Literature DB >> 35229716

Coil-to-α-helix transition at the Nup358-BicD2 interface activates BicD2 for dynein recruitment.

James M Gibson1, Heying Cui2, M Yusuf Ali3, Xiaoxin Zhao2, Erik W Debler4, Jing Zhao1, Kathleen M Trybus3, Sozanne R Solmaz2, Chunyu Wang1.   

Abstract

Nup358, a protein of the nuclear pore complex, facilitates a nuclear positioning pathway that is essential for many biological processes, including neuromuscular and brain development. Nup358 interacts with the dynein adaptor Bicaudal D2 (BicD2), which in turn recruits the dynein machinery to position the nucleus. However, the molecular mechanisms of the Nup358/BicD2 interaction and the activation of transport remain poorly understood. Here for the first time, we show that a minimal Nup358 domain activates dynein/dynactin/BicD2 for processive motility on microtubules. Using nuclear magnetic resonance titration and chemical exchange saturation transfer, mutagenesis, and circular dichroism spectroscopy, a Nup358 α-helix encompassing residues 2162-2184 was identified, which transitioned from a random coil to an α-helical conformation upon BicD2 binding and formed the core of the Nup358-BicD2 interface. Mutations in this region of Nup358 decreased the Nup358/BicD2 interaction, resulting in decreased dynein recruitment and impaired motility. BicD2 thus recognizes Nup358 through a 'cargo recognition α-helix,' a structural feature that may stabilize BicD2 in its activated state and promote processive dynein motility.
© 2022, Gibson et al.

Entities:  

Keywords:  BicD2; NMR; TIRF; bidirectional transport; dynein; molecular biophysics; none; nuclear positioning; structural biology

Mesh:

Substances:

Year:  2022        PMID: 35229716      PMCID: PMC8956292          DOI: 10.7554/eLife.74714

Source DB:  PubMed          Journal:  Elife        ISSN: 2050-084X            Impact factor:   8.713


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