Abstract

The overall goals of the proposed research are to understand how transmitter-gated membrane channels function and the mechanisms by which cells modulate the functional properties of these receptors. To reach these goals, it is necessary to determine the steps and rates in receptor activation, to determine the rates which are altered in cases in which function is altered, and to determine the likely structural basis for the changes. Further, physiological studies must be performed on cells which may be experimentally manipulated and on which biochemical studies may be done. Recent developments in eukaryotic gene expression allow generation of clonal lines which produce receptors of known subunit composition. These lines are ideal for biophysical, pharmacological and biochemical studies. The proposed work focusses on nicotinic acetylcholine receptors (AChR) which are the best studied representatives of an extended gene family which includes several other transmitter-gated channels. Biophysical methods will be used to study AChR function, biochemical methods to examine structure, and molecular biological methods to generate clonal cell lines. Our previous work has generated clonal cell lines which express mammalian adult and fetal muscle AChR. These cells provide an accessible system in which these receptors may be directly compared. Critical functional properties of these receptors will be determined, including the affinity of the receptor for acetylcholine and the intrinsic channel opening rate. The pharmacology of neuromuscular blocking agents on adult and fetal muscle AChR will then be examined. The work will be extended to examine modulation of adult muscle AChR. Neurons express structurally related nicotinic receptors, but studies of the physiology and pharmacology of these receptors have been hampered by the lack of stable sources of cells which express receptors of defined subunit composition. Therefore, the project proposes to generate stable clonal lines which express neuronal AChR and to use these cells to determine the physiological and pharmacological properties of the receptors. Further work will examine mechanisms for modulation of these neuronal receptors. Finally, the basis for the modulation of neuronal nicotinic AChR expressed by clonal PC12 cells will be determined. This work will provide precise information on the function of nicotinic acetylcholine receptors and on the mechanisms by which a cell can alter the functional properties of these receptors. This knowledge is required to understand both synaptic transmission and the actions of pharmacological agents, in normal and disease states. The understanding will provide insight into the mechanisms of blocking agents and the etiology of disease states involving nicotinic AChR, which are thought to include nicotine dependence and possibly Alzheimer's disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS022356-09
Application #
3404603
Study Section
Neurological Sciences Subcommittee 1 (NLS)
Project Start
1984-12-01
Project End
1996-11-30
Budget Start
1992-12-01
Budget End
1993-11-30
Support Year
9
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Type
Schools of Medicine
DUNS #
062761671
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Jin, Xiaochun; Germann, Allison L; Shin, Daniel J et al. (2017) Determination of the Residues in the Extracellular Domain of the Nicotinic ? Subunit Required for the Actions of Physostigmine on Neuronal Nicotinic Receptors. Mol Pharmacol 92:318-326
Jin, Xiaochun; McCollum, Megan M; Germann, Allison L et al. (2017) The E Loop of the Transmitter Binding Site Is a Key Determinant of the Modulatory Effects of Physostigmine on Neuronal Nicotinic ?4?2 Receptors. Mol Pharmacol 91:100-109
Bracamontes, John R; Akk, Gustav; Steinbach, Joe Henry (2016) Introduced Amino Terminal Epitopes Can Reduce Surface Expression of Neuronal Nicotinic Receptors. PLoS One 11:e0151071
Jin, Xiaochun; Steinbach, Joe Henry (2015) Potentiation of Neuronal Nicotinic Receptors by 17?-Estradiol: Roles of the Carboxy-Terminal and the Amino-Terminal Extracellular Domains. PLoS One 10:e0144631
Haller, Gabe; Li, Ping; Esch, Caroline et al. (2014) Functional characterization improves associations between rare non-synonymous variants in CHRNB4 and smoking behavior. PLoS One 9:e96753
Jin, Xiaochun; Bermudez, Isabel; Steinbach, Joe Henry (2014) The nicotinic ?5 subunit can replace either an acetylcholine-binding or nonbinding subunit in the ?4?2* neuronal nicotinic receptor. Mol Pharmacol 85:11-7
Akk, Gustav; Eaton, Megan; Li, Ping et al. (2013) Energetic contributions to channel gating of residues in the muscle nicotinic receptor ?1 subunit. PLoS One 8:e78539
Haller, Gabe; Druley, Todd; Vallania, Francesco L et al. (2012) Rare missense variants in CHRNB4 are associated with reduced risk of nicotine dependence. Hum Mol Genet 21:647-55
Tammimäki, Anne; Herder, Penelope; Li, Ping et al. (2012) Impact of human D398N single nucleotide polymorphism on intracellular calcium response mediated by ?3?4?5 nicotinic acetylcholine receptors. Neuropharmacology 63:1002-11
Hinrichs, Anthony L; Murphy, Sharon E; Wang, Jen C et al. (2011) Common polymorphisms in FMO1 are associated with nicotine dependence. Pharmacogenet Genomics 21:397-402

Showing the most recent 10 out of 54 publications