Microtubule Dynamic Instability Controls Podosome Patterning in Osteoclasts through EB1, Cortactin, and Src

Author:

Biosse Duplan Martin1,Zalli Detina1,Stephens Sebastien1,Zenger Serhan1,Neff Lynn1,Oelkers J. Margit23,Lai Frank P. L.2,Horne William1,Rottner Klemens23,Baron Roland14

Affiliation:

1. Harvard School of Dental Medicine, Department of Oral Medicine, Infection and Immunity, Boston, Massachusetts, USA

2. Helmholtz Center for Infection Research, Braunschweig, Germany

3. Institute of Genetics, University of Bonn, Bonn, Germany

4. Harvard Medical School, Department of Medicine, Endocrine Unit, Massachusetts General Hospital, Boston Massachusetts, USA

Abstract

ABSTRACT In osteoclasts (OCs) podosomes are organized in a belt, a feature critical for bone resorption. Although microtubules (MTs) promote the formation and stability of the belt, the MT and/or podosome molecules that mediate the interaction of the two systems are not identified. Because the growing “plus” ends of MTs point toward the podosome belt, plus-end tracking proteins (+TIPs) might regulate podosome patterning. Among the +TIPs, EB1 increased as OCs matured and was enriched in the podosome belt, and EB1-positive MTs targeted podosomes. Suppression of MT dynamic instability, displacement of EB1 from MT ends, or EB1 depletion resulted in the loss of the podosome belt. We identified cortactin as an Src-dependent interacting partner of EB1. Cortactin-deficient OCs presented a defective MT targeting to, and patterning of, podosomes and reduced bone resorption. Suppression of MT dynamic instability or EB1 depletion increased cortactin phosphorylation, decreasing its acetylation and affecting its interaction with EB1. Thus, dynamic MTs and podosomes interact to control bone resorption.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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