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Microtubule association induces a Mg-free apo-like ADP pre-release conformation in kinesin-1 that is unaffected by its autoinhibitory tail

Nature Communications. 2025-07; 
J Atherton, M S Chegkazi, M Leusciatti, M Di Palma, E Peirano, L S Pozzer, M V A Meli, S Pasqualato, T Foran, G Morra, R A Steiner Randall Centre for Cell and Molecular Biophysics, King's College London - New Hunt's House, Guy's Campus, London, UK.
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Mammalian Expression and CC1 (residues 1–357) fused via a flexible (Thr-Gly-Ser)9 linker to the C-terminal tail region encompassing the autoinhibitory IAK motif (residues 912–935) was purchased from Genscript Get A Quote

摘要

Kinesin-1 is a processive dimeric ATP-driven motor that transports vital intracellular cargos along microtubules (MTs). If not engaged in active transport, kinesin-1 limits futile ATP hydrolysis by adopting a compact autoinhibited conformation that involves an interaction between its C-terminal tail and the N-terminal motor domains. Here, using a chimeric kinesin-1 that fuses the N-terminal motor region to the tail and a tail variant unable to interact with the motors, we employ cryo-EM to investigate elements of the MT-associated mechanochemical cycle. We describe a missing structure for the proposed two-step allosteric mechanism of ADP release, the ATPase rate limiting step. It shows that MT association remod... More

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