Article
- The EMBO Journal (2006) 25, 267 - 277
- doi:10.1038/sj.emboj.7600937
Published online: 12 January 2006
Subject Category:
Processive movement of single kinesins on crowded microtubules visualized using quantum dots
Arne Seitz and Thomas Surrey
- European Molecular Biology Laboratory (EMBL), Cell Biology and Biophysics Unit, Heidelberg, Germany
Correspondence to:
Thomas Surrey, EMBL, Cell Biology and Biophysics Unit, Meyerhofstrasse 1, 69117 Heidelberg, Germany. Tel.: +49 6221 387 8360; Fax: +49 6221 387 8512; E-mail: surrey@embl.de
Received 11 July 2005; Accepted 6 December 2005
Abstract
Kinesin-1 is a processive molecular motor transporting cargo along microtubules. Inside cells, several motors and microtubule-associated proteins compete for binding to microtubules. Therefore, the question arises how processive movement of kinesin-1 is affected by crowding on the microtubule. Here we use total internal reflection fluorescence microscopy to image in vitro the runs of single quantum dot-labelled kinesins on crowded microtubules under steady-state conditions and to measure the degree of crowding on a microtubule at steady-state. We find that the runs of kinesins are little affected by high kinesin densities on a microtubule. However, the presence of high densities of a mutant kinesin that is not able to step efficiently reduces the average speed of wild-type kinesin, while hardly changing its processivity. This indicates that kinesin waits in a strongly bound state on the microtubule when encountering an obstacle until the obstacle unbinds and frees the binding site for kinesin's next step. A simple kinetic model can explain quantitatively the behaviour of kinesin under both crowding conditions.
Keywords:
- crowding,
- molecular motors,
- quantum dots,
- single-molecule imaging
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