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Long distance effect on ligand-gated ion channels extracellular domain may affect interactions with the intracellular machinery

机译:对配体门控离子通道细胞外结构域的长距离影响可能影响与细胞内机制的相互作用

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摘要

Modulation of receptor trafficking is critical for controlling neurotransmission. A γ2(R43Q) point mutation on GABAA receptor subunit is linked to epilepsy in human. We recently analyzed the effect of this amino-acid substitution on GABAA receptor trafficking and showed that this mutation as well as agonist application, both affecting GABAA receptor extracellular domain, have an effect on receptor endocytosis. By comparing homology models based on ligand gated ion channels in their active and resting states, we reveal that the γ2R43 domain is located in a loop that is affected by motion resulting from receptor activation. Taken together, these results suggest that endocytosis of GABAA receptors is linked to agonist induced conformational changes. We propose that ligand or modulator binding is followed by a whole chain of interconnections, including the intracellular domain, that may influence ligand-gated channel trafficking.
机译:受体运输的调节对于控制神经传递至关重要。 GABAA受体亚基上的γ2(R43Q)点突变与人的癫痫病有关。我们最近分析了这种氨基酸取代对GABAA受体运输的影响,并表明这种突变以及激动剂的应用均影响GABAA受体胞外域,对受体的内吞作用有影响。通过比较基于在活性和静止状态下的配体门控离子通道的同源性模型,我们揭示了γ2R43结构域位于一个受受体激活运动影响的环中。综上所述,这些结果表明,GABAA受体的内吞作用与激动剂诱导的构象变化有关。我们提出,配体或调节剂结合后是整个互连链,包括可能影响配体门控通道运输的细胞内结构域。

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