Abstract

The long-term objectives of this project are to develop long-acting Na+ channel blockers pertinent for pain management and to gain a better understanding of how these blockers work mechanistically. Traditional local anesthetics (LAs) are often inept for chronic or intractable cancer pain due to their insufficient duration of nerve block.
Our specific aims are (1) to identify and synthesize compounds that potently block the open and/or inactivated Na+ channels, (2) to assess the use- and state-dependent block of potent Na+ channel blockers, (3) to test their in vivo potency as long-acting LAs, and (4) to map their receptor site within the Na+ channel alpha-subunit. Recent screening has identified several new lead structures that block open Na+ channels with high affinities. Earlier screening demonstrated that drugs taken orally for neuropathic pain, such as amitriptyline, flecainide, and mexiletine, also block open Na+ channels effectively at their therapeutic plasma concentrations. We hypothesize that these drugs alleviate ectopic high-frequency discharges found in injured nerves due to their high-affinity block of open Na+ channels. Amitriptyline, which too potently blocks the inactivated Na+ channels, indeed acts as a long-acting LA. We plan to identify and synthesize novel open and/or inactivated-channel blockers based on these lead structures. Their use-dependent block of Na+ currents during repetitive pulses and the 50% inhibitory concentration (IC50) of resting-, open-, and inactivated-channel block will be determined in wild-type and/or in inactivation-deficient mutant Na+ channels expressed in human HEK293 cells. Sensory and motor functions of nerve block will be evaluated in rats or sheep before and after injection of potent Na + channel blockers via various routes. Finally, we plan to delimit the receptor for selected blockers within the Na+ channel alpha-subunit by site-directed mutagenesis and by computer simulation of the ligand-receptor complex. This information will in turn facilitate receptor-based drug design. Together, these studies should provide us new lead structures for the development of long-acting LAs that selectively target open and/or inactivated Na+ channels. Such drugs, either taken orally or injected locally, may be beneficial for patients with chronic and intractable cancer pain.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM048090-13
Application #
6826554
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Program Officer
Cole, Alison E
Project Start
1992-08-01
Project End
2008-07-31
Budget Start
2004-08-01
Budget End
2005-07-31
Support Year
13
Fiscal Year
2004
Total Cost
$349,465
Indirect Cost

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
030811269
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Wang, Sho-Ya; Calderon, Joanna; Kuo Wang, Ging (2010) Block of neuronal Na+ channels by antidepressant duloxetine in a state-dependent manner. Anesthesiology 113:655-65
Wang, Ging Kuo; Calderon, Joanna; Jaw, Shiow-Jiin et al. (2009) State-dependent block of Na+ channels by articaine via the local anesthetic receptor. J Membr Biol 229:1-9
Wang, Chi-Fei; Gerner, Peter; Schmidt, Birgitta et al. (2008) Use of bulleyaconitine A as an adjuvant for prolonged cutaneous analgesia in the rat. Anesth Analg 107:1397-405
Gerner, Peter; Binshtok, Alexander M; Wang, Chi-Fei et al. (2008) Capsaicin combined with local anesthetics preferentially prolongs sensory/nociceptive block in rat sciatic nerve. Anesthesiology 109:872-8
Wang, Ging Kuo; Mitchell, Jane; Wang, Sho-Ya (2008) Block of persistent late Na+ currents by antidepressant sertraline and paroxetine. J Membr Biol 222:79-90
Wang, Ging Kuo; Calderon, Joanna; Wang, Sho-Ya (2008) State- and use-dependent block of muscle Nav1.4 and neuronal Nav1.7 voltage-gated Na+ channel isoforms by ranolazine. Mol Pharmacol 73:940-8
Wang, Sho-Ya; Mitchell, Jane; Wang, Ging Kuo (2007) Preferential block of inactivation-deficient Na+ currents by capsaicin reveals a non-TRPV1 receptor within the Na+ channel. Pain 127:73-83
Wang, Chi-Fei; Gerner, Peter; Wang, Sho-Ya et al. (2007) Bulleyaconitine A isolated from aconitum plant displays long-acting local anesthetic properties in vitro and in vivo. Anesthesiology 107:82-90
Wang, Sho-Ya; Tikhonov, Denis B; Mitchell, Jane et al. (2007) Irreversible block of cardiac mutant Na+ channels by batrachotoxin. Channels (Austin) 1:179-88
Wang, G K; Wang, S Y (1994) Modification of cloned brain Na+ channels by batrachotoxin. Pflugers Arch 427:309-16

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