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Control of AMPA receptor activity by the extracellular loops of auxiliary proteins.


ABSTRACT: At synapses throughout the mammalian brain, AMPA receptors form complexes with auxiliary proteins, including TARPs. However, how TARPs modulate AMPA receptor gating remains poorly understood. We built structural models of TARP-AMPA receptor complexes for TARPs ?2 and ?8, combining recent structural studies and de novo structure predictions. These models, combined with peptide binding assays, provide evidence for multiple interactions between GluA2 and variable extracellular loops of TARPs. Substitutions and deletions of these loops had surprisingly rich effects on the kinetics of glutamate-activated currents, without any effect on assembly. Critically, by altering the two interacting loops of ?2 and ?8, we could entirely remove all allosteric modulation of GluA2, without affecting formation of AMPA receptor-TARP complexes. Likewise, substitutions in the linker domains of GluA2 completely removed any effect of ?2 on receptor kinetics, indicating a dominant role for this previously overlooked site proximal to the AMPA receptor channel gate.

SUBMITTER: Riva I 

PROVIDER: S-EPMC5599240 | biostudies-literature | 2017 Aug

REPOSITORIES: biostudies-literature

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Control of AMPA receptor activity by the extracellular loops of auxiliary proteins.

Riva Irene I   Eibl Clarissa C   Volkmer Rudolf R   Carbone Anna L AL   Plested Andrew Jr AJ  

eLife 20170830


At synapses throughout the mammalian brain, AMPA receptors form complexes with auxiliary proteins, including TARPs. However, how TARPs modulate AMPA receptor gating remains poorly understood. We built structural models of TARP-AMPA receptor complexes for TARPs γ2 and γ8, combining recent structural studies and de novo structure predictions. These models, combined with peptide binding assays, provide evidence for multiple interactions between GluA2 and variable extracellular loops of TARPs. Subst  ...[more]

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