Abstract
The persistence of increased excitability and spontaneous activity in injured peripheral neurons is imperative for the development and persistence of many forms of neuropathic pain. This aberrant activity involves increased activity and/or expression of voltage-gated Na+ and Ca2+ channels and hyperpolarization activated cyclic nucleotide gated (HCN) channels as well as decreased function of K+ channels. Because they display limited central side effects, peripherally restricted Na+ and Ca2+ channel blockers and K+ channel activators offer potential therapeutic approaches to pain management. This review outlines the current status and future therapeutic promise of peripherally acting channel modulators. Selective blockers of Nav1.3, Nav1.7, Nav1.8, Cav3.2, and HCN2 and activators of Kv7.2 abrogate signs of neuropathic pain in animal models. Unfortunately, their performance in the clinic has been disappointing; some substances fail to meet therapeutic end points whereas others produce dose-limiting side effects. Despite this, peripheral voltage-gated cation channels retain their promise as therapeutic targets. The way forward may include (i) further structural refinement of K+ channel activators such as retigabine and ASP0819 to improve selectivity and limit toxicity; use or modification of Na+ channel blockers such as vixotrigine, PF-05089771, A803467, PF-01247324, VX-150 or arachnid toxins such as Tap1a; the use of Ca2+ channel blockers such as TTA-P2, TTA-A2, Z 944, ACT709478, and CNCB-2; (ii) improving methods for assessing “pain” as opposed to nociception in rodent models; (iii) recognizing sex differences in pain etiology; (iv) tailoring of therapeutic approaches to meet the symptoms and etiology of pain in individual patients via quantitative sensory testing and other personalized medicine approaches; (v) targeting genetic and biochemical mechanisms controlling channel expression using anti-NGF antibodies such as tanezumab or re-purposed drugs such as vorinostat, a histone methyltransferase inhibitor used in the management of T-cell lymphoma, or cercosporamide a MNK 1/2 inhibitor used in treatment of rheumatoid arthritis; (vi) combination therapy using drugs that are selective for different channel types or regulatory processes; (vii) directing preclinical validation work toward the use of human or human-derived tissue samples; and (viii) application of molecular biological approaches such as clustered regularly interspaced short palindromic repeats (CRISPR) technology.
Highlights
Whilst opioids are extremely effective in managing deep and nociceptive pain, the drugs available for treatment of neuropathic pain display limited effectiveness [1, 2]
Df1a is active in vivo and reverses the Inhibitors of channel function μ-theraphotoxin-Pn3a Phoneutria nigriventer toxin 1 Grammostola porter Toxin 1 Jingzhaotoxin-V μ-theraphotoxin-Tp1a Theraphosa apophysis Toxin 1a Davus fasciatus Toxin 1a Huwentoxin-IV Hainantoxins Activator of channel function α-scorpion toxin OD1
We found ivabradine administered to nerve injured rats at a dose that significantly reduced mechanical allodynia was without noticeable effect on arterial pressure and produced only a 15% reduction in heart rate, its cardiovascular actions have detracted from its use as an analgesic agent in the clinic [430]
Summary
Whilst opioids are extremely effective in managing deep and nociceptive pain, the drugs available for treatment of neuropathic pain display limited effectiveness [1, 2]. The genetic and structural definitions of Nav1.1–Nav1.9 channel subtypes was established many years ago [116,117,118] and this has led to a mechanistic and molecular understanding of injury-induced changes [8, 114] This has paved the way for selective targeting of TTX-sensitive Nav1.3, 1.6, and 1.7 channels and TTX-resistant Nav1.8 channels as these are important in the generation and maintenance of neuropathic pain [114, 119,120,121,122]. Nerve injury upregulates and promotes re-expression of Nav1.3 in adult DRG neurons [127, 130, 131] as well as in spinal dorsal horn and thalamus [132, 133] This may reflect removal of suppression of the SCN3A gene by microRNAs such as miR-384-5p, mir-96 and/or miR-30b suggesting that their targeted delivery may be of use in pain management [41,42,43]. Structure activity studies starting with a diphenylmethyl amide adduct of an aryl sulphonamide has led to the development of TABLE 1 | Potential and actual therapeutic candidates
Sign-in/Register to view highlights & summary Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a callMore From: Frontiers in pain research (Lausanne, Switzerland)
Disclaimer: All third-party content on this website/platform is and will remain the property of their respective owners and is provided on "as is" basis without any warranties, express or implied. Use of third-party content does not indicate any affiliation, sponsorship with or endorsement by them. Any references to third-party content is to identify the corresponding services and shall be considered fair use under The CopyrightLaw.
