Potential Phosphorylation Site Modulates The Dimerization and Activity of KIF1A
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Huazhong University of Science and Technology,Institute of Biophysics, Chinese Academy of Sciences,Institute of Biophysics, Chinese Academy of Sciences,Institute of Biophysics, Chinese Academy of Sciences,Institute of Biophysics, Chinese Academy of Sciences,Institute of Biophysics, Chinese Academy of Sciences,Institute of Biophysics, Chinese Academy of Sciences

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This work was supported by grants from The National Basic Research Program of China (2010CB833701, 2011CB910503, 2014CB910202) and The National Natural Science Foundation of China (31130065, 31300611, 31190062, 31200577)

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    Abstract:

    Kinesin-3 KIF1A is responsible for the anterograde transport of synapse vesicle (SV) precursors in axons. The CC1-FHA tandem of KIF1A has been revealed as a stable dimer that can trigger motor activity, but the mechanism underlying the regulation of the CC1-FHA dimer is unclear. Based on the CC1-FHA dimer structure, we found a potential phosphorylation motif "487SPKK490" located at the dimer interface. We demonstrated that the phosphorylation-mimetic mutation of Ser487 leads to the dissociation of the CC1-FHA dimer. Moreover, the Ser487-mutation could regulate the motor activity of KIF1A and the KIF1A-mediated axonal transport activity of SVs in C. elegans. Thus, the highly conserved "487SPKK490" motif may be a key site in the CC1-FHA tandem for regulating CC1-FHA dimerization and the subsequent activity of KIF1A.

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LIU Bei, YUE Yang, YU Yong, REN Jin-Qi, FENG Wei, HUO Lin, XU Tao. Potential Phosphorylation Site Modulates The Dimerization and Activity of KIF1A[J]. Progress in Biochemistry and Biophysics,2014,41(9):870-876

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History
  • Received:March 17,2014
  • Revised:May 30,2014
  • Accepted:May 30,2014
  • Online: September 22,2014
  • Published: September 20,2014