The Journal of Membrane Biology

, Volume 170, Issue 2, pp 157–164

Alteration in Ion Channel Function of Mouse Nicotinic Acetylcholine Receptor by Mutations in the M4 Transmembrane Domain

  • S.  Tamamizu
  • Y.-H.  Lee
  • B.  Hung
  • M.G.  McNamee
  • J.A.  Lasalde-Dominicci

DOI: 10.1007/s002329900545

Cite this article as:
Tamamizu, S., Lee, YH., Hung, B. et al. J. Membrane Biol. (1999) 170: 157. doi:10.1007/s002329900545

Abstract.

The effect of structural alterations of the M4 transmembrane segment in the Torpedo californica AChR has shown that substitution of specific residues can be critical to the channel gating (Lasalde et al., 1996). In a previous study we found that phenylalanine and tryptophan substitutions at the αC418 residue in the M4 transmembrane segment of the Torpedo californica AChR significantly altered ion channel function (Lee et al., 1994; Ortiz-Miranda et al., 1997). Cassette mutagenesis was used to mutate the Cys residue at the corresponding C418 position in the α subunit of mouse AChR. A total of nine mutations on the mouse αC418 position were tested, including the αC418A, αC418V, αC418L, αC418S, αC418M, αC418W, αC418H, αC418E and αC418G mutants. All the mutants tested were functional except the αC418G which was not expressed on the surface of the oocyte. The data obtained from macroscopic and single channel currents demonstrate that different types of amino acids can be accommodated at this presumably lipid-exposed position without loss of ion-channel function. As with the Torpedo AChR, the mutation of Cys to Trp dramatically decreased the EC50 for acetylcholine and increased channel open time. The lack of expression of the mouse αC418G suggest that there are some differences in folding, oligomerization and perhaps transport to the surface membrane for this mutant between the Torpedo and the mammalian AChR.

Key words:Torpedo californica— Cassette mutagenesis — Single channel electrophysiology — Ion channel gating

Copyright information

© 1999 Springer-Verlag New York Inc.

Authors and Affiliations

  • S.  Tamamizu
    • 1
  • Y.-H.  Lee
    • 1
  • B.  Hung
    • 1
  • M.G.  McNamee
    • 1
  • J.A.  Lasalde-Dominicci
    • 2
  1. 1.Section of Molecular and Cellular Biology, University of California, Davis CA 95616, USAUS
  2. 2.University of Puerto Rico, Department of Biology, PO Box 23360, San Juan, Puerto Rico 00931-3360, USAUS