Molecular Dissection of Subunit Interfaces in the Acetylcholine Receptor

Agonists and antagonists select between the αγ and αδ binding sites of the fetal muscle acetylcholine receptor owing to different contributions by the γ and δ subunits. To identify determinants of selectivity for agonists, we constructed a panel of γ-δ subunit chimeras, co-expressed them wit...

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Bibliographic Details
Published in:The Journal of biological chemistry 1996-10, Vol.271 (42), p.25770-25777
Main Authors: Prince, Richard J., Sine, Steven M.
Format: Article
Language:English
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Summary:Agonists and antagonists select between the αγ and αδ binding sites of the fetal muscle acetylcholine receptor owing to different contributions by the γ and δ subunits. To identify determinants of selectivity for agonists, we constructed a panel of γ-δ subunit chimeras, co-expressed them with the α subunit in 293 HEK cells, and measured carbamylcholine binding affinity of intracellular complexes. Wild-type αδ complexes bind carbamylcholine about 30-fold more tightly than αγ complexes. This degree of selectivity is similar to that of the resting state of the receptor determined by kinetic analysis of single-channel events. We identify a primary set of determinants of selectivity, Lys γ34 /Ser δ36 and Phe γ172 /Ile δ178 , and a secondary set, Glu γ57 /Asp δ59 and Cys γ115 /Tyr δ117 . The contributions of all four determinants are subunit-dependent and are modified by interaction with one another. Coexpression of point mutant subunits with complementary wild-type subunits to form cell surface pentamers shows that Lys γ34 /Ser δ36 and Phe γ172 /Ile δ178 contribute in a manner consistent with affecting selectivity of the resting state of the receptor, while Glu γ57 appears to contribute to the affinity of the desensitized state. The four determinants either coincide with or are close to residues known to contribute to the acetylcholine binding site. These results suggest that a minimum of four loops in the γ and δ subunits contribute to the agonist binding site.
ISSN:0021-9258
1083-351X
DOI:10.1074/jbc.271.42.25770