PLoS ONE (Jan 2012)

14-3-3θ is a binding partner of rat Eag1 potassium channels.

  • Po-Hao Hsu,
  • Shi-Chuen Miaw,
  • Chau-Ching Chuang,
  • Pei-Yu Chang,
  • Ssu-Ju Fu,
  • Guey-Mei Jow,
  • Mei-Miao Chiu,
  • Chung-Jiuan Jeng

DOI
https://doi.org/10.1371/journal.pone.0041203
Journal volume & issue
Vol. 7, no. 7
p. e41203

Abstract

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The ether-à-go-go (Eag) potassium (K(+)) channel belongs to the superfamily of voltage-gated K(+) channel. In mammals, the expression of Eag channels is neuron-specific but their neurophysiological role remains obscure. We have applied the yeast two-hybrid screening system to identify rat Eag1 (rEag1)-interacting proteins from a rat brain cDNA library. One of the clones we identified was 14-3-3θ, which belongs to a family of small acidic protein abundantly expressed in the brain. Data from in vitro yeast two-hybrid and GST pull-down assays suggested that the direct association with 14-3-3θ was mediated by both the N- and the C-termini of rEag1. Co-precipitation of the two proteins was confirmed in both heterologous HEK293T cells and native hippocampal neurons. Electrophysiological studies showed that over-expression of 14-3-3θ led to a sizable suppression of rEag1 K(+) currents with no apparent alteration of the steady-state voltage dependence and gating kinetics. Furthermore, co-expression with 14-3-3θ failed to affect the total protein level, membrane trafficking, and single channel conductance of rEag1, implying that 14-3-3θ binding may render a fraction of the channel locked in a non-conducting state. Together these data suggest that 14-3-3θ is a binding partner of rEag1 and may modulate the functional expression of the K(+) channel in neurons.