Long-lasting Analgesia via Targeted<i>in vivo</i>Epigenetic Repression of Nav1.7

Moreno, Ana M.; Catroli, Glaucilene Ferreira; Alemán, Fernando; Pla, Andrew; Woller, Sarah A.; Hu, Michael; Yaksh, Tony L.; Mali, Prashant

doi:10.1101/711812

Cited by 7 publications

(3 citation statements)

References 112 publications

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“…12 For intractable chronic pain, gene therapy strategies that mimic genetic loss-of-function will likely be required. 56 Taken together, these data support a mechanism where pain insensitivity of mice and humans lacking NaV1.7 principally involves opioid receptors ( Figure S6). Diminished peripheral excitability and die-back may also contribute to analgesia, but opioid-mediated suppression of neurotransmitter release plays a major role.…”

Section: Discussionsupporting

confidence: 52%

The mechanism of analgesia in Na_V1.7 null mutants

MacDonald

Sikandar

Weiss

et al. 2020

Preprint

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Deletion of SCN9A encoding the voltage-gated sodium channel NaV1.7 in humans leads to profound pain insensitivity and anosmia. Conditional deletion of NaV1.7 in sensory neurons of mice also abolishes pain suggesting the locus of analgesia is the nociceptor.Here we demonstrate that NaV1.7 knockout mice have essentially normal nociceptor activity using in vivo calcium imaging and extracellular recording. However, glutamate and substance P release from nociceptor central terminals in the spinal cord is greatly reduced by an opioid-dependent mechanism. Analgesia is also substantially reversed by central but not peripheral application of opioid antagonists. In contrast, the lack of neurotransmitter release from olfactory sensory neurons is opioid-independent. Male and female humans with NaV1.7 null mutations show naloxone reversible analgesia. Thus opioid-dependent inhibition of neurotransmitter release is the principal mechanism of NaV1.7 null analgesia in mice and humans.deficits in thermal, mechanical, inflammatory and some forms of neuropathic pain. 15,16 To determine the mechanism of NaV1.7 null analgesia, we used complementary optical, electrophysiological and pharmacological methods to study nociceptor function in vivo in mice and humans lacking NaV1.7. ResultsDeletion of NaV1.7 in sensory neurons decreases pain sensitivity without silencing peripheral nociceptorsWe deleted Scn9a encoding NaV1.7 in peripheral sensory neurons of mice. Advillin-Cre or Wnt1-Cre was used to excise the floxed Scn9a allele, resulting in knockout of NaV1.7 restricted, respectively, to sensory neurons or to neural crest-derived neurons. 15 We performed whole-cell voltage-clamp recordings of voltage-gated sodium currents in cultured sensory neurons from solution contained 125 mM K-gluconate, 6 mM KCl, 10 mM HEPES, 0.1 mM EGTA, 2 mM Mg-ATP, pH 7.3 with KOH, and osmolarity of 290-310 mOsm. Cells were targeted for patching in the inner and outer Lamina II and visualized through an Eclipse E600FN Nikon microscope (Nikon, Japan) equipped with infrared differential interference contrast (IR-DIC) connected to a digital camera (Nikon, DS-Qi1Mc). Cells were voltage-clamped at -70 mV and spontaneous excitatory post synaptic currents (sEPSCs) recorded. sEPSCs were automatically detected using ClampFit in a 5 s window for each cell. Ex vivo olfactory bulb electrophysiology:Acute MOB slices were prepared from 4 -11 week old mice (male and female) anesthetized with CO2 before decapitation. OBs were rapidly dissected in ice-cold oxygenated (95% O2, 5% CO2) solution containing the following (in mM): 83 NaCl, 26.2 NaHCO3, 1 NaH2PO4, 2.5 KCl, 3.3 MgCl2, 0.5 CaCl2, 70 sucrose, pH 7.3 (osmolarity, 300 mOsm/l). The tissue was mounted on a

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Section: Discussionsupporting

confidence: 52%

The mechanism of analgesia in Na_V1.7 null mutants

MacDonald

Sikandar

Weiss

et al. 2020

Preprint

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“…Overexpression of the voltage-gated sodium channels Nav1.7 and Nav1.8 have also been observed in the DRG and SC of acute pain model animals [29]. Conversely, suppression of Nav1.7 was associated with long-lasting analgesia [30]. Furthermore, Nav1.8 is highly expressed by nociceptive sensory afferents, and expression increases during chronic pain [31].…”

Section: Discussionmentioning

confidence: 99%

Acupoint Injection of Dextrose Attenuates Chronic Inflammatory Pain In Mice Through Modulation of Transient Receptor Potential V1 Channel Expression

