Abstract

The permeation pathway of the voltage-gated Na/+ channel encompasses a selectivity filter, and an activation gate. Upon binding, local anesthetics (LAs) block this permeation pathway whereas batrachotoxin (BTX) alters ion selectivity and causes persistent Na/+ channel opening. Our long-term objectives are (1) to understand better the structure/function relationship of receptor sites for LAs and for BTX in the alpha-subunit of the voltage gated Na/+ channel and (2) to explore the interplay among the LA receptor, the BTX receptor, and the Na/+ permeation pathway. Such information will be beneficial for the design of therapeutic drugs. Two hypotheses will be tested: first, the receptors for LAs and for BTX change their conformations during state transitions and second, the LA receptor and the BTX receptor align in close proximity to each other within the Na/+ permeation pathway. Specifically, we will examine the structural basis of the static-ligand receptor interactions in the rat skeletal muscle Na/+ channel (SKM1), the successive changes in receptor sites during state transitions, and the functional roles of these receptors within the permeation pathway. Site-directed mutagenesis will be used to create mutants with point mutations at these two separate ligand binding sites. These mutants will be transiently expressed in human embryonic kidney cells. Both whole-cell and single-channel currents will be measured in order to obtain detailed kinetic information on the dynamic interactions between Na/+ channels and these ligands. A substituted- cysteine accessibility method will be used to scan the regions within or near the ligand binding sites that may change conformations during state transitions. Finally, the ion selected mutants will be examined to reveal the putative interactions between the selectivity locus and the receptors. Together, these studies should provide a better understanding of how BTX and LAs modulate the Na/+ permeation pathway at the molecular level as well as a clearer view of the dynamic interactions between these ligands and the alpha-subunit Na/+ channel.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM035401-16
Application #
6476463
Study Section
Cellular Biology and Physiology Subcommittee 1 (CBY)
Program Officer
Cole, Alison E
Project Start
1985-09-06
Project End
2003-11-30
Budget Start
2001-12-01
Budget End
2003-11-30
Support Year
16
Fiscal Year
2002
Total Cost
$387,089
Indirect Cost

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
071723621
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Xiao, Yong-Fu; Ke, Qingen; Wang, Sho-Ya et al. (2004) Electrophysiologic properties of lidocaine, cocaine, and n-3 fatty-acids block of cardiac Na+ channels. Eur J Pharmacol 485:31-41
Sudoh, Yukari; Desai, Sukumar P; Haderer, Anna E et al. (2004) Neurologic and histopathologic evaluation after high-volume intrathecal amitriptyline. Reg Anesth Pain Med 29:434-40
Nau, Carla; Wang, Sho-Ya; Wang, Ging Kuo (2003) Point mutations at L1280 in Nav1.4 channel D3-S6 modulate binding affinity and stereoselectivity of bupivacaine enantiomers. Mol Pharmacol 63:1398-406
O'Reilly, J P; Wang, S Y; Wang, G K (2003) Methanethiosulfonate-modification alters local anesthetic block in rNav1.4 cysteine-substituted mutants S1276C and L1280C. J Membr Biol 193:47-55
Wang, Ging Kuo; Wang, Sho-Ya (2003) Veratridine block of rat skeletal muscle Nav1.4 sodium channels in the inner vestibule. J Physiol 548:667-75
Sudoh, Yukari; Cahoon, Elaine Elliott; Gerner, Peter et al. (2003) Tricyclic antidepressants as long-acting local anesthetics. Pain 103:49-55
Wang, G K; Wang, S Y (2002) Modifications of human cardiac sodium channel gating by UVA light. J Membr Biol 189:153-65
Xiao, Y F; Ke, Q; Wang, S Y et al. (2001) Point mutations in alpha-subunit of human cardiac Na+ channels alter Na+ current kinetics. Biochem Biophys Res Commun 281:45-52
Xiao, Y F; Ke, Q; Wang, S Y et al. (2001) Single point mutations affect fatty acid block of human myocardial sodium channel alpha subunit Na+ channels. Proc Natl Acad Sci U S A 98:3606-11
Wang, S Y; Barile, M; Wang, G K (2001) A phenylalanine residue at segment D3-S6 in Nav1.4 voltage-gated Na(+) channels is critical for pyrethroid action. Mol Pharmacol 60:620-8

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