holds the potential to address at least some of the current limitations of analgesic therapy due to its unique mechanism of action and has shown to be safe and effective in the treatment of chronic pain of cancer and noncancer etiologies including nociceptive, neuropathic and mixed pain. In particular, the MOR component of tapentadol activity predominantly allows for analgesia in nociceptive pain; on the other hand, the NRI component contributes, now in a predominant manner, for analgesic efficacy in cases of neuropathic pain states. This paper will discuss recent pieces of evidence on the pathophysiology of pain, the background on tapentadol and then present some new studies on how the unique mechanism of action of tapentadol provides a key role in its analgesic efficacy in a number of pain states and with a favorable safety profile. Keywords: tapentadol, neuropathic pain, pain chronicization

Published

2019

3. Tapentadol: a new option for the treatment of cancer and noncancer pain

Author

Dickenson AH and Kress HG

Subjects

Cancer pain, non-cancer pain, tapentadol, Medicine (General), R5-920

Abstract

Anthony H Dickenson,1 Hans G Kress2 1Neuroscience, Physiology and Pharmacology, University College London, London WC1E6BT, UK; 2Department of Special Anaesthesia and Pain Medicine, Medical University, AKH of Vienna, Vienna, AustriaThe last years have witnessed major advances in the knowledge of the basic mechanisms underlying the onset and the chronification of pain. In particular, it has emerged that pain signaling and modulatory mechanisms change following physiopathological events, such as the two major types of pain, neuropathic and inflammatory pains. Very different chemical events and ion channel changes, respectively, underlie these pains at peripheral levels, so treatments have to differ. Low back pain and cancer pain can be one or the other or a combination of these different mechanisms, so-called mixed pains. The final pain experience is a combination of all these peripheral and central events, but within the central nervous system, the pain controlling systems are more common so that therapies acting on central modulation can span a range of pain conditions. Descending controls link the brain back to the spinal cord, where noradrenaline (NRI) is a key inhibitory transmitter in pain control in these pathways. Descending controls run from the brain to the spinal cord and can be gaged in patients – the balance between excitations and facilitations’ shift to the latter in persistent pain states, reinforcing pain transmission.1

Published

2019

4. Genes, molecules and patients - Emerging topics to guide clinical pain research

Author

Sikandar, S, Patel, R, Patel, S, Sikander, S, Bennett, DLH, and Dickenson, AH

Abstract

This review selectively explores some areas of pain research that, until recently, have been poorly understood. We have chosen four topics that relate to clinical pain and we discuss the underlying mechanisms and related pathophysiologies contributing to these pain states. A key issue in pain medicine involves crucial events and mediators that contribute to normal and abnormal pain signaling, but remain unseen without genetic, biomarker or imaging analysis. Here we consider how the altered genetic make-up of familial pains reveals the human importance of channels discovered by preclinical research, followed by the contribution of receptors as stimulus transducers in cold sensing and cold pain. Finally we review recent data on the neuro-immune interactions in chronic pain and the potential targets for treatment in cancer-induced bone pain. © 2013 Elsevier B.V. All rights reserved.

Published

2016

5. ENLARGEMENT OF THE RECEPTIVE FIELD SIZE TO LOW INTENSITY MECHANICAL STIMULATION IN THE RAT SPINAL NERVE LIGATION MODEL OF NEUROPATHY

Author

Suzuki, R, primary, Kontinen, Vk, additional, Matthews, E, additional, Williams, E, additional, and Dickenson, Ah, additional

Published

2000

6. EFFECTS OF MIDAZOLAM IN THE SPINAL NERVE LIGATION MODEL OF NEUROPATHIC PAIN IN RATS

Author

Kontinen, Vk, primary and Dickenson, Ah, additional

Published

2000

7. PEPTIDES AND AMINO ACIDS: SETTING THE LEVEL OF SPINAL OPIOID ANALGESIA

Author

Dickenson, AH, primary

Published

1995

8. Pregabalin suppresses spinal neuronal hyperexcitability and visceral hypersensitivity in the absence of peripheral pathophysiology.

Author

Bannister K, Sikandar S, Bauer CS, Dolphin AC, Porreca F, Dickenson AH, Bannister, Kirsty, Sikandar, Shafaq, Bauer, Claudia S, Dolphin, Annette C, Porreca, Frank, and Dickenson, Anthony H

Published

2011

9. Mu-opioid and noradrenergic α(2)-adrenoceptor contributions to the effects of tapentadol on spinal electrophysiological measures of nociception in nerve-injured rats.

Author

Bee LA, Bannister K, Rahman W, Dickenson AH, Bee, Lucy A, Bannister, Kirsty, Rahman, Wahida, and Dickenson, Anthony H

Published

2011

10. Spinal cord mechanisms of pain.

Author

D'Mello R, Dickenson AH, D'Mello, R, and Dickenson, A H

Abstract

The spinal cord is the first relay site in the transmission of nociceptive information from the periphery to the brain. Sensory signals are transmitted from the periphery by primary afferent fibres into the dorsal horn of the spinal cord, where these afferents synapse with intrinsic spinal dorsal horn neurones. Spinal projection neurones then convey this information to higher centres in the brain, where non-noxious and noxious signals can be perceived. During nociceptive transmission, the output of the spinal cord is dependent on various spinal mechanisms which can either increase or decrease the activity of dorsal horn neurones. Such mechanisms include local excitatory and inhibitory interneurones, N-methyl-D-aspartate receptor activation, and descending influences from the brainstem, which can be both inhibitory and excitatory in nature. After nerve injury or conditions of inflammation, shifts can occur in these excitatory and inhibitory mechanisms which modulate spinal excitability, often resulting in the heightened response of dorsal neurones to incoming afferent signals, and increased output to the brain, a phenomenon known as central sensitization. In this review, we consider the ways in which spinal cord activity may be altered in chronic pain states. In addition, we discuss the spinal mechanisms which are targeted by current analgesics used in the management of chronic pain. [ABSTRACT FROM AUTHOR]

Published

2008

11. The pharmacology of central sensitization.

Author

Suzuki R and Dickenson AH

Abstract

Objective: The purpose of this review is to show how central mechanisms of pain transmission relate to pharmacological systems that are responsible for the generation of central sensitization states.Findings: Pain transmission is a complex process involving the interplay between excitatory and inhibitory systems acting at different levels of the central nervous system. A balance between excitatory and inhibitory receptor mediated events determines the level of excitability within spinal circuits capable of contributing to the transmission of noxious messages. All of these systems are subject to plasticity and other alterations in pharmacological functions that characterize pathological conditions.Conclusions: A better understanding of the neuropharmacology of pain transmission within the spinal cord has the potential to improve the clinical management of pathologically severe and persistent pain. [ABSTRACT FROM AUTHOR]

Published

2002

12. Endogenous adenosine A3 receptor activation selectively alleviates persistent pain states

Author

Jennifer Y. Xie, Kenneth A. Jacobson, Joshua W. Little, Anthony H. Dickenson, Kirsty Bannister, Sabatino Maione, Todd W. Vanderah, Kali Janes, Zhoumou Chen, Amanda Ford, Ashley M. Symons-Liguori, Livio Luongo, Daniela Salvemini, Frank Porreca, Timothy M. Doyle, Dilip K. Tosh, Little, Jw, Ford, A, Symons Liguori, Am, Chen, Z, Janes, K, Doyle, T, Xie, J, Luongo, Livio, Tosh, Dk, Maione, Sabatino, Bannister, K, Dickenson, Ah, Vanderah, Tw, Porreca, F, Jacobson, Ka, and Salvemini, D.

Subjects

Male, Pain Threshold, Time Factors, Pyridines, Morpholines, Mice, Transgenic, Adenosine kinase, Pharmacology, Rats, Sprague-Dawley, Mice, Threshold of pain, medicine, Animals, spontaneous pain, Pain Measurement, Neurons, Medulla Oblongata, biology, Naloxone, business.industry, Receptor, Adenosine A3, Chronic pain, Adenosine A3 receptor, medicine.disease, Adenosine, Rats, Mice, Inbred C57BL, Disease Models, Animal, Pyrimidines, Gene Expression Regulation, Purinergic P1 Receptor Antagonists, Spinal Cord, Opioid, Hyperalgesia, adenosine, Neuropathic pain, biology.protein, Neuralgia, Neurology (clinical), medicine.symptom, rostral ventromedial medulla, business, A3AR, chronic pain, Neuroscience, Reports, medicine.drug

Abstract

Chronic pain is a global burden that promotes disability and unnecessary suffering. To date, efficacious treatment of chronic pain has not been achieved. Thus, new therapeutic targets are needed. Here, we demonstrate that increasing endogenous adenosine levels through selective adenosine kinase inhibition produces powerful analgesic effects in rodent models of experimental neuropathic pain through the A3 adenosine receptor (A3AR, now known as ADORA3) signalling pathway. Similar results were obtained by the administration of a novel and highly selective A3AR agonist. These effects were prevented by blockade of spinal and supraspinal A3AR, lost in A3AR knock-out mice, and independent of opioid and endocannabinoid mechanisms. A3AR activation also relieved non-evoked spontaneous pain behaviours without promoting analgesic tolerance or inherent reward. Further examination revealed that A3AR activation reduced spinal cord pain processing by decreasing the excitability of spinal wide dynamic range neurons and producing supraspinal inhibition of spinal nociception through activation of serotonergic and noradrenergic bulbospinal circuits. Critically, engaging the A3AR mechanism did not alter nociceptive thresholds in non-neuropathy animals and therefore produced selective alleviation of persistent neuropathic pain states. These studies reveal A3AR activation by adenosine as an endogenous anti-nociceptive pathway and support the development of A3AR agonists as novel therapeutics to treat chronic pain.

Published

2015

13. A back-translational study of descending interactions with the induction of hyperalgesia by high-frequency electrical stimulation in rats and humans.

