Inhibition of mechanical allodynia in neuropathic pain by TLR5-mediated A-fiber blockade

p38 mitogen-activated protein kinase (MAPK) consists of two major isoforms: p38α and p38β; however, it remains unclear which isoform is more important for chronic pain development. Recently, we developed potent, long-lasting, and p38 MAPK subtype-specific antisense oligonucleotides (ASOs). We examined the therapeutic effects of isoform-specific ASOs in several chronic pain models following single intrathecal injection (300 µg/10 µl) in CD1 mice. In the chronic constriction injury (CCI) model, p38α MAPK ASO, given on post-operative day 5, reduced CCI-induced mechanical allodynia in male but not female mice. In contrast, mechanical allodynia after CCI in both sexes was not affected by p38β MAPK ASO. Intrathecal injection of p38α or p38β ASO resulted in a partial reduction (≈50%) of spinal p38α or p38β mRNA level, respectively, in both sexes at two weeks. In contrast, intrathecal injection of the ASOs did not affect p38α and p38β MAPK mRNA levels in dorsal root ganglia. Intrathecal p38α ASO also reduced postoperative pain (mechanical and cold allodynia) in male mice after tibia fracture. However, intrathecal p38α ASO had no effect on mechanical allodynia in male mice after paclitaxel treatment. Intrathecal p38α MAPK ASO pre-treatment also prevented TLR4-mediated mechanical allodynia and downregulated levels of p38α MAPK and phosphorylated p38 MAPK following intrathecal treatment of lipopolysaccharide. In summary, our findings suggest that p38α MAPK is the major p38 MAPK isoform in the spinal cord and regulates chronic pain in a sex and model-dependent manner. Intrathecal p38α MAPK ASO may offer a new treatment for some chronic pain conditions.

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“…To produce chemotherapy-associated neuropathic pain, paclitaxel (2 mg/kg, i.p.) was injected at day 0, 2, 4, and 6 (Xu et al, 2015). …”

Section: Methodsmentioning

confidence: 99%

Intrathecal administration of antisense oligonucleotide against p38α but not p38β MAP kinase isoform reduces neuropathic and postoperative pain and TLR4-induced pain in male mice

Luo

Fitzsimmons

Mohan

et al. 2018

Brain, Behavior, and Immunity

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“…This may be achieved by direct activation of TRPV1 by capsaicin or indirect activation of other drug-permeable channels via Toll-like receptor 5 (TLR5) (Peirs and Seal, 2015;Xu et al, 2015). The TRPV1 channel pore is large enough to permit permeation of a quaternary derivative of lidocaine known as QX-314.…”

Section: B Improving Gabapeninoid Effectivenessmentioning

confidence: 99%

“…It is effective when introduced into the cytoplasm via the TRPV1 channel, and this allows selective targeting of classic C fiber nociceptors in nociceptive pain. Because TLR5 is expressed on medium to large A fibers, including Ab mechanoreceptors in both mice and humans (Xu et al, 2015), this may allow selective pharmacological blockade of transmission in fiber types that mediate allodynia. We recently noted that GBP is able to permeate TRPV1 channels activated by capsaicin, and this led to increased effectiveness (Biggs et al, 2015).…”

Section: B Improving Gabapeninoid Effectivenessmentioning

confidence: 99%

“…We recently noted that GBP is able to permeate TRPV1 channels activated by capsaicin, and this led to increased effectiveness (Biggs et al, 2015). Perhaps topical application of GBP (Shahid et al, 2017) combined with a TLR5 agonist such as flagellin (Xu et al, 2015) may facilitate its access to a2d-1 and thereby increase its effectiveness in the clinic.…”

Section: B Improving Gabapeninoid Effectivenessmentioning

confidence: 99%

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Etiology and Pharmacology of Neuropathic Pain

Alles¹,

Smith²

2018

Pharmacol Rev

283

229

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“…Because of the process of central sensitisation, large A b fibres are able to engage the nociceptive system, and ectopic activity in sensory neurons, more so in myelinated than unmyelinated fibres, is a hallmark of neuropathic pain caused by peripheral nerve injury [17]. Accordingly, blockade of these large fibres can completely attenuate the allodynia and spontaneous pain in neuropathic pain models [18]. LGI1 antibodies were also reported in some patients with pain [3] but their significance is less easy to assess as LGI1 is not typically expressed at nodes of Ranvier or known to play a role in peripheral nerve, dorsal roots or spinal cord.…”

Section: Voltage-gated Potassium Channel Complex Antibodiesmentioning

confidence: 99%