4.8 Article

Reconstitution of the augmin complex provides insights into its architecture and function

Journal

NATURE CELL BIOLOGY
Volume 16, Issue 9, Pages 852-863

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/ncb3030

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Funding

  1. National Institutes of Health (NIH) [1S10RR023748-01]
  2. National Institute of General Medical Sciences [9 P41 GM103310]
  3. Kimberly Lawrence-Netter Cancer Research Discovery Fund at The Rockefeller University
  4. Special Fellow Award from The Leukemia and Lymphoma Society
  5. NIH National Research Service Award Fellowship [F32GM099380]
  6. NIH [GM-052468, GM-65933]

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Proper microtubule nucleation during cell division requires augmin, a microtubule-associated hetero-octameric protein complex. In current models, augmin recruits y-tubulin, through the carboxyl terminus of its hDgt6 subunit to nucleate microtubules within spindles. However, augmin's biochemical complexity has restricted analysis of its structural organization and function. Here, we reconstitute human augmin and show that it is a Y-shaped complex that can adopt multiple conformations. Further, we find that a dimeric sub-complex retains in vitro microtubule-binding properties of octameric complexes, but not proper metaphase spindle localization. Addition of octameric augmin complexes to Xenopus egg extracts promotes microtubule aster formation, an activity enhanced by Ran-GTP. This activity requires microtubule binding, but not the characterized hDgt6 y-tubulin-recruitment domain. Tetrameric sub-complexes induce asters, but activity and microtubule bundling within asters are reduced compared with octameric complexes. Together, our findings shed light on augmin's structural organization and microtubule-binding properties, and define subunits required for its function in organizing microtubule-based structures.

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