Author

Patel R, Taylor JL, Dickenson AH, McMahon SB, and Bannister K

Subjects

Animals, Rats, Male, Humans, Adult, Female, Young Adult, Pain Measurement methods, Pain Threshold physiology, Spinal Cord, Translational Research, Biomedical, Hyperalgesia physiopathology, Electric Stimulation methods, Rats, Sprague-Dawley

Abstract

Abstract: In humans and animals, high-frequency electrocutaneous stimulation (HFS) induces an "early long-term potentiation-like" sensitisation, where synaptic plasticity is underpinned by an ill-defined interaction between peripheral input and central modulatory processes. The relative contributions of these processes to the initial pain or nociceptive response likely differ from those that underpin development of the heightened response. To investigate the impact of HFS-induced hyperalgesia on pain and nociception in perception and neural terms, respectively, and to explore the impact of descending inhibitory pathway activation on the development of HFS-induced hyperalgesia, we performed parallel studies utilising identical stimuli to apply HFS concurrent to (1) a conditioned pain modulation paradigm during psychophysical testing in healthy humans or (2) a diffuse noxious inhibitory controls paradigm during in vivo electrophysiological recording of spinal neurones in healthy anaesthetised rats. High-frequency electrocutaneous stimulation alone induced enhanced perceptual responses to pinprick stimuli in cutaneous areas secondary to the area of electrical stimulation in humans and increased the excitability of spinal neurones which exhibited stimulus intensity-dependent coded responses to pinprick stimulation in a manner that tracked with human psychophysics, supporting their translational validity. Application of a distant noxious conditioning stimulus during HFS did not alter perceived primary or secondary hyperalgesia in humans or the development of primary or secondary neuronal hyperexcitability in rats compared with HFS alone, suggesting that, upon HFS-response initiation in a healthy nervous system, excitatory signalling escapes inhibitory control. Therefore, in this model, dampening facilitatory mechanisms rather than augmenting top-down inhibitions could prevent pain development., (Copyright © 2024 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the International Association for the Study of Pain.)

Published

2024

14. Nerve injury increases native Ca V 2.2 trafficking in dorsal root ganglion mechanoreceptors.

Author

Nieto-Rostro M, Patel R, Dickenson AH, and Dolphin AC

Subjects

Animals, Mice, Rats, Nociceptors metabolism, Rats, Sprague-Dawley, Ganglia, Spinal metabolism, Mechanoreceptors, Peripheral Nervous System Diseases metabolism

Abstract

Abstract: Neuronal N-type (Ca V 2.2) voltage-gated calcium channels are essential for neurotransmission from primary afferent terminals in the dorsal horn. In this study, we have used a knockin mouse containing Ca V 2.2 with an inserted extracellular hemagglutinin tag (Ca V 2.2_HA), to visualise the pattern of expression of endogenous Ca V 2.2 in dorsal root ganglion (DRG) neurons and their primary afferents in the dorsal horn. We examined the effect of partial sciatic nerve ligation (PSNL) and found an increase in Ca V 2.2_HA only in large and medium dorsal root ganglion neurons and also in deep dorsal horn synaptic terminals. Furthermore, there is a parallel increase in coexpression with GFRα1, present in a population of low threshold mechanoreceptors, both in large DRG neurons and in their terminals. The increased expression of Ca V 2.2_HA in these DRG neurons and their terminals is dependent on the presence of the auxiliary subunit α 2 δ-1, which is required for channel trafficking to the cell surface and to synaptic terminals, and it likely contributes to enhanced synaptic transmission at these synapses following PSNL. By contrast, the increase in GFRα1 is not altered in α 2 δ-1-knockout mice. We also found that following PSNL, there is patchy loss of glomerular synapses immunoreactive for Ca V 2.2_HA and CGRP or IB4, restricted to the superficial layers of the dorsal horn. This reduction is not dependent on α 2 δ-1 and likely reflects partial deafferentation of C-nociceptor presynaptic terminals. Therefore, in this pain model, we can distinguish 2 different events affecting specific DRG terminals, with opposite consequences for Ca V 2.2_HA expression and function in the dorsal horn., (Copyright © 2023 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the International Association for the Study of Pain.)

Published

2023

15. Maximizing treatment efficacy through patient stratification in neuropathic pain trials.

Author

Baron R, Dickenson AH, Calvo M, Dib-Hajj SD, and Bennett DL

Subjects

Animals, Humans, Pain Measurement, Analgesics therapeutic use, Treatment Outcome, Neuralgia drug therapy

Abstract

Treatment of neuropathic pain remains inadequate despite the elucidation of multiple pathophysiological mechanisms and the development of promising therapeutic compounds. The lack of success in translating knowledge into clinical practice has discouraged pharmaceutical companies from investing in pain medicine; however, new patient stratification approaches could help bridge the translation gap and develop individualized therapeutic approaches. As we highlight in this article, subgrouping of patients according to sensory profiles and other baseline characteristics could aid the prediction of treatment success. Furthermore, novel outcome measures have been developed for patients with neuropathic pain. The extent to which sensory profiles and outcome measures can be employed in routine clinical practice and clinical trials and across distinct neuropathic pain aetiologies is yet to be determined. Improvements in animal models, drawing on our knowledge of human pain, and robust public-private partnerships will be needed to pave the way to innovative and effective pain medicine in the future., (© 2022. Springer Nature Limited.)

Published

2023

16. Ambroxol for neuropathic pain: hiding in plain sight?

Author

Russo MA, Baron R, Dickenson AH, Kern KU, and Santarelli DM

Subjects

Humans, Analgesics therapeutic use, Anesthetics, Local therapeutic use, Pain Measurement, Ambroxol therapeutic use, Ambroxol pharmacology, Neuralgia drug therapy

Abstract

Abstract: Ambroxol is a multifaceted drug with primarily mucoactive and secretolytic actions, along with anti-inflammatory, antioxidant, and local anaesthetic properties. It has a long history of use in the treatment of respiratory tract diseases and has shown to be efficacious in relieving sore throat. In more recent years, ambroxol has gained interest for its potential usefulness in treating neuropathic pain. Research into this area has been slow, despite clear preclinical evidence to support its primary analgesic mechanism of action-blockade of voltage-gated sodium (Na v ) channels in sensory neurons. Ambroxol is a commercially available inhibitor of Na v 1.8, a crucial player in the pathophysiology of neuropathic pain, and Na v 1.7, a particularly exciting target for the treatment of chronic pain. In this review, we discuss the analgesic mechanisms of action of ambroxol, as well as proposed synergistic properties, followed by the preclinical and clinical results of its use in the treatment of persistent pain and neuropathic pain symptoms, including trigeminal neuralgia, fibromyalgia, and complex regional pain syndrome. With its well-established safety profile, extensive preclinical and clinical drug data, and early evidence of clinical effectiveness, ambroxol is an old drug worthy of further investigation for repurposing. As a patent-expired drug, a push is needed to progress the drug to clinical trials for neuropathic pain. We encourage the pharmaceutical industry to look at patented drug formulations and take an active role in bringing an optimized version for neuropathic pain to market., (Copyright © 2022 International Association for the Study of Pain.)

Published

2023

17. Sodium-calcium exchanger-3 regulates pain "wind-up": From human psychophysics to spinal mechanisms.

Author

Trendafilova T, Adhikari K, Schmid AB, Patel R, Polgár E, Chisholm KI, Middleton SJ, Boyle K, Dickie AC, Semizoglou E, Perez-Sanchez J, Bell AM, Ramirez-Aristeguieta LM, Khoury S, Ivanov A, Wildner H, Ferris E, Chacón-Duque JC, Sokolow S, Saad Boghdady MA, Herchuelz A, Faux P, Poletti G, Gallo C, Rothhammer F, Bedoya G, Zeilhofer HU, Diatchenko L, McMahon SB, Todd AJ, Dickenson AH, Ruiz-Linares A, and Bennett DL

Subjects

Animals, Humans, Mice, Pain, Posterior Horn Cells, Psychophysics, Calcium, Sodium-Calcium Exchanger genetics

Abstract

Repeated application of noxious stimuli leads to a progressively increased pain perception; this temporal summation is enhanced in and predictive of clinical pain disorders. Its electrophysiological correlate is "wind-up," in which dorsal horn spinal neurons increase their response to repeated nociceptor stimulation. To understand the genetic basis of temporal summation, we undertook a GWAS of wind-up in healthy human volunteers and found significant association with SLC8A3 encoding sodium-calcium exchanger type 3 (NCX3). NCX3 was expressed in mouse dorsal horn neurons, and mice lacking NCX3 showed normal, acute pain but hypersensitivity to the second phase of the formalin test and chronic constriction injury. Dorsal horn neurons lacking NCX3 showed increased intracellular calcium following repetitive stimulation, slowed calcium clearance, and increased wind-up. Moreover, virally mediated enhanced spinal expression of NCX3 reduced central sensitization. Our study highlights Ca 2+ efflux as a pathway underlying temporal summation and persistent pain, which may be amenable to therapeutic targeting., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2022 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2022

18. The Life and Times of Stephen B. McMahon (1954-2021).

Author

Dickenson AH and Bennett DLH

Abstract

Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Published

2022

19. Neuropharmacological basis for multimodal analgesia in chronic pain.

Author

Patel R and Dickenson AH

Subjects

Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Humans, Pain Management, Quality of Life, Selective Serotonin Reuptake Inhibitors therapeutic use, Analgesia, Chronic Pain drug therapy

Abstract

Managing chronic pain remains a major unmet clinical challenge. Patients can be treated with a range of interventions, but pharmacotherapy is the most common. These include opioids, antidepressants, calcium channel modulators, sodium channel blockers, and nonsteroidal anti-inflammatory drugs. Many of these drugs target a particular mechanism; however, chronic pain in many diseases is multifactorial and induces plasticity throughout the sensory neuroaxis. Furthermore, comorbidities such as depression, anxiety, and sleep disturbances worsen quality of life. Given the complexity of mechanisms and symptoms in patients, it is unsurprising that many fail to achieve adequate pain relief from a single agent. The efforts to develop novel drug classes with better efficacy have not always proved successful; a multimodal or combination approach to analgesia is an important strategy in pain control. Many patients frequently take more than one medication, but high-quality evidence to support various combinations is often sparse. Ideally, combining drugs would produce synergistic action to maximize analgesia and reduce side effects, although sub-additive and additive analgesia is still advantageous if additive side-effects can be avoided. In this review, we discuss pain mechanisms, drug actions, and the rationale for mechanism-led treatment selection. Abbreviations : COX - cyclooxygenase, CGRP - calcitonin gene-related peptide, CPM - conditioned pain modulation, NGF - nerve growth factor, NNT - number needed to treat, NMDA - N -methyl-d-aspartate, NSAID - nonsteroidal anti-inflammatory drugs, TCA - tricyclic antidepressant, SNRI - serotonin-noradrenaline reuptake inhibitor, QST - quantitative sensory testing.

