During mitosis, microtubule dynamics are regulated to ensure proper alignment and segregation of chromosomes. The dynamics of kinetochore-attached microtubules are regulated by hepatoma-upregulated protein (HURP) and the mitotic kinesin-8 Kif18A, but the underlying mechanism remains elusive. Using single-molecule imaging , we demonstrate that Kif18A motility is regulated by HURP. While sparse decoration of HURP activates the motor, higher concentrations hinder processive motility. To shed light on this behavior, we determined the binding mode of HURP to microtubules using Cryo-EM. The structure reveals that one HURP motif spans laterally across β-tubulin, while a second motif binds between adjacent protofilaments. HURP partially overlaps with the microtubule-binding site of the Kif18A motor domain, indicating that excess HURP inhibits Kif18A motility by steric exclusion. We also observed that HURP and Kif18A function together to suppress dynamics of the microtubule plus-end, providing a mechanistic basis for how they collectively serve in spindle length control.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11030443PMC
http://dx.doi.org/10.1101/2024.04.11.589088DOI Listing

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Article Synopsis
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  • HURP stabilizes the microtubule structure and shifts its function toward facilitating branching by localizing to TPX2 condensates, which are crucial for spindle assembly, supported by high-resolution cryo-EM imaging of HURP on microtubules.
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