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The polarity protein Inturned links NPHP4 to Daam1 to control the subapical actin network in multiciliated cells
Authors:Takayuki Yasunaga  Sylvia Hoff  Christoph Schell  Martin Helmst?dter  Oliver Kretz  Sebastian Kuechlin  Toma A Yakulov  Christina Engel  Barbara Müller  Robert Bensch  Olaf Ronneberger  Tobias B Huber  Soeren S Lienkamp  Gerd Walz
Institution:1.Renal Division, Department of Medicine, University of Freiburg Medical Center, 79106 Freiburg, Germany;2.Neuroanatomy, University of Freiburg, 79104 Freiburg, Germany;3.Department of Computer Science, University of Freiburg, 79110 Freiburg, Germany;4.Centre for Biological Signaling Studies, 79104 Freiburg, Germany
Abstract:Motile cilia polarization requires intracellular anchorage to the cytoskeleton; however, the molecular machinery that supports this process remains elusive. We report that Inturned plays a central role in coordinating the interaction between cilia-associated proteins and actin-nucleation factors. We observed that knockdown of nphp4 in multiciliated cells of the Xenopus laevis epidermis compromised ciliogenesis and directional fluid flow. Depletion of nphp4 disrupted the subapical actin layer. Comparison to the structural defects caused by inturned depletion revealed striking similarities. Furthermore, coimmunoprecipitation assays demonstrated that the two proteins interact with each other and that Inturned mediates the formation of ternary protein complexes between NPHP4 and DAAM1. Knockdown of daam1, but not formin-2, resulted in similar disruption of the subapical actin web, whereas nphp4 depletion prevented the association of Inturned with the basal bodies. Thus, Inturned appears to function as an adaptor protein that couples cilia-associated molecules to actin-modifying proteins to rearrange the local actin cytoskeleton.
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