Published

2022

20. Studying Independent Kcna6 Knock-out Mice Reveals Toxicity of Exogenous LacZ to Central Nociceptor Terminals and Differential Effects of Kv1.6 on Acute and Neuropathic Pain Sensation.

Author

Peck LJ, Patel R, Diaz P, Wintle YM, Dickenson AH, Todd AJ, Calvo M, and Bennett DLH

Subjects

Animals, CRISPR-Cas Systems, Female, Gene Knockout Techniques methods, Integrases metabolism, Kv1.6 Potassium Channel metabolism, Male, Mice, Mice, Inbred C57BL, Nociceptors pathology, Synapses metabolism, Synapses pathology, Gene Knockout Techniques adverse effects, Genes, Reporter, Kv1.6 Potassium Channel genetics, Lac Operon, Neuralgia metabolism, Nociceptors metabolism

Abstract

The potassium channel Kv1.6 has recently been implicated as a major modulatory channel subunit expressed in primary nociceptors. Furthermore, its expression at juxtaparanodes of myelinated primary afferents is induced following traumatic nerve injury as part of an endogenous mechanism to reduce hyperexcitability and pain-related hypersensitivity. In this study, we compared two mouse models of constitutive Kv1.6 knock-out (KO) achieved by different methods: traditional gene trap via homologous recombination and CRISPR-mediated excision. Both Kv1.6 KO mouse lines exhibited an unexpected reduction in sensitivity to noxious heat stimuli, to differing extents: the Kv1.6 mice produced via gene trap had a far more significant hyposensitivity. These mice ( Kcna6 lacZ ) expressed the bacterial reporter enzyme LacZ in place of Kv1.6 as a result of the gene trap mechanism, and we found that their central primary afferent presynaptic terminals developed a striking neurodegenerative phenotype involving accumulation of lipid species, development of "meganeurites," and impaired transmission to dorsal horn wide dynamic range neurons. The anatomic defects were absent in CRISPR-mediated Kv1.6 KO mice ( Kcna6 -/- ) but were present in a third mouse model expressing exogenous LacZ in nociceptors under the control of a Nav1.8-promoted Cre recombinase. LacZ reporter enzymes are thus intrinsically neurotoxic to sensory neurons and may induce pathologic defects in transgenic mice, which has confounding implications for the interpretation of gene KOs using lacZ Nonetheless, in Kcna6 -/- mice not affected by LacZ, we demonstrated a significant role for Kv1.6 regulating acute noxious thermal sensitivity, and both mechanical and thermal pain-related hypersensitivity after nerve injury. SIGNIFICANCE STATEMENT In recent decades, the expansion of technologies to experimentally manipulate the rodent genome has contributed significantly to the field of neuroscience. While introduction of enzymatic or fluorescent reporter proteins to label neuronal populations is now commonplace, often potential toxicity effects are not fully considered. We show a role of Kv1.6 in acute and neuropathic pain states through analysis of two mouse models lacking Kv1.6 potassium channels: one with additional expression of LacZ and one without. We show that LacZ reporter enzymes induce unintended defects in sensory neurons, with an impact on behavioral data outcomes. To summarize we highlight the importance of Kv1.6 in recovery of normal sensory function following nerve injury, and careful interpretation of data from LacZ reporter models., (Copyright © 2021 the authors.)

Published

2021

21. The Stage-Specific Plasticity of Descending Modulatory Controls in a Rodent Model of Cancer-Induced Bone Pain.

Author

Kucharczyk MW, Derrien D, Dickenson AH, and Bannister K

Abstract

Pain resulting from metastatic bone disease is a major unmet clinical need. Studying spinal processing in rodent models of cancer pain is desirable since the percept of pain is influenced in part by modulation at the level of the transmission system in the dorsal horn of the spinal cord. Here, a rodent model of cancer-induced bone pain (CIBP) was generated following syngeneic rat mammary gland adenocarcinoma cell injection in the tibia of male Sprague Dawley rats. Disease progression was classified as "early" or "late" stage according to bone destruction. Even though wakeful CIBP rats showed progressive mechanical hypersensitivity, subsequent in vivo electrophysiological measurement of mechanically evoked deep dorsal horn spinal neuronal responses revealed no change. Rather, a dynamic reorganization of spinal neuronal modulation by descending controls was observed, and this was maladaptive only in the early stage of CIBP. Interestingly, this latter observation corresponded with the degree of damage to the primary afferents innervating the cancerous tissue. Plasticity in the modulation of spinal neuronal activity by descending control pathways reveals a novel opportunity for targeting CIBP in a stage-specific manner. Finally, the data herein have translational potential since the descending control pathways measured are present also in humans.

Published

2020

22. Capsaicin 8% dermal patch in clinical practice: an expert opinion.

Author

Bonezzi C, Costantini A, Cruccu G, Fornasari DMM, Guardamagna V, Palmieri V, Polati E, Zini P, and Dickenson AH

Subjects

Administration, Topical, Analgesics adverse effects, Capsaicin adverse effects, Cost-Benefit Analysis, Expert Testimony, Humans, Neuralgia metabolism, Pregabalin administration & dosage, Pregabalin adverse effects, Pregabalin therapeutic use, Quality of Life, TRPV Cation Channels metabolism, Transdermal Patch, Analgesics administration & dosage, Analgesics therapeutic use, Capsaicin administration & dosage, Capsaicin therapeutic use, Neuralgia drug therapy

Abstract

Introduction: Neuropathic pain (NP) is caused by a lesion or disease of the somatosensory system, which can severely impact patients' quality of life. The current-approved treatments for NP comprise of both centrally acting agents and topical drugs, including capsaicin 8% dermal patches, which is approved for the treatment of peripheral NP., Areas Covered: The authors summarize literature data regarding capsaicin use in patients who suffer from NP and discuss the clinical applications of this topical approach., Expert Opinion: Overall, the capsaicin 8% dermal patch is as effective in reducing pain intensity as other centrally active agents (i.e. pregabalin). Some studies have also reported fewer systemic side effects, a faster onset of action and superior treatment satisfaction compared with systemic agents. In our opinion, capsaicin 8% dermal patches also present additional advantages, such as a good systemic tolerability, the scarcity of adverse events, the possibility to combine it with other agents, and a good cost-effective profile. It is important to note that, as the mechanism of action of capsaicin 8% is the 'defunctionalization' of small afferent fibers through interaction with TRPV1 receptors, the peripheral expression of this receptor on nociceptor fibers, is crucial to predict patient's response to treatment.

Published

2020

23. The impact of bone cancer on the peripheral encoding of mechanical pressure stimuli.

Author

Kucharczyk MW, Chisholm KI, Denk F, Dickenson AH, Bannister K, and McMahon SB

Subjects

Animals, Female, Ganglia, Spinal, Male, Rats, Rats, Sprague-Dawley, Bone Neoplasms complications

Abstract

Skeletal metastases are frequently accompanied by chronic pain that is mechanoceptive in nature. Mechanistically, cancer-induced bone pain (CIBP) is mediated by peripheral sensory neurons innervating the cancerous site, the cell bodies of which are housed in the dorsal root ganglia (DRG). How these somatosensory neurons encode sensory information in CIBP remains only partly explained. Using a validated rat model, we first confirmed cortical bone destruction in CIBP but not sham-operated rats (day 14 after surgery, designated "late"-stage bone cancer). This occurred with behavioural mechanical hypersensitivity (Kruskal-Wallis H for independent samples; CIBP vs sham-operated, day 14; P < 0.0001). Next, hypothesising that the proportion and phenotype of primary afferents would be altered in the disease state, dorsal root ganglia in vivo imaging of genetically encoded calcium indicators and Markov Cluster Analysis were used to analyse 1748 late-stage CIBP (n = 10) and 757 sham-operated (n = 9), neurons. Distinct clusters of responses to peripheral stimuli were revealed. In CIBP rats, upon knee compression of the leg ipsilateral to the tumour, (1) 3 times as many sensory afferents responded (repeated-measures analysis of variance: P < 0.0001 [vs sham]); (2) there were significantly more small neurons responding (Kruskal-Wallis for independent samples (vs sham): P < 0.0001); and (3) approximately 13% of traced tibial cavity afferents responded (no difference observed between CIBP and sham-operated animals). We conclude that an increased sensory afferent response is present in CIBP rats, and this is likely to reflect afferent recruitment from outside of the bone rather than increased intraosseous afferent activity.