Liao¹,

Lin²,

Lin³

2021

Preprint

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Background: Neuroinflammatory processes initiated by injury, infection, and other insults induce long-term alterations in the signaling characteristics of nociceptive neurons and associated non-neuronal cells, resulting in chronic inflammatory pain (CIP). Prolotherapy, also termed acupoint injection (AI) therapy, utilizes anatomically based meridians derived from Chinese Medicinal Theory to attenuate chronic pain. In fact, AI has demonstrated superior results compared to traditional acupuncture methods without significant side effects. Methods: In this study, we explored the efficacy and underlying mechanisms of AI on CIP in mice. The mouse hindpaw was injected with complete Freund’s adjuvant (CFA) to induce CIP, followed AI treatment. Results: After two weeks, indices of mechanical and thermal hyperalgesia were significantly reduced by AI treatment. CIP was associated with elevated expression levels of transient receptor potential V1 (TRPV1) channels, various downstream kinases and transcription factors, and nociception-associated voltage-gated sodium channels (Navs) in dorsal root ganglion (DRG), spinal cord, thalamus, and somatosensory cortex, while AI-induced analgesia was associated with reversal of these expression changes. Further, upregulation of TRPV1-associated signaling factors was not observed in Trpv1 knockout mice following CFA injection. In addition, the activated microglial markers Iba-1 and S100B demonstrated similar expression changes and were colocalized with TRPV1. Conclusions: These findings suggest that AI can mitigate chronic pain (and sequel such as comorbid depression) by suppressing TRPV1 overexpression in neuronal or microglial cells.

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“…Although a recent study by Moreno AM et al, 2021, which was conducted in mice, suggests that the clustered regularly interspaced short palindromic repeats-Cas9 (CRISP-Cas9) new technique could reduce or block genes (polymorphisms) encoding channels (NaV1.7 at Neuro2A cells in lumbar dorsal root ganglia), so an effective reduction in pain sensitivity occurs. Maybe similar studies will be soon conducted in humans [ 46 ].…”

Section: Reviewmentioning

confidence: 99%

A Biopsychosocial Model-Based Clinical Approach in Myofascial Pain Syndrome: A Narrative Review

Koukoulithras

Plexousakis

Kolokotsios

et al. 2021

Cureus

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One of the most common chronic musculoskeletal pain syndromes is myofascial pain syndrome (MPS). Trigger points (TrPs) are hypersensitive taut bands that appear in two genres, each with a different ratio in specific areas of the muscles, and when triggered, they can produce pain, numbness, and tingling. Various underlying causes (mechanical, nutritional, and psychological) have been discovered to participate in the pathogenesis of MPS, activating trigger points and intensifying the pain. Furthermore, genetic, social, and psychological factors seem to exacerbate these patients' clinical appearance, according to the biopsychosocial model, which seems to be closely linked to the formation of trigger points. Chronic pain and psychological distress frequently coexist, and psychological and social factors have been found to worsen the patient's quality of life and perpetuate the existing pain. The diagnosis is formed following a comprehensive physical and clinical examination, and the appropriate management technique is selected. For MPS treatment, management techniques based on the biopsychosocial model are used in conjunction with various myofascial release strategies and pharmacologic care. Exercise, posture correction, and a vitamin balance in the diet, especially in the Vitamin B complex, appear to prevent trigger point (TrP) activation. The precise etiology of MPS is not clear yet, and further research is needed to determine the root cause. A holistic approach, which blends the basic clinical care with the management of the biopsychosocial model, is essential to patients with MPS to regain their function and improve their quality of life and wellbeing.

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Long-lasting Analgesia via Targetedin vivoEpigenetic Repression of Nav1.7

Cited by 7 publications

References 112 publications

The mechanism of analgesia in Na_V1.7 null mutants

The mechanism of analgesia in Na_V1.7 null mutants

Acupoint Injection of Dextrose Attenuates Chronic Inflammatory Pain In Mice Through Modulation of Transient Receptor Potential V1 Channel Expression

A Biopsychosocial Model-Based Clinical Approach in Myofascial Pain Syndrome: A Narrative Review

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Long-lasting Analgesia via Targetedin vivoEpigenetic Repression of Nav1.7

Cited by 7 publications

References 112 publications

The mechanism of analgesia in NaV1.7 null mutants

The mechanism of analgesia in NaV1.7 null mutants

Acupoint Injection of Dextrose Attenuates Chronic Inflammatory Pain In Mice Through Modulation of Transient Receptor Potential V1 Channel Expression

A Biopsychosocial Model-Based Clinical Approach in Myofascial Pain Syndrome: A Narrative Review

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The mechanism of analgesia in Na_V1.7 null mutants

The mechanism of analgesia in Na_V1.7 null mutants