Abstract

We propose to determine the three-dimensional architecture of the outer vestibule/pore region of the rat skeletal muscle subtype 1 (rSkM1) voltage-sensitive sodium channel. To accomplish this we will use mu- conotoxin GIIIA, the three-dimensional structure of which is known, as a molecular caliper to map out the position of channel residues on the extracellular surface of rSkM1. We will achieve this goal by several types of experiments. first, we will determine the residues on the channel surface that interact with the toxin. this will be accomplished by constructing and analyzing chimeric and site-specifically mutated channels and measuring the effects of these changes on wild-type (WT) toxin affinity. Second, we will mutate the toxin and measure the affinities of mutant toxins on the wild-type and mutant channels. From these thermodynamic measurements, mutant cycles can be constructed that reflect the interaction between a site on the channel and one in the toxin. If there is not interaction between two mutated sites, one in toxin and the other in rSkM1, the degree of interaction or coupling energy is zero (coupling coefficient of unity). Non-unity coupling coefficients enable the assignment of pairwise interactions. Using the toxin as a molecular caliper and electrostatic compliance measurements, estimates will be obtained for the distance between the two sites. Third, we will use di-cysteine substituted channels to form cross-links by oxidation (-SS-) or Me 2+ chelation and assess the effects on channel function including toxin binding. Positive results indicate proximal side chains and place distance constraints between these residues. Triangulation using a set of distance measurements will define the spatial arrangement of channel amino acids. Computer models of the rSkM1 external vestibule will be constructed and tested by further mutant cycle analysis. In the long-term, from the surface architecture, synthetic molecules will be designed as new candidate drugs that modify channel function.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR041762-08
Application #
6328837
Study Section
Physiology Study Section (PHY)
Program Officer
Lymn, Richard W
Project Start
1992-09-01
Project End
2002-11-30
Budget Start
2000-12-01
Budget End
2001-11-30
Support Year
8
Fiscal Year
2001
Total Cost
$284,642
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Biochemistry
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Ma, Zhongming; Kong, Jun; Kallen, Roland G (2009) Studies of alpha-helicity and intersegmental interactions in voltage-gated Na+ channels: S2D4. PLoS One 4:e7674
Zhang, H; Kolibal, S; Vanderkooi, J M et al. (2000) A carboxy-terminal alpha-helical segment in the rat skeletal muscle voltage-dependent Na+ channel is responsible for its interaction with the amino-terminus. Biochim Biophys Acta 1467:406-18
O'Reilly, J P; Wang, S Y; Kallen, R G et al. (1999) Comparison of slow inactivation in human heart and rat skeletal muscle Na+ channel chimaeras. J Physiol 515 ( Pt 1):61-73
Chahine, M; Sirois, J; Marcotte, P et al. (1998) Extrapore residues of the S5-S6 loop of domain 2 of the voltage-gated skeletal muscle sodium channel (rSkM1) contribute to the mu-conotoxin GIIIA binding site. Biophys J 75:236-46
Tang, L; Chehab, N; Wieland, S J et al. (1998) Glutamine substitution at alanine1649 in the S4-S5 cytoplasmic loop of domain 4 removes the voltage sensitivity of fast inactivation in the human heart sodium channel. J Gen Physiol 111:639-52
Wolska, B M; Averyhart-Fullard, V; Omachi, A et al. (1997) Changes in thyroid state affect pHi and Nai+ homeostasis in rat ventricular myocytes. J Mol Cell Cardiol 29:2653-63
Frohnwieser, B; Chen, L Q; Schreibmayer, W et al. (1997) Modulation of the human cardiac sodium channel alpha-subunit by cAMP-dependent protein kinase and the responsible sequence domain. J Physiol 498 ( Pt 2):309-18
Chahine, M; Deschenes, I; Trottier, E et al. (1997) Restoration of fast inactivation in an inactivation-defective human heart sodium channel by the cysteine modifying reagent benzyl-MTS: analysis of IFM-ICM mutation. Biochem Biophys Res Commun 233:606-10
Benzinger, G R; Drum, C L; Chen, L Q et al. (1997) Differences in the binding sites of two site-3 sodium channel toxins. Pflugers Arch 434:742-9
Marcotte, P; Chen, L Q; Kallen, R G et al. (1997) Effects of Tityus serrulatus scorpion toxin gamma on voltage-gated Na+ channels. Circ Res 80:363-9

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