Published

2020

24. Central Nervous System Targets: Supraspinal Mechanisms of Analgesia.

Author

Bannister K and Dickenson AH

Subjects

Analgesics metabolism, Analgesics, Opioid administration & dosage, Analgesics, Opioid metabolism, Animals, Anticonvulsants administration & dosage, Anticonvulsants metabolism, Antidepressive Agents administration & dosage, Antidepressive Agents metabolism, Brain metabolism, Central Nervous System drug effects, Central Nervous System metabolism, Humans, Nociception drug effects, Nociception physiology, Pain metabolism, Pain Management methods, Spinal Cord metabolism, Analgesia methods, Analgesics administration & dosage, Brain drug effects, Drug Delivery Systems methods, Pain drug therapy, Spinal Cord drug effects

Abstract

While the acute sensation of pain is protective, signaling the presence of actual or potential bodily harm, its persistence is unpleasant. When pain becomes chronic, it has limited evolutionarily advantage. Despite the differing nature of acute and chronic pain, a common theme is that sufferers seek pain relief. The possibility to medicate pain types as varied as a toothache or postsurgical pain reflects the diverse range of mechanism(s) by which pain-relieving "analgesic" therapies may reduce, eliminate, or prevent pain. Systemic application of an analgesic able to cross the blood-brain barrier can result in pain modulation via interaction with targets at different sites in the central nervous system. A so-called supraspinal mechanism of action indicates manipulation of a brain-defined circuitry. Pre-clinical studies demonstrate that, according to the brain circuitry targeted, varying therapeutic pain-relieving effects may be observed that relate to an impact on, for example, sensory and/or affective qualities of pain. In many cases, this translates to the clinic. Regardless of the brain circuitry manipulated, modulation of brain processing often directly impacts multiple aspects of nociceptive transmission, including spinal neuronal signaling. Consideration of supraspinal mechanisms of analgesia and ensuing pain relief must take into account nonbrain-mediated effects; therefore, in this review, the supraspinally mediated analgesic actions of opioidergic, anti-convulsant, and anti-depressant drugs are discussed. The persistence of poor treatment outcomes and/or side effect profiles of currently used analgesics highlight the need for the development of novel therapeutics or more precise use of available agents. Fully uncovering the complex biology of nociception, as well as currently used analgesic mechanism(s) and site(s) of action, will expedite this process.

Published

2020

25. Modulation of sensitization processes in the management of pain and the importance of descending pathways: a role for tapentadol?

Author

Caraci F, Coluzzi F, Marinangeli F, Mercadante S, Rinonapoli G, Romualdi P, Nicora M, and Dickenson AH

Subjects

Humans, Norepinephrine physiology, Receptors, Opioid, mu agonists, Adrenergic Uptake Inhibitors therapeutic use, Analgesics, Opioid therapeutic use, Chronic Pain drug therapy, Pain Management methods, Tapentadol therapeutic use

Abstract

Objective: This paper presents and discusses recent evidence on the pathophysiological mechanisms of pain. The role of tapentadol - an opioid characterized by an innovative mechanism of action (i.e. µ-opioid receptor [MOR] agonism and inhibition of noradrenaline [NA] reuptake [NRI]) - in the modulation of pain, and the most recent pharmacological evidence on this molecule (e.g. the µ-load concept) are also presented and commented upon. Methods: Narrative review. Results: Solid evidence has highlighted the importance of central sensitization in the transition from acute to chronic pain. In particular, the noradrenergic system holds a major role in limiting central sensitization and the progression to chronic pain. Therefore, pharmacological modulation of the noradrenergic system appears to be a well-grounded strategy for the control of chronic pain. Tapentadol is characterized by a to-date-unique mechanism of action, since it acts both as a MOR agonist and as an inhibitor of NA reuptake. The synergistic interaction of these two mechanisms allows a strong analgesic effect by acting on both ascending and descending pathways. Of note, the reduced µ-load of tapentadol limits the risk of opioid-related adverse events, such as gastrointestinal disturbances. Moreover, the NA component becomes predominant, at least, in some types of pain, with consequent specific clinical efficacy in the treatment of neuropathic and chronic pain. Conclusions: According to these characteristics, tapentadol appears suitable in the treatment of severe uncontrolled chronic pain characterized by both a nociceptive and a neuropathic component, such as osteoarthritis or back pain.

Published

2020

26. GPR160 de-orphanization reveals critical roles in neuropathic pain in rodents.

Author

Yosten GL, Harada CM, Haddock C, Giancotti LA, Kolar GR, Patel R, Guo C, Chen Z, Zhang J, Doyle TM, Dickenson AH, Samson WK, and Salvemini D

Subjects

Animals, Cell Line, Female, Humans, Ligands, Male, Mice, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Neuralgia genetics, PC12 Cells, RNA, Small Interfering genetics, Rats, Receptors, G-Protein-Coupled antagonists & inhibitors, Receptors, G-Protein-Coupled genetics, Sciatic Nerve injuries, Sciatic Nerve physiopathology, Signal Transduction, Spinal Cord metabolism, Up-Regulation, Neuralgia etiology, Neuralgia physiopathology, Receptors, G-Protein-Coupled physiology

Abstract

Treating neuropathic pain is challenging and novel non-opioid-based medicines are needed. Using unbiased receptomics, transcriptomic analyses, immunofluorescence, and in situ hybridization, we found that the expression of the orphan GPCR Gpr160 and GPR160 increased in the rodent dorsal horn of the spinal cord following traumatic nerve injury. Genetic and immunopharmacological approaches demonstrated that GPR160 inhibition in the spinal cord prevented and reversed neuropathic pain in male and female rodents without altering normal pain response. GPR160 inhibition in the spinal cord attenuated sensory processing in the thalamus, a key relay in the sensory discriminative pathways of pain. We also identified cocaine- and amphetamine-regulated transcript peptide (CARTp) as a GPR160 ligand. Inhibiting endogenous CARTp signaling in spinal cord attenuated neuropathic pain, whereas exogenous intrathecal CARTp evoked painful hypersensitivity through GPR160-dependent ERK and cAMP response element-binding protein (CREB). Our findings de-orphanize GPR160, identify it as a determinant of neuropathic pain and potential therapeutic target, and provide insights into its signaling pathways. CARTp is involved in many diseases including depression and reward and addiction; de-orphanization of GPR160 is a major step forward understanding the role of CARTp signaling in health and disease.

Published

2020

27. Supraspinal Opioid Circuits Differentially Modulate Spinal Neuronal Responses in Neuropathic Rats.

Author

Dickenson AH, Navratilova E, Patel R, Porreca F, and Bannister K

Subjects

Action Potentials drug effects, Action Potentials physiology, Amygdala physiology, Animals, Dose-Response Relationship, Drug, Gyrus Cinguli drug effects, Gyrus Cinguli physiology, Male, Medulla Oblongata drug effects, Medulla Oblongata physiology, Microinjections methods, Nerve Net physiology, Peripheral Nervous System Diseases physiopathology, Posterior Horn Cells drug effects, Posterior Horn Cells physiology, Rats, Rats, Sprague-Dawley, Spinal Nerves physiology, Amygdala drug effects, Analgesics, Opioid administration & dosage, Morphine administration & dosage, Nerve Net drug effects, Peripheral Nervous System Diseases drug therapy, Spinal Nerves drug effects

Abstract

Background: The anterior cingulate cortex and central nucleus of the amygdala connect widely with brainstem nuclei involved in descending modulation, including the rostral ventromedial medulla. Endogenous opioids in these circuits participate in pain modulation. The hypothesis was that a differential opioidergic role for the brain nuclei listed in regulation of spinal neuronal responses because separable effects on pain behaviors in awake animals were previously observed., Methods: This study utilized in vivo electrophysiology to determine the effects of morphine microinjection into the anterior cingulate cortex, right or left central nucleus of the amygdala, or the rostral ventromedial medulla on spinal wide dynamic range neuronal responses in isoflurane-anesthetized, male Sprague-Dawley rats. Ongoing activity in the ventrobasal thalamus was also measured. In total, 33 spinal nerve ligated and 26 control age- and weight-matched control rats were used., Results: Brainstem morphine reduced neuronal firing to 60-g von Frey stimulation in control rats (to 65 ± 12% of control response (means ± 95% CI), P < 0.001) with a greater inhibition in neuropathic rats (to 53 ± 17% of control response, P < 0.001). Contrasting anterior cingulate cortex morphine had only marginal modulatory effects on spinal neuronal responses with limited variance in effect between control and neuropathic rats. The inhibitory effects of morphine in the central nucleus of the amygdala were dependent on pain state and laterality; only right-side morphine reduced neuronal firing to 60-g stimulation in neuropathic rats (to 65 ± 14% of control response, P = 0.001). In addition, in neuropathic rats elevated ongoing neuronal activity in the ventral posterolateral thalamus was not inhibited by anterior cingulate cortex morphine, in contrast to evoked responses., Conclusions: Cumulatively the data support opioid modulation of evoked responses predominately through a lateralized output from the right amygdala, as well as from the brainstem that is enhanced in injured conditions. Minimal modulation of dorsal horn responses was observed after anterior cingulate cortex opioid administration regardless of injury state.

Published

2020

28. What goes up must come down: insights from studies on descending controls acting on spinal pain processing.

Author

Lockwood S and Dickenson AH

Subjects

Animals, Humans, Neural Pathways metabolism, Neural Pathways physiopathology, Brain drug effects, Brain metabolism, Brain physiopathology, Neurotransmitter Agents pharmacology, Osteoarthritis drug therapy, Osteoarthritis metabolism, Osteoarthritis physiopathology, Pain drug therapy, Pain metabolism, Pain physiopathology, Spinal Cord drug effects, Spinal Cord metabolism, Spinal Cord physiopathology

Abstract

Descending controls link higher processing of noxious signals to modulation of spinal cord responses to their noxious inputs. It has become possible to study one key inhibitory system in animals and humans using one painful stimulus to attenuate another distant response and so eliciting diffuse noxious inhibitory controls (DNIC) or the human counterpart, conditioned pain modulation (CPM). Here, we discuss the neuronal pathways in both species, their pharmacology and examine changes in descending controls with a focus on osteoarthritis. We will also discuss the opposing descending facilitatory system. Strong parallels between DNIC and CPM emphasize the possibility of forward and reverse translation.

Published

2020

29. Selective modulation of tonic aversive qualities of neuropathic pain by morphine in the central nucleus of the amygdala requires endogenous opioid signaling in the anterior cingulate cortex.

