. 2017 Jan 4:8:13999.

doi: 10.1038/ncomms13999.

The mitotic kinesin-14 KlpA contains a context-dependent directionality switch

Andrew R Popchock¹, Kuo-Fu Tseng², Pan Wang^{2

3}, P Andrew Karplus¹, Xin Xiang⁴, Weihong Qiu^{1

2}

Affiliations

¹ Department of Biochemistry and Biophysics, Oregon State University, Corvallis, Oregon 97331, USA.
² Department of Physics, Oregon State University, Corvallis, Oregon 97331, USA.
³ School of Physics and Electronics, Henan University, Kaifeng, Henan 475004, China.
⁴ Department of Biochemistry and Molecular Biology, The Uniformed Services University of the Health Sciences, Bethesda, Maryland 20814, USA.

PMID: 28051135
PMCID: PMC5216134
DOI: 10.1038/ncomms13999

The mitotic kinesin-14 KlpA contains a context-dependent directionality switch

Andrew R Popchock et al. Nat Commun. 2017.

. 2017 Jan 4:8:13999.

doi: 10.1038/ncomms13999.

Authors

Andrew R Popchock¹, Kuo-Fu Tseng², Pan Wang^{2

3}, P Andrew Karplus¹, Xin Xiang⁴, Weihong Qiu^{1

2}

Affiliations

¹ Department of Biochemistry and Biophysics, Oregon State University, Corvallis, Oregon 97331, USA.
² Department of Physics, Oregon State University, Corvallis, Oregon 97331, USA.
³ School of Physics and Electronics, Henan University, Kaifeng, Henan 475004, China.
⁴ Department of Biochemistry and Molecular Biology, The Uniformed Services University of the Health Sciences, Bethesda, Maryland 20814, USA.

PMID: 28051135
PMCID: PMC5216134
DOI: 10.1038/ncomms13999

Abstract

Kinesin-14s are commonly known as nonprocessive minus end-directed microtubule motors that function mainly for mitotic spindle assembly. Here we show using total internal reflection fluorescence microscopy that KlpA-a kinesin-14 from Aspergillus nidulans-is a context-dependent bidirectional motor. KlpA exhibits plus end-directed processive motility on single microtubules, but reverts to canonical minus end-directed motility when anchored on the surface in microtubule-gliding experiments or interacting with a pair of microtubules in microtubule-sliding experiments. Plus end-directed processive motility of KlpA on single microtubules depends on its N-terminal nonmotor microtubule-binding tail, as KlpA without the tail is nonprocessive and minus end-directed. We suggest that the tail is a de facto directionality switch for KlpA motility: when the tail binds to the same microtubule as the motor domain, KlpA is a plus end-directed processive motor; in contrast, when the tail detaches from the microtubule to which the motor domain binds, KlpA becomes minus end-directed.

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Figures

**Figure 1. Surface-immobilized KlpA molecules exhibit minus end-directed motility to glide microtubules.**
(a) Schematic diagrams of the full-length KlpA and the recombinant GFP-KlpA. The full-length KlpA consists of three consecutive coiled coils (CC1, aa 153–249; CC2, aa 250–297; and CC3, aa 298–416), a neck (aa 417–421) and a catalytic microtubule-binding motor domain (aa 422–756). GFP-KlpA contains an N-terminal polyhistidine-tag (not shown). (b) Coomassie-stained SDS–polyacrylamide gel electrophoresis (SDS–PAGE) of purified recombinant GFP-KlpA. (c) Schematic diagram of the microtubule-gliding assay. Movement of microtubules driven by surface-immobilized GFP-KlpA molecules was visualized by TIRF microscopy. Microtubules were fluorescently labelled with tetramethylrhodamine (TMR), and polarity-marked with a dim minus end and a bright plus end. (d) Representative TIRF microscopy images of polarity-marked microtubules moving on the coverslip surface with the bright plus ends leading (yellow arrowheads). (e) Histogram showing the microtubule-gliding velocity distribution of GFP-KlpA. Red line indicates a Gaussian fit to the velocity histogram. Scale bar, 5 μm.

