Abstract

Sensitization of the heat-activated ion channel transient receptor potential vanilloid 1 (TRPV1) through lipids is a fundamental mechanism during inflammation-induced peripheral sensitization. Leukotriene B4 is a proinflammatory lipid mediator whose role in peripheral nociceptive sensitization is not well understood to date. Two major G-protein-coupled receptors for leukotriene B4 have been identified: the high-affinity receptor BLT1 and the low-affinity receptor BLT2. Transcriptional screening for the expression G-protein-coupled receptors in murine dorsal root ganglia showed that both receptors were among the highest expressed in dorsal root ganglia. Calcium imaging revealed a sensitization of TRPV1-mediated calcium increases in a relative narrow concentration range for leukotriene B4 (100-200 nm). Selective antagonists and neurons from knock-out mice demonstrated a BLT1-dependent sensitization of TRPV1-mediated calcium increases. Accordingly, leukotriene B4-induced thermal hyperalgesia was mediated through BLT1 and TRPV1 as shown using the respective knock-out mice. Importantly, higher leukotriene B4 concentrations (>0.5 μm) and BLT2 agonists abolished sensitization of the TRPV1-mediated calcium increases. Also, BLT2 activation inhibited protein kinase C- and protein kinase A-mediated sensitization processes through the phosphatase calcineurin. Consequently, a selective BLT2-receptor agonist increased thermal and mechanical withdrawal thresholds during zymosan-induced inflammation. In accordance with these data, immunohistochemical analysis showed that both leukotriene B4 receptors were expressed in peripheral sensory neurons. Thus, the data show that the two leukotriene B4 receptors have opposing roles in the sensitization of peripheral sensory neurons forming a self-restricting system.

Highlights

  • Sensitization of the heat-activated ion channel transient receptor potential vanilloid 1 (TRPV1) through lipids is a fundamental mechanism during inflammation-induced peripheral sensitization

  • We describe that BLT1 and BLT2 are coexpressed in peripheral sensory neurons and that low concentrations of Leukotriene B4 (LTB4) sensitize TRPV1-mediated intracellular calcium increases through BLT1-induced PKC activation, whereas higher LTB4 concentrations desensitize TRPV1-mediated calcium increases through BLT2-induced calcineurin activation

  • Low concentrations of LTB4 sensitize TRPV1-mediated calcium increases through BLT1

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Summary

Introduction

Sensitization of the heat-activated ion channel transient receptor potential vanilloid 1 (TRPV1) through lipids is a fundamental mechanism during inflammation-induced peripheral sensitization. LTB4 reduces the proresolving lipid 18S-resolvin LTB4-induced NF-␬B activation, as well as neutrophil infiltration by antagonizing BLT1, thereby limiting inflammation in mice [9, 10]. Ion channels such as the transient receptor potential channels transduce physical (e.g. heat or cold) and chemical (e.g. endogenous lipids) stimuli in the peripheral nociceptive system [11,12,13].

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