AI Article Synopsis

  • Understanding how microtubules (MTs) are formed is crucial for grasping the structure of the cytoskeleton, with the γ-tubulin ring complex (γ-TuRC) being the key nucleator identified, though its exact mechanism remains unclear.
  • A novel single molecule assay was created to visualize how γ-TuRC nucleates MTs, showing that it has a strong affinity for γ-/αβ-tubulin, allowing for more efficient assembly compared to spontaneous nucleation, which needs more tubulin units.
  • The study found that factors like NME7, TPX2, and the activation domain of CDK5RAP2 help γ-TuRC in nucleation, while XMAP215 significantly boosts efficiency

Article Abstract

Determining how microtubules (MTs) are nucleated is essential for understanding how the cytoskeleton assembles. While the MT nucleator, γ-tubulin ring complex (γ-TuRC) has been identified, precisely how γ-TuRC nucleates a MT remains poorly understood. Here, we developed a single molecule assay to directly visualize nucleation of a MT from purified γ-TuRC. We reveal a high γ-/αβ-tubulin affinity, which facilitates assembly of a MT from γ-TuRC. Whereas spontaneous nucleation requires assembly of 8 αβ-tubulins, nucleation from γ-TuRC occurs efficiently with a cooperativity of 4 αβ-tubulin dimers. This is distinct from pre-assembled MT seeds, where a single dimer is sufficient to initiate growth. A computational model predicts our kinetic measurements and reveals the rate-limiting transition where laterally associated αβ-tubulins drive γ-TuRC into a closed conformation. NME7, TPX2, and the putative activation domain of CDK5RAP2 h γ-TuRC-mediated nucleation, while XMAP215 drastically increases the nucleation efficiency by strengthening the longitudinal γ-/αβ-tubulin interaction.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7338055PMC
http://dx.doi.org/10.7554/eLife.54253DOI Listing

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