Author

Navratilova E, Nation K, Remeniuk B, Neugebauer V, Bannister K, Dickenson AH, and Porreca F

Subjects

Animals, Central Amygdaloid Nucleus diagnostic imaging, Gyrus Cinguli diagnostic imaging, Injections, Intraventricular, Male, Microinjections methods, Neuralgia diagnostic imaging, Rats, Sprague-Dawley, Signal Transduction drug effects, Signal Transduction physiology, Analgesics, Opioid administration & dosage, Central Amygdaloid Nucleus drug effects, Gyrus Cinguli drug effects, Morphine administration & dosage, Neuralgia drug therapy, Receptors, Opioid agonists

Abstract

The amygdala is a key subcortical region believed to contribute to emotional components of pain. As opioid receptors are found in both the central (CeA) and basolateral (BLA) nuclei of the amygdala, we investigated the effects of morphine microinjection on evoked pain responses, pain-motivated behaviors, dopamine release in the nucleus accumbens (NAc), and descending modulation in rats with left-side spinal nerve ligation (SNL). Morphine administered into the right or left CeA had no effect on nerve injury-induced tactile allodynia or mechanical hyperalgesia. Right, but not left, CeA morphine produced conditioned place preference (CPP) and increased extracellular dopamine in the NAc selectively in SNL rats, suggesting relief of aversive qualities of ongoing pain. In SNL rats, CPP and NAc dopamine release following right CeA morphine was abolished by blocking mu opioid receptor signaling in the rostral anterior cingulate cortex (rACC). Right CeA morphine also significantly restored SNL-induced loss of the diffuse noxious inhibitory controls, a spino-bulbo-spinal pain modulatory mechanism, termed conditioned pain modulation in humans. Microinjection of morphine into the BLA had no effects on evoked behaviors and did not produce CPP in nerve-injured rats. These findings demonstrate that the amygdalar action of morphine is specific to the right CeA contralateral to the side of injury and results in enhancement of net descending inhibition. In addition, engagement of mu opioid receptors in the right CeA modulates affective qualities of ongoing pain through endogenous opioid neurotransmission within the rACC, revealing opioid-dependent functional connections from the CeA to the rACC.

Published

2020

30. A study of cortical and brainstem mechanisms of diffuse noxious inhibitory controls in anaesthetised normal and neuropathic rats.

Author

Patel R and Dickenson AH

Subjects

Animals, Brain Stem, Humans, Rats, Rats, Sprague-Dawley, Spinal Cord, Spinal Nerves, Diffuse Noxious Inhibitory Control

Abstract

Diffuse noxious inhibitory controls (DNIC) are a mechanism of endogenous descending pain modulation and are deficient in a large proportion of chronic pain patients. However, the pathways involved remain only partially determined with several cortical and brainstem structures implicated. This study examined the role of the dorsal reticular nucleus (DRt) and infralimbic (ILC) region of the medial prefrontal cortex in DNIC. In vivo electrophysiology was performed to record from dorsal horn lamina V/VI wide dynamic range neurones with left hind paw receptive fields in anaesthetised sham-operated and L5/L6 spinal nerve-ligated (SNL) rats. Evoked neuronal responses were quantified in the presence and absence of a conditioning stimulus (left ear clamp). In sham rats, DNIC were reproducibly recruited by a heterotopically applied conditioning stimulus, an effect that was absent in neuropathic rats. Intra-DRt naloxone had no effect on spinal neuronal responses to dynamic brush, punctate mechanical, evaporative cooling and heat stimuli in sham and SNL rats. In addition, intra-DRt naloxone blocked DNIC in sham rats, but had no effect in SNL rats. Intra-ILC lidocaine had no effect on spinal neuronal responses to dynamic brush, punctate mechanical, evaporative cooling and heat stimuli in sham and SNL rats. However, differential effects were observed in relation to the expression of DNIC; intra-ILC lidocaine blocked activation of DNIC in sham rats but restored DNIC in SNL rats. These data suggest that the ILC is not directly involved in mediating DNIC but can modulate its activation and that DRt involvement in DNIC requires opioidergic signalling., (© 2019 The Authors. European Journal of Neuroscience published by Federation of European Neuroscience Societies and John Wiley & Sons Ltd.)

Published

2020

31. Translational issues in precision medicine in neuropathic pain.

Author

Dickenson AH and Patel R

Abstract

Neuropathic pain remains poorly treated, with most new drugs falling through the translational gap. The traditional model of bench-to-bedside research has relied on identifying new mechanisms/targets in animal models and then developing clinical applications. Several have advocated bridging the translational gap by beginning with clinical observations and back-translating to animal models for further investigation of mechanisms. There is good evidence that phenotyping of patients through quantitative sensory testing can lead to improved treatment selection and hence improved patient outcomes. This practice has been widely adopted in clinical investigations, but its application in preclinical research is not mainstream. In this review, we retrospectively examine our historical rodent data sets with the aim of reconsidering drug effects on sensory neuronal endpoints, their alignment with clinical observations, and how these might guide future clinical studies., (© 2020 The Author(s). Published with license by Taylor & Francis Group, LLC.)

Published

2020

32. Neuropathic Pain: Mechanism-Based Therapeutics.

Author

Bannister K, Sachau J, Baron R, and Dickenson AH

Subjects

Animals, Humans, Neuralgia diagnosis, Neuralgia physiopathology, Phenotype, Translational Research, Biomedical, Analgesics pharmacology, Neuralgia drug therapy

Abstract

Neuropathic pain (NeP) can result from sources as varied as nerve compression, channelopathies, autoimmune disease, and incision. By identifying the neurobiological changes that underlie the pain state, it will be clinically possible to exploit mechanism-based therapeutics for maximum analgesic effect as diagnostic accuracy is optimized. Obtaining sufficient knowledge regarding the neuroadaptive alterations that occur in a particular NeP state will result in improved patient analgesia and a mechanism-based, as opposed to a disease-based, therapeutic approach to facilitate target identification. This will rely on comprehensive disease pathology insight; our knowledge is vastly improving due to continued forward and back translational preclinical and clinical research efforts. Here we discuss the clinical aspects of neuropathy and currently used drugs whose mechanisms of action are outlined alongside their clinical use. Finally, we consider sensory phenotypes, patient clusters, and predicting the efficacy of an analgesic for neuropathy.

Published

2020

33. Sigma-1 receptor modulates neuroinflammation associated with mechanical hypersensitivity and opioid tolerance in a mouse model of osteoarthritis pain.

Author

Carcolé M, Kummer S, Gonçalves L, Zamanillo D, Merlos M, Dickenson AH, Fernández-Pastor B, Cabañero D, and Maldonado R

Subjects

Analgesics, Opioid pharmacology, Animals, Dose-Response Relationship, Drug, Drug Tolerance, Hyperalgesia drug therapy, Inflammation drug therapy, Injections, Intra-Articular, Iodoacetic Acid administration & dosage, Male, Mice, Morphine pharmacology, Morpholines pharmacology, Osteoarthritis chemically induced, Osteoarthritis drug therapy, Pain chemically induced, Pain drug therapy, Pyrazoles pharmacology, Receptors, sigma antagonists & inhibitors, Sigma-1 Receptor, Disease Models, Animal, Hyperalgesia metabolism, Inflammation metabolism, Osteoarthritis metabolism, Pain metabolism, Receptors, sigma metabolism

Abstract

Background and Purpose: Osteoarthritic pain is a chronic disabling condition lacking effective treatment. Continuous use of opioid drugs during osteoarthritic pain induces tolerance and may result in dose escalation and abuse. Sigma-1 (σ1) receptors, a chaperone expressed in key areas for pain control, modulates μ-opioid receptor activity and represents a promising target to tackle these problems. The present study investigates the efficacy of the σ1 receptor antagonist E-52862 to inhibit pain sensitization, morphine tolerance, and associated electrophysiological and molecular changes in a murine model of osteoarthritic pain., Experimental Approach: Mice received an intra-knee injection of monoiodoacetate followed by 14-day treatment with E-52862, morphine, or vehicle, and mechanical sensitivity was assessed before and after the daily doses., Key Results: Monoiodoacetate-injected mice developed persistent mechanical hypersensitivity, which was dose-dependently inhibited by E-52862. Mechanical thresholds assessed before the daily E-52862 dose showed gradual recovery, reaching complete restoration by the end of the treatment. When repeated treatment started 15 days after knee injury, E-52862 produced enhanced short-term analgesia, but recovery to baseline threshold was slower. Both a σ1 receptor agonist and a μ receptor antagonist blocked the analgesic effects of E-52862. An acute, sub-effective dose of E-52862 restored morphine analgesia in opioid-tolerant mice. Moreover, E-52862 abolished spinal sensitization in osteoarthritic mice and inhibited pain-related molecular changes., Conclusion and Implications: These findings show dual effects of σ1 receptor antagonism alleviating both short- and long-lasting antinociception during chronic osteoarthritis pain. They identify E-52862 as a promising pharmacological agent to treat chronic pain and avoid opioid tolerance., (© 2019 The British Pharmacological Society.)

Published

2019

34. Kappa opioid signaling in the right central amygdala causes hind paw specific loss of diffuse noxious inhibitory controls in experimental neuropathic pain.

