CLIP-170 tracks growing microtubule ends by dynamically recognizing composite EB1/tubulin-binding sites

Author:

Bieling Peter1,Kandels-Lewis Stefanie1,Telley Ivo A.1,van Dijk Juliette2,Janke Carsten2,Surrey Thomas1

Affiliation:

1. European Molecular Biology Laboratory, Cell Biology and Biophysics Unit, 69117 Heidelberg, Germany

2. Centre de Recherche de Biochimie Macromoléculaire, Université Montpellier 2 and 1, Centre National de la Recherche Scientifique, 34293 Montpellier, France

Abstract

The microtubule cytoskeleton is crucial for the internal organization of eukaryotic cells. Several microtubule-associated proteins link microtubules to subcellular structures. A subclass of these proteins, the plus end–binding proteins (+TIPs), selectively binds to the growing plus ends of microtubules. Here, we reconstitute a vertebrate plus end tracking system composed of the most prominent +TIPs, end-binding protein 1 (EB1) and CLIP-170, in vitro and dissect their end-tracking mechanism. We find that EB1 autonomously recognizes specific binding sites present at growing microtubule ends. In contrast, CLIP-170 does not end-track by itself but requires EB1. CLIP-170 recognizes and turns over rapidly on composite binding sites constituted by end-accumulated EB1 and tyrosinated α-tubulin. In contrast to its fission yeast orthologue Tip1, dynamic end tracking of CLIP-170 does not require the activity of a molecular motor. Our results demonstrate evolutionary diversity of the plus end recognition mechanism of CLIP-170 family members, whereas the autonomous end-tracking mechanism of EB family members is conserved.

Publisher

Rockefeller University Press

Subject

Cell Biology

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