The Kinesin KIF1C and Microtubule Plus Ends Regulate Podosome Dynamics in Macrophages

Overview

Journal Mol Biol Cell

Specialties Cell Biology
Molecular Biology

Date 2006 Mar 24

PMID 16554367

Citations 52

Authors

Petra Kopp

Reiner Lammers

Martin Aepfelbacher

Gunther Woehlke

Thomas Rudel

Nikolaus Machuy

Walter Steffen

Stefan Linder

Affiliations

Soon will be listed here.

Abstract

Microtubules are important for the turnover of podosomes, dynamic, actin-rich adhesions implicated in migration and invasion of monocytic cells. The molecular basis for this functional dependency, however, remained unclear. Here, we show that contact by microtubule plus ends critically influences the cellular fate of podosomes in primary human macrophages. In particular, we identify the kinesin KIF1C, a member of the Kinesin-3 family, as a plus-end-enriched motor that targets regions of podosome turnover. Expression of mutation constructs or small interfering RNA-/short hairpin RNA-based depletion of KIF1C resulted in decreased podosome dynamics and ultimately in podosome deficiency. Importantly, protein interaction studies showed that KIF1C binds to nonmuscle myosin IIA via its PTPD-binding domain, thus providing an interface between the actin and tubulin cytoskeletons, which may facilitate the subcellular targeting of podosomes by microtubules. This is the first report to implicate a kinesin in podosome regulation and also the first to describe a function for KIF1C in human cells.

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