Coapplication of Lidocaine and the Permanently Charged Sodium Channel Blocker QX-314 Produces a Long-lasting Nociceptive Blockade in Rodents

Author:

Binshtok Alexander M.1,Gerner Peter2,Oh Seog Bae3,Puopolo Michelino4,Suzuki Suzuko5,Roberson David P.6,Herbert Teri7,Wang Chi-Fei6,Kim Donghoon8,Chung Gehoon9,Mitani Aya A.10,Wang Ging Kuo11,Bean Bruce P.12,Woolf Clifford J.13

Affiliation:

1. Instructor in Anesthesia.

2. Assistant Professor.

3. Associate Professor.

4. Instructor in Neurobiology.

5. Research Fellow.

6. Graduate Fellow.

7. Research Technician.

8. Doctoral Candidate, Department of Physiology, School of Dentistry, Seoul National University, Seoul, Korea.

9. Doctoral Candidate, National Research Laboratory for Pain and Dental Research Institute, Department of Physiology, School of Dentistry, Seoul National University, Seoul, Korea.

10. Biostatistician.

11. Associate Professor, Department of Anesthesiology, Perioperative, and Pain Medicine, Brigham and Women’s Hospital and Harvard Medical School, Boston, Massachusetts.

12. Professor, Department of Neurobiology, Harvard Medical School, Boston, Massachusetts.

13. Professor, Department of Anesthesia and Critical Care, Massachusetts General Hospital and Harvard Medical School, Charlestown, Massachusetts.

Abstract

Background Nociceptive-selective local anesthesia is produced by entry of the permanently charged lidocaine-derivative QX-314 into nociceptors when coadministered with capsaicin, a transient receptor potential vanilloid 1 (TRPV1) channel agonist. However, the pain evoked by capsaicin before establishment of the QX-314-mediated block would limit clinical utility. Because TRPV1 channels are also activated by lidocaine, the authors tested whether lidocaine can substitute for capsaicin to introduce QX-314 into nociceptors through TRPV1 channels and produce selective analgesia. Methods Lidocaine (0.5% [17.5 mM], 1% [35 mM], and 2% [70 mM]) alone, QX-314 (0.2% [5.8 mM]) alone, and a combination of the two were injected subcutaneously and adjacent to the sciatic nerve in rats and mice. Mechanical and thermal responsiveness were measured, as was motor block. Results Coapplication of 0.2% QX-314 with lidocaine prolonged the nociceptive block relative to lidocaine alone, an effect attenuated in TRPV1 knockout mice. The 0.2% QX-314 alone had no effect when injected intraplantary or perineurally, and it produced only weak short-lasting inhibition of the cutaneous trunci muscle reflex. Perisciatic nerve injection of lidocaine with QX-314 produced a differential nociceptive block much longer than the transient motor block, lasting 2 h (for 1% lidocaine) to 9 h (2% lidocaine). Triple application of lidocaine, QX-314, and capsaicin further increased the duration of the differential block. Conclusions Coapplication of lidocaine and its quaternary derivative QX-314 produces a long-lasting, predominantly nociceptor-selective block, likely by facilitating QX-314 entry through TRPV1 channels. Delivery of QX-314 into nociceptors by using lidocaine instead of capsaicin produces sustained regional analgesia without nocifensive behavior.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Anesthesiology and Pain Medicine

Reference36 articles.

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