Author

Phelps CE, Navratilova E, Dickenson AH, Porreca F, and Bannister K

Subjects

Animals, Chronic Pain physiopathology, Electrophysiological Phenomena, Functional Laterality, Hindlimb innervation, Hyperalgesia drug therapy, Hyperalgesia physiopathology, Ligation, Male, Naltrexone analogs & derivatives, Naltrexone pharmacology, Neuralgia psychology, Pain Measurement, Rats, Rats, Sprague-Dawley, Receptors, Opioid, kappa antagonists & inhibitors, Spinal Nerves physiopathology, Amygdala physiopathology, Diffuse Noxious Inhibitory Control drug effects, Hindlimb physiopathology, Neuralgia physiopathology, Receptors, Opioid, kappa drug effects, Signal Transduction

Abstract

Diffuse noxious inhibitory controls (DNICs) is a pain-inhibits-pain phenomenon demonstrated in humans and animals. Diffuse noxious inhibitory control is diminished in many chronic pain states, including neuropathic pain. The efficiency of DNIC has been suggested to prospectively predict both the likelihood of pain chronification and treatment response. Little is known as to why DNIC is dysfunctional in neuropathic pain. Here, we evaluated DNIC in the rat L5/L6 spinal nerve ligation (SNL) model of chronic pain using both behavioral and electrophysiological outcomes. For behavior, nociceptive thresholds were determined using response to noxious paw pressure on both hind paws as the test stimulus before, and after, injection of a conditioning stimulus of capsaicin into the left forepaw. Functionally, the spike firing of spinal wide-dynamic-range neuronal activity was evaluated before and during noxious ear pinch, while stimulating the ipsilateral paw with von Frey hairs of increased bending force. In both assays, the DNIC response was significantly diminished in the ipsilateral (ie, injured) paw of SNL animals. However, behavioral loss of DNIC was not observed on the contralateral (ie, uninjured) paw. Systemic application of nor-binaltorphimine, a kappa opioid antagonist, did not ameliorate SNL-induced hyperalgesia but reversed loss of the behavioral DNIC response. Microinjection of nor-binaltorphimine into the right central amygdala (RCeA) of SNL rats did not affect baseline thresholds but restored DNIC both behaviorally and electrophysiologically. Cumulatively, these data suggest that net enhanced descending facilitations may be mediated by kappa opioid receptor signaling from the right central amygdala to promote diminished DNIC after neuropathy.

Published

2019

35. A combination pharmacotherapy of tapentadol and pregabalin to tackle centrally driven osteoarthritis pain.

Author

Lockwood SM and Dickenson AH

Subjects

Analgesia, Analgesics therapeutic use, Animals, Chronic Pain drug therapy, Diffuse Noxious Inhibitory Control physiology, Humans, Male, Neurons drug effects, Norepinephrine, Spinal Cord metabolism, Osteoarthritis drug therapy, Pregabalin pharmacology, Tapentadol pharmacology

Abstract

Background: Many Osteoarthritis (OA) patients report with clinical features to their pain that cannot be explained by purely peripheral mechanisms. Yet, the analgesic agents available that tackle centrally driven chronic pain often provide only partial pain relief, or have dose-limiting side effects. We explored a combination therapy of the centrally acting analgesic agents tapentadol and pregabalin, to investigate if they could be used in combination to provide superior analgesia., Methods: Using electrophysiological single-unit recordings taken from spinal wide dynamic range neurons, Diffuse Noxious Inhibitory Controls (DNIC) were assessed as a marker of potential changes in descending controls in a monoiodoacetate (MIA) model of OA. We investigated if a subcutaneous injection of tapentadol or pregabalin, both alone and in combination, inhibited neuronal responses and restored the expression of DNIC, quantified as a reduction in neuronal firing in the presence of a conditioning noxious stimulus., Results: Tapentadol restored DNIC-induced neuronal inhibition in MIA animals, while pregabalin inhibited pre-conditioned mechanically evoked neuronal responses but did not restore DNIC. Given in combination, tapentadol and pregabalin restored DNIC expression and also inhibited spinal neuronal responses., Conclusions: We propose that there is both central sensitization and an imbalance in inhibitory and facilitatory descending controls in MIA animals. The combination therapy of tapentadol and pregabalin restored descending noradrenergic inhibitory tone and also inhibited nociceptive transmission at the level of the spinal cord., Significance: This study shows that pregabalin and tapentadol target different mechanisms of centrally driven chronic pain associated with osteoarthritis, and that when administered together can restore descending inhibitory tone whilst also tackling spinal neuronal hyperexcitability and may therefore provide superior analgesia., (© 2019 The Authors. European Journal of Pain published by John Wiley & Sons Ltd on behalf of European Pain Federation - EFIC ®.)

Published

2019

36. Issues in the future development of new analgesic drugs.

Author

David-Pereira A and Dickenson AH

Subjects

Analgesics administration & dosage, Analgesics adverse effects, Animals, Clinical Trials as Topic, Disease Models, Animal, Drug Evaluation, Preclinical methods, Humans, Perceptual Disorders genetics, Perceptual Disorders physiopathology, Analgesics therapeutic use, Drug Development organization & administration, Pain drug therapy

Abstract

Purpose of Review: There is a clear unmet need for either the development of new drugs for the treatment of painful pathologies or the better use of the existing agents denoted by the lack of efficacy of many existing drugs in a number of patients, limitations of their use due to severity of side effects, and by the high number of drugs that fail to reach clinical efficacy from preclinical development. This account considers the efforts being made to better validate new analgesic components and to improve translational efficacy of existing drugs., Recent Findings: A better use of the available models and tools can improve the predictive validity of new analgesic drugs, as well as using intermediate steps when translating drugs to clinical context such as characterizing drugs using stem cell-sensory derived neurones. Profiling patient sensory phenotypes can decrease the number of failed clinical trials and improve patient outcome., Summary: An integrative approach, comprising the use of complementary techniques to fully characterize drug profiles, is necessary to improve translational success of new analgesics.

Published

2019

37. Influence of behavioral traits in the inter-individual variability of nociceptive, emotional and cognitive manifestations of neuropathic pain.

Author

Martínez-Navarro M, Lara-Mayorga IM, Negrete R, Bilecki W, Wawrzczak-Bargieła A, Gonçalves L, Dickenson AH, Przewłocki R, Baños JE, and Maldonado R

Subjects

Animals, Behavior, Animal, Cell Cycle Proteins biosynthesis, Central Amygdaloid Nucleus metabolism, Central Amygdaloid Nucleus physiology, Enkephalins metabolism, Gene Expression, Interleukin-6 metabolism, Male, Mice, Neuralgia complications, Nociceptive Pain complications, Protein Precursors metabolism, Social Behavior, Cognition physiology, Emotions physiology, Individuality, Neuralgia physiopathology, Neuralgia psychology, Nociceptive Pain psychology

Abstract

Neuropathic pain is a complex disorder associated with emotional and cognitive deficits that may impair nociceptive manifestations. There is high inter-individual variability in the manifestations of human neuropathic pain, which largely depends on personality traits. We aim to identify the influence of different behavioral traits in the inter-individual vulnerability to neuropathic pain manifestations using behavioral, electrophysiological and genetic approaches. We first selected mice with extreme social and emotional traits and look for correlation with the spontaneous neuronal activity in the central amygdala. Neuropathic pain was induced to these mice to evaluate the influence of behavioral traits on nociceptive manifestations and gene expression profiles in the amygdala. Our results show an association of the spontaneous central amygdala neuronal activity with the sociability behavior. We demonstrate that low sociable, high anxious and low depressive phenotypes develop enhanced nociceptive hypersensitivity after nerve injury. However, greater emotional alterations and cognitive impairment are observed in high sociable, anxious-like and depressive-like mice, indicating that nociceptive, emotional and cognitive manifestations of neuropathic pain do not correlate with each other. Gene analyses identify high Pdyn and Il6 levels in the amygdala as indicative of enhanced nociceptive hypersensitivity and reveal an association between high Gadd45 expression and attenuated emotional and cognitive manifestations of neuropathic pain., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

38. Characterisation of peripheral and central components of the rat monoiodoacetate model of Osteoarthritis.

Author

Lockwood SM, Lopes DM, McMahon SB, and Dickenson AH

Subjects

Animals, Arthralgia diagnosis, Arthralgia etiology, Cartilage, Articular metabolism, Disease Models, Animal, Ganglia, Spinal pathology, Immunohistochemistry, Iodoacetic Acid toxicity, Knee Joint drug effects, Knee Joint metabolism, Male, Osteoarthritis, Knee chemically induced, Osteoarthritis, Knee complications, Rats, Rats, Sprague-Dawley, Cartilage, Articular pathology, Ganglia, Spinal metabolism, Interleukin-1beta metabolism, Knee Joint pathology, Osteoarthritis, Knee diagnosis

Abstract

Objective: Pain is the main reason patients report Osteoarthritis (OA), yet current analgesics remain relatively ineffective. This study investigated both peripheral and central mechanisms that lead to the development of OA associated chronic pain., Design: The monoiodoacetate (MIA) model of OA was investigated at early (2-6 days post injection) and late (>14 days post injection) time points. Pain-like behaviour and knee histology were assessed to understand the extent of pain due to cartilage degradation. Electrophysiological single-unit recordings were taken from spinal wide dynamic range (WDR) neurons to investigate Diffuse Noxious Inhibitory Controls (DNIC) as a marker of potential changes in descending controls. Immunohistochemistry was performed on dorsal root ganglion (DRG) neurons to assess any MIA induced neuronal damage. Furthermore, qPCR was used to measure levels of glia cells and cytokines in the dorsal horn., Results: Both MIA groups develop pain-like behaviour but only late phase (LP) animals display extensive cartilage degradation. Early phase animals have a normally functioning DNIC system but there is a loss of DNIC in LP animals. We found no evidence for neuronal damage caused by MIA in either group, yet an increase in IL-1β mRNA in the dorsal horn of LP animals., Conclusion: The loss of DNIC in LP MIA animals suggests an imbalance in inhibitory and facilitatory descending controls, and a rise in the mRNA expression of IL-1β mRNA suggest the development of central sensitisation. Therefore, the pain associated with OA in LP animals may not be attributed to purely peripheral mechanisms., (Copyright © 2019 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2019

39. An investigation into the noradrenergic and serotonergic contributions of diffuse noxious inhibitory controls in a monoiodoacetate model of osteoarthritis.

