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XB-ART-54372
J Cell Biol 2017 Nov 06;21611:3453-3462. doi: 10.1083/jcb.201705168.
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Regulation of mitotic spindle assembly factor NuMA by Importin-β.

Chang CC , Huang TL , Shimamoto Y , Tsai SY , Hsia KC .


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Ran-guanosine triphosphatase orchestrates mitotic spindle assembly by modulation of the interaction between Importin-α/-β and spindle assembly factors (SAFs). The inhibition of SAFs performed by importins needs to be done without much sequestration from abundant nuclear localization signal (NLS) -containing proteins. However, the molecular mechanisms that determine NLS-binding selectivity and that inhibit activity of Importin-β-regulated SAFs (e.g., nuclear mitotic apparatus protein [NuMA]) remain undefined. Here, we present a crystal structure of the Importin-α-NuMA C terminus complex showing a novel binding pattern that accounts for selective NLS recognition. We demonstrate that, in the presence of Importin-α, Importin-β inhibits the microtubule-binding function of NuMA. Further, we have identified a high-affinity microtubule-binding region that lies carboxyl-terminal to the NLS, which is sterically masked by Importin-β on being bound by Importin-α. Our study provides mechanistic evidence of how Importin-α/-β regulates the NuMA functioning required for assembly of higher-order microtubule structures, further illuminating how Ran-governed transport factors regulate diverse SAFs and accommodate various cell demands.

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Species referenced: Xenopus
Genes referenced: numa1 ran tpx2


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References [+] :
Brünger, Crystallography & NMR system: A new software suite for macromolecular structure determination. 1998, Pubmed