The nucleoporin MEL-28 promotes RanGTP-dependent γ-tubulin recruitment and microtubule nucleation in mitotic spindle formation

The GTP-bound form of the Ran GTPase (RanGTP), produced around chromosomes, drives nuclear envelope and nuclear pore complex (NPC) re-assembly after mitosis. The nucleoporin MEL-28/ELYS binds chromatin in a RanGTP-regulated manner and acts to seed NPC assembly. Here we show that, upon mitotic NPC di...

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Veröffentlicht in:Nature communications 2014, Vol.5 (1), p.3270-3270, Article 3270
Hauptverfasser: Yokoyama, Hideki, Koch, Birgit, Walczak, Rudolf, Ciray-Duygu, Fulya, González-Sánchez, Juan Carlos, Devos, Damien P., Mattaj, Iain W., Gruss, Oliver J.
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Sprache:eng
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Zusammenfassung:The GTP-bound form of the Ran GTPase (RanGTP), produced around chromosomes, drives nuclear envelope and nuclear pore complex (NPC) re-assembly after mitosis. The nucleoporin MEL-28/ELYS binds chromatin in a RanGTP-regulated manner and acts to seed NPC assembly. Here we show that, upon mitotic NPC disassembly, MEL-28 dissociates from chromatin and re-localizes to spindle microtubules and kinetochores. MEL-28 directly binds microtubules in a RanGTP-regulated way via its C-terminal chromatin-binding domain. Using Xenopus egg extracts, we demonstrate that MEL-28 is essential for RanGTP-dependent microtubule nucleation and spindle assembly, independent of its function in NPC assembly. Specifically, MEL-28 interacts with the γ-tubulin ring complex and recruits it to microtubule nucleation sites. Our data identify MEL-28 as a RanGTP target that functions throughout the cell cycle. Its cell cycle-dependent binding to chromatin or microtubules discriminates MEL-28 functions in interphase and mitosis, and ensures that spindle assembly occurs only after NPC breakdown. On mitotic exit, the nucleoporin MEL-28 binds to chromatin and seeds the formation of nuclear pore complexes. Here Yokoyama et al. show that upon mitotic entry, MEL-28 re-localizes to microtubules where it functions in assembling the mitotic spindle, revealing roles for MEL-28 throughout the cell cycle.
ISSN:2041-1723
2041-1723
DOI:10.1038/ncomms4270