Author

Lockwood SM, Bannister K, and Dickenson AH

Subjects

Action Potentials drug effects, Action Potentials physiology, Adrenergic alpha-2 Receptor Antagonists pharmacology, Animals, Diffuse Noxious Inhibitory Control drug effects, Disease Models, Animal, Disease Progression, Ganglia, Spinal drug effects, Ganglia, Spinal metabolism, Iodoacetic Acid, Male, Neural Inhibition drug effects, Neural Inhibition physiology, Neurons drug effects, Neurons metabolism, Norepinephrine metabolism, RNA, Messenger metabolism, Rats, Sprague-Dawley, Serotonin metabolism, Serotonin Antagonists pharmacology, Spinal Cord drug effects, Diffuse Noxious Inhibitory Control physiology, Osteoarthritis metabolism, Osteoarthritis therapy, Receptors, Adrenergic, alpha-2 metabolism, Receptors, Serotonin metabolism, Spinal Cord metabolism

Abstract

Osteoarthritis (OA) is a debilitating conditioning with pain as the major clinical symptom. Understanding the mechanisms that drive OA-associated chronic pain is crucial for developing the most effective analgesics. Although the degradation of the joint is the initial trigger for the development of chronic pain, the discordance between radiographic joint damage and the reported pain experience in patients, coupled with clinical features that cannot be explained by purely peripheral mechanisms, suggest there are often other factors at play. Therefore, this study considers the central contributions of chronic pain, using a monoiodoacetate (MIA) model of OA. Particularly, this study explores the functionality of descending controls over the course of the model by assessing diffuse noxious inhibitory controls (DNIC). Early-phase MIA animals have a functional DNIC system, whereas DNIC are abolished in late-phase MIA animals, indicating a dysregulation in descending modulation over the course of the model. In early-phase animals, blocking the actions of spinal α 2 -adrenergic receptors completely abolishes DNIC, whereas blocking the actions of spinal 5-HT 7 receptors only partially decreases the magnitude of DNIC. However, activating the spinal α 2 -adrenergic or 5-HT 7 receptors in late-phase MIA animals restored DNIC-induced neuronal inhibition. This study confirms that descending noradrenergic signaling is crucial for DNIC expression. Furthermore, we suggest a compensatory increase in descending serotonergic inhibition acting at 5-HT 7 receptors as the model progresses such that receptor activation is sufficient to override the imbalance in descending controls and mediate neuronal inhibition. NEW & NOTEWORTHY This study showed that there are both noradrenergic and serotonergic components contributing to the expression of diffuse noxious inhibitory controls (DNIC). Furthermore, although a tonic descending noradrenergic tone is always crucial for the expression of DNIC, variations in descending serotonergic signaling over the course of the model mean this component plays a more vital role in states of sensitization.

Published

2019

40. Neuropathy following spinal nerve injury shares features with the irritable nociceptor phenotype: A back-translational study of oxcarbazepine.

Author

Patel R, Kucharczyk M, Montagut-Bordas C, Lockwood S, and Dickenson AH

Subjects

Animals, Ligation, Male, Neuralgia physiopathology, Neurons drug effects, Nociceptors drug effects, Phenotype, Rats, Rats, Sprague-Dawley, Thalamus, Action Potentials drug effects, Nociceptors physiology, Oxcarbazepine pharmacology, Peripheral Nervous System Diseases physiopathology, Posterior Horn Cells drug effects, Spinal Nerves injuries, Ventral Thalamic Nuclei drug effects, Voltage-Gated Sodium Channel Blockers pharmacology

Abstract

Background: The term 'irritable nociceptor' was coined to describe neuropathic patients characterized by evoked hypersensitivity and preservation of primary afferent fibres. Oxcarbazepine is largely ineffectual in an overall patient population, but has clear efficacy in a subgroup with the irritable nociceptor profile. We examine whether neuropathy in rats induced by spinal nerve injury shares overlapping pharmacological sensitivity with the irritable nociceptor phenotype using drugs that target sodium channels., Methods: In vivo electrophysiology was performed in anaesthetized spinal nerve ligated (SNL) and sham-operated rats to record from wide dynamic range (WDR) neurones in the ventral posterolateral thalamus (VPL) and dorsal horn., Results: In neuropathic rats, spontaneous activity in the VPL was substantially attenuated by spinal lidocaine, an effect that was absent in sham rats. The former measure was in part dependent on ongoing peripheral activity as intraplantar lidocaine also reduced aberrant spontaneous thalamic firing. Systemic oxcarbazepine had no effect on wind-up of dorsal horn neurones in sham and SNL rats. However, in SNL rats, oxcarbazepine markedly inhibited punctate mechanical-, dynamic brush- and cold-evoked neuronal responses in the VPL and dorsal horn, with minimal effects on heat-evoked responses. In addition, oxcarbazepine inhibited spontaneous activity in the VPL. Intraplantar injection of the active metabolite licarbazepine replicated the effects of systemic oxcarbazepine, supporting a peripheral locus of action., Conclusions: We provide evidence that ongoing activity in primary afferent fibres drives spontaneous thalamic firing after spinal nerve injury and that oxcarbazepine through a peripheral mechanism exhibits modality-selective inhibitory effects on sensory neuronal processing., Significance: The inhibitory effects of lidocaine and oxcarbazepine in this rat model of neuropathy resemble the clinical observations in the irritable nociceptor patient subgroup and support a mechanism-based rationale for bench-to-bedside translation when screening novel drugs., (© 2018 The Authors. European Journal of Pain published by John Wiley & Sons Ltd on behalf of European Pain Federation - EFIC®.)

Published

2019

41. Modality selective roles of pro-nociceptive spinal 5-HT 2A and 5-HT 3 receptors in normal and neuropathic states.

Author

Patel R and Dickenson AH

Subjects

Animals, Disease Models, Animal, Ketanserin pharmacology, Male, Membrane Potentials drug effects, Membrane Potentials physiology, Neural Pathways drug effects, Neural Pathways metabolism, Neurons drug effects, Neurons metabolism, Ondansetron pharmacology, Rats, Sprague-Dawley, Serotonin Antagonists pharmacology, Spinal Cord drug effects, Spinal Nerves injuries, Thalamus metabolism, Neuralgia metabolism, Nociceptive Pain metabolism, Receptor, Serotonin, 5-HT2A metabolism, Receptors, Serotonin, 5-HT3 metabolism, Spinal Cord metabolism

Abstract

Descending brainstem control of spinal nociceptive processing permits a dynamic and adaptive modulation of ascending sensory information. Chronic pain states are frequently associated with enhanced descending excitatory drive mediated predominantly through serotonergic neurones in the rostral ventromedial medulla. In this study, we examine the roles of spinal 5-HT 2A and 5-HT 3 receptors in modulating ascending sensory output in normal and neuropathic states. In vivo electrophysiology was performed in anaesthetised spinal nerve ligated (SNL) and sham-operated rats to record from wide dynamic range neurones in the ventral posterolateral thalamus. In sham rats, block of spinal 5-HT 3 Rs with ondansetron revealed tonic facilitation of noxious punctate mechanical stimulation, whereas blocking 5-HT 2A Rs with ketanserin had minimal effect on neuronal responses to evoked stimuli. The inhibitory profiles of both drugs were altered in SNL rats; ondansetron additionally inhibited neuronal responses to lower intensity punctate mechanical stimuli and noxious heat evoked responses, whereas ketanserin inhibited innocuous and noxious evaporative cooling evoked responses. Neither drug had any effect on dynamic brush evoked responses nor on spontaneous firing rates in both sham and SNL rats. These data identify novel modality and intensity selective facilitatory roles of spinal 5-HT 2A and 5-HT 3 receptors on sensory neuronal processing within the spinothalamic-somatosensory cortical pathway., (Copyright © 2018 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2018

42. Morphine effects within the rodent anterior cingulate cortex and rostral ventromedial medulla reveal separable modulation of affective and sensory qualities of acute or chronic pain.

Author

Gomtsian L, Bannister K, Eyde N, Robles D, Dickenson AH, Porreca F, and Navratilova E

Subjects

Acute Pain drug therapy, Animals, Chronic Pain drug therapy, Conditioning, Operant drug effects, Disease Models, Animal, Exploratory Behavior drug effects, Hyperalgesia drug therapy, Hyperalgesia etiology, Male, Microinjections, Nociception drug effects, Pain Measurement, Rats, Rats, Sprague-Dawley, Acute Pain pathology, Analgesics, Opioid therapeutic use, Chronic Pain pathology, Gyrus Cinguli drug effects, Medulla Oblongata drug effects, Morphine therapeutic use

Abstract

Modulation of pain may result from engagement of opioid receptors in multiple brain regions. Whether sensory and affective qualities of pain are differentially affected by brain opioid receptor circuits remains unclear. We previously reported that opioid actions within the rostral anterior cingulate cortex (ACC) produce selective modulation of affective qualities of neuropathic pain in rodents, but whether such effects may occur in other areas of the ACC is not known. Here, morphine was microinjected into 3 regions of the ACC or into the rostral ventromedial medulla (RVM), and pain behaviors in naive, sham, or spinal nerve ligated (SNL) rats were evaluated. In naive animals, the tail-flick response was inhibited by RVM, but not ACC, morphine. Anterior cingulate cortex morphine did not affect tactile allodynia (the von Frey test) or mechanical (Randall-Selitto) or thermal (Hargreaves) hyperalgesia in spinal nerve ligated rats. In contrary, RVM morphine reduced tactile allodynia and produced both antihyperalgesic and analgesic effects against mechanical and thermal stimuli as well as conditioned place preference selectively in nerve-injured rats. Within the RVM, opioids inhibit nociceptive transmission reflected in both withdrawal thresholds and affective pain behaviors. Activation of mu opioid receptors within specific rostral ACC circuits, however, selectively modulates affective dimensions of ongoing pain without altering withdrawal behaviors. These data suggest that RVM and ACC opioid circuits differentially modulate sensory and affective qualities of pain, allowing for optimal behaviors that promote escape and survival. Targeting specific ACC opioid circuits may allow for treatment of chronic pain while preserving the physiological function of acute pain.

Published

2018

43. Selective deficiencies in descending inhibitory modulation in neuropathic rats: implications for enhancing noradrenergic tone.