**Figure 2. KlpA moves processively towards the plus end on single microtubules.**
(a) Schematic diagram of the *in vitro* KlpA motility assay. Microtubules were fluorescently labelled with Hilyte 647, and polarity-marked with a dim minus end and a bright plus end. (b) Example kymograph showing GFP-KlpA molecules (green), at relatively high protein input levels, form a plus end-directed flux and accumulate there on a surface-immobilized polarity-marked microtubule (red). Yellow arrow indicates GFP-KlpA accumulation at the microtubule plus end, and white arrow indicates minus end-directed movement of a GFP-KlpA aggregate. (c) Example kymographs showing that individual GFP-KlpA molecules (green) move towards the plus end on single polarity-marked microtubules (red) in a processive manner. (d) Velocity histogram of individual GFP-KlpA molecules on single microtubules. Red line indicates a Gaussian fit to the velocity histogram. (e) Run-length histogram of individual GFP-KlpA molecules on single microtubules. Red line indicates a single exponential fit to the run-length histogram. Scale bars, 1 min (vertical) and 5 μm (horizontal).

**Figure 3. Plus end-directed processive motility of KlpA on single microtubules requires its N-terminal nonmotor microtubule-binding tail.**
(a) Schematic diagrams of the full-length KlpA and the recombinant GFP-KlpA-Δtail. GFP-KlpA-Δtail contains a polyhistidine-tag (not shown) and a GFP at the N terminus, and residues 303–770 of KlpA. (b) Representative TIRF microscopy images of GFP-KlpA-Δtail driving polarity-marked microtubules (red) to glide with the bright plus ends leading (white arrowheads). (c) Velocity histogram of microtubule-gliding by GFP-KlpA-Δtail. Red line indicates a Gaussian fit to the velocity histogram. (d) Example kymograph showing that individual GFP-KlpA-Δtail molecules (yellow) exhibit nonprocessive movement on a single polarity-marked microtubule with a bright plus end. White arrow indicates minus end-directed movement of a rare GFP-KlpA-Δtail aggregate. Scale bars, 1 min (vertical) and 5 μm (horizontal).

**Figure 4. KlpA exhibits opposite directional preference inside and outside the microtubule overlaps.**
(a) Schematic diagram of the microtubule-sliding assay showing that KlpA contains context-dependent opposite directional preference. Track and cargo microtubules were fluorescently labelled with Hilyte 647 and TMR, respectively, and polarity-marked with a dim minus end and a bright plus end. (b) Example kymographs of GFP-KlpA motility inside and outside the antiparallel microtubule overlap. Yellow arrow indicates GFP-KlpA accumulation at the microtubule plus end outside the antiparallel microtubule overlap. White arrow indicates minus end-directed movement of GFP-KlpA inside the antiparallel microtubule overlap. (c) Example kymographs of GFP-KlpA motility inside and outside the parallel microtubule overlap. Yellow arrow indicates GFP-KlpA accumulation at the microtubule plus end outside the parallel microtubule overlap. White arrow indicates GFP-KlpA accumulation at the microtubule minus end inside the parallel microtubule overlap. Scale bars, 30 s (vertical) and 5 μm (horizontal).

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References

1. Vale R. D. The molecular motor toolbox for intracellular transport. Cell 112, 467–480 (2003). - PubMed
1. Drummond D. R. Regulation of microtubule dynamics by kinesins. Semin. Cell Dev. Biol. 22, 927–934 (2011). - PubMed
1. Vicente J. J. & Wordeman L. Mitosis, microtubule dynamics and the evolution of kinesins. Exp. Cell Res. 334, 61–69 (2015). - PMC - PubMed
1. Karsenti E. & Vernos I. The mitotic spindle: a self-made machine. Science 294, 543–547 (2001). - PubMed
1. Wordeman L. How kinesin motor proteins drive mitotic spindle function: lessons from molecular assays. Semin. Cell Dev. Biol. 21, 260–268 (2010). - PMC - PubMed

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The mitotic kinesin-14 KlpA contains a context-dependent directionality switch

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The mitotic kinesin-14 KlpA contains a context-dependent directionality switch

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