Abstract

The overall objective of the research program is to understand how the structure and function of membrane-spanning channels is determined by their amino acid sequence and the properties of the host bilayer. The proposed experiments will examine these problems using a family of prototypical channel-formers, the linear gramicidins. This system offers several advantages: there is a considerable amount of structural information to guide the experimental design; the channel-forming molecules are modified using peptide chemical methods, which allows the convenient introduction of non-genetic amino acids; and it is possible to obtain structural information about channels formed by sequence-modified gramicidins by making use of the inherent resolution of single-channel measurements. The experiments will address the following questions: what are the determinants of channel folding and membrane insertion; what are the energetics of peptide interactions in a membrane; specifically, what are the determinants of the voltage-dependent gating seen in asymmetrical gramicidin channels; what are the determinants of the channels' permeability characteristics; and how is channel function modulated by the chemical composition and physico-chemical properties of the host bilayer? These questions will be examined in single-channel experiments. The amplitude of the current transitions will be used to characterize the channels' catalytic efficiency. the formation of heterodimer (hybrid) channels and their stability and appearance rate relative to the homodimeric channels will be used to elucidate the structural questions.
The aim i s to understand how a """"""""simple"""""""" channel functions: how the anisotropic membrane environment and the primary amino acid sequence interact in determining the channel structure; how a """"""""stress"""""""" introduced by sequence modifications affect the structure; specifically, how relatively modest sequence alterations can introduce voltage control into the channels; how the rate of ion movement is determined by the channel structure and the amino acid sequence; and how alterations in the host bilayer alter channel function, in particular whether alterations in a bilayer's mechanical properties can alter the equilibrium distribution among different channel states.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM021342-18
Application #
3270412
Study Section
Physiology Study Section (PHY)
Project Start
1977-06-01
Project End
1995-06-30
Budget Start
1991-07-01
Budget End
1992-06-30
Support Year
18
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Weill Medical College of Cornell University
Department
Type
Schools of Medicine
DUNS #
201373169
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Dockendorff, Chris; Gandhi, Disha M; Kimball, Ian H et al. (2018) Synthetic Analogues of the Snail Toxin 6-Bromo-2-mercaptotryptamine Dimer (BrMT) Reveal That Lipid Bilayer Perturbation Does Not Underlie Its Modulation of Voltage-Gated Potassium Channels. Biochemistry 57:2733-2743
Zhang, Mike; Peyear, Thasin; Patmanidis, Ilias et al. (2018) Fluorinated Alcohols' Effects on Lipid Bilayer Properties. Biophys J 115:679-689
Posson, David J; Rusinova, Radda; Andersen, Olaf S et al. (2018) Stopped-Flow Fluorometric Ion Flux Assay for Ligand-Gated Ion Channel Studies. Methods Mol Biol 1684:223-235
Herold, Karl F; Andersen, Olaf S; Hemmings Jr, Hugh C (2017) Divergent effects of anesthetics on lipid bilayer properties and sodium channel function. Eur Biophys J 46:617-626
Beaven, Andrew H; Maer, Andreia M; Sodt, Alexander J et al. (2017) Gramicidin A Channel Formation Induces Local Lipid Redistribution I: Experiment and Simulation. Biophys J 112:1185-1197
Beaven, Andrew H; Sodt, Alexander J; Pastor, Richard W et al. (2017) Characterizing Residue-Bilayer Interactions Using Gramicidin A as a Scaffold and Tryptophan Substitutions as Probes. J Chem Theory Comput 13:5054-5064
O'Donnell, John P; Cooley, Richard B; Kelly, Carolyn M et al. (2017) Timing and Reset Mechanism of GTP Hydrolysis-Driven Conformational Changes of Atlastin. Structure 25:997-1010.e4
Herold, Karl F; Sanford, R Lea; Lee, William et al. (2017) Clinical concentrations of chemically diverse general anesthetics minimally affect lipid bilayer properties. Proc Natl Acad Sci U S A 114:3109-3114
Menny, Anaïs; Lefebvre, Solène N; Schmidpeter, Philipp Am et al. (2017) Identification of a pre-active conformation of a pentameric channel receptor. Elife 6:
Sodt, Alexander J; Beaven, Andrew H; Andersen, Olaf S et al. (2017) Gramicidin A Channel Formation Induces Local Lipid Redistribution II: A 3D Continuum Elastic Model. Biophys J 112:1198-1213

Showing the most recent 10 out of 109 publications