4.5 Article

Trafficking and potential assembly patterns of ε-containing GABAA receptors

Journal

JOURNAL OF NEUROCHEMISTRY
Volume 103, Issue 3, Pages 1258-1271

Publisher

WILEY
DOI: 10.1111/j.1471-4159.2007.04833.x

Keywords

chimera; epsilon; GABA(A) receptor; stoichiometry; trafficking

Funding

  1. NIDA NIH HHS [DA14137] Funding Source: Medline

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Incorporation of the epsilon subunit into the GABA(A) receptor has been suggested to confer unusual, but variable, biophysical and pharmacological characteristics to both recombinant and native receptors. Due to their structural similarity with the gamma subunits, epsilon subunits have been assumed to substitute at the single position of the gamma subunit in assembled receptors. However, prior work suggests that functional variability in epsilon-containing receptors may reflect alternative sites of incorporation and of not just one, but possibly multiple epsilon subunits in the pentameric receptor complex. Here we present data indicating that increased expression of epsilon, in conjunction with alpha(2) and beta(3) subunits, results in expression of GABA(A) receptors with correspondingly altered rectification, deactivation and levels of spontaneous openings, but not increased total current density. We also provide data that the epsilon subunit, like the beta(3) subunit, can self-export and data from chimeric receptors suggesting that similarities between the assembly domains of the beta(3) and the epsilon subunits may allow the epsilon subunit to replace the beta, as well as the gamma, subunit. The substitution of an epsilon for a beta, as well as the gamma subunit and formation of receptors with alternative patterns of assembly with respect to epsilon incorporation may underlie the observed variability in both biophysical and pharmacological properties noted not only in recombinant, but also in native receptors.

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