Literature DB >> 18945901

A cation-pi interaction in the binding site of the glycine receptor is mediated by a phenylalanine residue.

Stephan A Pless1, Kat S Millen, Ariele P Hanek, Joseph W Lynch, Henry A Lester, Sarah C R Lummis, Dennis A Dougherty.   

Abstract

Cys-loop receptor binding sites characteristically contain many aromatic amino acids. In nicotinic ACh and 5-HT3 receptors, a Trp residue forms a cation-pi interaction with the agonist, whereas in GABA(A) receptors, a Tyr performs this role. The glycine receptor binding site, however, contains predominantly Phe residues. Homology models suggest that two of these Phe side chains, Phe159 and Phe207, and possibly a third, Phe63, are positioned such that they could contribute to a cation-pi interaction with the primary amine of glycine. Here, we test this hypothesis by incorporation of a series of fluorinated Phe derivatives using unnatural amino acid mutagenesis. The data reveal a clear correlation between the glycine EC(50) value and the cation-pi binding ability of the fluorinated Phe derivatives at position 159, but not at positions 207 or 63, indicating a single cation-pi interaction between glycine and Phe159. The data thus provide an anchor point for locating glycine in its binding site, and demonstrate for the first time a cation-pi interaction between Phe and a neurotransmitter.

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Year:  2008        PMID: 18945901      PMCID: PMC2649377          DOI: 10.1523/JNEUROSCI.2540-08.2008

Source DB:  PubMed          Journal:  J Neurosci        ISSN: 0270-6474            Impact factor:   6.167


  32 in total

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  36 in total

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Authors:  Stephan A Pless; Lucia G Sivilotti
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3.  Ligand-specific conformational changes in the alpha1 glycine receptor ligand-binding domain.

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4.  The aromatic ring of phenylalanine 334 is essential for oligomerization of Vibrio vulnificus hemolysin.

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7.  A cation-π interaction at a phenylalanine residue in the glycine receptor binding site is conserved for different agonists.

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Review 8.  Incorporation of Non-Canonical Amino Acids.

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