4.8 Article

The BBSome controls IFT assembly and turnaround in cilia

Journal

NATURE CELL BIOLOGY
Volume 14, Issue 9, Pages 950-+

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/ncb2560

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Funding

  1. National Institutes of Health [1R01DK090038]
  2. P30 center grant [P30DK90728]
  3. Mayo Clinic Center for Cell Signaling in Gastroenterology [P30DK084567]
  4. PKD Foundation Young Investigator Award [04YI09a]
  5. FULK Career Development Award
  6. Zell PKD Research Award
  7. Upjohn PKD Research Fund
  8. National Cancer Institute (NCI) [1R01CA149039-0 1A1]
  9. Susan G. Komen for the Cure [KG100902]
  10. National Institute of Diabetes and Digestive and Kidney Diseases [P30DK90728]

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The bidirectional movement of intraflagellar transport (IFT) particles,which are composed of motors, IFT-A and IFT-B subcomplexes,and cargoes,is required for the biogenesis and signalling of cilia(1,2). A successful IFT cycle depends on the proper assembly of the massive IFT particle at the ciliary base and its turnaround from anterograde to retrograde transport at the ciliary tip. However,how IFT assembly and turnaround are regulated in vivo remains elusive. From a whole-genome mutagenesis screen in Caenorhabditis elegans, we identified two hypomorphic mutations in dyf-2 and bbs-1 as the only mutants showing normal anterograde IFT transport but defective IFT turnaround at the ciliary tip. Further analyses revealed that the BBSome (refs3,4), agroup of conserved proteins affected in human Bardet-Biedl syndrome(5) (BBS), assembles IFT complexes at the ciliary base, then binds to the anterograde IFT particleina DYF-2- (an orthologue of human WDR19) and BBS-1-dependent manner, and lastly reaches the ciliary tip to regulate proper IFT recycling. Our results identify the BBSome as the key player regulating IFT assembly and turnaround in cilia.

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