The Journal of Neuroscience, March 11, 2009, 29(10):3189-3199; doi:10.1523/JNEUROSCI.6185-08.2009
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Cellular/Molecular
Binding to Gating Transduction in Nicotinic Receptors: Cys-Loop Energetically Couples to Pre-M1 and M2–M3 Regions
Won Yong Lee,1,2
Chris R. Free,1,2 and
Steven M. Sine1,2,3
1Receptor Biology Laboratory and Departments of 2Physiology and Biomedical Engineering and 3Neurology, Mayo Clinic College of Medicine, Rochester, Minnesota 55905
Correspondence should be addressed to Steven M. Sine at the above address. Email: sine{at}mayo.edu
The nicotinic acetylcholine receptor (AChR) transduces binding of nerve-released ACh into opening of an intrinsic ion channel, yet the intraprotein interactions behind transduction remain to be fully elucidated. Attention has focused on the region of the AChR in which the β1–β2 and Cys-loops from the extracellular domain project into a cavity framed by residues preceding the first transmembrane domain (pre-M1) and the linker spanning transmembrane domains M2 and M3. Previous studies identified a principal transduction pathway in which the pre-M1 domain is coupled to the M2–M3 linker through the β1–β2 loop. Here we identify a parallel pathway in which the pre-M1 domain is coupled to the M2–M3 linker through the Cys-loop. Mutagenesis, single-channel kinetic analyses and thermodynamic mutant cycle analyses reveal energetic coupling among
Leu 210 from the pre-M1 domain,
Phe 135 and
Phe 137 from the Cys-loop, and
Leu 273 from the M2–M3 linker. Residues at equivalent positions of non-
-subunits show negligible coupling, indicating these interresidue couplings are specific to residues in the
-subunit. Thus, the extracellular β1–β2 and Cys-loops bridge the pre-M1 domain and M2–M3 linker to transduce agonist binding into channel gating.
Received Dec. 30, 2008;
revised Feb. 5, 2009;
accepted Feb. 6, 2009.
Correspondence should be addressed to Steven M. Sine at the above address. Email: sine{at}mayo.edu
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