| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 8536875 | Pharmacology & Therapeutics | 2018 | 64 Pages |
Abstract
One of the fundamental mechanisms whereby the innate immune system coordinates inflammatory signal transduction is through Toll-like receptors (TLRs), which function to protect and defend the host organism by initiating inflammatory signaling cascades in response to tissue damage or injury. TLRs are positioned at the neuroimmune interface, and accumulating evidence suggests that the inflammatory consequences of TLR activation on glia (including microglia and astrocytes), sensory neurons, and other cell types can influence nociceptive processing and lead to states of exaggerated and unresolved pain. In this review, we summarize our current understanding of how different TLRs and their accessory or adaptor molecules can contribute to the development and maintenance of persistent pain. The challenges and opportunities of targeting TLRs for new treatment strategies against chronic pain are discussed, including the therapeutic context of TLR-mediated signaling in opioid analgesia and chemotherapy-induced pain. Considering the prevalence of persistent pain and the insufficient efficacy and safety of current treatment options, a deeper understanding of Toll-like receptors holds the promise of novel therapies for managing pathological pain.
Keywords
NF-κBTRPA1LPSIL-6CCL2TRPV1JnkIL-1DRGmRNAMYD88GFAPNADPHIL-4DAMPERKLBPiNOSMCP-1CD36HspIL-1βIL-10AP-1ODNCCIoligodeoxynucleotideTLRCIPNHMGB1PRRCLRintegrin alpha MCD14CXCL1CD11BRAGEIL-1RIL-8NLRcluster of differentiation 11bCCL21IRFRLRITGAMCR3LPS-RSMD-2CSF-1TNFchemokine C-C motif ligand 2BDNFc-Jun N-terminal kinaseMAPKmessenger RNAshort interfering RNAsiRNATRIFAdenosine TriphosphateATPchronic constriction injuryMacrophage-1 antigenLet-7γ-aminobutyric acidRNAribonucleic acidinflammationdamage-associated molecular patternInnate immunityinterferonIFNinterleukin-4Interleukin-8Interleukin-10interleukin-6interleukin-1Interleukin-1βTIRToll-like receptorcluster of differentiation 14cluster of differentiation 36PainCNSinducible nitric oxide synthasecentral nervous systemchemotherapy-induced peripheral neuropathymyeloid differentiation factor 2IFN regulatory factornociceptionBrain-derived neurotrophic factortumor necrosis factornuclear factor-κBlipopolysaccharidecolony stimulating factor 1Mac-1MicroRNAMiRNAnicotinamide adenine dinucleotide phosphatepolymerase chain reactionPCRmyeloid differentiation primary response gene 88transient receptor potential ankyrin 1Transient receptor potential vanilloid 1LPS-binding proteinGlial fibrillary acidic proteinHigh-mobility group box protein 1Heat shock proteinmonocyte chemoattractant protein-1activator protein-1extracellular signal-regulated kinasemitogen-activated kinaseGABAdorsal root gangliaToll/interleukin-1 receptorinterleukin-1 receptorReceptor for advanced glycation end-productsComplement receptor 3pattern recognition receptorC-type lectin receptorGlia
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Authors
Michael J. Lacagnina, Linda R. Watkins, Peter M. Grace,