Author

Patel R, Qu C, Xie JY, Porreca F, and Dickenson AH

Subjects

Action Potentials drug effects, Adrenergic Neurons drug effects, Adrenergic alpha-2 Receptor Agonists pharmacology, Adrenergic alpha-2 Receptor Antagonists pharmacology, Animals, Avoidance Learning drug effects, Clonidine pharmacology, Conditioning, Operant drug effects, Evoked Potentials drug effects, Imidazoles pharmacology, Male, Pain Threshold drug effects, Pain Threshold physiology, Rats, Rats, Sprague-Dawley, Action Potentials physiology, Adrenergic Neurons metabolism, Avoidance Learning physiology, Conditioning, Operant physiology, Evoked Potentials physiology, Neuralgia metabolism

Abstract

Pontine noradrenergic neurones form part of a descending inhibitory system that influences spinal nociceptive processing. Weak or absent descending inhibition is a common feature of chronic pain patients. We examined the extent to which the descending noradrenergic system is tonically active, how control of spinal neuronal excitability is integrated into thalamic relays within sensory-discriminative projection pathways, and how this inhibitory control is altered after nerve injury. In vivo electrophysiology was performed in anaesthetised spinal nerve-ligated (SNL) and sham-operated rats to record from wide dynamic range neurones in the ventral posterolateral thalamus (VPL). In sham rats, spinal block of α2-adrenoceptors with atipamezole resulted in enhanced stimulus-evoked and spontaneous firing in the VPL, and produced conditioned place avoidance. However, in SNL rats, these conditioned avoidance behaviours were absent. Furthermore, inhibitory control of evoked neuronal responses was lost, but spinal atipamezole markedly increased spontaneous firing. Augmenting spinal noradrenergic tone in neuropathic rats with reboxetine, a selective noradrenergic reuptake inhibitor, modestly reinstated inhibitory control of evoked responses in the VPL but had no effect on spontaneous firing. By contrast, clonidine, an α2 agonist, inhibited both evoked and spontaneous firing, and exhibited increased potency in SNL rats compared with sham controls. These data suggest descending noradrenergic inhibitory pathways are tonically active in sham rats. Moreover, in neuropathic states, descending inhibitory control is diminished, but not completely absent, and distinguishes between spontaneous and evoked neuronal activity. These observations may have implications for how analgesics targeting the noradrenergic system provide relief.

Published

2018

44. Sense and sensibility-logical approaches to profiling in animal models.

Author

Dickenson AH and Patel R

Subjects

Animals, Models, Animal, Neuralgia

Published

2018

45. Editorial for Pain: Nonmalignant Diseases in 2018.

Author

Dickenson AH and Bannister K

Subjects

Analgesics pharmacology, Blood-Brain Barrier physiopathology, Chronic Pain drug therapy, Headache physiopathology, Humans, Inflammation physiopathology, Pericytes metabolism, Toxins, Biological pharmacology, Chronic Pain physiopathology

Published

2018

46. Calcium channel modulation as a target in chronic pain control.

Author

Patel R, Montagut-Bordas C, and Dickenson AH

Subjects

Animals, Chronic Pain metabolism, Humans, Calcium Channel Blockers pharmacology, Calcium Channels metabolism, Chronic Pain drug therapy

Abstract

Neuropathic pain remains poorly treated for large numbers of patients, and little progress has been made in developing novel classes of analgesics. To redress this issue, ziconotide (Prialt™) was developed and approved as a first-in-class synthetic version of ω-conotoxin MVIIA, a peptide blocker of Ca v 2.2 channels. Unfortunately, the impracticalities of intrathecal delivery, low therapeutic index and severe neurological side effects associated with ziconotide have restricted its use to exceptional circumstances. Ziconotide exhibits no state or use-dependent block of Ca v 2.2 channels; activation state-dependent blockers were hypothesized to circumvent the side effects of state-independent blockers by selectively targeting high-frequency firing of nociceptive neurones in chronic pain states, thus alleviating aberrant pain but not affecting normal sensory transduction. Unfortunately, numerous drugs, including state-dependent calcium channel blockers, have displayed efficacy in preclinical models but have subsequently been disappointing in clinical trials. In recent years, it has become more widely acknowledged that trans-aetiological sensory profiles exist amongst chronic pain patients and may indicate similar underlying mechanisms and drug sensitivities. Heterogeneity amongst patients, a reliance on stimulus-evoked endpoints in preclinical studies and a failure to utilize translatable endpoints, all are likely to have contributed to negative clinical trial results. We provide an overview of how electrophysiological and operant-based assays provide insight into sensory and affective aspects of pain in animal models and how these may relate to chronic pain patients in order to improve the bench-to-bedside translation of calcium channel modulators., Linked Articles: This article is part of a themed section on Recent Advances in Targeting Ion Channels to Treat Chronic Pain. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v175.12/issuetoc., (© 2017 The Authors. British Journal of Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society.)

Published

2018

47. Editorial for Pain: Cancer in 2018.

Author

Dickenson AH and Farquhar-Smith P

Subjects

Analgesics administration & dosage, Analgesics adverse effects, Humans, Palliative Care, Analgesics therapeutic use, Cancer Pain drug therapy, Pain, Postoperative drug therapy

Published

2018

48. Immune or Genetic-Mediated Disruption of CASPR2 Causes Pain Hypersensitivity Due to Enhanced Primary Afferent Excitability.

Author

Dawes JM, Weir GA, Middleton SJ, Patel R, Chisholm KI, Pettingill P, Peck LJ, Sheridan J, Shakir A, Jacobson L, Gutierrez-Mecinas M, Galino J, Walcher J, Kühnemund J, Kuehn H, Sanna MD, Lang B, Clark AJ, Themistocleous AC, Iwagaki N, West SJ, Werynska K, Carroll L, Trendafilova T, Menassa DA, Giannoccaro MP, Coutinho E, Cervellini I, Tewari D, Buckley C, Leite MI, Wildner H, Zeilhofer HU, Peles E, Todd AJ, McMahon SB, Dickenson AH, Lewin GR, Vincent A, and Bennett DL

Subjects

Animals, Cells, Cultured, Female, Humans, Immunization, Passive, Male, Mechanotransduction, Cellular, Membrane Proteins genetics, Membrane Proteins immunology, Mice, Inbred C57BL, Mice, Knockout, Nerve Tissue Proteins genetics, Nerve Tissue Proteins immunology, Posterior Horn Cells physiology, Shaker Superfamily of Potassium Channels physiology, Ganglia, Spinal physiopathology, Immunoglobulin G administration & dosage, Membrane Proteins physiology, Nerve Tissue Proteins physiology, Nociceptive Pain immunology, Nociceptive Pain physiopathology, Sensory Receptor Cells physiology

Abstract

Human autoantibodies to contactin-associated protein-like 2 (CASPR2) are often associated with neuropathic pain, and CASPR2 mutations have been linked to autism spectrum disorders, in which sensory dysfunction is increasingly recognized. Human CASPR2 autoantibodies, when injected into mice, were peripherally restricted and resulted in mechanical pain-related hypersensitivity in the absence of neural injury. We therefore investigated the mechanism by which CASPR2 modulates nociceptive function. Mice lacking CASPR2 (Cntnap2 -/- ) demonstrated enhanced pain-related hypersensitivity to noxious mechanical stimuli, heat, and algogens. Both primary afferent excitability and subsequent nociceptive transmission within the dorsal horn were increased in Cntnap2 -/- mice. Either immune or genetic-mediated ablation of CASPR2 enhanced the excitability of DRG neurons in a cell-autonomous fashion through regulation of Kv1 channel expression at the soma membrane. This is the first example of passive transfer of an autoimmune peripheral neuropathic pain disorder and demonstrates that CASPR2 has a key role in regulating cell-intrinsic dorsal root ganglion (DRG) neuron excitability., (Copyright © 2018 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2018

49. Holding down the pain.

Author

Dickenson AH

Subjects

Humans, Mutation, Pain, Pain Threshold, Synaptic Transmission, Hyperekplexia

Published

2018

50. Multiple sites and actions of gabapentin-induced relief of ongoing experimental neuropathic pain.

Author

Bannister K, Qu C, Navratilova E, Oyarzo J, Xie JY, King T, Dickenson AH, and Porreca F

Subjects

Animals, Disease Models, Animal, Gabapentin, Gyrus Cinguli drug effects, Male, Nucleus Accumbens drug effects, Posterior Horn Cells drug effects, Rats, Sprague-Dawley, Amines pharmacology, Cyclohexanecarboxylic Acids pharmacology, Neuralgia therapy, Pain Threshold drug effects, Spinal Nerves drug effects, gamma-Aminobutyric Acid pharmacology

Abstract

Gabapentin (GBP) is a first-line therapy for neuropathic pain, but its mechanisms and sites of action remain uncertain. We investigated GBP-induced modulation of neuropathic pain following spinal nerve ligation (SNL) in rats. Intravenous or intrathecal GBP reversed evoked mechanical hypersensitivity and produced conditioned place preference (CPP) and dopamine (DA) release in the nucleus accumbens (NAc) selectively in SNL rats. Spinal GBP also significantly inhibited dorsal horn wide-dynamic-range neuronal responses to a range of evoked stimuli in SNL rats. By contrast, GBP microinjected bilaterally into the rostral anterior cingulate cortex (rACC), produced CPP, and elicited NAc DA release selectively in SNL rats but did not reverse tactile allodynia and had marginal effects on wide-dynamic-range neuronal activity. Moreover, blockade of endogenous opioid signaling in the rACC prevented intravenous GBP-induced CPP and NAc DA release but failed to block its inhibition of tactile allodynia. Gabapentin, therefore, can potentially act to produce its pain relieving effects by (a) inhibition of injury-induced spinal neuronal excitability, evoked hypersensitivity, and ongoing pain and (b) selective supraspinal modulation of affective qualities of pain, without alteration of reflexive behaviors. Consistent with previous findings of pain relief from nonopioid analgesics, GBP requires engagement of rACC endogenous opioid circuits and downstream activation of mesolimbic reward circuits reflected in learned pain-motivated behaviors. These findings support the partial separation of sensory and affective dimensions of pain in this experimental model and suggest that modulation of affective-motivational qualities of pain may be the preferential mechanism of GBP's analgesic effects in patients.

Published

2017